Your search keyword '"82/80"' showing total 83 results

1. TEFM variants impair mitochondrial transcription causing childhood-onset neurological disease

Author

Lindsey Van Haute, Emily O’Connor, Héctor Díaz-Maldonado, Benjamin Munro, Kiran Polavarapu, Daniella H. Hock, Gautham Arunachal, Alkyoni Athanasiou-Fragkouli, Mainak Bardhan, Magalie Barth, Dominique Bonneau, Nicola Brunetti-Pierri, Gerarda Cappuccio, Nikeisha J. Caruana, Natalia Dominik, Himanshu Goel, Guy Helman, Henry Houlden, Guy Lenaers, Karine Mention, David Murphy, Bevinahalli Nandeesh, Catarina Olimpio, Christopher A. Powell, Veeramani Preethish-Kumar, Vincent Procaccio, Rocio Rius, Pedro Rebelo-Guiomar, Cas Simons, Seena Vengalil, Maha S. Zaki, Alban Ziegler, David R. Thorburn, David A. Stroud, Reza Maroofian, John Christodoulou, Claes Gustafsson, Atchayaram Nalini, Hanns Lochmüller, Michal Minczuk, Rita Horvath, Van Haute, Lindsey [0000-0001-7809-1473], Polavarapu, Kiran [0000-0002-8879-6001], Hock, Daniella H [0000-0002-6940-4420], Bardhan, Mainak [0000-0002-4106-409X], Brunetti-Pierri, Nicola [0000-0002-6895-8819], Caruana, Nikeisha J [0000-0002-0817-1686], Helman, Guy [0000-0002-4784-7423], Houlden, Henry [0000-0002-2866-7777], Lenaers, Guy [0000-0003-2736-3349], Rius, Rocio [0000-0002-9871-3126], Rebelo-Guiomar, Pedro [0000-0002-5060-7519], Simons, Cas [0000-0003-3147-8042], Vengalil, Seena [0000-0002-0629-9221], Zaki, Maha S [0000-0001-7840-0002], Thorburn, David R [0000-0002-7725-9470], Stroud, David A [0000-0002-2048-3383], Christodoulou, John [0000-0002-8431-0641], Gustafsson, Claes [0000-0003-3531-8468], Minczuk, Michal [0000-0001-8242-1420], Horvath, Rita [0000-0002-9841-170X], Apollo - University of Cambridge Repository, Van Haute, Lindsey, O'Connor, Emily, Díaz-Maldonado, Héctor, Munro, Benjamin, Polavarapu, Kiran, Hock, Daniella H, Arunachal, Gautham, Athanasiou-Fragkouli, Alkyoni, Bardhan, Mainak, Barth, Magalie, Bonneau, Dominique, Brunetti-Pierri, Nicola, Cappuccio, Gerarda, Caruana, Nikeisha J, Dominik, Natalia, Goel, Himanshu, Helman, Guy, Houlden, Henry, Lenaers, Guy, Mention, Karine, Murphy, David, Nandeesh, Bevinahalli, Olimpio, Catarina, Powell, Christopher A, Preethish-Kumar, Veeramani, Procaccio, Vincent, Rius, Rocio, Rebelo-Guiomar, Pedro, Simons, Ca, Vengalil, Seena, Zaki, Maha S, Ziegler, Alban, Thorburn, David R, Stroud, David A, Maroofian, Reza, Christodoulou, John, Gustafsson, Clae, Nalini, Atchayaram, Lochmüller, Hann, Minczuk, Michal, and Horvath, Rita

Subjects

Transcription, Genetic, RNA, Mitochondrial, General Physics and Astronomy, 38/90, 13/106, 692/1807/1693, 14, DNA, Mitochondrial, General Biochemistry, Genetics and Molecular Biology, 38, 38/91, 82/80, Mitochondrial Proteins, 38/1, 692/420/2489/144, 692/617/375/374, 38/23, 38/22, Animals, Humans, Child, Zebrafish, 64, Multidisciplinary, 64/116, 692/308/2056, article, General Chemistry, 13/51, Mutation, 38/77, 692/700/139/422, Transcription Factors

Abstract

Funder: EC | EC Seventh Framework Programm | FP7 Ideas: European Research Council (FP7-IDEAS-ERC - Specific Programme: "Ideas" Implementing the Seventh Framework Programme of the European Community for Research, Technological Development and Demonstration Activities (2007 to 2013)); doi: https://doi.org/10.13039/100011199; Grant(s): 309548, Funder: Lily Mae Foundation; doi: https://doi.org/10.13039/100012336, Mutations in the mitochondrial or nuclear genomes are associated with a diverse group of human disorders characterized by impaired mitochondrial respiration. Within this group, an increasing number of mutations have been identified in nuclear genes involved in mitochondrial RNA biology. The TEFM gene encodes the mitochondrial transcription elongation factor responsible for enhancing the processivity of mitochondrial RNA polymerase, POLRMT. We report for the first time that TEFM variants are associated with mitochondrial respiratory chain deficiency and a wide range of clinical presentations including mitochondrial myopathy with a treatable neuromuscular transmission defect. Mechanistically, we show muscle and primary fibroblasts from the affected individuals have reduced levels of promoter distal mitochondrial RNA transcripts. Finally, tefm knockdown in zebrafish embryos resulted in neuromuscular junction abnormalities and abnormal mitochondrial function, strengthening the genotype-phenotype correlation. Our study highlights that TEFM regulates mitochondrial transcription elongation and its defect results in variable, tissue-specific neurological and neuromuscular symptoms.

Published

2023

2. Deletion of SNX9 alleviates CD8 T cell exhaustion for effective cellular cancer immunotherapy

Author

Marcel P. Trefny, Nicole Kirchhammer, Priska Auf der Maur, Marina Natoli, Dominic Schmid, Markus Germann, Laura Fernandez Rodriguez, Petra Herzig, Jonas Lötscher, Maryam Akrami, Jane C. Stinchcombe, Michal A. Stanczak, Andreas Zingg, Melanie Buchi, Julien Roux, Romina Marone, Leyla Don, Didier Lardinois, Mark Wiese, Lukas T. Jeker, Mohamed Bentires-Alj, Jérémie Rossy, Daniela S. Thommen, Gillian M. Griffiths, Heinz Läubli, Christoph Hess, Alfred Zippelius, Trefny, Marcel P [0000-0001-6755-7899], Kirchhammer, Nicole [0000-0001-6043-5143], Auf der Maur, Priska [0000-0002-9059-8979], Schmid, Dominic [0000-0003-4821-6495], Stinchcombe, Jane C [0000-0003-1459-9299], Roux, Julien [0000-0002-4192-5099], Marone, Romina [0000-0003-1474-1689], Jeker, Lukas T [0000-0002-3359-8796], Bentires-Alj, Mohamed [0000-0001-6344-1127], Thommen, Daniela S [0000-0002-7431-2854], Griffiths, Gillian M [0000-0003-0434-5842], Hess, Christoph [0000-0003-0364-8825], Zippelius, Alfred [0000-0003-1933-8178], and Apollo - University of Cambridge Repository

Subjects

General Physics and Astronomy, 13/106, 45/23, CD8-Positive T-Lymphocytes, General Biochemistry, Genetics and Molecular Biology, 38/91, 82/80, Lymphocytes, Tumor-Infiltrating, ddc:570, Neoplasms, 692/308/575, 42/41, Humans, 692/4028/67/580, 14/19, Multidisciplinary, article, 631/250/251, General Chemistry, Translational research, 96/21, T-Cell Exhaustion, 13/31, 631/67/580, 13/95, Tumour immunology, 64/60, Immunotherapy, 82/1

Abstract

Funder: Dr. Arnold U. und Susanne Huggenberger-Bischoff Stiftung zur Krebsforschung (Huggenberger-Bischoff Foundationfor Cancer Research); doi: https://doi.org/10.13039/501100007878, Funder: Krebsliga Beider Basel (Cancer League of Basel-City and Basel-Country); doi: https://doi.org/10.13039/501100006069, Funder: Krebsliga Schweiz (Ligue Suisse Contre le Cancer); doi: https://doi.org/10.13039/501100004361, Funder: Swiss Personalized Health Network (Swiss Personalized Oncology driver project) Medical Faculty and Department of Surgery of the University Hospital Basel, Tumor-specific T cells are frequently exhausted by chronic antigenic stimulation. We here report on a human antigen-specific ex vivo model to explore new therapeutic options for T cell immunotherapies. T cells generated with this model resemble tumor-infiltrating exhausted T cells on a phenotypic and transcriptional level. Using a targeted pooled CRISPR-Cas9 screen and individual gene knockout validation experiments, we uncover sorting nexin-9 (SNX9) as a mediator of T cell exhaustion. Upon TCR/CD28 stimulation, deletion of SNX9 in CD8 T cells decreases PLCγ1, Ca2+, and NFATc2-mediated T cell signaling and reduces expression of NR4A1/3 and TOX. SNX9 knockout enhances memory differentiation and IFNγ secretion of adoptively transferred T cells and results in improved anti-tumor efficacy of human chimeric antigen receptor T cells in vivo. Our findings highlight that targeting SNX9 is a strategy to prevent T cell exhaustion and enhance anti-tumor immunity.

Published

2023

3. Activation mechanism of the class D fungal GPCR dimer Ste2

Author

Vaithish Velazhahan, Ning Ma, Nagarajan Vaidehi, Christopher G. Tate, Vaidehi, Nagarajan [0000-0001-8100-8132], Tate, Christopher G [0000-0002-2008-9183], and Apollo - University of Cambridge Repository

Subjects

Mammals, 82/29, Saccharomyces cerevisiae Proteins, Multidisciplinary, 101/28, Cell Membrane, article, Saccharomyces cerevisiae, 631/45/612/194, Heterotrimeric GTP-Binding Proteins, 631/45/535/1258/1259, Receptors, G-Protein-Coupled, 82/80, GTP-Binding Protein gamma Subunits, Receptors, Mating Factor, Animals, 82/83

Abstract

The fungal class D1 G-protein-coupled receptor (GPCR) Ste2 has a different arrangement of transmembrane helices compared with mammalian GPCRs and a distinct mode of coupling to the heterotrimeric G protein Gpa1–Ste2–Ste181. In addition, Ste2 lacks conserved sequence motifs such as DRY, PIF and NPXXY, which are associated with the activation of class A GPCRs2. This suggested that the activation mechanism of Ste2 may also differ. Here we determined structures of Saccharomyces cerevisiae Ste2 in the absence of G protein in two different conformations bound to the native agonist α-factor, bound to an antagonist and without ligand. These structures revealed that Ste2 is indeed activated differently from other GPCRs. In the inactive state, the cytoplasmic end of transmembrane helix H7 is unstructured and packs between helices H1–H6, blocking the G protein coupling site. Agonist binding results in the outward movement of the extracellular ends of H6 and H7 by 6 Å. On the intracellular surface, the G protein coupling site is formed by a 20 Å outward movement of the unstructured region in H7 that unblocks the site, and a 12 Å inward movement of H6. This is a distinct mechanism in GPCRs, in which the movement of H6 and H7 upon agonist binding facilitates G protein coupling.

Published

2022

4. Mechanism-based traps enable protease and hydrolase substrate discovery

Author

Shan Tang, Adam T. Beattie, Lucie Kafkova, Gianluca Petris, Nicolas Huguenin-Dezot, Marc Fiedler, Matthew Freeman, Jason W. Chin, Tang, Shan [0000-0003-4483-1108], Petris, Gianluca [0000-0002-2420-6359], Huguenin-Dezot, Nicolas [0000-0001-8816-2159], Fiedler, Marc [0000-0003-4269-7873], Freeman, Matthew [0000-0003-0410-5451], Chin, Jason [0000-0003-1219-4757], Apollo - University of Cambridge Repository, and Chin, Jason W [0000-0003-1219-4757]

Subjects

Mammals, 45/70, Multidisciplinary, 631/92/607, 82/58, Serine Endopeptidases, article, Intracellular Signaling Peptides and Proteins, Membrane Proteins, 13/106, Cell Cycle Proteins, 13/109, Neoplasm Proteins, Substrate Specificity, 631/92/96, 82/80, 13/31, Serine, Animals, Humans, 82/1, 82/83, Peptide Hydrolases

Abstract

Hydrolase enzymes, including proteases, are encoded by 2–3% of the genes in the human genome and 14% of these enzymes are active drug targets1. However, the activities and substrate specificities of many proteases—especially those embedded in membranes—and other hydrolases remain unknown. Here we report a strategy for creating mechanism-based, light-activated protease and hydrolase substrate traps in complex mixtures and live mammalian cells. The traps capture substrates of hydrolases, which normally use a serine or cysteine nucleophile. Replacing the catalytic nucleophile with genetically encoded 2,3-diaminopropionic acid allows the first step reaction to form an acyl-enzyme intermediate in which a substrate fragment is covalently linked to the enzyme through a stable amide bond2; this enables stringent purification and identification of substrates. We identify new substrates for proteases, including an intramembrane mammalian rhomboid protease RHBDL4 (refs. 3,4). We demonstrate that RHBDL4 can shed luminal fragments of endoplasmic reticulum-resident type I transmembrane proteins to the extracellular space, as well as promoting non-canonical secretion of endogenous soluble endoplasmic reticulum-resident chaperones. We also discover that the putative serine hydrolase retinoblastoma binding protein 9 (ref. 5) is an aminopeptidase with a preference for removing aromatic amino acids in human cells. Our results exemplify a powerful paradigm for identifying the substrates and activities of hydrolase enzymes.

Published

2022

5. Low-dose IL-2 reduces IL-21+ T cell frequency and induces anti-inflammatory gene expression in type 1 diabetes

Author

Zhang, Jia-Yuan, Hamey, Fiona, Trzupek, Dominik, Mickunas, Marius, Lee, Mercede, Godfrey, Leila, Yang, Jennie HM, Pekalski, Marcin L, Kennet, Jane, Waldron-Lynch, Frank, Evans, Mark L, Tree, Timothy IM, Wicker, Linda S, Todd, John A, Ferreira, Ricardo C, Zhang, Jia-Yuan [0000-0003-1321-0384], Mickunas, Marius [0000-0002-5457-9850], Godfrey, Leila [0000-0002-4454-1285], Yang, Jennie HM [0000-0001-6171-833X], Pekalski, Marcin L [0000-0001-7623-4370], Kennet, Jane [0000-0001-8615-0576], Waldron-Lynch, Frank [0000-0002-0597-4328], Evans, Mark L [0000-0001-8122-8987], Wicker, Linda S [0000-0001-7771-0324], Todd, John A [0000-0003-2740-8148], Ferreira, Ricardo C [0000-0001-5733-3285], and Apollo - University of Cambridge Repository

Subjects

45/91, 49/31, Multidisciplinary, 45, T-Lymphocytes, 692/699/249/2510, article, Anti-Inflammatory Agents, Gene Expression, General Physics and Astronomy, General Chemistry, General Biochemistry, Genetics and Molecular Biology, 631/250/249/1313/1418, 82/80, Diabetes Mellitus, Type 1, 692/308/575, Humans, Interleukin-2, 38/39, 631/1647/514/1949, 82/1

Abstract

Funder: China Scholarship Council, Despite early clinical successes, the mechanisms of action of low-dose interleukin-2 (LD-IL-2) immunotherapy remain only partly understood. Here we examine the effects of interval administration of low-dose recombinant IL-2 (iLD-IL-2) in type 1 diabetes using high-resolution single-cell multiomics and flow cytometry on longitudinally-collected peripheral blood samples. Our results confirm that iLD-IL-2 selectively expands thymic-derived FOXP3+HELIOS+ regulatory T cells and CD56bright NK cells, and show that the treatment reduces the frequency of IL-21-producing CD4+ T cells and of two innate-like mucosal-associated invariant T and Vγ9Vδ2 CD8+ T cell subsets. The cellular changes induced by iLD-IL-2 associate with an anti-inflammatory gene expression signature, which remains detectable in all T and NK cell subsets analysed one month after treatment. These findings warrant investigations into the potential longer-term clinical benefits of iLD-IL-2 in immunotherapy., This work was supported by the Sir Jules Thorn Trust (13/JTA (OCT2013/DR/1044)), the JDRF (1-SRA-2019-657-A-N), and the NIHR Cambridge Biomedical Research Centre. The Diabetes and Inflammation Laboratory was supported by a strategic award from the Wellcome (107212/A/15/Z) and the JDRF (4-SRA-2017-473-A-A). JYZ was supported by the China Scholarship Council-University of Oxford Scholarship. The research was supported by the Wellcome Trust Core Award Grant Number 203141/Z/16/Z with additional support from the NIHR Oxford BRC. The University of Cambridge has received salary support for ME through the National Health Service in the East of England through the Clinical Academic Reserve. The views expressed are those of the author(s) and not necessarily those of the NHS, the NIHR or the Department of Health.

Published

2022

6. Parkin regulates adiposity by coordinating mitophagy with mitochondrial biogenesis in white adipocytes

Author

Timothy M. Moore, Lijing Cheng, Dane M. Wolf, Jennifer Ngo, Mayuko Segawa, Xiaopeng Zhu, Alexander R. Strumwasser, Yang Cao, Bethan L. Clifford, Alice Ma, Philip Scumpia, Orian S. Shirihai, Thomas Q. de Aguiar Vallim, Markku Laakso, Aldons J. Lusis, Andrea L. Hevener, Zhenqi Zhou, Moore, Timothy M [0000-0003-4250-3370], Scumpia, Philip [0000-0002-2563-2042], Shirihai, Orian S [0000-0001-8466-3431], Lusis, Aldons J [0000-0001-9013-0228], Zhou, Zhenqi [0000-0001-6560-9704], and Apollo - University of Cambridge Repository

Subjects

Ubiquitin-Protein Ligases, 1.1 Normal biological development and functioning, Adipocytes, White, 38/90, General Physics and Astronomy, White, Neurodegenerative, DNA, Mitochondrial, General Biochemistry, Genetics and Molecular Biology, 38/91, 82/80, Mice, 14/34, 42/89, Underpinning research, Adipocytes, Genetics, Animals, Humans, 631/443/319, Obesity, 14/19, 631/337/458/582, 692/699/2743/393, Metabolic and endocrine, Adiposity, Nutrition, Organelle Biogenesis, Parkinson's Disease, Multidisciplinary, article, Mitophagy, Neurosciences, DNA, General Chemistry, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, 692/4017, Mitochondrial, Brain Disorders, 13/51, 140/131, 64/60

Abstract

Funder: UCLA Intercampus Medical Genetics Training Program (T32GM008243), NRSA predoctoral fellowship (F31DK108657), Carl V. Gisolfi Memorial Research grant from the American College of Sports Medicine, and a predoctoral graduate student award from the Dornsife College at the University of Southern California., Funder: EMBO long-term fellowship ALTF 828-2021, Funder: DK120342, DK117850, Funder: DK109724, P30DK063491, Funder: NIDDK DK125354, Parkin, an E3 ubiquitin ligase, plays an essential role in mitochondrial quality control. However, the mechanisms by which Parkin connects mitochondrial homeostasis with cellular metabolism in adipose tissue remain unclear. Here, we demonstrate that Park2 gene (encodes Parkin) deletion specifically from adipose tissue protects mice against high-fat diet and aging-induced obesity. Despite a mild reduction in mitophagy, mitochondrial DNA content and mitochondrial function are increased in Park2 deficient white adipocytes. Moreover, Park2 gene deletion elevates mitochondrial biogenesis by increasing Pgc1α protein stability through mitochondrial superoxide-activated NAD(P)H quinone dehydrogenase 1 (Nqo1). Both in vitro and in vivo studies show that Nqo1 overexpression elevates Pgc1α protein level and mitochondrial DNA content and enhances mitochondrial activity in mouse and human adipocytes. Taken together, our findings indicate that Parkin regulates mitochondrial homeostasis by balancing mitophagy and Pgc1α-mediated mitochondrial biogenesis in white adipocytes, suggesting a potential therapeutic target in adipocytes to combat obesity and obesity-associated disorders.

Published

2022

7. MicroRNA-7 regulates melanocortin circuits involved in mammalian energy homeostasis

Author

LaPierre, Mary P, Lawler, Katherine, Godbersen, Svenja, Farooqi, I Sadaf, Stoffel, Markus, LaPierre, Mary P [0000-0002-3863-9438], Lawler, Katherine [0000-0003-4188-1804], Stoffel, Markus [0000-0003-1304-5817], and Apollo - University of Cambridge Repository

Subjects

123, Immunoglobulins, 13/106, 13/109, 13, 82/80, Mice, 13/1, 42/44, 42/41, Animals, Homeostasis, Humans, Obesity, 631/337/384/331, 13/89, 692/699/2743/393, Mammals, 45/91, article, 631/443/319/367/1562, 45/77, 96/63, Melanocortins, MicroRNAs, 13/51, alpha-Synuclein, Receptor, Melanocortin, Type 4, 64/60, Transcription Factors

Abstract

MicroRNAs (miRNAs) modulate physiological responses by repressing the expression of gene networks. We found that global deletion of microRNA-7 (miR-7), the most enriched miRNA in the hypothalamus, causes obesity in mice. Targeted deletion of miR-7 in Single-minded homolog 1 (Sim1) neurons, a critical component of the hypothalamic melanocortin pathway, causes hyperphagia, obesity and increased linear growth, mirroring Sim1 and Melanocortin-4 receptor (MC4R) haplo-insufficiency in mice and humans. We identified Snca (α-Synuclein) and Igsf8 (Immunoglobulin Superfamily Member 8) as miR-7 target genes that act in Sim1 neurons to regulate body weight and endocrine axes. In humans, MIR-7-1 is located in the last intron of HNRNPK, whose promoter drives the expression of both genes. Genetic variants at the HNRNPK locus that reduce its expression are associated with increased height and truncal fat mass. These findings demonstrate that miR-7 suppresses gene networks involved in the hypothalamic melanocortin pathway to regulate mammalian energy homeostasis., Nature Communications, 13, ISSN:2041-1723

Published

2022

8. Mild dyslipidemia accelerates tumorigenesis through expansion of Ly6Chi monocytes and differentiation to pro-angiogenic myeloid cells

Author

Thi Tran, Jean-Remi Lavillegrand, Cedric Lereverend, Bruno Esposito, Lucille Cartier, Melanie Montabord, Jaouen Tran-Rajau, Marc Diedisheim, Nadège Gruel, Khadija Ouguerram, Lea Paolini, Olivia Lenoir, Emmanuel Pinteaux, Eva Brabencova, Corinne Tanchot, Pauline Urquia, Jacqueline Lehmann-Che, Richard Le Naour, Yacine Merrouche, Christian Stockmann, Ziad Mallat, Alain Tedgui, Hafid Ait-Oufella, Eric Tartour, Stephane Potteaux, Tran, Thi [0000-0003-4012-5898], Lereverend, Cedric [0000-0002-9399-5638], Cartier, Lucille [0000-0003-0170-8396], Diedisheim, Marc [0000-0002-0418-1107], Lenoir, Olivia [0000-0001-8107-6987], Lehmann-Che, Jacqueline [0000-0001-6685-3354], Le Naour, Richard [0000-0003-1925-6041], Tedgui, Alain [0000-0002-7229-4875], Ait-Oufella, Hafid [0000-0002-2955-0183], Potteaux, Stephane [0000-0003-3068-8769], Apollo - University of Cambridge Repository, University of Zurich, Potteaux, Stephane, Paris-Centre de Recherche Cardiovasculaire (PARCC (UMR_S 970/ U970)), Hôpital Européen Georges Pompidou [APHP] (HEGP), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpitaux Universitaires Paris Ouest - Hôpitaux Universitaires Île de France Ouest (HUPO)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpitaux Universitaires Paris Ouest - Hôpitaux Universitaires Île de France Ouest (HUPO)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Paris Cité (UPCité), Immuno-Régulation dans les Maladies Auto-Immunes Inflammatoires et le Cancer - EA 7509 (IRMAIC), Université de Reims Champagne-Ardenne (URCA), Institut Jean Godinot [Reims], UNICANCER, Hôpital Cochin [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Unité de génétique et biologie des cancers (U830), Institut Curie [Paris]-Institut National de la Santé et de la Recherche Médicale (INSERM), Physiopathologie des Adaptations Nutritionnelles (PhAN), Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE)-Nantes Université - UFR de Médecine et des Techniques Médicales (Nantes Univ - UFR MEDECINE), Nantes Université - pôle Santé, Nantes Université (Nantes Univ)-Nantes Université (Nantes Univ)-Nantes Université - pôle Santé, Nantes Université (Nantes Univ)-Nantes Université (Nantes Univ), University of Manchester [Manchester], Immunologie humaine, physiopathologie & immunothérapie (HIPI (UMR_S_976 / U976)), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Paris Cité (UPCité), Hopital Saint-Louis [AP-HP] (AP-HP), Universität Zürich [Zürich] = University of Zurich (UZH), University of Cambridge [UK] (CAM), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpitaux Universitaires Paris Ouest - Hôpitaux Universitaires Île de France Ouest (HUPO), ANR-11-INBS-0006,FLI,France Life Imaging(2011), Lenoir, Olivia, and Infrastructures - France Life Imaging - - FLI2011 - ANR-11-INBS-0006 - INBS - VALID

Subjects

10017 Institute of Anatomy, Carcinogenesis, General Physics and Astronomy, 610 Medicine & health, 1600 General Chemistry, 13/106, [SDV.BC.BC]Life Sciences [q-bio]/Cellular Biology/Subcellular Processes [q-bio.SC], Monocytes, General Biochemistry, Genetics and Molecular Biology, 14/1, 82/80, Mice, 1300 General Biochemistry, Genetics and Molecular Biology, [SDV.BC.BC] Life Sciences [q-bio]/Cellular Biology/Subcellular Processes [q-bio.SC], Tumor Microenvironment, 38/88, Animals, Myeloid Cells, 49/91, Dyslipidemias, Inflammation, 49/31, 1000 Multidisciplinary, Multidisciplinary, 82/16, article, 11401 Cancer Research Center (CRC), General Chemistry, 3100 General Physics and Astronomy, Mice, Inbred C57BL, Cell Transformation, Neoplastic, 692/4019/592/75/2099, 59/78, 570 Life sciences, biology, 64/60, 82/51, 631/67/327

Abstract

Funder: Association pour la recherche sur le cancer, Funder: Ligue Contre le Cancer, Cancer and cardiovascular disease (CVD) share common risk factors such as dyslipidemia, obesity and inflammation. However, the role of pro-atherogenic environment and its associated low-grade inflammation in tumor progression remains underexplored. Here we show that feeding C57BL/6J mice with a non-obesogenic high fat high cholesterol diet (HFHCD) for two weeks to induce mild dyslipidemia, increases the pool of circulating Ly6Chi monocytes available for initial melanoma development, in an IL-1β-dependent manner. Descendants of circulating myeloid cells, which accumulate in the tumor microenvironment of mice under HFHCD, heighten pro-angiogenic and immunosuppressive activities locally. Limiting myeloid cell accumulation or targeting VEGF-A production by myeloid cells decrease HFHCD-induced tumor growth acceleration. Reverting the HFHCD to a chow diet at the time of tumor implantation protects against tumor growth. Together, these data shed light on cross-disease communication between cardiovascular pathologies and cancer.

Published

2022

9. A conformational switch controlling the toxicity of the prion protein

Author

Simon Jurt, Mattia Pedotti, Marika Marino, Luca Varani, Anna Henzi, Georg Meisl, Seden Bedir, Tuomas P. J. Knowles, Rohanah Hussain, Asvin K. K. Lakkaraju, Marco Losa, Federica Mazzola, Karl Frontzek, Marco Bardelli, Oliver Zerbe, Petra Schwarz, Giuliano Siligardi, Assunta Senatore, Adriano Aguzzi, Regina Reimann, Luca Simonelli, Simone Hornemann, Caihong Zhu, Matthew Holt, Frontzek, Karl [0000-0002-0945-8857], Bedir, Seden [0000-0002-8509-1268], Marino, Marika [0000-0001-6773-6176], Hussain, Rohanah [0000-0001-6207-6631], Meisl, Georg [0000-0002-6562-7715], Zerbe, Oliver [0000-0003-0475-438X], Losa, Marco [0000-0003-3428-418X], Knowles, Tuomas [0000-0002-7879-0140], Hornemann, Simone [0000-0002-2674-9891], Holt, Matthew G [0000-0002-8958-4027], Varani, Luca [0000-0002-0963-0987], Aguzzi, Adriano [0000-0002-0344-6708], Apollo - University of Cambridge Repository, University of Zurich, Varani, Luca, and Aguzzi, Adriano

Subjects

PRP, animal diseases, Mutant, RESISTANT, Ligands, 14, 13/1, Mice, 1315 Structural Biology, Structural Biology, Cerebellum, 540 Chemistry, 14/19, biology, Chemistry, Neurodegeneration, article, Cell biology, 631/45/460, Toxicity, Antibody, Life Sciences & Biomedicine, Biochemistry & Molecular Biology, 101, Prions, Biophysics, 10208 Institute of Neuropathology, 101/6, 610 Medicine & health, Antibodies, Prion Proteins, 38, 82/80, Prion infection, 1312 Molecular Biology, medicine, Animals, PrPC Proteins, Prion protein, Molecular Biology, Science & Technology, 82, Neurotoxicity, Cell Biology, medicine.disease, NMR, nervous system diseases, MICE, 631/535/1267, REPLICATION, ANTIBODIES, 13/51, biology.protein, 570 Life sciences, Neurological impairment

Abstract

Funder: Ono PharmaceuticalsTheodo Ida Herzog-Egli Stiftung, Funder: Stavros Niarchos Foundation (SNF); doi: https://doi.org/10.13039/501100004343, Funder: RCUK | Biotechnology and Biological Sciences Research Council (BBSRC); doi: https://doi.org/10.13039/501100000268, Funder: EC | EU Framework Programme for Research and Innovation H2020 | H2020 Priority Excellent Science | H2020 European Research Council (H2020 Excellent Science - European Research Council); doi: https://doi.org/10.13039/100010663, Funder: Frances and Augustus Newman Foundation; doi: https://doi.org/10.13039/100007898, Funder: EC | EC Seventh Framework Programm | FP7 Ideas: European Research Council (FP7-IDEAS-ERC - Specific Programme: “Ideas” Implementing the Seventh Framework Programme of the European Community for Research, Technological Development and Demonstration Activities (2007 to 2013)); doi: https://doi.org/10.13039/100011199; Grant(s): H2020-WIDESPREAD-2018-2020-6; NCBio; 951923, Funder: FWO (Grant 1513616N), Funder: Lions Club Monteceneri, Funder: Schweizerischer Nationalfonds zur Förderung der Wissenschaftlichen Forschung (Swiss National Science Foundation); doi: https://doi.org/10.13039/501100001711, Funder: Gelu Foundation, Swiss Initiative in Systems Biology, SystemsX.ch (PrionX, SynucleiX), Prion infections cause conformational changes of the cellular prion protein (PrPC) and lead to progressive neurological impairment. Here we show that toxic, prion-mimetic ligands induce an intramolecular R208-H140 hydrogen bond ('H-latch'), altering the flexibility of the α2-α3 and β2-α2 loops of PrPC. Expression of a PrP2Cys mutant mimicking the H-latch was constitutively toxic, whereas a PrPR207A mutant unable to form the H-latch conferred resistance to prion infection. High-affinity ligands that prevented H-latch induction repressed prion-related neurodegeneration in organotypic cerebellar cultures. We then selected phage-displayed ligands binding wild-type PrPC, but not PrP2Cys. These binders depopulated H-latched conformers and conferred protection against prion toxicity. Finally, brain-specific expression of an antibody rationally designed to prevent H-latch formation prolonged the life of prion-infected mice despite unhampered prion propagation, confirming that the H-latch is an important reporter of prion neurotoxicity.

Published

2022

10. Perineuronal nets affect memory and learning after synapse withdrawal

Author

Ruzicka, Jiri, Dalecka, Marketa, Safrankova, Kristyna, Peretti, Diego, Jendelova, Pavla, Kwok, Jessica CF, Fawcett, James W, Ruzicka, Jiri [0000-0002-1269-1633], Dalecka, Marketa [0000-0003-4366-0255], Jendelova, Pavla [0000-0002-4644-9212], Kwok, Jessica CF [0000-0002-9798-9083], Fawcett, James W [0000-0002-7990-4568], and Apollo - University of Cambridge Repository

Subjects

Neurons, Extracellular Matrix Proteins, article, 631/378/1595/1554, 64/110, 631/378/1595/2167, 96/63, Extracellular Matrix, 82/80, Cellular and Molecular Neuroscience, Psychiatry and Mental health, Synapses, Animals, Learning, 64/60, 14/28, 14/19, 82/1, 82/51, Biological Psychiatry

Abstract

Perineuronal nets (PNNs) enwrap mature neurons, playing a role in the control of plasticity and synapse dynamics. PNNs have been shown to have effects on memory formation, retention and extinction in a variety of animal models. It has been proposed that the cavities in PNNs, which contain synapses, can act as a memory store and that they remain stable after events that cause synaptic withdrawal such as anoxia or hibernation. We examine this idea by monitoring place memory before and after synaptic withdrawal caused by acute hibernation-like state (HLS). Animals lacking hippocampal PNNs due to enzymatic digestion by chondroitinase ABC or knockout of the PNN component aggrecan were compared with wild type controls. HLS-induced synapse withdrawal caused a memory deficit, but not to the level of untreated naïve animals and not worsened by PNN attenuation. After HLS, only animals lacking PNNs showed memory restoration or relearning. Absence of PNNs affected the restoration of excitatory synapses on PNN-bearing neurons. The results support a role for hippocampal PNNs in learning, but not in long-term memory storage for correction of deficits.

Published

2022

11. ELF5 is a potential respiratory epithelial cell-specific risk gene for severe COVID-19

Author

Maik Pietzner, Robert Lorenz Chua, Eleanor Wheeler, Katharina Jechow, Julian D. S. Willett, Helena Radbruch, Saskia Trump, Bettina Heidecker, Hugo Zeberg, Frank L. Heppner, Roland Eils, Marcus A. Mall, J. Brent Richards, Leif-Erik Sander, Irina Lehmann, Sören Lukassen, Nicholas J. Wareham, Christian Conrad, Claudia Langenberg, Pietzner, Maik [0000-0003-3437-9963], Wheeler, Eleanor [0000-0002-8616-6444], Radbruch, Helena [0000-0001-6941-3397], Zeberg, Hugo [0000-0001-7118-1249], Heppner, Frank L [0000-0001-9816-8917], Mall, Marcus A [0000-0002-4057-2199], Richards, J Brent [0000-0002-3746-9086], Sander, Leif-Erik [0000-0002-0476-9947], Lukassen, Sören [0000-0001-7045-6327], Wareham, Nicholas J [0000-0003-1422-2993], Conrad, Christian [0000-0001-7036-342X], Langenberg, Claudia [0000-0002-5017-7344], and Apollo - University of Cambridge Repository

Subjects

Respiratory System, 45/43, General Physics and Astronomy, genetics [DNA-Binding Proteins], Peptidyl-Dipeptidase A, General Biochemistry, Genetics and Molecular Biology, 82/80, 692/699/255/2514, ELF5 protein, human, Humans, genetics [COVID-19], metabolism [Peptidyl-Dipeptidase A], metabolism [Epithelial Cells], 49/91, genetics [Angiotensin-Converting Enzyme 2], Multidisciplinary, SARS-CoV-2, article, COVID-19, Epithelial Cells, General Chemistry, 631/208/205, genetics [Transcription Factors], 692/4017, DNA-Binding Proteins, ddc:500, Angiotensin-Converting Enzyme 2, 692/499, Transcription Factors

Abstract

Funder: Wellcome Trust, Funder: National Institute for Health Research (NIHR), Despite two years of intense global research activity, host genetic factors that predispose to a poorer prognosis of COVID-19 infection remain poorly understood. Here, we prioritise eight robust (e.g., ELF5) or suggestive but unreported (e.g., RAB2A) candidate protein mediators of COVID-19 outcomes by integrating results from the COVID-19 Host Genetics Initiative with population-based plasma proteomics using statistical colocalisation. The transcription factor ELF5 (ELF5) shows robust and directionally consistent associations across different outcome definitions, including a >4-fold higher risk (odds ratio: 4.88; 95%-CI: 2.47-9.63; p-value < 5.0 × 10-6) for severe COVID-19 per 1 s.d. higher genetically predicted plasma ELF5. We show that ELF5 is specifically expressed in epithelial cells of the respiratory system, such as secretory and alveolar type 2 cells, using single-cell RNA sequencing and immunohistochemistry. These cells are also likely targets of SARS-CoV-2 by colocalisation with key host factors, including ACE2 and TMPRSS2. In summary, large-scale human genetic studies together with gene expression at single-cell resolution highlight ELF5 as a risk gene for severe COVID-19, supporting a role of epithelial cells of the respiratory system in the adverse host response to SARS-CoV-2.

Published

2022

12. The renal lineage factor PAX8 controls oncogenic signalling in kidney cancer

Author

Patel, Saroor A, Hirosue, Shoko, Rodrigues, Paulo, Vojtasova, Erika, Richardson, Emma K, Ge, Jianfeng, Syafruddin, Saiful E, Speed, Alyson, Papachristou, Eva, Baker, David, Clarke, David, Purvis, Stephenie, Wesolowski, Ludovic, Dyas, Anna, Castillon, Leticia, Caraffini, Veronica, Bihary, Dóra, Yong, Cissy, Harrison, David J, Stewart, Grant, Machiela, Mitchell J, Purdue, Mark P, Chanock, Stephen J, Warren, Anne, Samarajiwa, Shamith A, Carroll, Jason, Vanharanta, Sakari, Hirosue, Shoko [0000-0003-1287-471X], Vojtasova, Erika [0000-0001-9255-8551], Papachristou, Eva [0000-0002-5835-2055], Harrison, David J [0000-0001-9041-9988], Stewart, Grant [0000-0003-3188-9140], Machiela, Mitchell J [0000-0001-6538-9705], Chanock, Stephen J [0000-0002-2324-3393], Warren, Anne [0000-0002-1170-7867], Samarajiwa, Shamith A [0000-0003-1046-0601], Carroll, Jason [0000-0003-3643-0080], Vanharanta, Sakari [0000-0001-5619-7963], Apollo - University of Cambridge Repository, University of St Andrews. School of Medicine, University of St Andrews. Sir James Mackenzie Institute for Early Diagnosis, University of St Andrews. Cellular Medicine Division, CAN-PRO - Translational Cancer Medicine Program, Department of Physiology, Faculty of Medicine, University of Helsinki, Papachristou, Evangelia K [0000-0002-5835-2055], Stewart, Grant D [0000-0003-3188-9140], Warren, Anne Y [0000-0002-1170-7867], and Carroll, Jason S [0000-0003-3643-0080]

Subjects

82/29, PROMOTES, Carcinogenesis, 45/41, 692/699/67/589/1588/1351, 45/43, SUSCEPTIBILITY, Kidney, 13, 59/5, 59, BINDING, Basic Helix-Loop-Helix Transcription Factors, Cyclin D1, SPECIFICITY, CYCLIN D1, 64, Multidisciplinary, Kidney Neoplasms, Multidisciplinary Sciences, Gene Expression Regulation, Neoplastic, 38/32, 13/31, TARGET, Von Hippel-Lindau Tumor Suppressor Protein, 38/35, Science & Technology - Other Topics, 38/39, 64/60, 631/67/70, Signal Transduction, 3122 Cancers, 13/106, QH426 Genetics, 631/67/69, Article, 38/91, RC0254, ENHANCER, Proto-Oncogene Proteins c-myc, 82/80, PAX8 Transcription Factor, SDG 3 - Good Health and Well-being, 38/89, 631/208/200, HIF, Humans, QH426, Carcinoma, Renal Cell, Alleles, 38/109, 42, Science & Technology, 45, RC0254 Neoplasms. Tumors. Oncology (including Cancer), 82/58, DAS, 45/15, GENE, Mutation, 631/208/191

Abstract

Large-scale human genetic data1-3 have shown that cancer mutations display strong tissue-selectivity, but how this selectivity arises remains unclear. Here, using experimental models, functional genomics and analyses of patient samples, we demonstrate that the lineage transcription factor paired box 8 (PAX8) is required for oncogenic signalling by two common genetic alterations that cause clear cell renal cell carcinoma (ccRCC) in humans: the germline variant rs7948643 at 11q13.3 and somatic inactivation of the von Hippel-Lindau tumour suppressor (VHL)4-6. VHL loss, which is observed in about 90% of ccRCCs, can lead to hypoxia-inducible factor 2α (HIF2A) stabilization6,7. We show that HIF2A is preferentially recruited to PAX8-bound transcriptional enhancers, including a pro-tumorigenic cyclin D1 (CCND1) enhancer that is controlled by PAX8 and HIF2A. The ccRCC-protective allele C at rs7948643 inhibits PAX8 binding at this enhancer and downstream activation of CCND1 expression. Co-option of a PAX8-dependent physiological programme that supports the proliferation of normal renal epithelial cells is also required for MYC expression from the ccRCC metastasis-associated amplicons at 8q21.3-q24.3 (ref. 8). These results demonstrate that transcriptional lineage factors are essential for oncogenic signalling and that they mediate tissue-specific cancer risk associated with somatic and inherited genetic variants., Medical Research Council (MC_UU_12022/7 and MC_UU_12022/10) and Kidney Research UK (RP_033_20170303).

Published

2022

13. Substrate binding in the mitochondrial ADP/ATP carrier is a step-wise process guiding the structural changes in the transport cycle

Author

Vasiliki Mavridou, Edmund R.S. Kunji, Sotiria Tavoulari, Shane M. Palmer, Jonathan J. Ruprecht, Martin S. King, Mavridou, Vasiliki [0000-0002-1019-1256], King, Martin [0000-0001-6030-5154], Tavoulari, Sotiria [0000-0002-4263-8905], Ruprecht, Jonathan [0000-0002-1838-7245], Kunji, Edmund [0000-0002-0610-4500], Apollo - University of Cambridge Repository, King, Martin S [0000-0001-6030-5154], Ruprecht, Jonathan J [0000-0002-1838-7245], and Kunji, Edmund RS [0000-0002-0610-4500]

Subjects

History, Cytoplasm, Polymers and Plastics, General Physics and Astronomy, Oxidative phosphorylation, Industrial and Manufacturing Engineering, General Biochemistry, Genetics and Molecular Biology, 82/80, Adenosine Triphosphate, Business and International Management, Binding site, 631/57/1464, 82/83, Multidisciplinary, Binding Sites, biology, Chemistry, Adenine nucleotide translocator, article, Substrate (chemistry), 101/47, General Chemistry, Mitochondria, Adenosine Diphosphate, Cytosol, 631/1647/2204, Mitochondrial matrix, 631/57/2283, Adenine nucleotide transport, 9, Biophysics, biology.protein, ATP–ADP translocase, 631/80/642/333, 119, Mitochondrial ADP, ATP Translocases, 631/535

Abstract

Mitochondrial ADP/ATP carriers import ADP into the mitochondrial matrix and export ATP to the cytosol to fuel cellular processes. Structures of the inhibited cytoplasmic- and matrix-open states have confirmed an alternating access transport mechanism, but the molecular details of substrate binding remain unresolved. Here, we evaluate the role of the solvent-exposed residues of the translocation pathway in the process of substrate binding. We identify the main binding site, comprising three positively charged and a set of aliphatic and aromatic residues, which bind ADP and ATP in both states. Additionally, there are two pairs of asparagine/arginine residues on opposite sides of this site that are involved in substrate binding in a state-dependent manner. Thus, the substrates are directed through a series of binding poses, inducing the conformational changes of the carrier that lead to their translocation. The properties of this site explain the electrogenic and reversible nature of adenine nucleotide transport.

Published

2022

14. ID proteins promote the survival and primed-to-naive transition of human embryonic stem cells through TCF3-mediated transcription

Author

Jiang, Haibin, Du, Mingxia, Li, Yaning, Zhou, Tengfei, Lei, Jia, Liang, Hongqing, Zhong, Zhen, Al-Lamki, Rafia S, Jiang, Ming, Yang, Jun, Yang, Jun [0000-0001-9715-8100], and Apollo - University of Cambridge Repository

Subjects

Inhibitor of Differentiation Protein 1, Cancer Research, 82, Immunology, Human Embryonic Stem Cells, 96, article, Cell Differentiation, Cell Biology, 38, 96/100, 82/80, DNA-Binding Proteins, 631/532/2117, Cellular and Molecular Neuroscience, embryonic structures, Basic Helix-Loop-Helix Transcription Factors, Humans, 38/39, 631/80/86/2364, Proto-Oncogene Proteins c-akt, Inhibitor of Differentiation Protein 2, Signal Transduction

Abstract

Funder: National Key Research and Development Program of China Stem Cell and Translational Research, 2016YFA0102300, Funder: Zhejiang University Education Foundation Global Partnership Fund(188170+194452115/011), Inhibition of DNA binding proteins 1 and 3 (ID1 and ID3) are important downstream targets of BMP signalling that are necessary for embryonic development. However, their specific roles in regulating the pluripotency of human embryonic stem cells (hESCs) remain unclear. Here, we examined the roles of ID1 and ID3 in primed and naive-like hESCs and showed that ID1 and ID3 knockout lines (IDs KO) exhibited decreased survival in both primed and naive-like state. IDs KO lines in the primed state also tended to undergo pluripotent dissolution and ectodermal differentiation. IDs KO impeded the primed-to-naive transition (PNT) of hESCs, and overexpression of ID1 in primed hESCs promoted PNT. Furthermore, single-cell RNA sequencing demonstrated that ID1 and ID3 regulated the survival and pluripotency of hESCs through the AKT signalling pathway. Finally, we showed that TCF3 mediated transcriptional inhibition of MCL1 promotes AKT phosphorylation, which was confirmed by TCF3 knockdown in KO lines. Our study suggests that IDs/TCF3 acts through AKT signalling to promote survival and maintain pluripotency of both primed and naive-like hESCs.

Published

2022

15. The structure of EXTL3 helps to explain the different roles of bi-domain exostosins in heparan sulfate synthesis

Author

L. F. L. Wilson, T. Dendooven, S. W. Hardwick, A. Echevarría-Poza, T. Tryfona, K. B. R. M. Krogh, D. Y. Chirgadze, B. F. Luisi, D. T. Logan, K. Mani, P. Dupree, Dupree, Paul [0000-0001-9270-6286], Hardwick, Steven [0000-0001-9246-1864], Tryfona, Theodora [0000-0002-1618-3521], Chirgadze, Dima [0000-0001-9942-0993], Luisi, Ben [0000-0003-1144-9877], and Apollo - University of Cambridge Repository

Subjects

82/29, Multidisciplinary, 631/535/1258/1259, 82/58, 101/28, article, General Physics and Astronomy, 13/106, 631/45/221, 13/109, General Chemistry, N-Acetylglucosaminyltransferases, 631/45/173, General Biochemistry, Genetics and Molecular Biology, 82/80, Mice, Animals, Heparitin Sulfate, 82/83, 631/45/607

Abstract

Funder: University of Cambridge; doi: https://doi.org/10.13039/501100000735, Funder: AstraZeneca; doi: https://doi.org/10.13039/100004325, Funder: RCUK | Biotechnology and Biological Sciences Research Council (BBSRC); doi: https://doi.org/10.13039/501100000268, Funder: RCUK | Engineering and Physical Sciences Research Council (EPSRC); doi: https://doi.org/10.13039/501100000266, Funder: OpenPlant, BB/L014130/1, Heparan sulfate is a highly modified O-linked glycan that performs diverse physiological roles in animal tissues. Though quickly modified, it is initially synthesised as a polysaccharide of alternating β-d-glucuronosyl and N-acetyl-α-d-glucosaminyl residues by exostosins. These enzymes generally possess two glycosyltransferase domains (GT47 and GT64)—each thought to add one type of monosaccharide unit to the backbone. Although previous structures of murine exostosin-like 2 (EXTL2) provide insight into the GT64 domain, the rest of the bi-domain architecture is yet to be characterised; hence, how the two domains co-operate is unknown. Here, we report the structure of human exostosin-like 3 (EXTL3) in apo and UDP-bound forms. We explain the ineffectiveness of EXTL3’s GT47 domain to transfer β-d-glucuronosyl units, and we observe that, in general, the bi-domain architecture would preclude a processive mechanism of backbone extension. We therefore propose that heparan sulfate backbone polymerisation occurs by a simple dissociative mechanism.

Published

2022

16. Genetic architecture of host proteins involved in SARS-CoV-2 infection

Author

Eric R. Gamazon, Erin Oerton, Nicola D. Kerrison, Nicholas J. Wareham, Aroon D. Hingorani, Maik Pietzner, Juan P Casas, Chris Finan, Rachel Ostroff, Gabi Kastenmüller, Steve A. Williams, Johannes Raffler, Eleanor Wheeler, Julia Carrasco-Zanini, Jian'an Luan, Markus Ralser, Victoria P W Auyeung, Claudia Langenberg, Wheeler, Eleanor [0000-0002-8616-6444], Raffler, Johannes [0000-0003-2495-4020], Auyeung, Victoria P. W. [0000-0002-0823-3963], Luan, Jian’an [0000-0003-3137-6337], Finan, Chris [0000-0002-3319-1937], Williams, Steve A. [0000-0002-8661-4315], Kastenmüller, Gabi [0000-0002-2368-7322], Gamazon, Eric R. [0000-0003-4204-8734], Wareham, Nicholas J. [0000-0003-1422-2993], Hingorani, Aroon D. [0000-0001-8365-0081], Langenberg, Claudia [0000-0002-5017-7344], Apollo - University of Cambridge Repository, Pietzner, Maik [0000-0003-3437-9963], Carrasco Zanini Sánchez, Julia [0000-0002-3988-7505], Au Yeung, Victoria [0000-0002-0823-3963], Luan, Jian'an [0000-0003-3137-6337], and Wareham, Nicholas [0000-0003-1422-2993]

Subjects

0301 basic medicine, Male, 45/61, Science, Quantitative Trait Loci, education, General Physics and Astronomy, Computational biology, Host-Derived Cellular Factors, 030204 cardiovascular system & hematology, Phenome, Quantitative trait locus, Biology, DNA sequencing, General Biochemistry, Genetics and Molecular Biology, ABO Blood-Group System, 82/80, 03 medical and health sciences, 631/208, 0302 clinical medicine, Immune system, Drug Delivery Systems, 692/53, Humans, Blood Coagulation, Repurposing, health care economics and organizations, Regulation of gene expression, Internet, Multidisciplinary, 45, SARS-CoV-2, article, COVID-19, Proteins, General Chemistry, Middle Aged, Genetic architecture, humanities, 030104 developmental biology, Drug development, Gene Expression Regulation, Host-Pathogen Interactions, Female, Aptamers, Peptide

Abstract

Funder: Medical Research Council, Understanding the genetic architecture of host proteins interacting with SARS-CoV-2 or mediating the maladaptive host response to COVID-19 can help to identify new or repurpose existing drugs targeting those proteins. We present a genetic discovery study of 179 such host proteins among 10,708 individuals using an aptamer-based technique. We identify 220 host DNA sequence variants acting in cis (MAF 0.01-49.9%) and explaining 0.3-70.9% of the variance of 97 of these proteins, including 45 with no previously known protein quantitative trait loci (pQTL) and 38 encoding current drug targets. Systematic characterization of pQTLs across the phenome identified protein-drug-disease links and evidence that putative viral interaction partners such as MARK3 affect immune response. Our results accelerate the evaluation and prioritization of new drug development programmes and repurposing of trials to prevent, treat or reduce adverse outcomes. Rapid sharing and detailed interrogation of results is facilitated through an interactive webserver (https://omicscience.org/apps/covidpgwas/).

Published

2020

17. Microbial communities form rich extracellular metabolomes that foster metabolic interactions and promote drug tolerance

Author

Jason S. L. Yu, Clara Correia-Melo, Francisco Zorrilla, Lucia Herrera-Dominguez, Mary Y. Wu, Johannes Hartl, Kate Campbell, Sonja Blasche, Marco Kreidl, Anna-Sophia Egger, Christoph B. Messner, Vadim Demichev, Anja Freiwald, Michael Mülleder, Michael Howell, Judith Berman, Kiran R. Patil, Mohammad Tauqeer Alam, Markus Ralser, Yu, Jason SL [0000-0001-5203-3603], Correia-Melo, Clara [0000-0001-6062-1472], Herrera-Dominguez, Lucia [0000-0001-8276-2241], Wu, Mary Y [0000-0002-2074-6171], Hartl, Johannes [0000-0001-8470-5355], Egger, Anna-Sophia [0000-0002-5204-7121], Howell, Michael [0000-0003-0912-0079], Berman, Judith [0000-0002-8577-0084], Alam, Mohammad Tauqeer [0000-0002-6872-0691], Ralser, Markus [0000-0001-9535-7413], Apollo - University of Cambridge Repository, and Apollo-University Of Cambridge Repository

Subjects

Microbiology (medical), 631/326/2565/855, RM, Immunology, Applied Microbiology and Biotechnology, Microbiology, 82/80, 13/44, 14/34, Ecology,Evolution & Ethology, 38/47, Genetics, 14/35, Computational & Systems Biology, Chemical Biology & High Throughput, 82/58, Microbiota, article, Cell Biology, Drug Tolerance, 631/326/22, QP, 96/63, QR, 13/31, Metabolism, Metabolome, bacteria, Microbial Interactions, Synthetic Biology, Metabolic Networks and Pathways

Abstract

Funder: United Arab Emirates University (UAEU); doi: https://doi.org/10.13039/501100006013, Microbial communities are composed of cells of varying metabolic capacity, and regularly include auxotrophs that lack essential metabolic pathways. Through analysis of auxotrophs for amino acid biosynthesis pathways in microbiome data derived from >12,000 natural microbial communities obtained as part of the Earth Microbiome Project (EMP), and study of auxotrophic-prototrophic interactions in self-establishing metabolically cooperating yeast communities (SeMeCos), we reveal a metabolically imprinted mechanism that links the presence of auxotrophs to an increase in metabolic interactions and gains in antimicrobial drug tolerance. As a consequence of the metabolic adaptations necessary to uptake specific metabolites, auxotrophs obtain altered metabolic flux distributions, export more metabolites and, in this way, enrich community environments in metabolites. Moreover, increased efflux activities reduce intracellular drug concentrations, allowing cells to grow in the presence of drug levels above minimal inhibitory concentrations. For example, we show that the antifungal action of azoles is greatly diminished in yeast cells that uptake metabolites from a metabolically enriched environment. Our results hence provide a mechanism that explains why cells are more robust to drug exposure when they interact metabolically.

Published

2022

18. Normalizing and denoising protein expression data from droplet-based single cell profiling

Author

Matthew P. Mulé, Andrew J. Martins, John S. Tsang, Mulè, Matthew P [0000-0001-8457-2716], Martins, Andrew J [0000-0002-1832-1924], Tsang, John S [0000-0003-3186-3047], and Apollo - University of Cambridge Repository

Subjects

Normalization (statistics), 631/61/475, Population, General Physics and Astronomy, Computational biology, General Biochemistry, Genetics and Molecular Biology, Transcriptome, Bioconductor, Database normalization, Background noise, 82/80, Single-cell analysis, Cluster analysis, education, education.field_of_study, Multidisciplinary, Chemistry, Gene Expression Profiling, 631/1647/48, article, General Chemistry, 631/114/2415, 631/114/794, 38/39, Single-Cell Analysis, Software

Abstract

Funder: NIAID Intramural Grant: 1ZIAAI001152, Multimodal single-cell profiling methods that measure protein expression with oligo-conjugated antibodies hold promise for comprehensive dissection of cellular heterogeneity, yet the resulting protein counts have substantial technical noise that can mask biological variations. Here we integrate experiments and computational analyses to reveal two major noise sources and develop a method called "dsb" (denoised and scaled by background) to normalize and denoise droplet-based protein expression data. We discover that protein-specific noise originates from unbound antibodies encapsulated during droplet generation; this noise can thus be accurately estimated and corrected by utilizing protein levels in empty droplets. We also find that isotype control antibodies and the background protein population average in each cell exhibit significant correlations across single cells, we thus use their shared variance to correct for cell-to-cell technical noise in each cell. We validate these findings by analyzing the performance of dsb in eight independent datasets spanning multiple technologies, including CITE-seq, ASAP-seq, and TEA-seq. Compared to existing normalization methods, our approach improves downstream analyses by better unmasking biologically meaningful cell populations. Our method is available as an open-source R package that interfaces easily with existing single cell software platforms such as Seurat, Bioconductor, and Scanpy and can be accessed at "dsb [ https://cran.r-project.org/package=dsb ]".

Published

2022

19. Structural and molecular determinants for the interaction of ExbB from Serratia marcescens and HasB, a TonB paralog

Author

Valérie Biou, Ricardo Jorge Diogo Adaixo, Mohamed Chami, Pierre-Damien Coureux, Benoist Laurent, Véronique Yvette Ntsogo Enguéné, Gisele Cardoso de Amorim, Nadia Izadi-Pruneyre, Christian Malosse, Julia Chamot-Rooke, Henning Stahlberg, Philippe Delepelaire, Laboratoire de biologie physico-chimique des protéines membranaires (LBPC-PM (UMR_7099)), Institut de biologie physico-chimique (IBPC (FR_550)), Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité), Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS), Center for Cellular Imaging and Nanoanalytics, University of Basel (Unibas), Laboratoire de Biologie Structurale de la Cellule (BIOC), École polytechnique (X)-Centre National de la Recherche Scientifique (CNRS), University of Cambridge [UK] (CAM), Bioinformatique structurale - Structural Bioinformatics, Institut Pasteur [Paris] (IP)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité), Centre de Bioinformatique, Biostatistique et Biologie Intégrative (C3BI), Institut Pasteur [Paris] (IP)-Centre National de la Recherche Scientifique (CNRS), Universidade Federal do Rio de Janeiro (UFRJ), Spectrométrie de Masse pour la Biologie – Mass Spectrometry for Biology (UTechS MSBio), Institut Pasteur [Paris] (IP)-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité), This work was supported by grants from the ANR (HEMESTOCKEXCHANGE ANR-12-BSV3-0022-01 and LABEX DYNAMO ANR-11-LABEX-0011-01)., ANR-12-BSV3-0022,HEMESTOCKEXCHANGE,Hème et porphyrine chez des bactéries modèle: des fonctions aux mécanismes(2012), ANR-11-LABX-0011,DYNAMO,Dynamique des membranes transductrices d'énergie : biogénèse et organisation supramoléculaire.(2011), Biou, Valérie [0000-0003-1600-6717], Coureux, Pierre-Damien [0000-0002-1328-7229], Enguéné, Véronique Yvette Ntsogo [0000-0003-0096-3192], de Amorim, Gisele Cardoso [0000-0003-4348-9515], Izadi-Pruneyre, Nadia [0000-0002-6864-2961], Chamot-Rooke, Julia [0000-0002-9427-543X], Delepelaire, Philippe [0000-0002-5190-7118], and Apollo - University of Cambridge Repository

Subjects

[SDV.BBM.BS]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Structural Biology [q-bio.BM], MESH: Escherichia coli, 101, Escherichia coli Proteins, 101/28, 101/6, article, Medicine (miscellaneous), MESH: Escherichia coli Proteins, Heme, [SDV.MP.BAC]Life Sciences [q-bio]/Microbiology and Parasitology/Bacteriology, General Biochemistry, Genetics and Molecular Biology, 631/45/535/1258/1259, 82/80, MESH: Serratia marcescens, MESH: Heme, Escherichia coli, MESH: Protein Binding, 631/326/41/2536, General Agricultural and Biological Sciences, 82/83, Serratia marcescens, Protein Binding

Abstract

Funder: LABEX DYNAMO ANR-11-LABEX-0011-01, Funder: ANR HEMESTOCKEXCHANGE ANR-12-BSV3-0022-01, Funder: ANR HEMESTOCKEXCHANGE ANR-12-BSV3-0022-01 ANR LABEX DYNAMO ANR-11-LABEX-0011-01, ExbB and ExbD are cytoplasmic membrane proteins that associate with TonB to convey the energy of the proton-motive force to outer membrane receptors in Gram-negative bacteria for iron uptake. The opportunistic pathogen Serratia marcescens (Sm) possesses both TonB and a heme-specific TonB paralog, HasB. ExbBSm has a long periplasmic extension absent in other bacteria such as E. coli (Ec). Long ExbB’s are found in several genera of Alphaproteobacteria, most often in correlation with a hasB gene. We investigated specificity determinants of ExbBSm and HasB. We determined the cryo-EM structures of ExbBSm and of the ExbB-ExbDSm complex from S. marcescens. ExbBSm alone is a stable pentamer, and its complex includes two ExbD monomers. We showed that ExbBSm extension interacts with HasB and is involved in heme acquisition and we identified key residues in the membrane domain of ExbBSm and ExbBEc, essential for function and likely involved in the interaction with TonB/HasB. Our results shed light on the class of inner membrane energy machinery formed by ExbB, ExbD and HasB.

Published

2022

20. Coiled-coil structure of meiosis protein TEX12 and conformational regulation by its C-terminal tip

Author

Dunce, James M, Salmon, Lucy J, Davies, Owen R, Davies, Owen R [0000-0002-3806-5403], and Apollo - University of Cambridge Repository

Subjects

631/67, 101, Chromosomal Proteins, Non-Histone, Synaptonemal Complex, 631/80/641/1633, synaptonemal complex, article, Molecular Conformation, Medicine (miscellaneous), General Biochemistry, Genetics and Molecular Biology, 82/80, Chromosome Pairing, Meiosis, chromosomal proteins, molecular conformation, non-histone, chromosome pairing, 9, meiosis, 631/45/535/1261, General Agricultural and Biological Sciences, 631/45/535/1266, 631/45/535/1267, 82/83

Abstract

Meiosis protein TEX12 is an essential component of the synaptonemal complex (SC), which mediates homologous chromosome synapsis. It is also recruited to centrosomes in meiosis, and aberrantly in certain cancers, leading to centrosome dysfunction. Within the SC, TEX12 forms an intertwined complex with SYCE2 that undergoes fibrous assembly, driven by TEX12’s C-terminal tip. However, we hitherto lack structural information regarding SYCE2-independent functions of TEX12. Here, we report X-ray crystal structures of TEX12 mutants in three distinct conformations, and utilise solution light and X-ray scattering to determine its wild-type dimeric four-helical coiled-coil structure. TEX12 undergoes conformational change upon C-terminal tip mutations, indicating that the sequence responsible for driving SYCE2-TEX12 assembly within the SC also controls the oligomeric state and conformation of isolated TEX12. Our findings provide the structural basis for SYCE2-independent roles of TEX12, including the possible regulation of SC assembly, and its known functions in meiotic centrosomes and cancer.

Published

2022

21. Mechanisms of inhibition and activation of extrasynaptic ���� GABAA receptors

Author

Kasaragod, Vikram Babu, Mortensen, Martin, Hardwick, Steven, Wahid, Ayla, Dorovykh, Valentina, Chirgadze, Dima, Smart, Trevor G, and Miller, Paul

Subjects

631/378/340, 82/80, 13/1, 631/535/1258/1259, 9/74, 101/28, article, 631/378/2586, 13/106, 13/109, 82/83

Abstract

Type A GABA (��-aminobutyric acid) receptors represent a diverse population in the mammalian brain, forming pentamers from combinations of ��-, ��-, ��-, ��-, ��-, ��-, ��- and ��-subunits1. ����, ��4����, ��6���� and ��5���� receptors favour extrasynaptic localization, and mediate an essential persistent (tonic) inhibitory conductance in many regions of the mammalian brain1,2. Mutations of these receptors in humans are linked to epilepsy and insomnia3,4. Altered extrasynaptic receptor function is implicated in insomnia, stroke and Angelman and Fragile X syndromes1,5, and drugs targeting these receptors are used to treat postpartum depression6. Tonic GABAergic responses are moderated to avoid excessive suppression of neuronal communication, and can exhibit high sensitivity to Zn2+ blockade, in contrast to synapse-preferring ��1����, ��2���� and ��3���� receptor responses5,7-12. Here, to resolve these distinctive features, we determined structures of the predominantly extrasynaptic ���� GABAA receptor class. An inhibited state bound by both the lethal paralysing agent ��-cobratoxin13 and Zn2+ was used in comparisons with GABA-Zn2+ and GABA-bound structures. Zn2+ nullifies the GABA response by non-competitively plugging the extracellular end of the pore to block chloride conductance. In the absence of Zn2+, the GABA signalling response initially follows the canonical route until it reaches the pore. In contrast to synaptic GABAA receptors, expansion of the midway pore activation gate is limited and it remains closed, reflecting the intrinsic low efficacy that characterizes the extrasynaptic receptor. Overall, this study explains distinct traits adopted by ���� receptors that adapt them to a role in tonic signalling., This work was supported by a Department of Pharmacology new lab start-up fund, the University of Cambridge Isaac Newton & Wellcome Trust Institutional Strategic Support Fund, and Academy of Medical Sciences Springboard Award (SBF004\1074). Electrophysiology work in the laboratory of Professor Trevor Smart was funded by an MRC programme grant (MR/T002581/1) and Wellcome Trust Collaborative Award (217199/Z/19/Z). The cryo-EM facility receives funding from the Wellcome Trust (206171/Z/17/Z; 202905/Z/16/Z) and University of Cambridge.

Published

2022

22. The C-terminal tail of ��-synuclein protects against aggregate replication but is critical for oligomerization

Author

Farzadfard, Azad, Pedersen, Jannik Nedergaard, Meisl, Georg, Somavarapu, Arun Kumar, Alam, Parvez, Goks��yr, Louise, Nielsen, Morten Agertoug, Sander, Adam Frederik, Knowles, Tuomas, Pedersen, Jan Skov, and Otzen, Daniel Erik

Subjects

82/80, 631/57, 82/29, 82/16, 101/28, article, 82/83, 631/337

Abstract

Aggregation of the 140-residue protein ��-synuclein (��SN) is a key factor in the etiology of Parkinson's disease. Although the intensely anionic C-terminal domain (CTD) of ��SN does not form part of the amyloid core region or affect membrane binding ability, truncation or reduction of charges in the CTD promotes fibrillation through as yet unknown mechanisms. Here, we study stepwise truncated CTDs and identify a threshold region around residue 121; constructs shorter than this dramatically increase their fibrillation tendency. Remarkably, these effects persist even when as little as 10% of the truncated variant is mixed with the full-length protein. Increased fibrillation can be explained by a substantial increase in self-replication, most likely via fragmentation. Paradoxically, truncation also suppresses toxic oligomer formation, and oligomers that can be formed by chemical modification show reduced membrane affinity and cytotoxicity. These remarkable changes correlate to the loss of negative electrostatic potential in the CTD and highlight a double-edged electrostatic safety guard.

Published

2022

23. Mechanisms of inhibition and activation of extrasynaptic αβ GABAA receptors

Author

Kasaragod, Vikram Babu, Mortensen, Martin, Hardwick, Steven, Wahid, Ayla, Dorovykh, Valentina, Chirgadze, Dima, Smart, Trevor G, Miller, Paul, Mortensen, Martin [0000-0002-5873-7107], Hardwick, Steven [0000-0001-9246-1864], Wahid, Ayla [0000-0001-8128-9632], Chirgadze, Dima [0000-0001-9942-0993], Smart, Trevor G [0000-0002-9089-5375], Miller, Paul [0000-0002-6512-9441], and Apollo - University of Cambridge Repository

Subjects

631/378/340, 82/80, 13/1, 631/535/1258/1259, 9/74, 101/28, article, 631/378/2586, 13/106, 13/109, 82/83

Abstract

Type A GABA (γ-aminobutyric acid) receptors represent a diverse population in the mammalian brain, forming pentamers from combinations of α-, β-, γ-, δ-, ε-, ρ-, θ- and π-subunits1. αβ, α4βδ, α6βδ and α5βγ receptors favour extrasynaptic localization, and mediate an essential persistent (tonic) inhibitory conductance in many regions of the mammalian brain1,2. Mutations of these receptors in humans are linked to epilepsy and insomnia3,4. Altered extrasynaptic receptor function is implicated in insomnia, stroke and Angelman and Fragile X syndromes1,5, and drugs targeting these receptors are used to treat postpartum depression6. Tonic GABAergic responses are moderated to avoid excessive suppression of neuronal communication, and can exhibit high sensitivity to Zn2+ blockade, in contrast to synapse-preferring α1βγ, α2βγ and α3βγ receptor responses5,7-12. Here, to resolve these distinctive features, we determined structures of the predominantly extrasynaptic αβ GABAA receptor class. An inhibited state bound by both the lethal paralysing agent α-cobratoxin13 and Zn2+ was used in comparisons with GABA-Zn2+ and GABA-bound structures. Zn2+ nullifies the GABA response by non-competitively plugging the extracellular end of the pore to block chloride conductance. In the absence of Zn2+, the GABA signalling response initially follows the canonical route until it reaches the pore. In contrast to synaptic GABAA receptors, expansion of the midway pore activation gate is limited and it remains closed, reflecting the intrinsic low efficacy that characterizes the extrasynaptic receptor. Overall, this study explains distinct traits adopted by αβ receptors that adapt them to a role in tonic signalling., This work was supported by a Department of Pharmacology new lab start-up fund, the University of Cambridge Isaac Newton & Wellcome Trust Institutional Strategic Support Fund, and Academy of Medical Sciences Springboard Award (SBF004\1074). Electrophysiology work in the laboratory of Professor Trevor Smart was funded by an MRC programme grant (MR/T002581/1) and Wellcome Trust Collaborative Award (217199/Z/19/Z). The cryo-EM facility receives funding from the Wellcome Trust (206171/Z/17/Z; 202905/Z/16/Z) and University of Cambridge.

Published

2022

24. Coding and regulatory variants are associated with serum protein levels and disease

Author

Valur Emilsson, Valborg Gudmundsdottir, Alexander Gudjonsson, Thorarinn Jonmundsson, Brynjolfur G. Jonsson, Mohd A. Karim, Marjan Ilkov, James R. Staley, Elias F. Gudmundsson, Lenore J. Launer, Jan H. Lindeman, Nicholas M. Morton, Thor Aspelund, John R. Lamb, Lori L. Jennings, Vilmundur Gudnason, Emilsson, Valur [0000-0001-9982-0524], Gudmundsdottir, Valborg [0000-0002-7459-1603], Jonmundsson, Thorarinn [0000-0001-9158-0087], Gudmundsson, Elias F [0000-0002-7661-4872], Launer, Lenore J [0000-0002-3238-7612], Morton, Nicholas M [0000-0001-8218-8462], Aspelund, Thor [0000-0002-7998-5433], Jennings, Lori L [0000-0001-5130-8417], Gudnason, Vilmundur [0000-0001-5696-0084], and Apollo - University of Cambridge Repository

Subjects

Proteomics, Male, Genotype, Proteome, Science, 631/208/205/2138, 45/43, Iceland, General Physics and Astronomy, 631/45/475, Genome-wide association studies, Polymorphism, Single Nucleotide, General Biochemistry, Genetics and Molecular Biology, 82/80, Prognostic markers, 692/53/2422, Humans, Disease, Exome, Genetic Predisposition to Disease, Aged, Multidisciplinary, article, General Chemistry, Blood Proteins, Female

Abstract

Circulating proteins can be used to diagnose and predict disease-related outcomes. A deep serum proteome survey recently revealed close associations between serum protein networks and common disease. In the current study, 54,469 low-frequency and common exome-array variants were compared to 4782 protein measurements in the serum of 5343 individuals from the AGES Reykjavik cohort. This analysis identifies a large number of serum proteins with genetic signatures overlapping those of many diseases. More specifically, using a study-wide significance threshold, we find that 2021 independent exome array variants are associated with serum levels of 1942 proteins. These variants reside in genetic loci shared by hundreds of complex disease traits, highlighting serum proteins’ emerging role as biomarkers and potential causative agents of a wide range of diseases., Finding the genetic basis of protein expression can elucidate the genetic mechanisms of disease. Here, the authors link low-frequency and common DNA sequence variants to thousands of serum proteins, finding genetic overlap between circulating proteins and a wide range of common diseases.

Published

2022

25. The role of the tryptophan-NAD + pathway in a mouse model of severe malnutrition induced liver dysfunction

Author

Guanlan Hu, Catriona Ling, Lijun Chi, Mehakpreet K. Thind, Samuel Furse, Albert Koulman, Jonathan R. Swann, Dorothy Lee, Marjolein M. Calon, Celine Bourdon, Christian J. Versloot, Barbara M. Bakker, Gerard Bryan Gonzales, Peter K. Kim, Robert H. J. Bandsma, Furse, Samuel [0000-0003-4267-2051], Koulman, Albert [0000-0001-9998-051X], Versloot, Christian J [0000-0002-3991-6652], Kim, Peter K [0000-0001-6626-0575], Bandsma, Robert HJ [0000-0001-6358-4750], Apollo - University of Cambridge Repository, Center for Liver, Digestive and Metabolic Diseases (CLDM), Molecular Cell Physiology, and AIMMS

Subjects

96, General Physics and Astronomy, 631/80/642/333/1465, 59, General Biochemistry, Genetics and Molecular Biology, 82/80, Mice, Voeding, Metabolisme en Genomica, 14/34, Voeding, Animals, Life Science, 96/1, Nutrition, 64, Multidisciplinary, 692/4020/4021/1607, Liver Diseases, article, Tryptophan, General Chemistry, NAD, Metabolism and Genomics, Metabolisme en Genomica, 64/60, Nutrition, Metabolism and Genomics, 692/699/1702/295

Abstract

Mortality in children with severe malnutrition is strongly related to signs of metabolic dysfunction, such as hypoglycemia. Lower circulating tryptophan levels in children with severe malnutrition suggest a possible disturbance in the tryptophan-nicotinamide adenine dinucleotide (TRP-NAD+) pathway and subsequently in NAD+ dependent metabolism regulator sirtuin1 (SIRT1). Here we show that severe malnutrition in weanling mice, induced by 2-weeks of low protein diet feeding from weaning, leads to an impaired TRP-NAD+ pathway with decreased NAD+ levels and affects hepatic mitochondrial turnover and function. We demonstrate that stimulating the TRP-NAD+ pathway with NAD+ precursors improves hepatic mitochondrial and overall metabolic function through SIRT1 modulation. Activating SIRT1 is sufficient to induce improvement in metabolic functions. Our findings indicate that modulating the TRP-NAD+ pathway can improve liver metabolic function in a mouse model of severe malnutrition. These results could lead to the development of new interventions for children with severe malnutrition.

Published

2022

26. Male-Specific Protein Disulphide Isomerase Function is Essential for Plasmodium Transmission and a Vulnerable Target for Intervention

Author

Sofia Tapanelli, Katarzyna A. Sala, George K. Christophides, Andrew M. Blagborough, Fiona Angrisano, Christophides, George K [0000-0002-3323-1687], Apollo - University of Cambridge Repository, Medical Research Council (MRC), Bill & Melinda Gates Foundation, and Christophides, George K. [0000-0002-3323-1687]

Subjects

0301 basic medicine, Male, GAMETE FUSION, Plasmodium berghei, Protozoan Proteins, lcsh:Medicine, Isomerase, Pharmacology, 0601 Biochemistry and Cell Biology, law.invention, Mice, law, Parasite physiology, 631/326/417/1716, HAP2, BERGHEI, lcsh:Science, CANDIDATES, 64, 631/326/417/2552, Multidisciplinary, SURFACE PROTEIN, article, 631/80/470, IMMUNIZATION, 3. Good health, Parasite biology, Multidisciplinary Sciences, medicine.anatomical_structure, Transmission (mechanics), Mechanisms of disease, BLOCKING IMMUNITY, Gamete, Science & Technology - Other Topics, Female, 64/60, 631/80/304, Antibody, 82/1, medicine.drug, inorganic chemicals, Isomerase activity, 0299 Other Physical Sciences, 030106 microbiology, Protein Disulfide-Isomerases, Bacitracin, Biology, 14/1, 82/80, 03 medical and health sciences, Antimalarials, MALARIA, Malaria Vaccines, medicine, KINASE, Animals, Protein folding, PDI FAMILY, 14/35, 38/109, Science & Technology, 82, lcsh:R, medicine.disease, nervous system diseases, body regions, 030104 developmental biology, biology.protein, lcsh:Q, Malaria, Function (biology)

Abstract

Inhibiting transmission of Plasmodium is an essential strategy in malaria eradication, and the biological process of gamete fusion during fertilization is a proven target for this approach. Lack of knowledge of the mechanisms underlying fertilization have been a hindrance in the development of transmission-blocking interventions. Here we describe a protein disulphide isomerase essential for malarial transmission (PDI-Trans/PBANKA_0820300) to the mosquito. We show that PDI-Trans activity is male-specific, surface-expressed, essential for fertilization/transmission, and exhibits disulphide isomerase activity which is up-regulated post-gamete activation. We demonstrate that PDI-Trans is a viable anti-malarial drug and vaccine target blocking malarial transmission with the use of PDI inhibitor bacitracin (98.21%/92.48% reduction in intensity/prevalence), and anti-PDI-Trans antibodies (66.22%/33.16% reduction in intensity/prevalence). To our knowledge, these results provide the first evidence that PDI function is essential for malarial transmission, and emphasize the potential of anti-PDI agents to act as anti-malarials, facilitating the future development of novel transmission-blocking interventions.

Published

2019

27. Mapping the serum proteome to neurological diseases using whole genome sequencing

Author

Xia Shen, Eleftheria Zeggini, Eleanor Wheeler, Maik Pietzner, Andrei Barysenka, James F. Wilson, Nicholas J. Wareham, Anders Mälarstig, George Dedoussis, Linda Repetto, Maria Karaleftheri, Pau Navarro, Emmanouil Tsafantakis, Grace Png, Claudia Langenberg, Arthur Gilly, Png, Grace [0000-0003-3962-7436], Navarro, Pau [0000-0001-5576-8584], Shen, Xia [0000-0003-4390-1979], Pietzner, Maik [0000-0003-3437-9963], Wheeler, Eleanor [0000-0002-8616-6444], Wareham, Nicholas [0000-0003-1422-2993], Langenberg, Claudia [0000-0002-5017-7344], Mälarstig, Anders [0000-0003-2608-1358], Wilson, James F [0000-0001-5751-9178], Zeggini, Eleftheria [0000-0003-4238-659X], Apollo - University of Cambridge Repository, and Wareham, Nicholas J [0000-0003-1422-2993]

Subjects

Proteome, Sialic Acid Binding Ig-like Lectin 3, 45/43, General Physics and Astronomy, Gene Expression, Disease, Genome-wide association studies, Cohort Studies, Multidisciplinary, Membrane Glycoproteins, Neurodevelopmental disorders, Scavenger Receptors, Class A, Parkinson Disease, symbols, 82/1, Science, Quantitative Trait Loci, 631/208/205/2138, 45/23, Computational biology, Biology, Quantitative trait locus, Predictive markers, General Biochemistry, Genetics and Molecular Biology, Article, MSR1, 82/80, symbols.namesake, Alzheimer Disease, 692/53/2423, 631/208/366, 692/699/375, Humans, Genetic Predisposition to Disease, Whole genome sequencing, GPNMB, 45, Whole Genome Sequencing, Genome, Human, Molecular Sequence Annotation, General Chemistry, Mendelian Randomization Analysis, Genetic architecture, Gene Ontology, Mendelian inheritance, Schizophrenia, Neurological disorders, Biomarkers

Abstract

Despite the increasing global burden of neurological disorders, there is a lack of effective diagnostic and therapeutic biomarkers. Proteins are often dysregulated in disease and have a strong genetic component. Here, we carry out a protein quantitative trait locus analysis of 184 neurologically-relevant proteins, using whole genome sequencing data from two isolated population-based cohorts (N = 2893). In doing so, we elucidate the genetic landscape of the circulating proteome and its connection to neurological disorders. We detect 214 independently-associated variants for 107 proteins, the majority of which (76%) are cis-acting, including 114 variants that have not been previously identified. Using two-sample Mendelian randomisation, we identify causal associations between serum CD33 and Alzheimer’s disease, GPNMB and Parkinson’s disease, and MSR1 and schizophrenia, describing their clinical potential and highlighting drug repurposing opportunities., Serum proteins are easily accessible biomarkers and drug targets. Here, the authors use whole genome sequencing data to describe the genetic architecture of neurologically-relevant serum proteins and establish causal protein-neurological disease relationships.

Published

2021

28. Somatic genetic rescue of a germline ribosome assembly defect

Author

Vasileios Kargas, Mélanie Parisot, Norberto Escudero-Urquijo, Alexis Bertrand, Christine Bellanné-Chantelot, Jean Donadieu, Mohammed Zarhrate, Patrick Nitschke, Cécile Masson, Laëtitia Kermasson, Beatriz Goyenechea, Sophie Kaltenbach, Alan J. Warren, David Traynor, Stefano Fumagalli, Li Jin, Blandine Beaupain, Bruno Reversade, Ahmed Z. Boukerrou, Peter J. Bond, M. Rossmann, Olivier Alibeu, Jean-Alain Martignoles, Christine Bole-Feysot, Jonathan Moreil, Shengjiang Tan, François Delhommeau, Patrick Revy, Kong Boo Phua, Alexandre Faille, Aurore Pouliet, Christine Hilcenko, Frédéric Tores, Isabelle Radford-Weiss, Ai Ling Koh, Isabelle Callebaut, Jean-Pierre de Villartay, Cambridge Institute for Medical Research (CIMR), University of Cambridge [UK] (CAM), Wellcome Trust-Medical Research Council Cambridge Stem Cell Institute, Imagine - Institut des maladies génétiques (IHU) (Imagine - U1163), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Paris (UP), MRC Laboratory of Molecular Biology [Cambridge, UK] (LMB), University of Cambridge [UK] (CAM)-Medical Research Council, Structure Fédérative de Recherche Necker (SFR Necker - UMS 3633 / US24), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université de Paris (UP), CHU Trousseau [APHP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), Institut Necker Enfants-Malades (INEM - UM 111 (UMR 8253 / U1151)), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université de Paris (UP), Université Paris Descartes - Paris 5 (UPD5), CHU Necker - Enfants Malades [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Centre de Recherche Saint-Antoine (CR Saint-Antoine), Sorbonne Université (SU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-CHU Saint-Antoine [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), KK Women's and Children's Hospital [Singapore], Genome Institute of Singapore (GIS), Bioinformatics Institute [Singapore], Agency for science, technology and research [Singapore] (A*STAR), National University of Singapore (NUS), CHU Pitié-Salpêtrière [AP-HP], Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Sorbonne Université (SU), Institut de minéralogie, de physique des matériaux et de cosmochimie (IMPMC), Muséum national d'Histoire naturelle (MNHN)-Institut de recherche pour le développement [IRD] : UR206-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Paris Cité (UPCité), Babraham Research Campus [Cambridge, Royaume-Uni], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité), Université Sorbonne Paris Cité (USPC), Centre de Recherche Saint-Antoine (CRSA), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU), ACS - Heart failure & arrhythmias, ARD - Amsterdam Reproduction and Development, Escudero-Urquijo, Norberto [0000-0002-8201-5884], Parisot, Mélanie [0000-0003-4312-2035], Reversade, Bruno [0000-0002-4070-7997], Bond, Peter J. [0000-0003-2900-098X], Bellanné-Chantelot, Christine [0000-0001-8415-6771], Warren, Alan J. [0000-0001-9277-4553], Revy, Patrick [0000-0003-0758-8022], Apollo - University of Cambridge Repository, Service de Génétique Cytogénétique et Embryologie [CHU Pitié-Salpêtrière], Hilcenko, Christine [0000-0002-9596-7833], Rossmann, Maxim [0000-0001-8811-3277], Bond, Peter J [0000-0003-2900-098X], Warren, Alan [0000-0001-9277-4553], Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Paris Cité (UPC), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPC), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPC), HAL-SU, Gestionnaire, ANR-18-IDEX-0001,Université de Paris,Université de Paris(2018), Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), and Warren, Alan J [0000-0001-9277-4553]

Subjects

Somatic cell, [SDV]Life Sciences [q-bio], General Physics and Astronomy, [SDV.BC.BC]Life Sciences [q-bio]/Cellular Biology/Subcellular Processes [q-bio.SC], Germline, 631/208/737, 692/699/1541, Ribosome assembly, 13/1, 0302 clinical medicine, hemic and lymphatic diseases, 38/22, Dictyostelium, Eukaryotic Initiation Factors, Child, Cells, Cultured, Biological Phenomena, Genetics, 0303 health sciences, Multidisciplinary, 631/208/514/2254, article, [SDV.MHEP.HEM]Life Sciences [q-bio]/Human health and pathology/Hematology, Ribosome Subunits, Large, Eukaryotic, Ribosome, Shwachman-Diamond Syndrome, 3. Good health, [SDV] Life Sciences [q-bio], 64/24, [SDV.IMM.IA]Life Sciences [q-bio]/Immunology/Adaptive immunology, 030220 oncology & carcinogenesis, Child, Preschool, Drosophila, Haematological diseases, Protein Binding, Adult, congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, Science, 45/23, Saccharomyces cerevisiae, Biology, Molecular Dynamics Simulation, General Biochemistry, Genetics and Molecular Biology, 82/80, 03 medical and health sciences, Young Adult, Germline mutation, Animals, Humans, Gene, Ribonucleoprotein, U5 Small Nuclear, 030304 developmental biology, Sequence Homology, Amino Acid, Eukaryotic Large Ribosomal Subunit, Point mutation, Infant, Proteins, [SDV.BBM.BM]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Molecular biology, General Chemistry, SBDS, 96/44, Peptide Elongation Factors, Germ Cells, [SDV.GEN.GH]Life Sciences [q-bio]/Genetics/Human genetics, Protein Biosynthesis, Mutation, Next-generation sequencing, 631/337/574/1789, Ribosomes

Abstract

Indirect somatic genetic rescue (SGR) of a germline mutation is thought to be rare in inherited Mendelian disorders. Here, we establish that acquired mutations in the EIF6 gene are a frequent mechanism of SGR in Shwachman-Diamond syndrome (SDS), a leukemia predisposition disorder caused by a germline defect in ribosome assembly. Biallelic mutations in the SBDS or EFL1 genes in SDS impair release of the anti-association factor eIF6 from the 60S ribosomal subunit, a key step in the translational activation of ribosomes. Here, we identify diverse mosaic somatic genetic events (point mutations, interstitial deletion, reciprocal chromosomal translocation) in SDS hematopoietic cells that reduce eIF6 expression or disrupt its interaction with the 60S subunit, thereby conferring a selective advantage over non-modified cells. SDS-related somatic EIF6 missense mutations that reduce eIF6 dosage or eIF6 binding to the 60S subunit suppress the defects in ribosome assembly and protein synthesis across multiple SBDS-deficient species including yeast, Dictyostelium and Drosophila. Our data suggest that SGR is a universal phenomenon that may influence the clinical evolution of diverse Mendelian disorders and support eIF6 suppressor mimics as a therapeutic strategy in SDS., Shwachman-Diamond syndrome (SDS) is a leukemia predisposition disorder that is caused by defective release of eIF6 during ribosome assembly. Here the authors show that acquired somatic EIF6 mutations are frequent in the hematopoietic cells from individuals with SDS and provide a selective advantage over non-modified cells.

Published

2021

29. StemBond hydrogels control the mechanical microenvironment for pluripotent stem cells

Author

Bao Xiu Tan, Céline Labouesse, Carla Mulas, Alexander K. Winkel, Moritz Hofer, Christophe M. Verstreken, Chibeza C. Agley, Kevin J. Chalut, José C. R. Silva, Giuliano Giuseppe Stirparo, Paul Bertone, Kristian Franze, William Mansfield, Hannah T. Stuart, Labouesse, Céline [0000-0002-9791-898X], Hofer, Moritz [0000-0002-9714-0143], Stirparo, Giuliano G. [0000-0002-5911-8682], Verstreken, Christophe M. [0000-0001-9038-1094], Mulas, Carla [0000-0002-9492-6482], Franze, Kristian [0000-0002-8425-7297], Silva, José C. R. [0000-0001-5487-1117], Chalut, Kevin J. [0000-0001-6200-9690], Apollo - University of Cambridge Repository, Stirparo, Giuliano G [0000-0002-5911-8682], Verstreken, Christophe M [0000-0001-9038-1094], Silva, José CR [0000-0001-5487-1117], Chalut, Kevin J [0000-0001-6200-9690], and Chalut, Kevin [0000-0001-6200-9690]

Subjects

Pluripotent Stem Cells, Embryonic stem cells, 631/61/54/2295, Science, Cell Culture Techniques, General Physics and Astronomy, 631/61/2320, macromolecular substances, Matrix (biology), 13, Mechanotransduction, Cellular, 14, Stem-cell biotechnology, General Biochemistry, Genetics and Molecular Biology, 38, 38/91, Extracellular matrix, 631/532/2435, 82/80, Mice, 631/532/2117, Stem cell fate specification, 13/100, 14/3, Cell Adhesion, 38/88, Animals, Humans, 14/19, Induced pluripotent stem cell, Cells, Cultured, Multidisciplinary, Chemistry, technology, industry, and agriculture, article, Reprogramming, Cell Differentiation, Hydrogels, General Chemistry, Embryonic stem cell, Cell biology, Biomechanical Phenomena, Extracellular Matrix, Self-healing hydrogels, 14/63, Biomaterials - cells, Stem cell

Abstract

Funder: Medical Research Council (UK) Career Development Award (G1100312/1), Funder: Medical Research Council (UK) MR/M011089/1 Wellcome Trust-Medical Research Council core funding to the Wellcome-MRC Cambridge Stem Cell Institute, Studies of mechanical signalling are typically performed by comparing cells cultured on soft and stiff hydrogel-based substrates. However, it is challenging to independently and robustly control both substrate stiffness and extracellular matrix tethering to substrates, making matrix tethering a potentially confounding variable in mechanical signalling investigations. Moreover, unstable matrix tethering can lead to poor cell attachment and weak engagement of cell adhesions. To address this, we developed StemBond hydrogels, a hydrogel in which matrix tethering is robust and can be varied independently of stiffness. We validate StemBond hydrogels by showing that they provide an optimal system for culturing mouse and human pluripotent stem cells. We further show how soft StemBond hydrogels modulate stem cell function, partly through stiffness-sensitive ERK signalling. Our findings underline how substrate mechanics impact mechanosensitive signalling pathways regulating self-renewal and differentiation, indicating that optimising the complete mechanical microenvironment will offer greater control over stem cell fate specification.

Published

2021

30. Higher-order phosphatase–substrate contacts terminate the integrated stress response

Author

David Ron, Yahui Yan, Heather P. Harding, Yan, Yahui [0000-0001-6934-9874], Harding, Heather P. [0000-0002-7359-7974], Ron, David [0000-0002-3014-5636], and Apollo - University of Cambridge Repository

Subjects

Models, Molecular, Hydrolases, Protein subunit, 631/535/1258/1259, Phosphatase, 13/106, CHO Cells, 13/109, Crystallography, X-Ray, 631/45/173, 631/45/607/1164, Dephosphorylation, 82/80, chemistry.chemical_compound, Phosphoserine, eIF-2 Kinase, Cricetulus, Structural Biology, Stress, Physiological, Catalytic Domain, Protein Phosphatase 1, Integrated stress response, Animals, Humans, Phosphorylation, Molecular Biology, 14/35, 82/83, biology, 82/16, Kinase, 9/10, Cryoelectron Microscopy, 101/28, article, Active site, Reproducibility of Results, Actins, Cell biology, 13/31, chemistry, 631/80/458/1733, Enzyme mechanisms, 14/63, biology.protein

Abstract

Many regulatory PPP1R subunits join few catalytic PP1c subunits to mediate phosphoserine and phosphothreonine dephosphorylation in metazoans. Regulatory subunits engage the surface of PP1c, locally affecting flexible access of the phosphopeptide to the active site. However, catalytic efficiency of holophosphatases towards their phosphoprotein substrates remains unexplained. Here we present a cryo-EM structure of the tripartite PP1c–PPP1R15A–G-actin holophosphatase that terminates signaling in the mammalian integrated stress response (ISR) in the pre-dephosphorylation complex with its substrate, translation initiation factor 2α (eIF2α). G-actin, whose essential role in eIF2α dephosphorylation is supported crystallographically, biochemically and genetically, aligns the catalytic and regulatory subunits, creating a composite surface that engages the N-terminal domain of eIF2α to position the distant phosphoserine-51 at the active site. Substrate residues that mediate affinity for the holophosphatase also make critical contacts with eIF2α kinases. Thus, a convergent process of higher-order substrate recognition specifies functionally antagonistic phosphorylation and dephosphorylation in the ISR., Structures of the dephosphorylation complex for phosphorylated eIF2α reveal how contacts with the regulatory PPP1R15A subunit mediate substrate selectivity, providing a paradigm for dephosphorylation reactions by diverse combinatorially assembled holophosphatases.

Published

2021

31. SMARCA4/2 loss inhibits chemotherapy-induced apoptosis by restricting IP3R3-mediated Ca 2+ flux to mitochondria

Author

Sophie Camilleri-Broët, Fraser Johnson, Anie Monast, Janusz Rak, Walter H. Gotlieb, Jonathan Spicer, Zheng Fu, Virginie Pilon, Sidong Huang, William W. Lockwood, Jordan L. Morris, Yibo Xue, Pierre Fiset, William D. Foulkes, Tunde Golenar, Mackenzie Coatham, Julien Prudent, Brian Meehan, Marie-Christine Guiot, Lynne-Marie Postovit, Leora Witkowski, Geneviève Morin, Lili Fu, Sungmi Jung, Xianbing Zhu, Kangning Yang, Anne V. Gonzalez, Morag Park, Amber Yasmeen, Xue, Yibo [0000-0003-4252-4446], Morris, Jordan L. [0000-0002-4663-4776], Yang, Kangning [0000-0002-5211-913X], Witkowski, Leora [0000-0002-5736-2534], Camilleri-Broet, Sophie [0000-0002-3453-636X], Spicer, Jonathan [0000-0003-2708-1309], Rak, Janusz [0000-0002-2912-5566], Park, Morag [0000-0001-5400-606X], Lockwood, William [0000-0001-9831-3408], Foulkes, William D. [0000-0001-7427-4651], Prudent, Julien [0000-0003-3821-6088], Huang, Sidong [0000-0002-2838-4726], Apollo - University of Cambridge Repository, Morris, Jordan L [0000-0002-4663-4776], and Foulkes, William D [0000-0001-7427-4651]

Subjects

Male, 49/47, General Physics and Astronomy, Apoptosis, Mice, SCID, 13/2, 0302 clinical medicine, 13/44, Intracellular organelle, Mice, Inbred NOD, Neoplasms, Inositol 1,4,5-Trisphosphate Receptors, 14/19, 13/89, Mice, Knockout, 0303 health sciences, Multidisciplinary, Chemistry, Histone deacetylase inhibitor, article, Nuclear Proteins, 3. Good health, Chromatin, Mitochondria, 631/67/68/2486, Gene Expression Regulation, Neoplastic, 13/31, 030220 oncology & carcinogenesis, 631/67/1244, SMARCA4, 38/39, medicine.drug, 631/80/82/23, medicine.drug_class, 631/67/1059/2326, Science, Antineoplastic Agents, 13/106, General Biochemistry, Genetics and Molecular Biology, Chromatin remodeling, 82/80, 03 medical and health sciences, Cell Line, Tumor, medicine, Animals, Humans, 030304 developmental biology, Cisplatin, Ion Transport, Gene Expression Profiling, DNA Helicases, General Chemistry, Xenograft Model Antitumor Assays, HEK293 Cells, Cancer cell, Mutation, 13/95, 13/51, Cancer research, Calcium, 38/15, Transcription Factors

Abstract

Acknowledgements: The authors thank A. Leary for sharing RNA-seq data and R. Hass for sharing the SCCOHT-1 cells. The authors thank members of the Pelletier Laboratory for assistance with flow cytometry studies. This work was supported by Canadian Institutes of Health Research (CIHR) grants MOP-130540, PJT-156233, and PJT-438303 to S.H. and grant FDN-148390 to W.D.F. and a core grant from Medical Research Council (MRC) MC_UU_00015/7 to J.P. Author Y.X. was supported by CIHR Fellowship (MFE-171249), J.L.M. was supported by a MRC-funded graduate student fellowship, and S.H. was supported by a CRC Chair in Functional Genomics., Inactivating mutations in SMARCA4 and concurrent epigenetic silencing of SMARCA2 characterize subsets of ovarian and lung cancers. Concomitant loss of these key subunits of SWI/SNF chromatin remodeling complexes in both cancers is associated with chemotherapy resistance and poor prognosis. Here, we discover that SMARCA4/2 loss inhibits chemotherapy-induced apoptosis through disrupting intracellular organelle calcium ion (Ca2+) release in these cancers. By restricting chromatin accessibility to ITPR3, encoding Ca2+ channel IP3R3, SMARCA4/2 deficiency causes reduced IP3R3 expression leading to impaired Ca2+ transfer from the endoplasmic reticulum to mitochondria required for apoptosis induction. Reactivation of SMARCA2 by a histone deacetylase inhibitor rescues IP3R3 expression and enhances cisplatin response in SMARCA4/2-deficient cancer cells both in vitro and in vivo. Our findings elucidate the contribution of SMARCA4/2 to Ca2+-dependent apoptosis induction, which may be exploited to enhance chemotherapy response in SMARCA4/2-deficient cancers.

Published

2021

32. Structures of a deAMPylation complex rationalise the switch between antagonistic catalytic activities of FICD

Author

David Ron, Luke A. Perera, Nathan R. Zaccai, Juliette M. Devos, Michael Haertlein, Steffen Preissler, Sylvain Prévost, Perera, Luke A [0000-0002-0032-1176], Preissler, Steffen [0000-0001-7936-9836], Zaccai, Nathan R [0000-0002-1476-2044], Prévost, Sylvain [0000-0002-6008-1987], Devos, Juliette M [0000-0001-5989-6794], Ron, David [0000-0002-3014-5636], Apollo - University of Cambridge Repository, Perera, Luke A. [0000-0002-0032-1176], Zaccai, Nathan R. [0000-0002-1476-2044], and Devos, Juliette M. [0000-0001-5989-6794]

Subjects

82/29, genetic structures, Amino Acid Motifs, General Physics and Astronomy, 631/45/173, 0302 clinical medicine, Adenosine Triphosphate, Chaperones, Endoplasmic Reticulum Chaperone BiP, Heat-Shock Proteins, 631/337/458, chemistry.chemical_classification, 0303 health sciences, Multidisciplinary, biology, article, Nucleotidyltransferases, 3. Good health, Tetratricopeptide, Enzyme mechanisms, 631/45/470/1981, 82/1, Dimerization, Stereochemistry, 145, Science, 13/106, 13/109, 631/337/470/1463, General Biochemistry, Genetics and Molecular Biology, Catalysis, 82/80, 03 medical and health sciences, Residue (chemistry), Humans, Adenylylation, 82/83, X-ray crystallography, 030304 developmental biology, 82/16, Endoplasmic reticulum, Membrane Proteins, General Chemistry, Solution structure, Adenosine Monophosphate, Enzyme, chemistry, 631/535/1266, Chaperone (protein), biology.protein, Biocatalysis, Protein Processing, Post-Translational, 030217 neurology & neurosurgery, Post-translational modifications

Abstract

The endoplasmic reticulum (ER) Hsp70 chaperone BiP is regulated by AMPylation, a reversible inactivating post-translational modification. Both BiP AMPylation and deAMPylation are catalysed by a single ER-localised enzyme, FICD. Here we present crystallographic and solution structures of a deAMPylation Michaelis complex formed between mammalian AMPylated BiP and FICD. The latter, via its tetratricopeptide repeat domain, binds a surface that is specific to ATP-state Hsp70 chaperones, explaining the exquisite selectivity of FICD for BiP’s ATP-bound conformation both when AMPylating and deAMPylating Thr518. The eukaryotic deAMPylation mechanism thus revealed, rationalises the role of the conserved Fic domain Glu234 as a gatekeeper residue that both inhibits AMPylation and facilitates hydrolytic deAMPylation catalysed by dimeric FICD. These findings point to a monomerisation-induced increase in Glu234 flexibility as the basis of an oligomeric state-dependent switch between FICD’s antagonistic activities, despite a similar mode of engagement of its two substrates — unmodified and AMPylated BiP., The ER chaperone BiP is regulated by FICD-mediated AMPylation and deAMPylation. Here, the authors characterise the structure of mammalian AMPylated BiP bound to FICD, by X-ray crystallography and neutron scattering, providing insights into the mechanism of BiP AMPylation and deAMPylation.

Published

2021

33. Synaptic control of DNA methylation involves activity-dependent degradation of DNMT3A1 in the nucleus

Author

Gonca Bayraktar, Oliver Stork, Ferah Yildirim, Guilherme M. Gomes, Anna Karpova, Shoji Tajima, Michael R. Kreutz, PingAn Yuanxiang, Alessandro D. Confettura, Syed Ahsan Raza, Isao Suetake, Bayraktar, Gonca [0000-0001-5476-4346], Yuanxiang, PingAn [0000-0002-3746-3282], Gomes, Guilherme M. [0000-0001-8566-4284], Suetake, Isao [0000-0002-1246-8474], Kreutz, Michael R. [0000-0003-0575-6950], Apollo - University of Cambridge Repository, Gomes, Guilherme M [0000-0001-8566-4284], and Kreutz, Michael R [0000-0003-0575-6950]

Subjects

Methyltransferase, Protein subunit, 96, 13/106, 13/109, 14, NEDD8, Receptors, N-Methyl-D-Aspartate, 82/80, 13/1, Memory, genetics [Receptors, N-Methyl-D-Aspartate], ddc:610, Epigenetics, 14/19, metabolism [Receptors, N-Methyl-D-Aspartate], 14/35, Pharmacology, Neurons, Neuronal Plasticity, Chemistry, Epigenetics and plasticity, 9/30, article, metabolism [Synapses], DNA Methylation, Neuroscience, Cell biology, Psychiatry and Mental health, metabolism [Neurons], 13/51, 13/95, 14/63, DNA methylation, Synaptic plasticity, Synapses, NMDA receptor, 64/60, Neddylation, 631/378, 631/378/2584/1695

Abstract

DNA methylation is a crucial epigenetic mark for activity-dependent gene expression in neurons. Very little is known about how synaptic signals impact promoter methylation in neuronal nuclei. In this study we show that protein levels of the principal de novo DNA-methyltransferase in neurons, DNMT3A1, are tightly controlled by activation of N-methyl-D-aspartate receptors (NMDAR) containing the GluN2A subunit. Interestingly, synaptic NMDARs drive degradation of the methyltransferase in a neddylation-dependent manner. Inhibition of neddylation, the conjugation of the small ubiquitin-like protein NEDD8 to lysine residues, interrupts degradation of DNMT3A1. This results in deficits in promoter methylation of activity-dependent genes, as well as synaptic plasticity and memory formation. In turn, the underlying molecular pathway is triggered by the induction of synaptic plasticity and in response to object location learning. Collectively, the data show that plasticity-relevant signals from GluN2A-containing NMDARs control activity-dependent DNA-methylation involved in memory formation.

Published

2021

34. The architecture and stabilisation of flagellotropic tailed bacteriophages

Author

Derek Pickard, Jiawei Wang, Trevor Lithgow, Joshua M. Hardy, Gordon Dougan, Matthew J. Belousoff, Rhys Grinter, Rhys A. Dunstan, Fasséli Coulibaly, Hariprasad Venugopal, Hardy, Joshua M [0000-0002-8014-8552], Dunstan, Rhys A [0000-0002-7161-3993], Grinter, Rhys [0000-0002-8195-5348], Lithgow, Trevor [0000-0002-0102-7884], Coulibaly, Fasséli [0000-0003-3380-2117], Apollo - University of Cambridge Repository, Hardy, Joshua M. [0000-0002-8014-8552], and Dunstan, Rhys A. [0000-0002-7161-3993]

Subjects

0301 basic medicine, 145, Science, Amino Acid Motifs, Phage biology, General Physics and Astronomy, Flagellum, Protein Structure, Secondary, General Biochemistry, Genetics and Molecular Biology, 631/326/596/432, Bacteriophage, 82/80, 03 medical and health sciences, chemistry.chemical_compound, Protein structure, Viral genetics, Dna genetics, 631/45/535/1258, Electron microscopy, Bacteriophages, lcsh:Science, Herpesviridae, Multidisciplinary, 030102 biochemistry & molecular biology, biology, 82/16, Chemistry, 101/28, Virion, article, DNA, General Chemistry, Virus structures, biology.organism_classification, Dna translocation, Vitrification, 030104 developmental biology, Capsid, Flagella, 631/326/596/2148, DNA, Viral, Biophysics, Capsid Proteins, lcsh:Q, Protein Multimerization

Abstract

Funder: Sir Henry Wellcome Fellow (106077/Z/14/Z), Funder: Australian Research Council Laureate Fellow (FL130100038), Flagellotropic bacteriophages engage flagella to reach the bacterial surface as an effective means to increase the capture radius for predation. Structural details of these viruses are of great interest given the substantial drag forces and torques they face when moving down the spinning flagellum. We show that the main capsid and auxiliary proteins form two nested chainmails that ensure the integrity of the bacteriophage head. Core stabilising structures are conserved in herpesviruses suggesting their ancestral origin. The structure of the tail also reveals a robust yet pliable assembly. Hexameric rings of the tail-tube protein are braced by the N-terminus and a β-hairpin loop, and interconnected along the tail by the splayed β-hairpins. By contrast, we show that the β-hairpin has an inhibitory role in the tail-tube precursor, preventing uncontrolled self-assembly. Dyads of acidic residues inside the tail-tube present regularly-spaced motifs well suited to DNA translocation into bacteria through the tail.

Published

2021

35. Defective folate metabolism causes germline epigenetic instability and distinguishes Hira as a phenotype inheritance biomarker

Author

Georgina E T Blake, Hong Wa Yung, Russell S. Hamilton, Erica D. Watson, Anne C. Ferguson-Smith, Graham J Burton, Xiaohui Zhao, Zhao, Xiaohui [0000-0001-9922-2815], Burton, Graham J [0000-0001-8677-4143], Hamilton, Russell S [0000-0002-0598-3793], Watson, Erica D [0000-0003-4496-2271], Apollo - University of Cambridge Repository, Burton, Graham J. [0000-0001-8677-4143], Hamilton, Russell S. [0000-0002-0598-3793], and Watson, Erica D. [0000-0003-4496-2271]

Subjects

Epigenomics, Male, 0301 basic medicine, Heredity, Inheritance Patterns, 45/88, General Physics and Astronomy, Cell Cycle Proteins, Germline, Epigenesis, Genetic, Mice, 0302 clinical medicine, 38/22, 45/90, Genetics, Multidisciplinary, Methylation, Spermatozoa, Phenotype, Pedigree, Trophoblasts, Ferredoxin-NADP Reductase, 631/208/176, Liver, DNA methylation, 64/60, Epigenetics, Female, Maternal Inheritance, Reprogramming, Epigenetic memory, 631/136/2442, Science, 45/23, Biology, Polymorphism, Single Nucleotide, Article, General Biochemistry, Genetics and Molecular Biology, 82/80, 03 medical and health sciences, Folic Acid, Animals, Histone Chaperones, 631/443/319, Gene, Whole Genome Sequencing, 82/58, General Chemistry, DNA Methylation, Embryo, Mammalian, MTRR, Mice, Inbred C57BL, Metabolism, Germ Cells, 030104 developmental biology, Biomarkers, 030217 neurology & neurosurgery, Transcription Factors

Abstract

Funder: Center for Trophoblast Research, The mechanism behind transgenerational epigenetic inheritance is unclear, particularly through the maternal grandparental line. We previously showed that disruption of folate metabolism in mice by the Mtrr hypomorphic mutation results in transgenerational epigenetic inheritance of congenital malformations. Either maternal grandparent can initiate this phenomenon, which persists for at least four wildtype generations. Here, we use genome-wide approaches to reveal genetic stability in the Mtrr model and genome-wide differential DNA methylation in the germline of Mtrr mutant maternal grandfathers. We observe that, while epigenetic reprogramming occurs, wildtype grandprogeny and great grandprogeny exhibit transcriptional changes that correlate with germline methylation defects. One region encompasses the Hira gene, which is misexpressed in embryos for at least three wildtype generations in a manner that distinguishes Hira transcript expression as a biomarker of maternal phenotypic inheritance.

Published

2021

36. The C-terminal tail of α-synuclein protects against aggregate replication but is critical for oligomerization

Author

Azad Farzadfard, Jannik Nedergaard Pedersen, Georg Meisl, Arun Kumar Somavarapu, Parvez Alam, Louise Goksøyr, Morten Agertoug Nielsen, Adam Frederik Sander, Tuomas P. J. Knowles, Jan Skov Pedersen, Daniel Erik Otzen, Meisl, Georg [0000-0002-6562-7715], Goksøyr, Louise [0000-0003-4508-9857], Nielsen, Morten Agertoug [0000-0003-2668-4992], Sander, Adam Frederik [0000-0002-8782-7830], Knowles, Tuomas PJ [0000-0002-7879-0140], Pedersen, Jan Skov [0000-0002-7768-0206], Otzen, Daniel Erik [0000-0002-2918-8989], Apollo - University of Cambridge Repository, and Knowles, Tuomas [0000-0002-7879-0140]

Subjects

DISRUPTION, MECHANISM, 82/29, Amyloid, INFLUX, QH301-705.5, Static Electricity, Medicine (miscellaneous), TOXICITY, General Biochemistry, Genetics and Molecular Biology, 82/80, FIBRIL, Humans, Biology (General), 82/83, 631/57, Membranes, 82/16, 101/28, article, TRUNCATION, Parkinson Disease, NMR, X-RAY-SCATTERING, alpha-Synuclein, General Agricultural and Biological Sciences, 631/337

Abstract

Aggregation of the 140-residue protein α-synuclein (αSN) is a key factor in the etiology of Parkinson’s disease. Although the intensely anionic C-terminal domain (CTD) of αSN does not form part of the amyloid core region or affect membrane binding ability, truncation or reduction of charges in the CTD promotes fibrillation through as yet unknown mechanisms. Here, we study stepwise truncated CTDs and identify a threshold region around residue 121; constructs shorter than this dramatically increase their fibrillation tendency. Remarkably, these effects persist even when as little as 10% of the truncated variant is mixed with the full-length protein. Increased fibrillation can be explained by a substantial increase in self-replication, most likely via fragmentation. Paradoxically, truncation also suppresses toxic oligomer formation, and oligomers that can be formed by chemical modification show reduced membrane affinity and cytotoxicity. These remarkable changes correlate to the loss of negative electrostatic potential in the CTD and highlight a double-edged electrostatic safety guard.

Published

2021

37. MyD88 TIR domain higher-order assembly interactions revealed by microcrystal electron diffraction and serial femtosecond crystallography

Author

Andrew Aquila, Emma Sierecki, Chun Hong Yoon, Jingjing Zhao, Connie Darmanin, Tristan I. Croll, Md. Habibur Rahaman, Yann Gambin, Alpeshkumar K. Malde, Timothy W. Muusse, Parimala R. Vajjhala, Hongyi Xu, Max T. B. Clabbers, Sara J. Thygesen, Leonie Flueckiger, Mark S. Hunter, Brian Abbey, Bostjan Kobe, Nadia A. Zatsepin, Jeffrey D. Nanson, Katryn J. Stacey, Thomas Ve, Dominic J. B. Hunter, Susannah Holmes, Mengning Liang, Clabbers, Max T B [0000-0002-5466-6508], Muusse, Timothy W [0000-0003-4384-5647], Malde, Alpeshkumar K [0000-0002-8181-1619], Nanson, Jeffrey D [0000-0003-1306-1948], Aquila, Andrew [0000-0003-0358-2774], Hunter, Mark S [0000-0002-0110-7075], Zhao, Jingjing [0000-0001-8444-6883], Zatsepin, Nadia A [0000-0003-1757-0205], Abbey, Brian [0000-0001-6504-0503], Sierecki, Emma [0000-0001-9970-868X], Darmanin, Connie [0000-0002-4449-2233], Kobe, Bostjan [0000-0001-9413-9166], Xu, Hongyi [0000-0002-8271-3906], Ve, Thomas [0000-0002-0113-1905], Apollo - University of Cambridge Repository, Clabbers, Max T. B. [0000-0002-5466-6508], Muusse, Timothy W. [0000-0003-4384-5647], Malde, Alpeshkumar K. [0000-0002-8181-1619], Nanson, Jeffrey D. [0000-0003-1306-1948], Hunter, Mark S. [0000-0002-0110-7075], Zatsepin, Nadia A. [0000-0003-1757-0205], and Clabbers, Max TB [0000-0002-5466-6508]

Subjects

Models, Molecular, Protein Conformation, alpha-Helical, 631/45/535, 631/535/1258/1259, Beta sheet, General Physics and Astronomy, 96/31, Biochemistry, Molecular dynamics, 0302 clinical medicine, Protein structure, Cryoelectron microscopy, General Materials Science, 0303 health sciences, Multidisciplinary, Membrane Glycoproteins, Crystallography, Nanocrystallography, hemic and immune systems, Condensed Matter Physics, Recombinant Proteins, 3. Good health, Electron diffraction, Femtosecond, lipids (amino acids, peptides, and proteins), ddc:500, 631/535/1266/1265, Structural biology, Dimerization, Signal Transduction, Materials science, 145, Science, Protein domain, Molecular Dynamics Simulation, digestive system, General Biochemistry, Genetics and Molecular Biology, Article, 96/95, 82/80, Inorganic Chemistry, 03 medical and health sciences, Protein Domains, parasitic diseases, Humans, Physical and Theoretical Chemistry, 82/83, 631/250/262/2106/2108, 030304 developmental biology, 101/28, Mutagenesis, Receptors, Interleukin-1, General Chemistry, biochemical phenomena, metabolism, and nutrition, Toll-like receptors, Toll-Like Receptor 4, HEK293 Cells, Mutation, Myeloid Differentiation Factor 88, Protein Conformation, beta-Strand, sense organs, 030217 neurology & neurosurgery

Abstract

MyD88 and MAL are Toll-like receptor (TLR) adaptors that signal to induce pro-inflammatory cytokine production. We previously observed that the TIR domain of MAL (MALTIR) forms filaments in vitro and induces formation of crystalline higher-order assemblies of the MyD88 TIR domain (MyD88TIR). These crystals are too small for conventional X-ray crystallography, but are ideally suited to structure determination by microcrystal electron diffraction (MicroED) and serial femtosecond crystallography (SFX). Here, we present MicroED and SFX structures of the MyD88TIR assembly, which reveal a two-stranded higher-order assembly arrangement of TIR domains analogous to that seen previously for MALTIR. We demonstrate via mutagenesis that the MyD88TIR assembly interfaces are critical for TLR4 signaling in vivo, and we show that MAL promotes unidirectional assembly of MyD88TIR. Collectively, our studies provide structural and mechanistic insight into TLR signal transduction and allow a direct comparison of the MicroED and SFX techniques., MAL and MyD88 are downstream adaptors of Toll-like receptors (TLR) and the MAL TIR domain forms filaments in vitro, which in turn nucleate the assembly of crystalline arrays of the MyD88 TIR domain. Here, the authors present the structure of these MyD88 TIR crystalline arrays solved by both microcrystal electron diffraction and serial femtosecond crystallography, and they show with mutagenesis experiments that MyD88 interface residues are important for TLR4 signaling in vivo.

Published

2021

38. Maternal iron deficiency perturbs embryonic cardiovascular development in mice

Author

Dorota Szumska, Jack J. Miller, Magda Wolna, Aimée Jacquemot, Victor L. J. Tybulewicz, Michael Troup, Fabrice Prin, Eleni Giannoulatou, Helena Rodriguez-Caro, Eleanor M. Stuart, Emily Hardman, Jacob E Munro, Elizabeth M. C. Fisher, Samira Lakhal-Littleton, Nikita Ved, Sarah De Val, Eva Lana-Elola, Rifdat Aoidi, Jacinta I. Kalisch-Smith, Shelley Harris, Duncan B. Sparrow, Timothy J. Mohun, Kalisch-Smith, Jacinta I. [0000-0002-5071-3805], Munro, Jacob [0000-0002-2751-0989], Miller, Jack J. [0000-0002-6258-1299], Hardman, Emily [0000-0002-3073-0309], Fisher, Elizabeth M. C. [0000-0003-2850-9936], Tybulewicz, Victor L. J. [0000-0003-2439-0798], Sparrow, Duncan B. [0000-0002-1141-6613], Apollo - University of Cambridge Repository, Kalisch-Smith, Jacinta I [0000-0002-5071-3805], Miller, Jack J [0000-0002-6258-1299], Fisher, Elizabeth MC [0000-0003-2850-9936], Tybulewicz, Victor LJ [0000-0003-2439-0798], and Sparrow, Duncan B [0000-0002-1141-6613]

Subjects

0301 basic medicine, Heart disease, General Physics and Astronomy, Physiology, Aorta, Thoracic, Penetrance, 96/35, Cardiovascular System, 14, 38/1, 0302 clinical medicine, Pregnancy, Edema, Myocytes, Cardiac, Transgenes, 14/19, 692/308/1426, 64, Multidisciplinary, Stem Cells, article, food and beverages, Cell Differentiation, Iron deficiency, Iron Deficiencies, Coronary Vessels, humanities, 3. Good health, Experimental models of disease, Phenotype, In utero, Embryogenesis, Female, 64/60, 38/39, 82/1, 692/499, Signal Transduction, Down syndrome, Offspring, Science, Iron, Green Fluorescent Proteins, 631/136/2086, Embryonic Development, Tretinoin, General Biochemistry, Genetics and Molecular Biology, 38/91, 82/80, 14/1, 14/32, 03 medical and health sciences, 14/5, medicine, Genetic predisposition, Animals, 631/136/1425, Lymphatic Vessels, business.industry, Disease model, Gene Expression Profiling, Myocardium, General Chemistry, medicine.disease, Embryo, Mammalian, Teratology, Mice, Inbred C57BL, 030104 developmental biology, Risk factors, Dietary Supplements, 13/51, 14/63, 59/57, Gene-Environment Interaction, business, 030217 neurology & neurosurgery, Biomarkers

Abstract

Congenital heart disease (CHD) is the most common class of human birth defects, with a prevalence of 0.9% of births. However, two-thirds of cases have an unknown cause, and many of these are thought to be caused by in utero exposure to environmental teratogens. Here we identify a potential teratogen causing CHD in mice: maternal iron deficiency (ID). We show that maternal ID in mice causes severe cardiovascular defects in the offspring. These defects likely arise from increased retinoic acid signalling in ID embryos. The defects can be prevented by iron administration in early pregnancy. It has also been proposed that teratogen exposure may potentiate the effects of genetic predisposition to CHD through gene–environment interaction. Here we show that maternal ID increases the severity of heart and craniofacial defects in a mouse model of Down syndrome. It will be important to understand if the effects of maternal ID seen here in mice may have clinical implications for women., From mouse experiments, the authors link iron deficiency in mothers with cardiovascular defects and increased retinoic acid signalling in their offspring, and giving iron early in pregnancy can prevent most defects.

Published

2021

39. SWI/SNF subunit BAF155 N-terminus structure informs the impact of cancer-associated mutations and reveals a potential drug binding site

Author

Mark D. Allen, Giovanna Zinzalla, Stefan M.V. Freund, Mark Bycroft, Bycroft, Mark [0000-0002-0673-2216], Zinzalla, Giovanna [0000-0002-1130-4865], and Apollo - University of Cambridge Repository

Subjects

Models, Molecular, Cancer therapy, QH301-705.5, Protein Conformation, Protein subunit, 631/67/1059, 101/6, Medicine (miscellaneous), General Biochemistry, Genetics and Molecular Biology, Chromodomain, 82/80, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, Missense mutation, Humans, Binding site, Biology (General), 82/83, 030304 developmental biology, X-ray crystallography, 0303 health sciences, Binding Sites, Chemistry, article, Small molecule, SWI/SNF, Cell biology, BRCT domain, Pharmaceutical Preparations, 631/535/1266, 030220 oncology & carcinogenesis, Mutation, Drug Binding Site, General Agricultural and Biological Sciences, Transcription Factors

Abstract

SWI/SNF (BAF) chromatin remodelling complexes are key regulators of gene expression programs, and attractive drug targets for cancer therapies. Here we show that the N-terminus of the BAF155/SMARCC1 subunit contains a putative DNA-binding MarR-like domain, a chromodomain and a BRCT domain that are interconnected to each other to form a distinct module. In this structure the chromodomain makes interdomain interactions and has lost its canonical function to bind to methylated lysines. The structure provides new insights into the missense mutations that target this module in cancer. This study also reveals two adjacent, highly-conserved pockets in a cleft between the domains that form a potential binding site, which can be targeted with small molecules, offering a new strategy to target SWI/SNF complexes., Allen et al. determine crystal structure of the N-terminus of SWI/SNF chromatin remodelling factor subunit BAF155. They identify an interconnected structure of MarR-like, BRCT and chromodomains, visualise the potential effect of cancer-associated missense mutations and suggest a binding site and target for small molecule inhibitors.

Published

2021

40. Systemic α-synuclein injection triggers selective neuronal pathology as seen in patients with Parkinson’s disease

Author

Yanyan Zhao, Roger A. Barker, Xiaoling He, Franklin I. Aigbirhio, Katherine Stott, Jessica C. F. Kwok, Wei-Li Kuan, Sujeong Yang, Tobias C. Wood, Katie Hall, Anthony C. Vernon, Ole Tietz, Kuan, Wei-Li [0000-0002-0273-1320], Stott, Katherine [0000-0002-4014-1188], Kwok, Jessica CF [0000-0002-9798-9083], Vernon, Anthony C [0000-0001-7305-1069], Apollo - University of Cambridge Repository, Kwok, Jessica C. F. [0000-0002-9798-9083], and Vernon, Anthony C. [0000-0001-7305-1069]

Subjects

0301 basic medicine, Cellular pathology, Pathology, medicine.medical_specialty, Parkinson's disease, Endogeny, Neuropathology, Disease, Article, Enteric Nervous System, 82/80, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, medicine, Animals, Humans, 14/19, Molecular Biology, Pathological, Neurons, 96/106, 631/1647, business.industry, Neurodegeneration, Biological techniques, Brain, Parkinson Disease, medicine.disease, Psychiatry and Mental health, 030104 developmental biology, 59/57, Systemic administration, alpha-Synuclein, 82/6, 14/28, 631/378, 82/51, 82/1, business, 030217 neurology & neurosurgery, Neuroscience

Abstract

Parkinson’s disease (PD) is an α-synucleinopathy characterized by the progressive loss of specific neuronal populations. Here, we develop a novel approach to transvascularly deliver proteins of complex quaternary structures, including α-synuclein preformed fibrils (pff). We show that a single systemic administration of α-synuclein pff triggers pathological transformation of endogenous α-synuclein in non-transgenic rats, which leads to neurodegeneration in discrete brain regions. Specifically, pff-exposed animals displayed a progressive deterioration in gastrointestinal and olfactory functions, which corresponded with the presence of cellular pathology in the central and enteric nervous systems. The α-synuclein pathology generated was both time dependent and region specific. Interestingly, the most significant neuropathological changes were observed in those brain regions affected in the early stages of PD. Our data therefore demonstrate for the first time that a single, transvascular administration of α-synuclein pff can lead to selective regional neuropathology resembling the premotor stage of idiopathic PD. Furthermore, this novel delivery approach could also be used to deliver a range of other pathogenic, as well as therapeutic, protein cargos transvascularly to the brain.

Published

2019

41. Adaptation of Plasmodium falciparum to humans involved the loss of an ape-specific erythrocyte invasion ligand

Author

Manoj T. Duraisingh, Alison Kemp, Julian C. Rayner, Selasi Dankwa, William R. Proto, Paul M. Sharp, Gavin J. Wright, Zenon A. Zenonos, Steve Unwin, Weimin Liu, Sasha V. Siegel, Sarah Marsden, Beatrice H. Hahn, Proto, William R [0000-0003-2311-920X], Siegel, Sasha V [0000-0002-1458-4348], Dankwa, Selasi [0000-0002-1837-2924], Sharp, Paul M [0000-0001-9771-543X], Hahn, Beatrice H [0000-0002-9400-9887], Rayner, Julian C [0000-0002-9835-1014], Apollo - University of Cambridge Repository, Proto, William R. [0000-0003-2311-920X], Siegel, Sasha V. [0000-0002-1458-4348], Sharp, Paul M. [0000-0001-9771-543X], Hahn, Beatrice H. [0000-0002-9400-9887], and Rayner, Julian C. [0000-0002-9835-1014]

Subjects

0301 basic medicine, Erythrocytes, Protozoan Proteins, General Physics and Astronomy, medicine.disease_cause, 13, law.invention, 0302 clinical medicine, law, Loss of Function Mutation, 631/326/417/1716, Malaria, Falciparum, lcsh:Science, Frameshift Mutation, Cell Engineering, Genetics, Gene Editing, Mutation, Multidisciplinary, biology, article, Ligand (biochemistry), 3. Good health, Parasite biology, 13/31, Parasite evolution, Recombinant DNA, Pan troglodytes, Science, Plasmodium falciparum, 13/106, General Biochemistry, Genetics and Molecular Biology, Laverania, Host Specificity, Frameshift mutation, 38/91, 82/80, Evolution, Molecular, 03 medical and health sciences, parasitic diseases, medicine, 692/699/255/1629, Animals, Humans, 631/326/417/2548, Gene, HEK 293 cells, General Chemistry, biology.organism_classification, Malaria, 030104 developmental biology, HEK293 Cells, Sialic Acids, lcsh:Q, CRISPR-Cas Systems, 030217 neurology & neurosurgery

Abstract

Plasmodium species are frequently host-specific, but little is currently known about the molecular factors restricting host switching. This is particularly relevant for P. falciparum, the only known human-infective species of the Laverania sub-genus, all other members of which infect African apes. Here we show that all tested P. falciparum isolates contain an inactivating mutation in an erythrocyte invasion associated gene, PfEBA165, the homologues of which are intact in all ape-infective Laverania species. Recombinant EBA165 proteins only bind ape, not human, erythrocytes, and this specificity is due to differences in erythrocyte surface sialic acids. Correction of PfEBA165 inactivating mutations by genome editing yields viable parasites, but is associated with down regulation of both PfEBA165 and an adjacent invasion ligand, which suggests that PfEBA165 expression is incompatible with parasite growth in human erythrocytes. Pseudogenization of PfEBA165 may represent a key step in the emergence and evolution of P. falciparum., Here, Proto et al. show that human infective Plasmodium falciparum isolates contain an inactivating mutation in the erythrocyte invasion associated gene PfEBA165, while homologues of ape-infective Laverania species are intact, and that expression of intact PfEBA165 is incompatible with parasite growth in human erythrocytes.

Published

2019

42. Genome-wide CRISPR/Cas9 deletion screen defines mitochondrial gene essentiality and identifies routes for tumour cell viability in hypoxia

Author

Stacey Price, Cinzia Esposito, Ultan McDermott, Rachel E. Morgan, Jamie Young, Lucas A. Maddalena, Steven P. Williams, Margaret Ashcroft, Luke W. Thomas, Thomas, Luke W [0000-0002-2246-0361], Ashcroft, Margaret [0000-0002-0066-3707], Apollo - University of Cambridge Repository, and Thomas, Luke W. [0000-0002-2246-0361]

Subjects

Cancer microenvironment, 0301 basic medicine, Mitochondrial DNA, 82/29, QH301-705.5, 45/41, Medicine (miscellaneous), Biology, Mitochondrion, 631/67/2327, Genome informatics, Genome, Oxidative Phosphorylation, General Biochemistry, Genetics and Molecular Biology, 45/29, 38/43, 82/80, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, Tumor Cells, Cultured, Humans, CRISPR, Viability assay, Biology (General), Hypoxia, Gene, 13/89, Cell Proliferation, 96/106, Cas9, Cell growth, article, 45/77, Cancer metabolism, Mitochondria, Cell biology, Genes, Mitochondrial, 030104 developmental biology, 030220 oncology & carcinogenesis, Genome, Mitochondrial, 631/114/2785, 38/39, CRISPR-Cas Systems, General Agricultural and Biological Sciences, 82/1, Glycolysis, 631/67/327

Abstract

Funder: EC | EC Seventh Framework Programm | FP7 Ideas: European Research Council (FP7-IDEAS-ERC - Specific Programme: "Ideas" Implementing the Seventh Framework Programme of the European Community for Research, Technological Development and Demonstration Activities (2007 to 2013)); doi: https://doi.org/10.13039/100011199; Grant(s): FP7/2007-2013, Mitochondria are typically essential for the viability of eukaryotic cells, and utilize oxygen and nutrients (e.g. glucose) to perform key metabolic functions that maintain energetic homeostasis and support proliferation. Here we provide a comprehensive functional annotation of mitochondrial genes that are essential for the viability of a large panel (625) of tumour cell lines. We perform genome-wide CRISPR/Cas9 deletion screening in normoxia-glucose, hypoxia-glucose and normoxia-galactose conditions, and identify both unique and overlapping genes whose loss influences tumour cell viability under these different metabolic conditions. We discover that loss of certain oxidative phosphorylation (OXPHOS) genes (e.g. SDHC) improves tumour cell growth in hypoxia-glucose, but reduces growth in normoxia, indicating a metabolic switch in OXPHOS gene function. Moreover, compared to normoxia-glucose, loss of genes involved in energy-consuming processes that are energetically demanding, such as translation and actin polymerization, improve cell viability under both hypoxia-glucose and normoxia-galactose. Collectively, our study defines mitochondrial gene essentiality in tumour cells, highlighting that essentiality is dependent on the metabolic environment, and identifies routes for regulating tumour cell viability in hypoxia.

Published

2021

43. Engineered MATE multidrug transporters reveal two functionally distinct ion-coupling pathways in NorM from Vibrio cholerae

Author

Asha V. Nair, Boyan Bai, Himansha Singh, Hendrik W. van Veen, Keiko Shinoda, Hideaki Fujitani, Sagar Raturi, Satoshi Murakami, Raturi, Sagar [0000-0003-4040-7799], Nair, Asha V. [0000-0002-2037-1138], Murakami, Satoshi [0000-0001-5553-7663], van Veen, Hendrik W. [0000-0002-9658-8077], Apollo - University of Cambridge Repository, Nair, Asha V [0000-0002-2037-1138], and van Veen, Hendrik W [0000-0002-9658-8077]

Subjects

Organic Cation Transport Proteins, QH301-705.5, education, Mutant, Medicine (miscellaneous), 96/34, Plasma protein binding, Antimicrobial resistance, medicine.disease_cause, 631/45/173, 38/70, Antiporters, General Biochemistry, Genetics and Molecular Biology, 82/80, 38/1, 03 medical and health sciences, 0302 clinical medicine, Protein structure, Bacterial Proteins, medicine, Biology (General), Binding site, 82/83, Vibrio cholerae, 030304 developmental biology, Ions, 0303 health sciences, Binding Sites, Chemistry, Sodium, article, Biological Transport, Transporter, humanities, Drug Resistance, Multiple, Cell biology, Transport protein, Enzyme mechanisms, 631/326/22/1434, behavior and behavior mechanisms, Efflux, General Agricultural and Biological Sciences, 030217 neurology & neurosurgery, Hydrogen, Protein Binding

Abstract

Funder: Cambridge Commonwealth, European and International Trust (Cambridge Commonwealth, European & International Trust); doi: https://doi.org/10.13039/501100003343, Funder: The Nehru Trust for Cambridge University, Funder: H.F. and K.S. were supported in part by the Innovative Drug Discovery Infrastructure through the Functional Control of Biomolecular Systems Priority Issue1 in Post-K Supercomputer Development from MEXT (Project ID: hp190171, hp170255, hp180191, and hp150269. K.S. was also supported in part by JSPS KAKENHI Grant Number JP20H05453., Funder: H.F. and K.S. were supported in part by the Innovative Drug Discovery Infrastructure through the Functional Control of Biomolecular Systems Priority Issue1 in Post-K Supercomputer Development from MEXT (Project ID: hp190171, hp170255, hp180191, and hp150269)., Multidrug and toxic compound extrusion (MATE) transport proteins confer multidrug resistance on pathogenic microorganisms and affect pharmacokinetics in mammals. Our understanding of how MATE transporters work, has mostly relied on protein structures and MD simulations. However, the energetics of drug transport has not been studied in detail. Many MATE transporters utilise the electrochemical H+ or Na+ gradient to drive substrate efflux, but NorM-VC from Vibrio cholerae can utilise both forms of metabolic energy. To dissect the localisation and organisation of H+ and Na+ translocation pathways in NorM-VC we engineered chimaeric proteins in which the N-lobe of H+-coupled NorM-PS from Pseudomonas stutzeri is fused to the C-lobe of NorM-VC, and vice versa. Our findings in drug binding and transport experiments with chimaeric, mutant and wildtype transporters highlight the versatile nature of energy coupling in NorM-VC, which enables adaptation to fluctuating salinity levels in the natural habitat of V. cholerae.

Published

2021

44. The double-stranded DNA-binding proteins TEBP-1 and TEBP-2 form a telomeric complex with POT-1

Author

Christian Renz, Miguel Vasconcelos Almeida, Emily Nischwitz, Jan Schreier, Albert Fradera-Sola, Nikenza Viceconte, Dennis Kappei, Helle D. Ulrich, Alejandro Ceron-Noriega, Falk Butter, René F. Ketting, Sabrina Dietz, Dietz, Sabrina [0000-0003-3227-9264], Almeida, Miguel Vasconcelos [0000-0002-4816-3111], Viceconte, Nikenza [0000-0002-5101-4125], Fradera-Sola, Albert [0000-0002-4780-9312], Kappei, Dennis [0000-0002-3582-2253], Ketting, René F [0000-0001-6161-5621], Butter, Falk [0000-0002-7197-7279], Apollo - University of Cambridge Repository, and Ketting, René F. [0000-0001-6161-5621]

Subjects

DNA damage, Science, Mutant, Telomere-Binding Proteins, Biology, 631/45/475, Double-stranded DNA binding, Germline, 38/70, 570 Life sciences, Animals, Genetically Modified, 82/80, 14/32, 38/23, 64/11, Animals, Protein Isoforms, 14/19, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Mitosis, 82/83, Phylogeny, Binding Sites, Base Sequence, 82/58, article, DNA, 631/80/103/560, Telomere, Shelterin, Phenotype, Cell biology, DNA-Binding Proteins, Germ Cells, Microscopy, Fluorescence, Multiprotein Complexes, 38/35, Mutation, 14/63, 570 Biowissenschaften, Protein Binding, 82/111

Abstract

Telomeres are bound by dedicated protein complexes, like shelterin in mammals, which protect telomeres from DNA damage. In the nematodeCaenorhabditis elegans, a comprehensive understanding of the proteins interacting with the telomere sequence is lacking. Here, we harnessed a quantitative proteomics approach to screen for proteins binding toC. elegans telomeres, and identified TEBP-1 and TEBP-2, two paralogs that associate to telomeres in vitro and in vivo. TEBP-1 and TEBP-2 are expressed in the germline and during embryogenesis.tebp-1andtebp-2mutants display strikingly distinct phenotypes:tebp-1mutants have longer telomeres than wild-type animals, whiletebp-2mutants display shorter telomeres and a mortal germline, a phenotype characterized by transgenerational germline deterioration. Notably,tebp-1;tebp-2double mutant animals have synthetic sterility, with germlines showing signs of severe mitotic and meiotic arrest. TEBP-1 and TEBP-2 form a telomeric complex with the known single-stranded telomere-binding proteins POT-1, POT-2, and MRT-1. Furthermore, we find that POT-1 bridges the double- stranded binders TEBP-1 and TEBP-2, with the single-stranded binders POT-2 and MRT-1. These results describe the first telomere-binding complex inC. elegans, with TEBP-1 and TEBP-2, two double-stranded telomere binders required for fertility and that mediate opposite telomere dynamics.

Published

2021

45. A fast and efficient colocalization algorithm for identifying shared genetic risk factors across multiple traits

Author

Paul D. W. Kirk, James R Staley, Benjamin B. Sun, Stephen Burgess, Philip G. Breen, Joanna M. M. Howson, Christopher N. Foley, Foley, Christopher N [0000-0002-0970-2610], Kirk, Paul DW [0000-0002-5931-7489], Burgess, Stephen [0000-0001-5365-8760], Howson, Joanna MM [0000-0001-7618-0050], Apollo - University of Cambridge Repository, Foley, Christopher N. [0000-0002-0970-2610], Kirk, Paul D. W. [0000-0002-5931-7489], and Howson, Joanna M. M. [0000-0001-7618-0050]

Subjects

0301 basic medicine, Linkage disequilibrium, 45/41, 45/43, General Physics and Astronomy, Coronary Disease, Genome-wide association study, 030204 cardiovascular system & hematology, Genome-wide association studies, Linkage Disequilibrium, 0302 clinical medicine, Risk Factors, Pleiotropy, 129, 0303 health sciences, Multidisciplinary, 030305 genetics & heredity, Functional genomics, Genomics, Trait, 139, Algorithms, 141, Science, Quantitative Trait Loci, 631/208/205/2138, Computational biology, Quantitative trait locus, Biology, Polymorphism, Single Nucleotide, Article, General Biochemistry, Genetics and Molecular Biology, 38, 82/80, 03 medical and health sciences, 692/4019/592/2727, Humans, Genetic Predisposition to Disease, Gene, 030304 developmental biology, Genetic association, 45, Computational Biology, Reproducibility of Results, Multiple traits, Colocalization, Cardiovascular genetics, General Chemistry, 030104 developmental biology, 631/114/794, 631/208/191, 119, Software, Genome-Wide Association Study

Abstract

Genome-wide association studies (GWAS) have identified thousands of genomic regions affecting complex diseases. The next challenge is to elucidate the causal genes and mechanisms involved. One approach is to use statistical colocalization to assess shared genetic aetiology across multiple related traits (e.g. molecular traits, metabolic pathways and complex diseases) to identify causal pathways, prioritize causal variants and evaluate pleiotropy. We propose HyPrColoc (Hypothesis Prioritisation for multi-trait Colocalization), an efficient deterministic Bayesian algorithm using GWAS summary statistics that can detect colocalization across vast numbers of traits simultaneously (e.g. 100 traits can be jointly analysed in around 1 s). We perform a genome-wide multi-trait colocalization analysis of coronary heart disease (CHD) and fourteen related traits, identifying 43 regions in which CHD colocalized with ≥1 trait, including 5 previously unknown CHD loci. Across the 43 loci, we further integrate gene and protein expression quantitative trait loci to identify candidate causal genes., Statistical colocalisation is a method to identify causal genes and shared genetic aetiology across traits. Here, the authors describe HyPrColoc, an efficient Bayesian divisive clustering algorithm which integrates summary statistics from genome-wide association studies to detect clusters of colocalised traits from large numbers of traits.

Published

2021

46. Endogenous aldehyde accumulation generates genotoxicity and exhaled biomarkers in esophageal adenocarcinoma

Author

Christopher J. Peters, Haonan Lu, Mina E. Adam, Piers R. Boshier, Hani Gabra, George B. Hanna, Tom Wiggins, Zoltan Takats, Zsolt Bodai, Francesca Rosini, Nagy A. Habib, Robert D. Goldin, Yan Mei Goh, Sheraz R. Markar, Hiromi Kudo, Catherine M. Green, Daniela Moralli, Rebecca C. Fitzgerald, Stefan Antonowicz, Imperial College London, The Wellcome Trust Centre for Human Genetics [Oxford], University of Oxford, University of Cambridge [UK] (CAM), Antonowicz, Stefan [0000-0002-9182-7753], Goh, Yan Mei [0000-0001-6964-0979], Goldin, Robert [0000-0001-5184-4519], Moralli, Daniela [0000-0001-7977-8496], Gabra, Hani [0000-0002-3322-4399], Fitzgerald, Rebecca C [0000-0002-3434-3568], Hanna, George B [0000-0003-2897-0140], Apollo - University of Cambridge Repository, INSERM, Université de Lille, Protéomique, Réponse Inflammatoire, Spectrométrie de Masse (PRISM) - U1192, University of Cambridge [UK] [CAM], Fitzgerald, Rebecca C. [0000-0002-3434-3568], and Hanna, George B. [0000-0003-2897-0140]

Subjects

0301 basic medicine, Esophageal Neoplasms, [SDV]Life Sciences [q-bio], General Physics and Astronomy, 692/4028/67/1504/1477, Endogeny, medicine.disease_cause, Aldehyde, chemistry.chemical_compound, DNA Adducts, 0302 clinical medicine, chemistry.chemical_classification, Multidisciplinary, Chemistry, Oesophageal cancer, food and beverages, 140/58, Aldehyde Oxidoreductases, Metformin, Multidisciplinary Sciences, 030220 oncology & carcinogenesis, Toxicity, 38/77, Science & Technology - Other Topics, medicine.drug, Science, 631/337/1427/1979, Adenocarcinoma, Article, General Biochemistry, Genetics and Molecular Biology, 82/80, 03 medical and health sciences, Esophagus, Detoxification, medicine, Biomarkers, Tumor, Metabolomics, Humans, DNA adducts, Aldehydes, Science & Technology, 631/45/320, General Chemistry, Decanal, Aldehyde Dehydrogenase, Genes, p53, In vitro, 030104 developmental biology, Cancer research, sense organs, Genotoxicity, DNA Damage

Abstract

Volatile aldehydes are enriched in esophageal adenocarcinoma (EAC) patients’ breath and could improve early diagnosis, however the mechanisms of their production are unknown. Here, we show that weak aldehyde detoxification characterizes EAC, which is sufficient to cause endogenous aldehyde accumulation in vitro. Two aldehyde groups are significantly enriched in EAC biopsies and adjacent tissue: (i) short-chain alkanals, and (ii) medium-chain alkanals, including decanal. The short-chain alkanals form DNA-adducts, which demonstrates genotoxicity and confirms inadequate detoxification. Metformin, a putative aldehyde scavenger, reduces this toxicity. Tissue and breath concentrations of the medium-chain alkanal decanal are correlated, and increased decanal is linked to reduced ALDH3A2 expression, TP53 deletion, and adverse clinical features. Thus, we present a model for increased exhaled aldehydes based on endogenous accumulation from reduced detoxification, which also causes therapeutically actionable genotoxicity. These results support EAC early diagnosis trials using exhaled aldehyde analysis., Volatile aldehydes can be enriched in esophageal adenocarcinoma patients’ breath. Here, the authors reveal corresponding metabolic changes in EAC tumours, which may be caused by impaired detoxification of endogenous metabolites.

Published

2021

47. The placenta protects the fetal circulation from anxiety-driven elevations in maternal serum levels of brain-derived neurotrophic factor

Author

Rosalind M. John, Isabel Martinez-Garay, Hayley Dingsdale, Samantha M. Garay, Cedric Ghevaert, Xinsheng Nan, Annett Mueller, Pedro Chacón-Fernández, Lorna Sumption, Yves-Alain Barde, Dingsdale, Hayley [0000-0002-2919-8722], Nan, Xinsheng [0000-0002-0865-7934], Chacón-Fernández, Pedro [0000-0003-0925-814X], Martinez-Garay, Isabel [0000-0001-6849-7496], Barde, Yves-Alain [0000-0002-7627-461X], John, Rosalind M. [0000-0002-3827-7617], Apollo - University of Cambridge Repository, and John, Rosalind M [0000-0002-3827-7617]

Subjects

Male, Serum, medicine.medical_specialty, Placenta, Anxiety, 38, lcsh:RC321-571, 82/80, Cellular and Molecular Neuroscience, 38/1, Pregnancy, Internal medicine, 692/699/476/1414, medicine, Psychology, Humans, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Biological Psychiatry, Brain-derived neurotrophic factor, 64, Fetus, business.industry, Depression, Brain-Derived Neurotrophic Factor, article, medicine.disease, Fetal Blood, Psychiatry and Mental health, Endocrinology, Fetal circulation, medicine.anatomical_structure, Mood disorders, nervous system, Cord blood, Female, 64/60, medicine.symptom, 631/477, business

Abstract

Funder: European Union’s Horizon 2020 Research and Innovation Programme under the Marie Skłodowska-Curie Grant Agreement 663830, Funder: Welsh Government’s Sêr Cymru programme, Funder: NHS Blood and Transplant, Brain-derived neurotrophic factor (BDNF) plays crucial roles in brain function. Numerous studies report alterations in BDNF levels in human serum in various neurological conditions, including mood disorders such as depression. However, little is known about BDNF levels in the blood during pregnancy. We asked whether maternal depression and/or anxiety during pregnancy were associated with altered serum BDNF levels in mothers (n = 251) and their new-born infants (n = 212). As prenatal exposure to maternal mood disorders significantly increases the risk of neurological conditions in later life, we also examined the possibility of placental BDNF transfer by developing a new mouse model. We found no association between maternal symptoms of depression and either maternal or infant cord blood serum BDNF. However, maternal symptoms of anxiety correlated with significantly raised maternal serum BDNF exclusively in mothers of boys (r = 0.281; P = 0.005; n = 99). Serum BDNF was significantly lower in male infants than female infants but neither correlated with maternal anxiety symptoms. Consistent with this observation, we found no evidence for BDNF transfer across the placenta. We conclude that the placenta protects the developing fetus from maternal changes in serum BDNF that could otherwise have adverse consequences for fetal development.

Published

2021

48. Prophage exotoxins enhance colonization fitness in epidemic scarlet fever-causing Streptococcus pyogenes

Author

Tania Rivera-Hernandez, Yuanhai You, Diane Ly, Johanna Richter, Gordon Dougan, Timothy C. Barnett, Amanda J. Cork, Mark J. Walker, Katherine J. Kasper, Mark R. Davies, Magnus G. Jespersen, Martina L. Sanderson-Smith, Victor Nizet, Liam McIntyre, Kwok Yung Yuen, David M. P. De Oliveira, John K. McCormick, Stephan Brouwer, Benjamin L. Schulz, Barnett, Timothy C. [0000-0002-3346-5117], De Oliveira, David M. P. [0000-0002-5085-7163], Jespersen, Magnus G. [0000-0001-9751-9877], Nizet, Victor [0000-0003-3847-0422], Yuen, Kwok-Yung [0000-0002-2083-1552], McCormick, John K. [0000-0003-3742-7289], Sanderson-Smith, Martina L. [0000-0002-6366-4993], Davies, Mark R. [0000-0001-6141-5179], Walker, Mark J. [0000-0001-7423-2769], Apollo - University of Cambridge Repository, Barnett, Timothy C [0000-0002-3346-5117], De Oliveira, David MP [0000-0002-5085-7163], Jespersen, Magnus G [0000-0001-9751-9877], McCormick, John K [0000-0003-3742-7289], Sanderson-Smith, Martina L [0000-0002-6366-4993], Davies, Mark R [0000-0001-6141-5179], and Walker, Mark J [0000-0001-7423-2769]

Subjects

0301 basic medicine, Male, 82/29, Erythrocytes, 631/326/1320, Prophages, General Physics and Astronomy, medicine.disease_cause, Group A, 38/70, 13/1, 38/1, Superantigen, 38/22, lcsh:Science, Multidisciplinary, Superantigens, Streptococcus, article, Glutathione, Streptolysins, 38/77, Streptolysin, 38/39, Female, Infection, Scarlet Fever, Streptococcus pyogenes, Science, 030106 microbiology, Virulence, Exotoxins, 13/106, Mice, Transgenic, Biology, General Biochemistry, Genetics and Molecular Biology, Microbiology, 38/91, Cell Line, 82/80, 03 medical and health sciences, 14/34, Bacterial Proteins, medicine, Animals, Humans, 82/83, Prophage, 692/420/254, Bacteriology, General Chemistry, 64/110, biochemical phenomena, metabolism, and nutrition, medicine.disease, Mice, Inbred C57BL, 030104 developmental biology, 14/63, Mutation, Scarlet fever, bacteria, Pharynx, lcsh:Q

Abstract

The re-emergence of scarlet fever poses a new global public health threat. The capacity of North-East Asian serotype M12 (emm12) Streptococcus pyogenes (group A Streptococcus, GAS) to cause scarlet fever has been linked epidemiologically to the presence of novel prophages, including prophage ΦHKU.vir encoding the secreted superantigens SSA and SpeC and the DNase Spd1. Here, we report the molecular characterization of ΦHKU.vir-encoded exotoxins. We demonstrate that streptolysin O (SLO)-induced glutathione efflux from host cellular stores is a previously unappreciated GAS virulence mechanism that promotes SSA release and activity, representing the first description of a thiol-activated bacterial superantigen. Spd1 is required for resistance to neutrophil killing. Investigating single, double and triple isogenic knockout mutants of the ΦHKU.vir-encoded exotoxins, we find that SpeC and Spd1 act synergistically to facilitate nasopharyngeal colonization in a mouse model. These results offer insight into the pathogenesis of scarlet fever-causing GAS mediated by prophage ΦHKU.vir exotoxins., The pathogenesis of Streptococcus pyogenes (GAS) causing scarlet fever has been associated with the presence of prophages, such as ΦHKU.vir, and their products. Here, the authors characterize the exotoxins SpeC and Spd1 of ΦHKU.vir and show these to act synergistically to facilitate nasopharyngeal colonization in mice.

Published

2020

49. Exome reanalysis and proteomic profiling identified TRIP4 as a novel cause of cerebellar hypoplasia and spinal muscular atrophy (PCH1)

Author

Töpf, Ana, Pyle, Angela, Griffin, Helen, Matalonga, Leslie, Schon, Katherine, Sickmann, Albert, Schara–Schmidt, Ulrike, Hentschel, Andreas, Chinnery, Patrick F., Kölbel, Heike, Roos, Andreas, Horvath, Rita, Cohen, Enzo, Cuesta, Isabel, Danis, Daniel, Denommé-Pichon, Anne-Sophie, Duffourd, Yannis, Gilissen, Christian, Johari, Mridul, Laurie, Steven, Li, Shuang, Nelson, Isabelle, Paramonov, Ida, Peters, Sophia, Prasanth, Sivakumar, Robinson, Peter, Sablauskas, Karolis, Savarese, Marco, Steyaert, Wouter, Van Der Velde, Joeri K., Vitobello, Antonio, Baets, Jonathan, Beijer, Danique, Bonne, Gisèle, Cossins, Judith, Evangelista, Teresinha, Ferlini, Alessandra, Hackman, Peter, Hanna, Michael G., Houlden, Henry, Lau, Jarred, Lochmüller, Hanns, Macken, William L., Musacchia, Francesco, Nascimento, Andres, Natera-De Benito, Daniel, Nigro, Vincenzo, Piluso, Giulio, Pini, Veronica, Pitceathly, Robert D. S., Polavarapu, Kiran, Cruz, Pedro M. Rodriguez, Sarkozy, Anna, Selvatici, Rita, Thompson, Rachel, Torella, Annalaura, Udd, Bjarne, Van De Vondel, Liedewei, Vandrovcova, Jana, Zaharieva, Irina, Schon, Katherine [0000-0001-8054-8954], Horvath, Rita [0000-0002-9841-170X], Apollo - University of Cambridge Repository, Newcastle Upon Tyne Hospitals NHS Foundation Trust, Barcelona Institute of Science and Technology (BIST), University of Cambridge [UK] (CAM), Leibniz-Institut für Analytische Wissenschaften - ISAS - e.V., University of Aberdeen, Ruhr-Universität Bochum [Bochum], University Children's Hospital of Essen [Essen, Germany], Enzo Cohen, Isabel Cuesta, Daniel Danis, Anne-Sophie Denommé-Pichon, Yannis Duffourd, Christian Gilissen, Mridul Johari, Steven Laurie, Shuang Li, Isabelle Nelson, Ida Paramonov, Sophia Peters, Sivakumar Prasanth, Peter Robinson, Karolis Sablauskas, Marco Savarese, Wouter Steyaert, Joeri K van der Velde, Antonio Vitobello, Jonathan Baets, Danique Beijer, Gisèle Bonne, Judith Cossins, Teresinha Evangelista, Alessandra Ferlini, Peter Hackman, Michael G Hanna, Henry Houlden, Jarred Lau, Hanns Lochmüller, William L Macken, Francesco Musacchia, Andres Nascimento, Daniel Natera-de Benito, Vincenzo Nigro, Giulio Piluso, Veronica Pini, Robert D S Pitceathly, Kiran Polavarapu, Pedro M Rodriguez Cruz, Anna Sarkozy, Rita Selvatici, Rachel Thompson, Annalaura Torella, Bjarne Udd, Liedewei Van de Vondel, Jana Vandrovcova, Irina Zaharieva, Töpf, Ana, Pyle, Angela, Griffin, Helen, Matalonga, Leslie, Schon, Katherine, Sickmann, Albert, Schara-Schmidt, Ulrike, Hentschel, Andrea, Chinnery, Patrick F, Kölbel, Heike, Roos, Andrea, Horvath, Rita, Nigro, Vincenzo, Torella, Annalaura, and Piluso, Giulio

Subjects

0301 basic medicine, Male, Proteome, 45/41, Developmental Disabilities, Medizin, 45/22, Biology, Bioinformatics, Nervous System Malformations, Brief Communication, 82/80, Muscular Atrophy, Spinal, 03 medical and health sciences, 0302 clinical medicine, Cerebellum, 38/23, Genetics research, Genetics, medicine, [SDV.MHEP.AHA]Life Sciences [q-bio]/Human health and pathology/Tissues and Organs [q-bio.TO], Humans, Exome, Genetic Testing, Gene, Cerebellar hypoplasia, Genetics (clinical), Exome sequencing, Proteomic Profile, Proteomic Profiling, 82/58, 631/208/514/2254, brief-communication, 692/308/2056, Infant, Metabolic Disorders Radboud Institute for Molecular Life Sciences [Radboudumc 6], Spinal muscular atrophy, medicine.disease, 3. Good health, 030104 developmental biology, Congenital muscular dystrophy, Next-generation sequencing, 030217 neurology & neurosurgery, Transcription Factors

Abstract

TRIP4 is one of the subunits of the transcriptional coregulator ASC-1, a ribonucleoprotein complex that participates in transcriptional coactivation and RNA processing events. Recessive variants in the TRIP4 gene have been associated with spinal muscular atrophy with bone fractures as well as a severe form of congenital muscular dystrophy. Here we present the diagnostic journey of a patient with cerebellar hypoplasia and spinal muscular atrophy (PCH1) and congenital bone fractures. Initial exome sequencing analysis revealed no candidate variants. Reanalysis of the exome data by inclusion in the Solve-RD project resulted in the identification of a homozygous stop-gain variant in the TRIP4 gene, previously reported as disease-causing. This highlights the importance of analysis reiteration and improved and updated bioinformatic pipelines. Proteomic profile of the patient's fibroblasts showed altered RNA-processing and impaired exosome activity supporting the pathogenicity of the detected variant. In addition, we identified a novel genetic form of PCH1, further strengthening the link of this characteristic phenotype with altered RNA metabolism. The Solve-RD project has received funding from the European Union’s Horizon 2020 research and innovation programme under grant agreement No 779257. Several authors of this study are members of the European Reference Network for Neuromuscular disease, Project ID No 739543. This study was supported by the AFM (grant 21644 to AR), the framework of the NME-GPS project by the European Regional Development Fund (AR/US/AS), the support by the Ministerium für Kultur und Wissenschaft des Landes Nordrhein-Westfalen, the Regierende Bürgermeister von Berlin-inkl. Wissenschaft und Forschung, and the Bundesministerium für Bildung und Forschung (AH and AS), the European Research Council (RH), the Wellcome Investigator Award (109915/Z/15/Z to RH), the Medical Research Council UK (MR/N025431/1 to RH), the Newton Fund (MR/N027302/1 to RH), the Lily Foundation (RH) and the Evelyn Trust (RH). This research was supported by an MRC strategic award to establish an International Centre for Genomic Medicine in Neuromuscular Diseases (ICGNMD) MR/S005021/1 and the NIHR Cambridge Biomedical Research Centre (BRC-1215-20014). The views expressed are those of the authors and not necessarily those of the NIHR or the Department of Health and Social Care

Published

2020

50. The GATA3 X308_Splice breast cancer mutation is a hormone context-dependent oncogenic driver

Author

Begoña Bermejo, Laia Paré Brunet, Mark Kalisz, Ana Sagrera, Natascha Hruschka, Igor Chernukhin, Carlos Caldas, Jason S. Carroll, Maria Subijana, Osvaldo Graña-Castro, Aurélien de Reyniès, Francisco X. Real, Octavio Burgues, Francisco Del Caño-Ochoa, Suet-Feung Chin, Bernhard Kloesch, David Andreu, Aleix Prat, Santiago Ramón-Maiques, Joseph Sutton, Paola Martinelli, Juan Miguel Cejalvo, Kalisz, Mark [0000-0002-8770-2798], Del Cano-Ochoa, Francisco [0000-0003-3093-3103], Andreu, David [0000-0002-6317-6666], Caldas, Carlos [0000-0003-3547-1489], Ramón-Maiques, Santiago [0000-0001-9674-8088], Carroll, Jason S. [0000-0003-3643-0080], Prat, Aleix [0000-0003-2377-540X], Real, Francisco X. [0000-0001-9501-498X], Martinelli, Paola [0000-0002-1643-8731], Apollo - University of Cambridge Repository, Medical University of Vienna, Austrian Science Fund, Ministerio de Economía y Competitividad (España), Fundación Científica Asociación Española Contra el Cáncer, Ministerio de Ciencia, Innovación y Universidades (España), Carroll, Jason S [0000-0003-3643-0080], and Real, Francisco X [0000-0001-9501-498X]

Subjects

0301 basic medicine, Cancer Research, medicine.drug_class, RNA Splicing, T-Lymphocytes, 45/22, Breast Neoplasms, Context (language use), GATA3 Transcription Factor, Biology, medicine.disease_cause, 82/80, 03 medical and health sciences, 13/1, 0302 clinical medicine, Breast cancer, 631/67/68, Genetics, medicine, Humans, splice, RNA, Messenger, Molecular Biology, Transcription factor, Cancer genetics, 45/90, Mutation, 96/106, Cell Cycle, GATA3, article, Cancer, Oncogenes, 631/67/1347, medicine.disease, 030104 developmental biology, Receptors, Estrogen, Estrogen, 030220 oncology & carcinogenesis, 13/51, Cancer research, Female, 38/39, Receptors, Progesterone

Abstract

Funder: Spanish Ministry of Science, Innovation, and University. BFU2016-80570-R, Funder: Cancer Research UK (CRUK); doi: https://doi.org/10.13039/501100000289, Funder: Fundación Científica Asociación Española Contra el Cáncer (Scientific Foundation, Spanish Association Against Cancer); doi: https://doi.org/10.13039/501100002704, As the catalog of oncogenic driver mutations is expanding, it becomes clear that alterations in a given gene might have different functions and should not be lumped into one class. The transcription factor GATA3 is a paradigm of this. We investigated the functions of the most common GATA3 mutation (X308_Splice) and five additional mutations, which converge into a neoprotein that we called “neoGATA3,” associated with excellent prognosis in patients. Analysis of available molecular data from >3000 breast cancer patients revealed a dysregulation of the ER-dependent transcriptional response in tumors carrying neoGATA3-generating mutations. Mechanistic studies in vitro showed that neoGATA3 interferes with the transcriptional programs controlled by estrogen and progesterone receptors, without fully abrogating them. ChIP-Seq analysis indicated that ER binding is reduced in neoGATA3-expressing cells, especially at distal regions, suggesting that neoGATA3 interferes with the fine tuning of ER-dependent gene expression. This has opposite outputs in distinct hormonal context, having pro- or anti-proliferative effects, depending on the estrogen/progesterone ratio. Our data call for functional analyses of putative cancer drivers to guide clinical application.

Published

2020