Your search keyword '"Carsten Russ"' showing total 106 results

1. Cancer lineage-specific regulation of YAP responsive elements revealed through large-scale functional epigenomic screens

Author

Inês A. M. Barbosa, Rajaraman Gopalakrishnan, Samuele Mercan, Thanos P. Mourikis, Typhaine Martin, Simon Wengert, Caibin Sheng, Fei Ji, Rui Lopes, Judith Knehr, Marc Altorfer, Alicia Lindeman, Carsten Russ, Ulrike Naumann, Javad Golji, Kathleen Sprouffske, Louise Barys, Luca Tordella, Dirk Schübeler, Tobias Schmelzle, and Giorgio G. Galli

Subjects

Science

Abstract

Abstract YAP is a key transcriptional co-activator of TEADs, it regulates cell growth and is frequently activated in cancer. In Malignant Pleural Mesothelioma (MPM), YAP is activated by loss-of-function mutations in upstream components of the Hippo pathway, while, in Uveal Melanoma (UM), YAP is activated in a Hippo-independent manner. To date, it is unclear if and how the different oncogenic lesions activating YAP impact its oncogenic program, which is particularly relevant for designing selective anti-cancer therapies. Here we show that, despite YAP being essential in both MPM and UM, its interaction with TEAD is unexpectedly dispensable in UM, limiting the applicability of TEAD inhibitors in this cancer type. Systematic functional interrogation of YAP regulatory elements in both cancer types reveals convergent regulation of broad oncogenic drivers in both MPM and UM, but also strikingly selective programs. Our work reveals unanticipated lineage-specific features of the YAP regulatory network that provide important insights to guide the design of tailored therapeutic strategies to inhibit YAP signaling across different cancer types.

Published

2023

2. Cell adhesion molecule KIRREL1 is a feedback regulator of Hippo signaling recruiting SAV1 to cell-cell contact sites

Author

Atanu Paul, Stefano Annunziato, Bo Lu, Tianliang Sun, Olivera Evrova, Lara Planas-Paz, Vanessa Orsini, Luigi M. Terracciano, Olga Charlat, Zinger Yang Loureiro, Lei Ji, Raffaella Zamponi, Frederic Sigoillot, Hong Lei, Alicia Lindeman, Carsten Russ, John S. Reece-Hoyes, Thomas B. Nicholson, Jan S. Tchorz, and Feng Cong

Subjects

Science

Abstract

How cell-cell contact is sensed by Hippo pathway is poorly understood. Here, the authors show that KIRREL1 functions as a feedback regulator of the mammalian Hippo pathway by sensing cell-cell interaction and recruiting SAV1 to cell-cell contacts.

Published

2022

3. Genome-wide CRISPR screen identifies protein pathways modulating tau protein levels in neurons

Author

Carlos G. Sanchez, Christopher M. Acker, Audrey Gray, Malini Varadarajan, Cheng Song, Nadire R. Cochran, Steven Paula, Alicia Lindeman, Shaojian An, Gregory McAllister, John Alford, John Reece-Hoyes, Carsten Russ, Lucas Craig, Ketthsy Capre, Christian Doherty, Gregory R. Hoffman, Sarah J. Luchansky, Manuela Polydoro, Ricardo Dolmetsch, and Fiona Elwood

Subjects

Biology (General), QH301-705.5

Abstract

Using an unbiased genome-wide CRISPR screen approach, Sanchez et al. identified modulators of endogenous tau protein. This study suggests that chromatin modifiers, neddylation, ubiquitination, and the mTOR pathways regulate overall levels of tau protein in neurons, which could help in future identification of therapeutics for neurodegenerative diseases.

Published

2021

4. IRF2 is a master regulator of human keratinocyte stem cell fate

Author

Nicolas Mercado, Gabi Schutzius, Christian Kolter, David Estoppey, Sebastian Bergling, Guglielmo Roma, Caroline Gubser Keller, Florian Nigsch, Adrian Salathe, Remi Terranova, John Reece-Hoyes, John Alford, Carsten Russ, Judith Knehr, Dominic Hoepfner, Alexandra Aebi, Heinz Ruffner, Tanner C. Beck, Sajjeev Jagannathan, Calla M. Olson, Hadley E. Sheppard, Selma Z. Elsarrag, Tewis Bouwmeester, Mathias Frederiksen, Felix Lohmann, Charles Y. Lin, and Susan Kirkland

Subjects

Science

Abstract

Epidermal homeostasis requires long term stem cell function. Here, the authors apply transcriptional circuitry analysis based on integrated epigenomic profiling of primary human keratinocytes with high and low stem cell function to identify IRF2 as a negative regulator of stemness.

Published

2019

5. USP7 inhibits Wnt/β-catenin signaling through promoting stabilization of Axin

Author

Lei Ji, Bo Lu, Raffaella Zamponi, Olga Charlat, Robert Aversa, Zinger Yang, Frederic Sigoillot, Xiaoping Zhu, Tiancen Hu, John S. Reece-Hoyes, Carsten Russ, Gregory Michaud, Jan S. Tchorz, Xiaomo Jiang, and Feng Cong

Subjects

Science

Abstract

Axin is a scaffolding protein known for its role in Wnt signalling that can be marked with a variety of post-translational modifications. Here, Cong et al. demonstrate that USP7 de-ubiquinates Axin and that canonical Wnt signaling output can be increased with USP7 inhibitors.

Published

2019

6. An iron-dependent metabolic vulnerability underlies VPS34-dependence in RKO cancer cells.

Author

Marek J Kobylarz, Jonathan M Goodwin, Zhao B Kang, John W Annand, Sarah Hevi, Ellen O'Mahony, Gregory McAllister, John Reece-Hoyes, Qiong Wang, John Alford, Carsten Russ, Alicia Lindeman, Martin Beibel, Guglielmo Roma, Walter Carbone, Judith Knehr, Joseph Loureiro, Christophe Antczak, Dmitri Wiederschain, Leon O Murphy, Suchithra Menon, and Beat Nyfeler

Subjects

Medicine, Science

Abstract

VPS34 is a key regulator of endomembrane dynamics and cargo trafficking, and is essential in cultured cell lines and in mice. To better characterize the role of VPS34 in cell growth, we performed unbiased cell line profiling studies with the selective VPS34 inhibitor PIK-III and identified RKO as a VPS34-dependent cellular model. Pooled CRISPR screen in the presence of PIK-III revealed endolysosomal genes as genetic suppressors. Dissecting VPS34-dependent alterations with transcriptional profiling, we found the induction of hypoxia response and cholesterol biosynthesis as key signatures. Mechanistically, acute VPS34 inhibition enhanced lysosomal degradation of transferrin and low-density lipoprotein receptors leading to impaired iron and cholesterol uptake. Excess soluble iron, but not cholesterol, was sufficient to partially rescue the effects of VPS34 inhibition on mitochondrial respiration and cell growth, indicating that iron limitation is the primary driver of VPS34-dependency in RKO cells. Loss of RAB7A, an endolysosomal marker and top suppressor in our genetic screen, blocked transferrin receptor degradation, restored iron homeostasis and reversed the growth defect as well as metabolic alterations due to VPS34 inhibition. Altogether, our findings suggest that impaired iron mobilization via the VPS34-RAB7A axis drive VPS34-dependence in certain cancer cells.

Published

2020

7. TRIAMF: A New Method for Delivery of Cas9 Ribonucleoprotein Complex to Human Hematopoietic Stem Cells

Author

Jonathan Yen, Michael Fiorino, Yi Liu, Steve Paula, Scott Clarkson, Lisa Quinn, William R. Tschantz, Heath Klock, Ning Guo, Carsten Russ, Vionnie W. C. Yu, Craig Mickanin, Susan C. Stevenson, Cameron Lee, and Yi Yang

Subjects

Hematopoietic Stem And Progenitor Cells (HSPCs), Purified Cas9 Protein, HSPC Expansion, Neon Electroporation, Syringe Connector, Medicine, Science

Abstract

Abstract CRISPR/Cas9 mediated gene editing of patient-derived hematopoietic stem and progenitor cells (HSPCs) ex vivo followed by autologous transplantation of the edited HSPCs back to the patient can provide a potential cure for monogenic blood disorders such as β-hemoglobinopathies. One challenge for this strategy is efficient delivery of the ribonucleoprotein (RNP) complex, consisting of purified Cas9 protein and guide RNA, into HSPCs. Because β-hemoglobinopathies are most prevalent in developing countries, it is desirable to have a reliable, efficient, easy-to-use and cost effective delivery method. With this goal in mind, we developed TRansmembrane Internalization Assisted by Membrane Filtration (TRIAMF), a new method to quickly and effectively deliver RNPs into HSPCs by passing a RNP and cell mixture through a filter membrane. We achieved robust gene editing in HSPCs using TRIAMF and demonstrated that the multilineage colony forming capacities and the competence for engraftment in immunocompromised mice of HSPCs were preserved post TRIAMF treatment. TRIAMF is a custom designed system using inexpensive components and has the capacity to process HSPCs at clinical scale.

Published

2018

8. A Genome-wide CRISPR Screen Identifies ZCCHC14 as a Host Factor Required for Hepatitis B Surface Antigen Production

Author

Anastasia Hyrina, Christopher Jones, Darlene Chen, Scott Clarkson, Nadire Cochran, Paul Feucht, Gregory Hoffman, Alicia Lindeman, Carsten Russ, Frederic Sigoillot, Tiffany Tsang, Kyoko Uehara, Lili Xie, Don Ganem, and Meghan Holdorf

Subjects

Biology (General), QH301-705.5

Abstract

Summary: A hallmark of chronic hepatitis B (CHB) virus infection is the presence of high circulating levels of non-infectious small lipid HBV surface antigen (HBsAg) vesicles. Although rare, sustained HBsAg loss is the idealized endpoint of any CHB therapy. A small molecule, RG7834, has been previously reported to inhibit HBsAg expression by targeting terminal nucleotidyltransferase proteins 4A and 4B (TENT4A and TENT4B). In this study, we describe a genome-wide CRISPR screen to identify other potential host factors required for HBsAg expression and to gain further insights into the mechanism of RG7834. We report more than 60 genes involved in regulating HBsAg and identify additional factors involved in RG7834 activity, including a zinc finger CCHC-type containing 14 (ZCCHC14) protein. We show that ZCCHC14, together with TENT4A/B, stabilizes HBsAg expression through HBV RNA tailing, providing a potential new therapeutic target to achieve functional cure in CHB patients. : Hyrina et al. employ a non-biased functional CRISPR screening approach to identify host factors regulating HBsAg expression as well as those targeted by RG7834, a HBsAg inhibitor. The screen highlighted over 60 genes and identified a mechanism by which ZCCHC14, together with TENT4A/B, stabilizes HBsAg expression through HBV RNA tailing. Keywords: HBV, HBsAg, CRISPR, genome-wide screen, RG7834, ZCCHC14, TENT4B, RNA tailing

Published

2019

9. The Natural Product Cavinafungin Selectively Interferes with Zika and Dengue Virus Replication by Inhibition of the Host Signal Peptidase

Author

David Estoppey, Chia Min Lee, Marco Janoschke, Boon Heng Lee, Kah Fei Wan, Hongping Dong, Philippe Mathys, Ireos Filipuzzi, Tim Schuhmann, Ralph Riedl, Thomas Aust, Olaf Galuba, Gregory McAllister, Carsten Russ, Martin Spiess, Tewis Bouwmeester, Ghislain M.C. Bonamy, and Dominic Hoepfner

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Flavivirus infections by Zika and dengue virus impose a significant global healthcare threat with no US Food and Drug Administration (FDA)-approved vaccination or specific antiviral treatment available. Here, we present the discovery of an anti-flaviviral natural product named cavinafungin. Cavinafungin is a potent and selectively active compound against Zika and all four dengue virus serotypes. Unbiased, genome-wide genomic profiling in human cells using a novel CRISPR/Cas9 protocol identified the endoplasmic-reticulum-localized signal peptidase as the efficacy target of cavinafungin. Orthogonal profiling in S. cerevisiae followed by the selection of resistant mutants pinpointed the catalytic subunit of the signal peptidase SEC11 as the evolutionary conserved target. Biochemical analysis confirmed a rapid block of signal sequence cleavage of both host and viral proteins by cavinafungin. This study provides an effective compound against the eukaryotic signal peptidase and independent confirmation of the recently identified critical role of the signal peptidase in the replicative cycle of flaviviruses. : Recent outbreaks and lack of effective treatments against dengue and Zika virus have caused public concerns. Estoppey et al. have identified cavinafungin as exerting potent and selective antiviral activity by targeting the signal-binding cleft of the catalytic subunit of the endoplasmic reticulum signal peptidase. Keywords: Zika virus, dengue virus, cavinafungin, signal peptidase, SEC11A, SEC11, CRISPR/Cas9, chemogenomic profiling

Published

2017

10. Genome-wide CRISPR screening reveals genetic modifiers of mutant EGFR dependence in human NSCLC

Author

Hao Zeng, Johnny Castillo-Cabrera, Mika Manser, Bo Lu, Zinger Yang, Vaik Strande, Damien Begue, Raffaella Zamponi, Shumei Qiu, Frederic Sigoillot, Qiong Wang, Alicia Lindeman, John S Reece-Hoyes, Carsten Russ, Debora Bonenfant, Xiaomo Jiang, Youzhen Wang, and Feng Cong

Subjects

CRISPR screen, EGFR TKI resistance, GPCR signaling, RIC8A, YAP signaling, ARIH2-CUL5 complex, Medicine, Science, Biology (General), QH301-705.5

Abstract

EGFR-mutant NSCLCs frequently respond to EGFR tyrosine kinase inhibitors (TKIs). However, the responses are not durable, and the magnitude of tumor regression is variable, suggesting the existence of genetic modifiers of EGFR dependency. Here, we applied a genome-wide CRISPR-Cas9 screening to identify genetic determinants of EGFR TKI sensitivity and uncovered putative candidates. We show that knockout of RIC8A, essential for G-alpha protein activation, enhanced EGFR TKI-induced cell death. Mechanistically, we demonstrate that RIC8A is a positive regulator of YAP signaling, activation of which rescued the EGFR TKI sensitizing phenotype resulting from RIC8A knockout. We also show that knockout of ARIH2, or other components in the Cullin-5 E3 complex, conferred resistance to EGFR inhibition, in part by promoting nascent protein synthesis through METAP2. Together, these data uncover a spectrum of previously unidentified regulators of EGFR TKI sensitivity in EGFR-mutant human NSCLC, providing insights into the heterogeneity of EGFR TKI treatment responses.

Published

2019

11. Genome-Scale CRISPR Screens Identify Human Pluripotency-Specific Genes

Author

Robert J. Ihry, Max R. Salick, Daniel J. Ho, Marie Sondey, Sravya Kommineni, Steven Paula, Joe Raymond, Beata Henry, Elizabeth Frias, Qiong Wang, Kathleen A. Worringer, Chaoyang Ye, Carsten Russ, John S. Reece-Hoyes, Robert C. Altshuler, Ranjit Randhawa, Zinger Yang, Gregory McAllister, Gregory R. Hoffman, Ricardo Dolmetsch, and Ajamete Kaykas

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Human pluripotent stem cells (hPSCs) generate a variety of disease-relevant cells that can be used to improve the translation of preclinical research. Despite the potential of hPSCs, their use for genetic screening has been limited by technical challenges. We developed a scalable and renewable Cas9 and sgRNA-hPSC library in which loss-of-function mutations can be induced at will. Our inducible mutant hPSC library can be used for multiple genome-wide CRISPR screens in a variety of hPSC-induced cell types. As proof of concept, we performed three screens for regulators of properties fundamental to hPSCs: their ability to self-renew and/or survive (fitness), their inability to survive as single-cell clones, and their capacity to differentiate. We identified the majority of known genes and pathways involved in these processes, as well as a plethora of genes with unidentified roles. This resource will increase the understanding of human development and genetics. This approach will be a powerful tool to identify disease-modifying genes and pathways. : Ihry et al. develop a CRISPR/Cas9 genetic screening platform for hPSCs that enables unbiased genome-scale genetic screening. The platform exhibits high performance and accurately detects the dropout of essential genes. Furthermore, proof-of-concept screens exploit hPSC-specific phenotypes to identify regulators of fitness, survival after single-cell dissociation, and pluripotency. Keywords: CRISPR genome-wide screening, human pluripotent stem cells, iPSC, hESC, PAWR, PMAIP1, DDR

Published

2019

12. Structure of the germline genome of Tetrahymena thermophila and relationship to the massively rearranged somatic genome

Author

Eileen P Hamilton, Aurélie Kapusta, Piroska E Huvos, Shelby L Bidwell, Nikhat Zafar, Haibao Tang, Michalis Hadjithomas, Vivek Krishnakumar, Jonathan H Badger, Elisabet V Caler, Carsten Russ, Qiandong Zeng, Lin Fan, Joshua Z Levin, Terrance Shea, Sarah K Young, Ryan Hegarty, Riza Daza, Sharvari Gujja, Jennifer R Wortman, Bruce W Birren, Chad Nusbaum, Jainy Thomas, Clayton M Carey, Ellen J Pritham, Cédric Feschotte, Tomoko Noto, Kazufumi Mochizuki, Romeo Papazyan, Sean D Taverna, Paul H Dear, Donna M Cassidy-Hanley, Jie Xiong, Wei Miao, Eduardo Orias, and Robert S Coyne

Subjects

Tetrahymena thermophila, chromosome breakage, intermal eliminated sequence, genome rearrangement, transposable element, centromere, Medicine, Science, Biology (General), QH301-705.5

Abstract

The germline genome of the binucleated ciliate Tetrahymena thermophila undergoes programmed chromosome breakage and massive DNA elimination to generate the somatic genome. Here, we present a complete sequence assembly of the germline genome and analyze multiple features of its structure and its relationship to the somatic genome, shedding light on the mechanisms of genome rearrangement as well as the evolutionary history of this remarkable germline/soma differentiation. Our results strengthen the notion that a complex, dynamic, and ongoing interplay between mobile DNA elements and the host genome have shaped Tetrahymena chromosome structure, locally and globally. Non-standard outcomes of rearrangement events, including the generation of short-lived somatic chromosomes and excision of DNA interrupting protein-coding regions, may represent novel forms of developmental gene regulation. We also compare Tetrahymena’s germline/soma differentiation to that of other characterized ciliates, illustrating the wide diversity of adaptations that have occurred within this phylum.

Published

2016

13. Functional CRISPR screening identifies the ufmylation pathway as a regulator of SQSTM1/p62

Author

Rowena DeJesus, Francesca Moretti, Gregory McAllister, Zuncai Wang, Phil Bergman, Shanming Liu, Elizabeth Frias, John Alford, John S Reece-Hoyes, Alicia Lindeman, Jennifer Kelliher, Carsten Russ, Judith Knehr, Walter Carbone, Martin Beibel, Guglielmo Roma, Aylwin Ng, John A Tallarico, Jeffery A Porter, Ramnik J Xavier, Craig Mickanin, Leon O Murphy, Gregory R Hoffman, and Beat Nyfeler

Subjects

autophagy, SQSTM1, ER stress, CRISPR, Medicine, Science, Biology (General), QH301-705.5

Abstract

SQSTM1 is an adaptor protein that integrates multiple cellular signaling pathways and whose expression is tightly regulated at the transcriptional and post-translational level. Here, we describe a forward genetic screening paradigm exploiting CRISPR-mediated genome editing coupled to a cell selection step by FACS to identify regulators of SQSTM1. Through systematic comparison of pooled libraries, we show that CRISPR is superior to RNAi in identifying known SQSTM1 modulators. A genome-wide CRISPR screen exposed MTOR signalling and the entire macroautophagy machinery as key regulators of SQSTM1 and identified several novel modulators including HNRNPM, SLC39A14, SRRD, PGK1 and the ufmylation cascade. We show that ufmylation regulates SQSTM1 by eliciting a cell type-specific ER stress response which induces SQSTM1 expression and results in its accumulation in the cytosol. This study validates pooled CRISPR screening as a powerful method to map the repertoire of cellular pathways that regulate the fate of an individual target protein.

Published

2016

14. Massively parallel sequencing of human urinary exosome/microvesicle RNA reveals a predominance of non-coding RNA.

Author

Kevin C Miranda, Daniel T Bond, Joshua Z Levin, Xian Adiconis, Andrey Sivachenko, Carsten Russ, Dennis Brown, Chad Nusbaum, and Leileata M Russo

Subjects

Medicine, Science

Abstract

Intact RNA from exosomes/microvesicles (collectively referred to as microvesicles) has sparked much interest as potential biomarkers for the non-invasive analysis of disease. Here we use the Illumina Genome Analyzer to determine the comprehensive array of nucleic acid reads present in urinary microvesicles. Extraneous nucleic acids were digested using RNase and DNase treatment and the microvesicle inner nucleic acid cargo was analyzed with and without DNase digestion to examine both DNA and RNA sequences contained in microvesicles. Results revealed that a substantial proportion (∼87%) of reads aligned to ribosomal RNA. Of the non-ribosomal RNA sequences, ∼60% aligned to non-coding RNA and repeat sequences including LINE, SINE, satellite repeats, and RNA repeats (tRNA, snRNA, scRNA and srpRNA). The remaining ∼40% of non-ribosomal RNA reads aligned to protein coding genes and splice sites encompassing approximately 13,500 of the known 21,892 protein coding genes of the human genome. Analysis of protein coding genes specific to the renal and genitourinary tract revealed that complete segments of the renal nephron and collecting duct as well as genes indicative of the bladder and prostate could be identified. This study reveals that the entire genitourinary system may be mapped using microvesicle transcript analysis and that the majority of non-ribosomal RNA sequences contained in microvesicles is potentially functional non-coding RNA, which play an emerging role in cell regulation.

Published

2014

15. Regulated aggregative multicellularity in a close unicellular relative of metazoa

Author

Arnau Sebé-Pedrós, Manuel Irimia, Javier del Campo, Helena Parra-Acero, Carsten Russ, Chad Nusbaum, Benjamin J Blencowe, and Iñaki Ruiz-Trillo

Subjects

opisthokonts, Capsaspora, alternative splicing, cell differentiation, evolutionary transition, Medicine, Science, Biology (General), QH301-705.5

Abstract

The evolution of metazoans from their unicellular ancestors was one of the most important events in the history of life. However, the cellular and genetic changes that ultimately led to the evolution of multicellularity are not known. In this study, we describe an aggregative multicellular stage in the protist Capsaspora owczarzaki, a close unicellular relative of metazoans. Remarkably, transition to the aggregative stage is associated with significant upregulation of orthologs of genes known to establish multicellularity and tissue architecture in metazoans. We further observe transitions in regulated alternative splicing during the C. owczarzaki life cycle, including the deployment of an exon network associated with signaling, a feature of splicing regulation so far only observed in metazoans. Our results reveal the existence of a highly regulated aggregative stage in C. owczarzaki and further suggest that features of aggregative behavior in an ancestral protist may had been co-opted to develop some multicellular properties currently seen in metazoans.

Published

2013

16. Distinctive expansion of potential virulence genes in the genome of the oomycete fish pathogen Saprolegnia parasitica.

Author

Rays H Y Jiang, Irene de Bruijn, Brian J Haas, Rodrigo Belmonte, Lars Löbach, James Christie, Guido van den Ackerveken, Arnaud Bottin, Vincent Bulone, Sara M Díaz-Moreno, Bernard Dumas, Lin Fan, Elodie Gaulin, Francine Govers, Laura J Grenville-Briggs, Neil R Horner, Joshua Z Levin, Marco Mammella, Harold J G Meijer, Paul Morris, Chad Nusbaum, Stan Oome, Andrew J Phillips, David van Rooyen, Elzbieta Rzeszutek, Marcia Saraiva, Chris J Secombes, Michael F Seidl, Berend Snel, Joost H M Stassen, Sean Sykes, Sucheta Tripathy, Herbert van den Berg, Julio C Vega-Arreguin, Stephan Wawra, Sarah K Young, Qiandong Zeng, Javier Dieguez-Uribeondo, Carsten Russ, Brett M Tyler, and Pieter van West

Subjects

Genetics, QH426-470

Abstract

Oomycetes in the class Saprolegniomycetidae of the Eukaryotic kingdom Stramenopila have evolved as severe pathogens of amphibians, crustaceans, fish and insects, resulting in major losses in aquaculture and damage to aquatic ecosystems. We have sequenced the 63 Mb genome of the fresh water fish pathogen, Saprolegnia parasitica. Approximately 1/3 of the assembled genome exhibits loss of heterozygosity, indicating an efficient mechanism for revealing new variation. Comparison of S. parasitica with plant pathogenic oomycetes suggests that during evolution the host cellular environment has driven distinct patterns of gene expansion and loss in the genomes of plant and animal pathogens. S. parasitica possesses one of the largest repertoires of proteases (270) among eukaryotes that are deployed in waves at different points during infection as determined from RNA-Seq data. In contrast, despite being capable of living saprotrophically, parasitism has led to loss of inorganic nitrogen and sulfur assimilation pathways, strikingly similar to losses in obligate plant pathogenic oomycetes and fungi. The large gene families that are hallmarks of plant pathogenic oomycetes such as Phytophthora appear to be lacking in S. parasitica, including those encoding RXLR effectors, Crinkler's, and Necrosis Inducing-Like Proteins (NLP). S. parasitica also has a very large kinome of 543 kinases, 10% of which is induced upon infection. Moreover, S. parasitica encodes several genes typical of animals or animal-pathogens and lacking from other oomycetes, including disintegrins and galactose-binding lectins, whose expression and evolutionary origins implicate horizontal gene transfer in the evolution of animal pathogenesis in S. parasitica.

Published

2013

17. Quantitative deep sequencing reveals dynamic HIV-1 escape and large population shifts during CCR5 antagonist therapy in vivo.

Author

Athe M N Tsibris, Bette Korber, Ramy Arnaout, Carsten Russ, Chien-Chi Lo, Thomas Leitner, Brian Gaschen, James Theiler, Roger Paredes, Zhaohui Su, Michael D Hughes, Roy M Gulick, Wayne Greaves, Eoin Coakley, Charles Flexner, Chad Nusbaum, and Daniel R Kuritzkes

Subjects

Medicine, Science

Abstract

High-throughput sequencing platforms provide an approach for detecting rare HIV-1 variants and documenting more fully quasispecies diversity. We applied this technology to the V3 loop-coding region of env in samples collected from 4 chronically HIV-infected subjects in whom CCR5 antagonist (vicriviroc [VVC]) therapy failed. Between 25,000-140,000 amplified sequences were obtained per sample. Profound baseline V3 loop sequence heterogeneity existed; predicted CXCR4-using populations were identified in a largely CCR5-using population. The V3 loop forms associated with subsequent virologic failure, either through CXCR4 use or the emergence of high-level VVC resistance, were present as minor variants at 0.8-2.8% of baseline samples. Extreme, rapid shifts in population frequencies toward these forms occurred, and deep sequencing provided a detailed view of the rapid evolutionary impact of VVC selection. Greater V3 diversity was observed post-selection. This previously unreported degree of V3 loop sequence diversity has implications for viral pathogenesis, vaccine design, and the optimal use of HIV-1 CCR5 antagonists.

Published

2009

18. Genome-wide CRISPR screen identifies protein pathways modulating tau protein levels in neurons

Author

Fiona Elwood, John Alford, Carsten Russ, Christopher Acker, Audrey Gray, John S. Reece-Hoyes, Carlos G Sanchez, Sarah J. Luchansky, Christian Doherty, Lucas Craig, Gregory McAllister, Steven Paula, Ricardo E. Dolmetsch, Shaojian An, Cheng Song, Alicia Lindeman, Malini Varadarajan, Nadire Cochran, Manuela Polydoro, Ketthsy Capre, and Gregory R. Hoffman

Subjects

CRISPR-Cas9 genome editing, 0301 basic medicine, Candidate gene, QH301-705.5, Tau protein, Medicine (miscellaneous), tau Proteins, Molecular neuroscience, Article, General Biochemistry, Genetics and Molecular Biology, Progressive supranuclear palsy, Mice, Neuroblastoma, 03 medical and health sciences, 0302 clinical medicine, Ubiquitin, CRISPR-Associated Protein 9, Cell Line, Tumor, mental disorders, medicine, Animals, Humans, CRISPR, Genetic Testing, Biology (General), PI3K/AKT/mTOR pathway, Gene Editing, Neurons, biology, TOR Serine-Threonine Kinases, Alzheimer's disease, medicine.disease, Cellular neuroscience, Rats, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Genes, biology.protein, Neddylation, TSC1, CRISPR-Cas Systems, General Agricultural and Biological Sciences, Metabolic Networks and Pathways, 030217 neurology & neurosurgery, Genome-Wide Association Study

Abstract

Aggregates of hyperphosphorylated tau protein are a pathological hallmark of more than 20 distinct neurodegenerative diseases, including Alzheimer’s disease, progressive supranuclear palsy, and frontotemporal dementia. While the exact mechanism of tau aggregation is unknown, the accumulation of aggregates correlates with disease progression. Here we report a genome-wide CRISPR screen to identify modulators of endogenous tau protein for the first time. Primary screens performed in SH-SY5Y cells, identified positive and negative regulators of tau protein levels. Hit validation of the top 43 candidate genes was performed using Ngn2-induced human cortical excitatory neurons. Using this approach, genes and pathways involved in modulation of endogenous tau levels were identified, including chromatin modifying enzymes, neddylation and ubiquitin pathway members, and components of the mTOR pathway. TSC1, a critical component of the mTOR pathway, was further validated in vivo, demonstrating the relevance of this screening strategy. These findings may have implications for treating neurodegenerative diseases in the future., Using an unbiased genome-wide CRISPR screen approach, Sanchez et al. identified modulators of endogenous tau protein. This study suggests that chromatin modifiers, neddylation, ubiquitination, and the mTOR pathways regulate overall levels of tau protein in neurons, which could help in future identification of therapeutics for neurodegenerative diseases.

Published

2021

19. CRISPR/Cas9 Genome-Edited Autologous Hematopoietic Stem Cell Transplantation Therapies for Sickle Cell Disease

Author

Yi Liu, Vionnie W. Yu, Qi Zhang, Madhura Panditrao, Yi Yang, Alberto Del Rio-Espinola, Daher Ibrahim Aibo, Azeddine Elhajouji, Konrad Mueller, Karin Abitorabi, Daniel O'Connell, Bo Han, Nishit Patel, Carsten Russ, Craig Mickanin, Timothy K. MacLachlan, and Susan C. Stevenson

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

20. DRUG-seq Provides Unbiased Biological Activity Readouts for Neuroscience Drug Discovery

Author

Jingyao Li, Daniel J. Ho, Martin Henault, Chian Yang, Marilisa Neri, Robin Ge, Steffen Renner, Leandra Mansur, Alicia Lindeman, Brian Kelly, Tayfun Tumkaya, Xiaoling Ke, Gilberto Soler-Llavina, Gopi Shanker, Carsten Russ, Marc Hild, Caroline Gubser Keller, Jeremy L. Jenkins, Kathleen A. Worringer, Frederic D. Sigoillot, and Robert J. Ihry

Subjects

Sequence Analysis, RNA, Drug Discovery, Molecular Medicine, Humans, RNA, Reproducibility of Results, General Medicine, Transcriptome, Biochemistry

Abstract

Unbiased transcriptomic RNA-seq data has provided deep insights into biological processes. However, its impact in drug discovery has been narrow given high costs and low throughput. Proof-of-concept studies with Digital RNA with pertUrbation of Genes (DRUG)-seq demonstrated the potential to address this gap. We extended the DRUG-seq platform by subjecting it to rigorous testing and by adding an open-source analysis pipeline. The results demonstrate high reproducibility and ability to resolve the mechanism(s) of action for a diverse set of compounds. Furthermore, we demonstrate how this data can be incorporated into a drug discovery project aiming to develop therapeutics for schizophrenia using human stem cell-derived neurons. We identified both an on-target activation signature, induced by a set of chemically distinct positive allosteric modulators of the

Published

2022

21. DRUG-seq Provides Unbiased Biological Activity Readouts for Drug Discovery

Author

Kathleen A. Worringer, Robert J. Ihry, Marc Hild, Carsten Russ, Marilisa Neri, Leandra Mansur, Alicia Lindeman, Frederic Sigoillot, Chian Yang, Robin Ge, Jeremy L. Jenkins, Daniel J. Ho, Caroline Gubser Keller, Tayfun Tumkaya, Jingyao Li, Steffen Renner, and Martin Henault

Subjects

Drug, High complexity, Drug discovery, Mechanism (biology), Computer science, media_common.quotation_subject, Pipeline (computing), natural sciences, Biological activity, Computational biology, Throughput (business), media_common

Abstract

Unbiased transcriptomic RNA-seq data has provided deep insights about biological processes. However, its impact in drug discovery has been narrow given high costs and low throughput. Proof-of-concept studies with Digital RNA with pertUrbation of Genes (DRUG)-seq demonstrated the potential to address this gap. We extended the DRUG-seq platform by subjecting it to rigorous testing and by adding an open-source analysis pipeline. The results demonstrate high reproducibility and ability to resolve the mechanism(s) of action for a diverse set of compounds. Overall, the protocol and open-source analysis pipeline are a step towards industrializing RNA-seq for high complexity transcriptomics studies performed at a saturating scale.

Published

2021

22. IRF2 is a master regulator of human keratinocyte stem cell fate

Author

Carsten Russ, Adrian Salathe, Charles Y. Lin, John Alford, Mathias Frederiksen, Caroline Gubser Keller, Gabi Schutzius, Sajjeev Jagannathan, Sebastian Bergling, Dominic Hoepfner, Heinz Ruffner, Nicolas Mercado, Judith Knehr, Alexandra Aebi, John S. Reece-Hoyes, Guglielmo Roma, David Estoppey, Remi Terranova, Hadley E. Sheppard, Calla M. Olson, Tewis Bouwmeester, Tanner C. Beck, Susan Kirkland, Florian Nigsch, Christian Kolter, Felix Lohmann, and Selma Z. Elsarrag

Subjects

Keratinocytes, Transcriptional Activation, 0301 basic medicine, Cell type, Science, Antigen presentation, General Physics and Astronomy, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Gene regulatory networks, 03 medical and health sciences, 0302 clinical medicine, Interferon, Transcription (biology), medicine, Humans, Regeneration, lcsh:Science, Transcription factor, Tissue homeostasis, Multidisciplinary, Stem Cells, Cell Differentiation, General Chemistry, Cell biology, Chromatin, 030104 developmental biology, Self-renewal, lcsh:Q, Stem cell, Interferon Regulatory Factor-2, 030217 neurology & neurosurgery, Transcription Factors, Skin stem cells, medicine.drug

Abstract

Resident adult epithelial stem cells maintain tissue homeostasis by balancing self-renewal and differentiation. The stem cell potential of human epidermal keratinocytes is retained in vitro but lost over time suggesting extrinsic and intrinsic regulation. Transcription factor-controlled regulatory circuitries govern cell identity, are sufficient to induce pluripotency and transdifferentiate cells. We investigate whether transcriptional circuitry also governs phenotypic changes within a given cell type by comparing human primary keratinocytes with intrinsically high versus low stem cell potential. Using integrated chromatin and transcriptional profiling, we implicate IRF2 as antagonistic to stemness and show that it binds and regulates active cis-regulatory elements at interferon response and antigen presentation genes. CRISPR-KD of IRF2 in keratinocytes with low stem cell potential increases self-renewal, migration and epidermis formation. These data demonstrate that transcription factor regulatory circuitries, in addition to maintaining cell identity, control plasticity within cell types and offer potential for therapeutic modulation of cell function., Epidermal homeostasis requires long term stem cell function. Here, the authors apply transcriptional circuitry analysis based on integrated epigenomic profiling of primary human keratinocytes with high and low stem cell function to identify IRF2 as a negative regulator of stemness.

Published

2019

23. Bile acid analogues are activators of pyrin inflammasome

Author

Xinming Cai, Zinger Yang, John S. Reece-Hoyes, Edmund Harrington, John Alford, Tim Schuhmann, Luis Llamas, Rob Maher, Alicia Lindeman, Stephen M. Canham, Irina Alimov, Nadire Cochran, Carsten Russ, Suchithra Menon, Gregory R. Hoffman, Qiong Wang, and John Concannon

Subjects

0301 basic medicine, Inflammasomes, THP-1 Cells, medicine.drug_class, Gut flora, digestive system, Biochemistry, Pyrin domain, Bile Acids and Salts, 03 medical and health sciences, Immune system, medicine, Humans, Myeloid Cells, Editors' Picks, Microbiome, Intestinal Mucosa, Immunity, Mucosal, Molecular Biology, 030102 biochemistry & molecular biology, biology, Bile acid, Chemistry, Pyroptosis, Epithelial Cells, Inflammasome, Cell Biology, Pyrin, biology.organism_classification, MEFV, Gastrointestinal Microbiome, 030104 developmental biology, medicine.drug

Abstract

Bile acids are critical metabolites in the gastrointestinal tract and contribute to maintaining intestinal immune homeostasis through cross-talk with the gut microbiota. The conversion of bile acids by the gut microbiome is now recognized as a factor affecting both host metabolism and immune responses, but its physiological roles remain unclear. We conducted a screen for microbiome metabolites that would function as inflammasome activators and herein report the identification of 12-oxo-lithocholic acid (BAA485), a potential microbiome-derived bile acid metabolite. We demonstrate that the more potent analogue 11-oxo-12S-hydroxylithocholic acid methyl ester (BAA473) can induce secretion of interleukin-18 (IL-18) through activation of the inflammasome in both myeloid and intestinal epithelial cells. Using a genome-wide CRISPR screen with compound induced pyroptosis in THP-1 cells, we identified that inflammasome activation by BAA473 is pyrin-dependent (MEFV). To our knowledge, the bile acid analogues BAA485 and BAA473 are the first small molecule activators of the pyrin inflammasome. We surmise that pyrin inflammasome activation through microbiota-modified bile acid metabolites such as BAA473 and BAA485 plays a role in gut microbiota regulated intestinal immune response. The discovery of these two bioactive compounds may help to further unveil the importance of pyrin in gut homeostasis and autoimmune diseases.

Published

2019

24. Cell adhesion molecule KIRREL1 is a feedback regulator of Hippo signaling recruiting SAV1 to cell-cell contact sites

Author

Atanu Paul, Stefano Annunziato, Bo Lu, Tianliang Sun, Olivera Evrova, Lara Planas-Paz, Vanessa Orsini, Luigi M. Terracciano, Olga Charlat, Zinger Yang Loureiro, Lei Ji, Raffaella Zamponi, Frederic Sigoillot, Hong Lei, Alicia Lindeman, Carsten Russ, John S. Reece-Hoyes, Thomas B. Nicholson, Jan S. Tchorz, and Feng Cong

Subjects

Adult, Aged, 80 and over, Feedback, Physiological, Male, Multidisciplinary, General Physics and Astronomy, Membrane Proteins, Cell Cycle Proteins, Mice, Transgenic, YAP-Signaling Proteins, General Chemistry, Cell Communication, Middle Aged, General Biochemistry, Genetics and Molecular Biology, Gene Knockout Techniques, Mice, HEK293 Cells, Cell Line, Tumor, Hepatocytes, Animals, Humans, Female, Hippo Signaling Pathway, Cell Proliferation

Abstract

The Hippo/YAP pathway controls cell proliferation through sensing physical and spatial organization of cells. How cell-cell contact is sensed by Hippo signaling is poorly understood. Here, we identified the cell adhesion molecule KIRREL1 as an upstream positive regulator of the mammalian Hippo pathway. KIRREL1 physically interacts with SAV1 and recruits SAV1 to cell-cell contact sites. Consistent with the hypothesis that KIRREL1-mediated cell adhesion suppresses YAP activity, knockout of KIRREL1 increases YAP activity in neighboring cells. Analyzing pan-cancer CRISPR proliferation screen data reveals KIRREL1 as the top plasma membrane protein showing strong correlation with known Hippo regulators, highlighting a critical role of KIRREL1 in regulating Hippo signaling and cell proliferation. During liver regeneration in mice, KIRREL1 is upregulated, and its genetic ablation enhances hepatic YAP activity, hepatocyte reprogramming and biliary epithelial cell proliferation. Our data suggest that KIRREL1 functions as a feedback regulator of the mammalian Hippo pathway through sensing cell-cell interaction and recruiting SAV1 to cell-cell contact sites.

Published

2020

25. Previously Uncharacterized Vacuolar-type ATPase Binding Site Discovered from Structurally Similar Compounds with Distinct Mechanisms of Action

Author

John A. Tallarico, Yan Feng, Jennifer Lipps, Jason R. Thomas, Rishi K. Jain, Frederick J. King, Carsten Russ, Markus Schirle, Xuewen Pan, Edmund Harrington, Andrew C Wang, Helen Trinh Pham, Scott M. Brittain, Dominic Hoepfner, and Yuan Wang

Subjects

Vacuolar Proton-Translocating ATPases, Protein subunit, ATPase, Saccharomyces cerevisiae, Biochemistry, chemistry.chemical_compound, Humans, Amino Acid Sequence, Enzyme Inhibitors, Binding site, Biological Products, Reporter gene, Binding Sites, Molecular Structure, Neurospora crassa, Sequence Homology, Amino Acid, Photoaffinity labeling, biology, Mutagenesis, Bafilomycin, General Medicine, HCT116 Cells, HEK293 Cells, chemistry, biology.protein, Molecular Medicine, Chemical genetics

Abstract

Using a comprehensive chemical genetics approach, we identified a member of the lignan natural product family, HTP-013, which exhibited significant cytotoxicity across various cancer cell lines. Correlation of compound activity across a panel of reporter gene assays suggested the vacuolar-type ATPase (v-ATPase) as a potential target for this compound. Additional cellular studies and a yeast haploinsufficiency screen strongly supported this finding. Competitive photoaffinity labeling experiments demonstrated that the ATP6V0A2 subunit of the v-ATPase complex binds directly to HTP-013, and further mutagenesis library screening identified resistance-conferring mutations in ATP6V0A2. The positions of these mutations suggest the molecule binds a novel pocket within the domain of the v-ATPase complex responsible for proton translocation. While other mechanisms of v-ATPase regulation have been described, such as dissociation of the complex or inhibition by natural products including bafilomycin A1 and concanamycin, this work provides detailed insight into a distinct binding pocket within the v-ATPase complex.

Published

2018

26. The Natural Product Cavinafungin Selectively Interferes with Zika and Dengue Virus Replication by Inhibition of the Host Signal Peptidase

Author

Chia Min Lee, Kah Fei Wan, Ralph Riedl, Marco Janoschke, Ghislain M. C. Bonamy, Tewis Bouwmeester, Olaf Galuba, Hongping Dong, Philippe Mathys, Tim Schuhmann, David Estoppey, Martin Spiess, Carsten Russ, Dominic Hoepfner, Ireos Filipuzzi, Boon Heng Lee, Gregory McAllister, and Thomas Aust

Subjects

0301 basic medicine, Signal peptide, Protein subunit, 030106 microbiology, Saccharomyces cerevisiae, Dengue virus, medicine.disease_cause, Virus Replication, General Biochemistry, Genetics and Molecular Biology, Zika virus, 03 medical and health sciences, Lipopeptides, Viral Proteins, medicine, CRISPR, Humans, Flavivirus Infections, lcsh:QH301-705.5, Signal peptidase, Biological Products, biology, Cas9, Genome, Human, Serine Endopeptidases, Membrane Proteins, Genomics, Zika Virus, Dengue Virus, biology.organism_classification, HCT116 Cells, Virology, Protein Subunits, 030104 developmental biology, lcsh:Biology (General), Gene Knockdown Techniques, CRISPR-Cas Systems

Abstract

Summary: Flavivirus infections by Zika and dengue virus impose a significant global healthcare threat with no US Food and Drug Administration (FDA)-approved vaccination or specific antiviral treatment available. Here, we present the discovery of an anti-flaviviral natural product named cavinafungin. Cavinafungin is a potent and selectively active compound against Zika and all four dengue virus serotypes. Unbiased, genome-wide genomic profiling in human cells using a novel CRISPR/Cas9 protocol identified the endoplasmic-reticulum-localized signal peptidase as the efficacy target of cavinafungin. Orthogonal profiling in S. cerevisiae followed by the selection of resistant mutants pinpointed the catalytic subunit of the signal peptidase SEC11 as the evolutionary conserved target. Biochemical analysis confirmed a rapid block of signal sequence cleavage of both host and viral proteins by cavinafungin. This study provides an effective compound against the eukaryotic signal peptidase and independent confirmation of the recently identified critical role of the signal peptidase in the replicative cycle of flaviviruses. : Recent outbreaks and lack of effective treatments against dengue and Zika virus have caused public concerns. Estoppey et al. have identified cavinafungin as exerting potent and selective antiviral activity by targeting the signal-binding cleft of the catalytic subunit of the endoplasmic reticulum signal peptidase. Keywords: Zika virus, dengue virus, cavinafungin, signal peptidase, SEC11A, SEC11, CRISPR/Cas9, chemogenomic profiling

Published

2017

27. Genome-wide CRISPR screening reveals genetic modifiers of mutant EGFR dependence in human NSCLC

Author

Feng Cong, Bo Lu, Damien Begue, Youzhen Wang, Mika Manser, Alicia Lindeman, John S. Reece-Hoyes, Qiong Wang, Hao Zeng, Xiaomo Jiang, Debora Bonenfant, Carsten Russ, Raffaella Zamponi, Shumei Qiu, Johnny Castillo-Cabrera, Frederic Sigoillot, Vaik Strande, and Zinger Yang

Subjects

0301 basic medicine, Mutant, Regulator, Genome, CRISPR screen, Gene Knockout Techniques, Mice, 0302 clinical medicine, Carcinoma, Non-Small-Cell Lung, GPCR signaling, Guanine Nucleotide Exchange Factors, Methionyl Aminopeptidases, CRISPR, Clustered Regularly Interspaced Short Palindromic Repeats, Receptors, Lysophosphatidic Acid, Biology (General), Cancer Biology, General Neuroscience, EGFR TKI resistance, General Medicine, Cullin Proteins, Phenotype, ErbB Receptors, Gene Expression Regulation, Neoplastic, 030220 oncology & carcinogenesis, Medicine, Female, Research Article, Human, Signal Transduction, YAP signaling, Programmed cell death, QH301-705.5, Ubiquitin-Protein Ligases, Science, Mice, Nude, Biology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Cell Line, Tumor, Animals, Humans, Adaptor Proteins, Signal Transducing, RIC8A, General Immunology and Microbiology, Egfr inhibition, YAP-Signaling Proteins, Cell Biology, METAP2, respiratory tract diseases, HEK293 Cells, 030104 developmental biology, A549 Cells, ARIH2-CUL5 complex, Cancer research, CRISPR-Cas Systems, Transcriptome, rhoA GTP-Binding Protein, Transcription Factors

Abstract

EGFR-mutant NSCLCs frequently respond to EGFR tyrosine kinase inhibitors (TKIs). However, the responses are not durable, and the magnitude of tumor regression is variable, suggesting the existence of genetic modifiers of EGFR dependency. Here, we applied a genome-wide CRISPR-Cas9 screening to identify genetic determinants of EGFR TKI sensitivity and uncovered putative candidates. We show that knockout of RIC8A, essential for G-alpha protein activation, enhanced EGFR TKI-induced cell death. Mechanistically, we demonstrate that RIC8A is a positive regulator of YAP signaling, activation of which rescued the EGFR TKI sensitizing phenotype resulting from RIC8A knockout. We also show that knockout of ARIH2, or other components in the Cullin-5 E3 complex, conferred resistance to EGFR inhibition, in part by promoting nascent protein synthesis through METAP2. Together, these data uncover a spectrum of previously unidentified regulators of EGFR TKI sensitivity in EGFR-mutant human NSCLC, providing insights into the heterogeneity of EGFR TKI treatment responses., eLife digest Cancer is caused by cells growing and dividing uncontrollably as a result of mutations in certain genes. Many human lung cancers have a mutation in the gene that makes the protein EGFR. In healthy cells, EGFR allows a cell to respond to chemical signals that encourage healthy growth. In cancer, the altered EGFR is always on, which allows the cell to rapidly grow without any control, resulting in cancer. One approach to treating these cancers is with drugs that block the activity of mutant EGFR. Although these drugs have been very successful, they do not always succeed in completely treating the cancer. This is because over time the cancer cells can become resistant to the drug and start forming new tumors. One way that this can happen is if random mutations lead to changes in other proteins that make the drug less effective or stop it from accessing the EGFR proteins. However, it is unclear how other proteins in cancer cells affect the response to these EGFR inhibiting drugs. Now, Zeng et al. have used gene editing to systematically remove every protein from human lung cancer cells grown in the laboratory to see how this affects resistance to EGFR inhibitor treatment. This revealed that a number of different proteins could change how cancer cells responded to the drug. For instance, cells lacking the protein RIC8A were more sensitive to EGFR inhibitors and less likely to develop resistance. This is because loss of RIC8A turns down a key cell survival pathway in cancer cells. Whereas, cancer cells lacking the ARIH2 protein were able to produce more proteins that are needed for cancer cell growth, which resulted in them having increased resistance to EGFR inhibitors. The proteins identified in this study could be used to develop new drugs that improve the effectiveness of EGFR inhibitors. Understanding how cancer cells respond to EGFR inhibitor treatment could help determine how likely a patient is to develop resistance to these drugs.

Published

2019

28. Author response: Genome-wide CRISPR screening reveals genetic modifiers of mutant EGFR dependence in human NSCLC

Author

Johnny Castillo-Cabrera, Alicia Lindeman, Xiaomo Jiang, Carsten Russ, Frederic Sigoillot, Debora Bonenfant, Damien Begue, Shumei Qiu, Raffaella Zamponi, Feng Cong, Hao Zeng, Mika Manser, Bo Lu, Youzhen Wang, Qiong Wang, Vaik Strande, Zinger Yang, and John S. Reece-Hoyes

Subjects

Genetics, Mutant, CRISPR, Biology, Genome

Published

2019

29. USP7 inhibits Wnt/β-catenin signaling through promoting stabilization of Axin

Author

Gregory A. Michaud, Zinger Yang, Frederic Sigoillot, Carsten Russ, Tiancen Hu, Olga Charlat, Raffaella Zamponi, Robert J. Aversa, John S. Reece-Hoyes, Lei Ji, Xiaoping Zhu, Feng Cong, Jan S. Tchorz, Xiaomo Jiang, and Bo Lu

Subjects

0301 basic medicine, Scaffold protein, Ubiquitylation, General Physics and Astronomy, Deubiquitylating enzymes, Deubiquitinating enzyme, Ubiquitin-Specific Peptidase 7, Mice, 0302 clinical medicine, Ubiquitin, Adipocytes, lcsh:Science, Wnt Signaling Pathway, beta Catenin, Multidisciplinary, biology, Chemistry, Protein Stability, Reverse Transcriptase Polymerase Chain Reaction, Wnt signaling pathway, food and beverages, Osteoblast, Flow Cytometry, Cell biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Deubiquitination, Cell signalling, Immunoprecipitation, Science, macromolecular substances, General Biochemistry, Genetics and Molecular Biology, Article, Morphogen signalling, Cell Line, 03 medical and health sciences, Axin Protein, 3T3-L1 Cells, Cell Line, Tumor, medicine, Animals, Humans, Osteoblasts, fungi, Ubiquitination, General Chemistry, HCT116 Cells, 030104 developmental biology, biology.protein, lcsh:Q

Abstract

Axin is a key scaffolding protein responsible for the formation of the β-catenin destruction complex. Stability of Axin protein is regulated by the ubiquitin-proteasome system, and modulation of cellular concentration of Axin protein has a profound effect on Wnt/β-catenin signaling. Although E3s promoting Axin ubiquitination have been identified, the deubiquitinase responsible for Axin deubiquitination and stabilization remains unknown. Here, we identify USP7 as a potent negative regulator of Wnt/β-catenin signaling through CRISPR screens. Genetic ablation or pharmacological inhibition of USP7 robustly increases Wnt/β-catenin signaling in multiple cellular systems. USP7 directly interacts with Axin through its TRAF domain, and promotes deubiquitination and stabilization of Axin. Inhibition of USP7 regulates osteoblast differentiation and adipocyte differentiation through increasing Wnt/β-catenin signaling. Our study reveals a critical mechanism that prevents excessive degradation of Axin and identifies USP7 as a target for sensitizing cells to Wnt/β-catenin signaling., Axin is a scaffolding protein known for its role in Wnt signalling that can be marked with a variety of post-translational modifications. Here, Cong et al. demonstrate that USP7 de-ubiquinates Axin and that canonical Wnt signaling output can be increased with USP7 inhibitors.

Published

2019

30. A genome-wide CRISPR screen identifies ZCCHC14 as a host factor required for hepatitis B surface antigen production

Author

Meghan Holdorf, Nadire Cochran, Lili Xie, Paul Feucht, Scott Clarkson, Kyoko Uehara, Gregory R. Hoffman, Darlene Chen, Don Ganem, Frederic Sigoillot, Carsten Russ, Anastasia Hyrina, Alicia Lindeman, and Christopher T. Jones

Subjects

Zinc finger, HBsAg, Antigen, CRISPR, virus diseases, Biology, Nucleotidyltransferase, Gene, Virology, Virus, digestive system diseases, Host factor

Abstract

GRAPHICAL ABSTRACTSUMMARYA hallmark of chronic hepatitis B virus (CHB) infection is the presence of high circulating levels of non-infectious small lipid HBV surface antigen (HBsAg) vesicles. Although rare, sustained HBsAg loss is the idealized endpoint of any CHB therapy. A novel small molecule RG7834 has been previously reported to inhibit HBsAg expression by targeting terminal nucleotidyltransferase protein 4A and 4B (TENT4A and TENT4B). In this study, we describe a genome-wide CRISPR screen to identify other potential novel host factors required for HBsAg expression and to gain further insights into the mechanism of RG7834. We report more than 60 genes involved in regulating HBsAg and identified novel factors involved in RG7834 activity, including a zinc finger CCHC-type containing 14 (ZCCHC14) protein. We show that ZCCHC14, together with TENT4A/B, stabilizes HBsAg expression through HBV RNA tailing, providing a potential new therapeutic target to achieve functional cure in CHB patients.

Published

2019

31. A Genome-wide CRISPR Screen Identifies ZCCHC14 as a Host Factor Required for Hepatitis B Surface Antigen Production

Author

Frederic Sigoillot, Lili Xie, Don Ganem, Kyoko Uehara, Scott Clarkson, Carsten Russ, Nadire Cochran, Tiffany Tsang, Gregory R. Hoffman, Darlene Chen, Meghan Holdorf, Paul Feucht, Anastasia Hyrina, Christopher T. Jones, and Alicia Lindeman

Subjects

0301 basic medicine, HBsAg, Hepatitis B virus, Biology, Antiviral Agents, General Biochemistry, Genetics and Molecular Biology, Virus, 03 medical and health sciences, 0302 clinical medicine, Hepatitis B, Chronic, Antigen, Cell Line, Tumor, CRISPR, Humans, Clustered Regularly Interspaced Short Palindromic Repeats, lcsh:QH301-705.5, Gene, Host factor, Zinc finger, Hepatitis B Surface Antigens, Host Microbial Interactions, virus diseases, Nuclear Proteins, Polynucleotide Adenylyltransferase, Hep G2 Cells, Viral Load, Nucleotidyltransferase, Virology, digestive system diseases, 030104 developmental biology, lcsh:Biology (General), Antigens, Surface, DNA, Viral, 030217 neurology & neurosurgery, Genome-Wide Association Study

Abstract

Summary: A hallmark of chronic hepatitis B (CHB) virus infection is the presence of high circulating levels of non-infectious small lipid HBV surface antigen (HBsAg) vesicles. Although rare, sustained HBsAg loss is the idealized endpoint of any CHB therapy. A small molecule, RG7834, has been previously reported to inhibit HBsAg expression by targeting terminal nucleotidyltransferase proteins 4A and 4B (TENT4A and TENT4B). In this study, we describe a genome-wide CRISPR screen to identify other potential host factors required for HBsAg expression and to gain further insights into the mechanism of RG7834. We report more than 60 genes involved in regulating HBsAg and identify additional factors involved in RG7834 activity, including a zinc finger CCHC-type containing 14 (ZCCHC14) protein. We show that ZCCHC14, together with TENT4A/B, stabilizes HBsAg expression through HBV RNA tailing, providing a potential new therapeutic target to achieve functional cure in CHB patients. : Hyrina et al. employ a non-biased functional CRISPR screening approach to identify host factors regulating HBsAg expression as well as those targeted by RG7834, a HBsAg inhibitor. The screen highlighted over 60 genes and identified a mechanism by which ZCCHC14, together with TENT4A/B, stabilizes HBsAg expression through HBV RNA tailing. Keywords: HBV, HBsAg, CRISPR, genome-wide screen, RG7834, ZCCHC14, TENT4B, RNA tailing

Published

2019

32. DNA Repair Profiling Reveals Nonrandom Outcomes at Cas9-Mediated Breaks

Author

Scott Gradia, Matthew S. Thompson, Megan van Overbeek, Gregory R. Hoffman, Carsten Russ, Elizabeth Frias, Christopher D. Nye, Andrew May, John S. Reece-Hoyes, Daniel Capurso, Bastien Vidal, Chris R. Fuller, Jiashun Zheng, and Matthew Merrill Carter

Subjects

0301 basic medicine, DNA End-Joining Repair, Time Factors, DNA repair, Computational biology, Biology, Transfection, 03 medical and health sciences, chemistry.chemical_compound, Bacterial Proteins, Genome editing, CRISPR-Associated Protein 9, Humans, DNA Breaks, Double-Stranded, Molecular Biology, Gene, Gene Editing, Genetics, Cas9, Gene Expression Profiling, Cell Biology, Endonucleases, HCT116 Cells, HEK293 Cells, 030104 developmental biology, chemistry, RNA Interference, DNA mismatch repair, Human genome, CRISPR-Cas Systems, K562 Cells, DNA, RNA, Guide, Kinetoplastida

Abstract

Summary The repair outcomes at site-specific DNA double-strand breaks (DSBs) generated by the RNA-guided DNA endonuclease Cas9 determine how gene function is altered. Despite the widespread adoption of CRISPR-Cas9 technology to induce DSBs for genome engineering, the resulting repair products have not been examined in depth. Here, the DNA repair profiles of 223 sites in the human genome demonstrate that the pattern of DNA repair following Cas9 cutting at each site is nonrandom and consistent across experimental replicates, cell lines, and reagent delivery methods. Furthermore, the repair outcomes are determined by the protospacer sequence rather than genomic context, indicating that DNA repair profiling in cell lines can be used to anticipate repair outcomes in primary cells. Chemical inhibition of DNA-PK enabled dissection of the DNA repair profiles into contributions from c-NHEJ and MMEJ. Finally, this work elucidates a strategy for using "error-prone" DNA-repair machinery to generate precise edits.

Published

2016

33. Tankyrase Inhibitor Sensitizes Lung Cancer Cells to Endothelial Growth Factor Receptor (EGFR) Inhibition via Stabilizing Angiomotins and Inhibiting YAP Signaling

Author

Gregory McAllister, Zinger Yang, Carsten Russ, Johnny Castillo, Greg Hoffman, Alicia Lindeman, Feng Cong, John S. Reece-Hoyes, Bo Lu, John A. Tallarico, Wenqing Xu, Markus Schirle, Yue Zhang, and Hui Wang

Subjects

0301 basic medicine, Lung Neoplasms, Ubiquitin-Protein Ligases, Down-Regulation, Antineoplastic Agents, Protein degradation, Biochemistry, Erlotinib Hydrochloride, Gene Knockout Techniques, 03 medical and health sciences, 0302 clinical medicine, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, medicine, Humans, Protein Interaction Domains and Motifs, RNA, Small Interfering, Molecular Biology, Tissue homeostasis, Adaptor Proteins, Signal Transducing, EGFR inhibitors, Tankyrases, biology, Protein Stability, Microfilament Proteins, Wnt signaling pathway, Membrane Proteins, YAP-Signaling Proteins, Cell Biology, Phosphoproteins, Angiomotin, Ubiquitin ligase, Cell biology, ErbB Receptors, HEK293 Cells, 030104 developmental biology, Angiomotins, 030220 oncology & carcinogenesis, biology.protein, Intercellular Signaling Peptides and Proteins, Erlotinib, CRISPR-Cas Systems, Signal transduction, Signal Transduction, Transcription Factors, medicine.drug

Abstract

YAP signaling pathway plays critical roles in tissue homeostasis, and aberrant activation of YAP signaling has been implicated in cancers. To identify tractable targets of YAP pathway, we have performed a pathway-based pooled CRISPR screen and identified tankyrase and its associated E3 ligase RNF146 as positive regulators of YAP signaling. Genetic ablation or pharmacological inhibition of tankyrase prominently suppresses YAP activity and YAP target gene expression. Using a proteomic approach, we have identified angiomotin family proteins, which are known negative regulators of YAP signaling, as novel tankyrase substrates. Inhibition of tankyrase or depletion of RNF146 stabilizes angiomotins. Angiomotins physically interact with tankyrase through a highly conserved motif at their N terminus, and mutation of this motif leads to their stabilization. Tankyrase inhibitor-induced stabilization of angiomotins reduces YAP nuclear translocation and decreases downstream YAP signaling. We have further shown that knock-out of YAP sensitizes non-small cell lung cancer to EGFR inhibitor Erlotinib. Tankyrase inhibitor, but not porcupine inhibitor, which blocks Wnt secretion, enhances growth inhibitory activity of Erlotinib. This activity is mediated by YAP inhibition and not Wnt/β-catenin inhibition. Our data suggest that tankyrase inhibition could serve as a novel strategy to suppress YAP signaling for combinatorial targeted therapy.

Published

2016

34. mTORC1 signaling suppresses Wnt/β-catenin signaling through DVL-dependent regulation of Wnt receptor FZD level

Author

Sebastian Bergling, Paola Capodieci, John S. Reece-Hoyes, Hao Zeng, Martin Beibel, Raffaella Zamponi, Jan S. Tchorz, Feng Cong, Bo Lu, Zinger Yang, Sina Mohammadi, Joseph Loureiro, Carsten Russ, Kristie Wetzel, and Guglielmo Roma

Subjects

0301 basic medicine, Frizzled, Adaptor Protein Complex 2, Dishevelled Proteins, Down-Regulation, Gene Expression, mTORC1, Biology, Cell Line, Mice, 03 medical and health sciences, Animals, Humans, Wnt Signaling Pathway, beta Catenin, PI3K/AKT/mTOR pathway, Tissue homeostasis, chemistry.chemical_classification, Multidisciplinary, TOR Serine-Threonine Kinases, Wnt signaling pathway, Frizzled Receptors, Dishevelled, Cell biology, Wnt Proteins, HEK293 Cells, 030104 developmental biology, PNAS Plus, chemistry, Receptors, Wnt, Stem cell, Signal transduction

Abstract

Wnt/β-catenin signaling plays pivotal roles in cell proliferation and tissue homeostasis by maintaining somatic stem cell functions. The mammalian target of rapamycin (mTOR) signaling functions as an integrative rheostat that orchestrates various cellular and metabolic activities that shape tissue homeostasis. Whether these two fundamental signaling pathways couple to exert physiological functions still remains mysterious. Using a genome-wide CRISPR-Cas9 screening, we discover that mTOR complex 1 (mTORC1) signaling suppresses canonical Wnt/β-catenin signaling. Deficiency in tuberous sclerosis complex 1/2 (TSC1/2), core negative regulators of mTORC1 activity, represses Wnt/β-catenin target gene expression, which can be rescued by RAD001. Mechanistically, mTORC1 signaling regulates the cell surface level of Wnt receptor Frizzled (FZD) in a Dishevelled (DVL)-dependent manner by influencing the association of DVL and clathrin AP-2 adaptor. Sustained mTORC1 activation impairs Wnt/β-catenin signaling and causes loss of stemness in intestinal organoids ex vivo and primitive intestinal progenitors in vivo. Wnt/β-catenin-dependent liver metabolic zonation gene expression program is also down-regulated by mTORC1 activation. Our study provides a paradigm that mTORC1 signaling cell autonomously regulates Wnt/β-catenin pathway to influence stem cell maintenance.

Published

2018

35. Guide Swap enables genome-scale pooled CRISPR-Cas9 screening in human primary cells

Author

Loren Miraglia, S. Whitney Barnes, Jennifer Snead, Carsten Russ, Peter McNamara, John Lamb, Albert E. Parker, Chris Trussell, J. Scott Lee, Orzala Sharif, Pamela Y. Ting, John R. Walker, Michael P. Cooke, Anthony E. Boitano, Scott Clarkson, Fabio Luna, Heath E. Klock, Julie Vance, Mu-Yun Gao, Christian Schmedt, and Glenn C. Federe

Subjects

0301 basic medicine, Computer science, High-throughput screening, Computational biology, CD8-Positive T-Lymphocytes, Biochemistry, Genome, 03 medical and health sciences, Genome editing, CRISPR-Associated Protein 9, CRISPR, Humans, Guide RNA, Progenitor cell, Molecular Biology, Cells, Cultured, Gene Editing, Cas9, Genome, Human, Cell Biology, Hematopoietic Stem Cells, 030104 developmental biology, HEK293 Cells, CRISPR-Cas Systems, Functional genomics, Biotechnology, RNA, Guide, Kinetoplastida

Abstract

CRISPR–Cas9 screening allows genome-wide interrogation of gene function. Currently, to achieve the high and uniform Cas9 expression desirable for screening, one needs to engineer stable and clonal Cas9-expressing cells—an approach that is not applicable in human primary cells. Guide Swap permits genome-scale pooled CRISPR–Cas9 screening in human primary cells by exploiting the unexpected finding that editing by lentivirally delivered, targeted guide RNAs (gRNAs) occurs efficiently when Cas9 is introduced in complex with nontargeting gRNA. We validated Guide Swap in depletion and enrichment screens in CD4+ T cells. Next, we implemented Guide Swap in a model of ex vivo hematopoiesis, and identified known and previously unknown regulators of CD34+ hematopoietic stem and progenitor cell (HSPC) expansion. We anticipate that this platform will be broadly applicable to other challenging cell types, and thus will enable discovery in previously inaccessible but biologically relevant human primary cell systems.

Published

2018

36. TMEM41B is a novel regulator of autophagy and lipid mobilization

Author

Leon Murphy, Zhao Kang, Zinger Yang, Debora Bonenfant, Isabelle Claerr, Rowena DeJesus, Carsten Russ, Matthias Mueller, Damien Begue, John S. Reece-Hoyes, Christophe Antczak, Alexandra Graff, Christel Genoud, Beat Nyfeler, Jonathan M. Goodwin, Phil Bergman, Gregory R. Hoffman, Stacie Dodgson, Ramnik J. Xavier, David Marcellin, and Francesca Moretti

Subjects

0301 basic medicine, Autophagosome, Regulator, Cellular homeostasis, Autophagy-Related Proteins, Endoplasmic Reticulum, Biochemistry, 03 medical and health sciences, Gene Knockout Techniques, 0302 clinical medicine, Lipid droplet, Phagosomes, CRISPR-Associated Protein 9, Genetics, Autophagy, Homeostasis, Humans, Clustered Regularly Interspaced Short Palindromic Repeats, News & Views, Molecular Biology, Chemistry, Endoplasmic reticulum, Scientific Reports, Fatty Acids, Lentivirus, Lipid Mobilization, Autophagosomes, Membrane Proteins, Lipid Droplets, Transmembrane protein, Cell biology, 030104 developmental biology, Lysosomes, Microtubule-Associated Proteins, 030217 neurology & neurosurgery, Biogenesis, HeLa Cells

Abstract

Autophagy maintains cellular homeostasis by targeting damaged organelles, pathogens, or misfolded protein aggregates for lysosomal degradation. The autophagic process is initiated by the formation of autophagosomes, which can selectively enclose cargo via autophagy cargo receptors. A machinery of well-characterized autophagy-related proteins orchestrates the biogenesis of autophagosomes; however, the origin of the required membranes is incompletely understood. Here, we have applied sensitized pooled CRISPR screens and identify the uncharacterized transmembrane protein TMEM41B as a novel regulator of autophagy. In the absence of TMEM41B, autophagosome biogenesis is stalled, LC3 accumulates at WIPI2- and DFCP1-positive isolation membranes, and lysosomal flux of autophagy cargo receptors and intracellular bacteria is impaired. In addition to defective autophagy, TMEM41B knockout cells display significantly enlarged lipid droplets and reduced mobilization and β-oxidation of fatty acids. Immunostaining and interaction proteomics data suggest that TMEM41B localizes to the endoplasmic reticulum (ER). Taken together, we propose that TMEM41B is a novel ER-localized regulator of autophagosome biogenesis and lipid mobilization.

Published

2018

37. Genome-Scale CRISPR Screening Identifies Novel Human Pluripotent Gene Networks

Author

Gregory R. Hoffman, Kathleen A. Worringer, Ranjit Randhawa, Sravya Kommineni, Robert J. Ihry, Gregory McAllister, Marie Sondey, Steven Paula, Ricardo E. Dolmetsch, Zinger Yang, Ajamete Kaykas, Elizabeth Frias, Daniel J. Ho, Joe Raymond, Bob Altshuler, Max R. Salick, Carsten Russ, and John S. Reece-Hoyes

Subjects

Cas9, Somatic cell, Genome scale, Gene regulatory network, CRISPR, Computational biology, Stem cell, Biology, Induced pluripotent stem cell, Gene

Abstract

Human pluripotent stem cells (hPSCs) generate a wide variety of disease-relevant cells that can be used to improve the translation of preclinical research. Despite the potential of hPSCs, their use for genetic screening has been limited because of technical challenges. We developed a renewable Cas9/sgRNA-hPSC library where loss-of-function mutations can be induced at will. Our inducible-mutant hPSC library can be used for an unlimited number of genome-wide screens. We screened for novel genes involved in 3 of the fundamental properties of hPSCs: Their ability to self-renew/survive, their capacity to differentiate into somatic cells, and their inability to survive as single-cell clones. We identified a plethora of novel genes with unidentified roles in hPSCs. These results are available as a resource for the community to increase the understanding of both human development and genetics. In the future, our stem cell library approach will be a powerful tool to identify disease-modifying genes.VISUAL ABSTRACT

Published

2018

38. Genome-wide CRISPR screen for PARKIN regulators reveals transcriptional repression as a determinant of mitophagy

Author

Rowena DeJesus, Andreas W. Sailer, Stephen B. Helliwell, Gregory McAllister, John S. Reece-Hoyes, Christophe Crochemore, Florian Nigsch, Carsten Russ, Christoph Potting, Walter Carbone, Matthias Müller, Judith Knehr, Gregory R. Hoffman, Alicia Lindeman, Carole Manneville, Isabel Schmidt, Guglielmo Roma, Francesca Moretti, and Rob Maher

Subjects

0301 basic medicine, Ubiquitin-Protein Ligases, Induced Pluripotent Stem Cells, Repressor, PINK1, Parkin, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Mitophagy, CRISPR, Humans, Phosphorylation, Cells, Cultured, Regulation of gene expression, Neurons, Multidisciplinary, biology, Cas9, Genome, Human, Ubiquitin, Infant, Newborn, HCT116 Cells, nervous system diseases, Ubiquitin ligase, Cell biology, Repressor Proteins, 030104 developmental biology, HEK293 Cells, Gene Expression Regulation, SI Correction, biology.protein, CRISPR-Cas Systems, Protein Kinases, 030217 neurology & neurosurgery

Abstract

PARKIN, an E3 ligase mutated in familial Parkinson's disease, promotes mitophagy by ubiquitinating mitochondrial proteins for efficient engagement of the autophagy machinery. Specifically, PARKIN-synthesized ubiquitin chains represent targets for the PINK1 kinase generating phosphoS65-ubiquitin (pUb), which constitutes the mitophagy signal. Physiological regulation of PARKIN abundance, however, and the impact on pUb accumulation are poorly understood. Using cells designed to discover physiological regulators of PARKIN abundance, we performed a pooled genome-wide CRISPR/Cas9 knockout screen. Testing identified genes individually resulted in a list of 53 positive and negative regulators. A transcriptional repressor network including THAP11 was identified and negatively regulates endogenous PARKIN abundance. RNAseq analysis revealed the PARKIN-encoding locus as a prime THAP11 target, and THAP11 CRISPR knockout in multiple cell types enhanced pUb accumulation. Thus, our work demonstrates the critical role of PARKIN abundance, identifies regulating genes, and reveals a link between transcriptional repression and mitophagy, which is also apparent in human induced pluripotent stem cell-derived neurons, a disease-relevant cell type.

Published

2017

39. Mitochondrial genome sequences reveal evolutionary relationships of the Phytophthora 1c clade species

Author

Jean B. Ristaino, Jeffrey L. Thorne, Andaine Seguin-Orlando, Erica S. Lassiter, José Alfredo Samaniego, Chad Nusbaum, Ignazio Carbone, Carsten Russ, Chia Hui Hu, Rodrigo A. Olarte, Qiandong Zeng, and Amanda C. Saville

Subjects

Phytophthora, Mitochondrial DNA, Phytophthora infestans, Colombia, DNA, Mitochondrial, Genome, Article, Solanum lycopersicum, Phylogenetics, Peru, Botany, Genetics, Clade, Phylogeny, Plant Diseases, Solanum tuberosum, biology, Phylogenetic tree, Chimera, food and beverages, Sequence Analysis, DNA, General Medicine, biology.organism_classification, Biological Evolution, Mitochondria, Phylogeography, Evolutionary biology, Genome, Mitochondrial, Ecuador

Abstract

Phytophthora infestans is one of the most destructive plant pathogens of potato and tomato globally. The pathogen is closely related to four other Phytophthora species including P. phaseoli, P. ipomoeae, P. mirabilis, and P. andina that are important pathogens of other wild and domesticated hosts. P. andina is an interspecific hybrid between P. infestans and an unknown Phytophthora species. We have sequenced mitochondrial genomes of the sister species of P. infestans in order to resolve the evolutionary relationships within the clade. Phylogenetic analysis indicates that the P. phaseoli mitochondrial lineage is basal within the clade. P. mirabilis and P. ipomoeae are sister lineages and share a common ancestor with the Ic mitochondrial lineage of P. andina. These lineages in turn are sister to the P. infestans and P. andina Ia mitochondrial lineages. The P. andina Ic lineage diverged much earlier than the P. andina Ia mitochondrial lineage and P. infestans. The presence of two mitochondrial lineages in P. andina supports the hybrid nature of this species. The ancestral state of the P. andina Ic lineage in the tree and its occurrence only in the Andean regions of Ecuador, Colombia and Peru suggests further sampling in the Americasis warranted to understand the distribution of this species hybrid in nature.

Published

2015

40. p53 inhibits CRISPR-Cas9 engineering in human pluripotent stem cells

Author

Elizabeth Frias, Carsten Russ, Sravya Kommineni, Robert J. Ihry, William C. Forrester, Marie Sondey, Kraig M. Theriault, Chaoyang Ye, Ajamete Kaykas, Daniel J. Ho, Ricardo E. Dolmetsch, Kathleen A. Worringer, Max R. Salick, Gregory R. Hoffman, Gregory McAllister, Tripti Kulkarni, Julie Chen, Zinger Yang, Ranjit Randhawa, and John S. Reece-Hoyes

Subjects

0301 basic medicine, Cyclin-Dependent Kinase Inhibitor p21, Pluripotent Stem Cells, Transcription, Genetic, Biology, Genome, General Biochemistry, Genetics and Molecular Biology, Genome engineering, 03 medical and health sciences, CRISPR-Associated Protein 9, CRISPR, Humans, DNA Breaks, Double-Stranded, RNA, Messenger, fas Receptor, Induced pluripotent stem cell, Cas9, Gene targeting, General Medicine, Embryonic stem cell, Cell biology, 030104 developmental biology, Stem cell, CRISPR-Cas Systems, Tumor Suppressor Protein p53, Genetic Engineering, Gene Deletion, RNA, Guide, Kinetoplastida

Abstract

CRISPR/Cas9 has revolutionized our ability to engineer genomes and conduct genome-wide screens in human cells1–3. Whereas some cell types are amenable to genome engineering, genomes of human pluripotent stem cells (hPSCs) have been difficult to engineer, with reduced efficiencies relative to tumour cell lines or mouse embryonic stem cells3–13. Here, using hPSC lines with stable integration of Cas9 or transient delivery of Cas9-ribonucleoproteins (RNPs), we achieved an average insertion or deletion (indel) efficiency greater than 80%. This high efficiency of indel generation revealed that double-strand breaks (DSBs) induced by Cas9 are toxic and kill most hPSCs. In previous studies, the toxicity of Cas9 in hPSCs was less apparent because of low transfection efficiency and subsequently low DSB induction 3 . The toxic response to DSBs was P53/TP53-dependent, such that the efficiency of precise genome engineering in hPSCs with a wild-type P53 gene was severely reduced. Our results indicate that Cas9 toxicity creates an obstacle to the high-throughput use of CRISPR/Cas9 for genome engineering and screening in hPSCs. Moreover, as hPSCs can acquire P53 mutations 14 , cell replacement therapies using CRISPR/Cas9-enginereed hPSCs should proceed with caution, and such engineered hPSCs should be monitored for P53 function.

Published

2017

41. P53 toxicity is a hurdle to CRISPR/CAS9 screening and engineering in human pluripotent stem cells

Author

Elizabeth Frias, Sravya Kommineni, Robert J. Ihry, William C. Forrester, Gregory R. Hoffman, Zinger Yang, Julie Chen, John S. Reece-Hoyes, Kraig M. Theriault, Ricardo E. Dolmetsch, Kathleen A. Worringer, Ranjit Randhawa, Gregory McAllister, Chaoyang Ye, Ajamete Kaykas, Marie Sondey, Daniel J. Ho, Carsten Russ, Max R. Salick, and Tripti Kulkarni

Subjects

Genetics, Cell type, Cas9, Cell culture, Toxicity, CRISPR, Biology, Tp53 mutation, Induced pluripotent stem cell, Function (biology), Cell biology

Abstract

SUMMARYCRISPR/Cas9 has revolutionized our ability to engineer genomes and to conduct genome-wide screens in human cells. While some cell types are easily modified with Cas9, human pluripotent stem cells (hPSCs) poorly tolerate Cas9 and are difficult to engineer. Using a stable Cas9 cell line or transient delivery of ribonucleoproteins (RNPs) we achieved an average insertion or deletion efficiency greater than 80%. This high efficiency made it apparent that double strand breaks (DSBs) induced by Cas9 are toxic and kill most treated hPSCs. Cas9 toxicity creates an obstacle to the high-throughput use CRISPR/Cas9 for genome-engineering and screening in hPSCs. We demonstrated the toxic response istp53-dependent and the toxic effect oftp53severely reduces the efficiency of precise genome-engineering in hPSCs. Our results highlight that CRISPR-based therapies derived from hPSCs should proceed with caution. Following engineering, it is critical to monitor fortp53function, especially in hPSCs which spontaneously acquiretp53mutations.

Published

2017

42. TRRAP is a central regulator of human multiciliated cell formation

Author

Carsten Russ, Nicole A. Renaud, John S. Reece-Hoyes, Guglielmo Roma, Rob Maher, Gregory R. Hoffman, Zinger Yang, Angelica D. Pessotti, Walter Carbone, Nadire Cochran, Rayman Choo-Wing, Lindsey W. Plasschaert, Shivani Aryal, Aron B. Jaffe, Alicia Lindeman, Nathaniel D. Kirkpatrick, Zhao Wang, and Gregory McAllister

Subjects

0301 basic medicine, Cell type, Xenopus, Cell Cycle Proteins, Cell Line, Epigenesis, Genetic, Small hairpin RNA, 03 medical and health sciences, Report, Humans, Cell Lineage, Cilia, Receptor, Notch2, Progenitor cell, RNA, Small Interfering, Transcription factor, Zebrafish, Lung, Research Articles, Adaptor Proteins, Signal Transducing, Regulation of gene expression, biology, food and beverages, Nuclear Proteins, Epithelial Cells, Forkhead Transcription Factors, Cell Biology, biology.organism_classification, Cell biology, 030104 developmental biology, Gene Expression Regulation, Motile cilium, Signal Transduction, Transcription Factors

Abstract

Multiciliated cells (MCCs) function to promote directional fluid flow across epithelial tissues. Wang et al. show that TRRAP, a component of multiple histone acetyltransferase complexes, is required for airway MCC formation and regulates a network of genes involved in MCC differentiation and function., The multiciliated cell (MCC) is an evolutionarily conserved cell type, which in vertebrates functions to promote directional fluid flow across epithelial tissues. In the conducting airway, MCCs are generated by basal stem/progenitor cells and act in concert with secretory cells to perform mucociliary clearance to expel pathogens from the lung. Studies in multiple systems, including Xenopus laevis epidermis, murine trachea, and zebrafish kidney, have uncovered a transcriptional network that regulates multiple steps of multiciliogenesis, ultimately leading to an MCC with hundreds of motile cilia extended from their apical surface, which beat in a coordinated fashion. Here, we used a pool-based short hairpin RNA screening approach and identified TRRAP, an essential component of multiple histone acetyltransferase complexes, as a central regulator of MCC formation. Using a combination of immunofluorescence, signaling pathway modulation, and genomic approaches, we show that (a) TRRAP acts downstream of the Notch2-mediated basal progenitor cell fate decision and upstream of Multicilin to control MCC differentiation; and (b) TRRAP binds to the promoters and regulates the expression of a network of genes involved in MCC differentiation and function, including several genes associated with human ciliopathies.

Published

2017

43. Identification of a novel NAMPT inhibitor by CRISPR/Cas9 chemogenomic profiling in mammalian cells

Author

Chantale T. Guy, Markus Schirle, Bertran Gerrits, David Estoppey, Xuewen Pan, Jason R. Thomas, Malini Varadarajan, Annick Waldt, Gregory McAllister, Jeffrey Hewett, Kevin Xie, Nadire Ramadan, Sven Schuierer, Guglielmo Roma, Judith Knehr, Elizabeth Frias, Qiong Wang, Zinger Yang, Tewis Bouwmeester, Alicia Lindeman, John S. Reece-Hoyes, Walter Carbone, Edmund Harrington, Dominic Hoepfner, Carsten Russ, Xin Chen, Rachel Cuttat, and Gregory R. Hoffman

Subjects

0301 basic medicine, Induced Pluripotent Stem Cells, Nicotinamide phosphoribosyltransferase, Computational biology, Biology, Chemical genetics, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Target identification, Drug Discovery, medicine, Humans, CRISPR, Enzyme Inhibitors, Nicotinamide Phosphoribosyltransferase, Induced pluripotent stem cell, Cells, Cultured, Genetics, Multidisciplinary, Drug discovery, Cas9, Gene deletion, Pharmacogenomic Testing, 030104 developmental biology, Mechanism of action, chemistry, 030220 oncology & carcinogenesis, CRISPR-Cas Systems, medicine.symptom, Gene Deletion

Abstract

Scientific Reports, 7, ISSN:2045-2322

Published

2017

44. Comprehensive variation discovery in single human genomes

Author

Iain MacCallum, Ryan Hegarty, Brian Sogoloff, Laurie Holmes, David B. Jaffe, Eric S. Lander, Shuangye Yin, Bayo Lau, Chad Nusbaum, Ted Sharpe, Diana Tabbaa, Carsten Russ, Neil I. Weisenfeld, Louise Williams, Massachusetts Institute of Technology. Department of Biology, and Lander, Eric S.

Subjects

Molecular Sequence Data, Genomics, Computational biology, Biology, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Sensitivity and Specificity, Genome, Article, 03 medical and health sciences, 0302 clinical medicine, Gene Frequency, Genetic variation, Genetics, Humans, Allele frequency, Oligonucleotide Array Sequence Analysis, 030304 developmental biology, Segmental duplication, Sequence (medicine), 0303 health sciences, Base Sequence, Genome, Human, Chromosome Mapping, Genetic Variation, High-Throughput Nucleotide Sequencing, Reproducibility of Results, 3. Good health, Fosmid, Human genome, Algorithms, Software, 030217 neurology & neurosurgery

Abstract

Complete knowledge of the genetic variation in individual human genomes is a crucial foundation for understanding the etiology of disease. Genetic variation is typically characterized by sequencing individual genomes and comparing reads to a reference. Existing methods do an excellent job of detecting variants in approximately 90% of the human genome; however, calling variants in the remaining 10% of the genome (largely low-complexity sequence and segmental duplications) is challenging. To improve variant calling, we developed a new algorithm, DISCOVAR, and examined its performance on improved, low-cost sequence data. Using a newly created reference set of variants from the finished sequence of 103 randomly chosen fosmids, we find that some standard variant call sets miss up to 25% of variants. We show that the combination of new methods and improved data increases sensitivity by several fold, with the greatest impact in challenging regions of the human genome., National Human Genome Research Institute (U.S.) (Grant R01HG003474), National Human Genome Research Institute (U.S.) (Grant U54HG003067), National Institute of Allergy and Infectious Diseases (U.S.) (Contract HHSN272200900018C)

Published

2014

45. YAP, but Not RSPO-LGR4/5, Signaling in Biliary Epithelial Cells Promotes a Ductular Reaction in Response to Liver Injury

Author

Florian Nigsch, Lapo Morelli, Zinger Yang, Tianliang Sun, Maryam Syed, Linda E. Greenbaum, Guglielmo Roma, John S. Reece-Hoyes, Jan S. Tchorz, Luigi Terracciano, Thomas B. Nicholson, Andreas W. Sailer, Caroline Gubser Keller, Lara Planas-Paz, Nadire Cochran, Sven Schuierer, Tewis Bouwmeester, Yi Yang, Carlos M. Cobos, Jesse J. Lugus, Annick Waldt, Vanessa Orsini, John Alford, Jasna Jetzer, Xiaohong Mao, Philipp S. Hoppe, Frederic Sigoillot, Wibke Schwarzer, Monika Pikiolek, Nicole Carballido-Perrig, Gregory McAllister, Carsten Russ, Feng Cong, Sebastian Bergling, Le Zhang, Gregory R. Hoffman, Marilisa Neri, Rachel Cuttat, and Bernd Kinzel

Subjects

Liver injury, 0303 health sciences, LGR5, Wnt signaling pathway, Liver Stem Cell, Cell Biology, Biology, medicine.disease, Liver regeneration, Cell biology, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Genetics, medicine, AXIN2, Molecular Medicine, Signal transduction, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

Summary Biliary epithelial cells (BECs) form bile ducts in the liver and are facultative liver stem cells that establish a ductular reaction (DR) to support liver regeneration following injury. Liver damage induces periportal LGR5+ putative liver stem cells that can form BEC-like organoids, suggesting that RSPO-LGR4/5-mediated WNT/β-catenin activity is important for a DR. We addressed the roles of this and other signaling pathways in a DR by performing a focused CRISPR-based loss-of-function screen in BEC-like organoids, followed by in vivo validation and single-cell RNA sequencing. We found that BECs lack and do not require LGR4/5-mediated WNT/β-catenin signaling during a DR, whereas YAP and mTORC1 signaling are required for this process. Upregulation of AXIN2 and LGR5 is required in hepatocytes to enable their regenerative capacity in response to injury. Together, these data highlight heterogeneity within the BEC pool, delineate signaling pathways involved in a DR, and clarify the identity and roles of injury-induced periportal LGR5+ cells.

Published

2019

46. Genome-Scale CRISPR Screens Identify Human Pluripotency-Specific Genes

Author

Max R. Salick, Carsten Russ, Sravya Kommineni, Ranjit Randhawa, Robert J. Ihry, Gregory R. Hoffman, John S. Reece-Hoyes, Marie Sondey, Elizabeth Frias, Kathleen A. Worringer, Beata Henry, Robert C. Altshuler, Gregory McAllister, Qiong Wang, Joe Raymond, Zinger Yang, Daniel J. Ho, Chaoyang Ye, Ajamete Kaykas, Steven Paula, and Ricardo E. Dolmetsch

Subjects

Pluripotent Stem Cells, 0301 basic medicine, Cell type, Genome, Cas9, Mutant, Genome scale, Computational biology, Biology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Preclinical research, 030104 developmental biology, 0302 clinical medicine, lcsh:Biology (General), Humans, CRISPR, Genetic Testing, CRISPR-Cas Systems, Induced pluripotent stem cell, lcsh:QH301-705.5, Gene, 030217 neurology & neurosurgery

Abstract

Summary: Human pluripotent stem cells (hPSCs) generate a variety of disease-relevant cells that can be used to improve the translation of preclinical research. Despite the potential of hPSCs, their use for genetic screening has been limited by technical challenges. We developed a scalable and renewable Cas9 and sgRNA-hPSC library in which loss-of-function mutations can be induced at will. Our inducible mutant hPSC library can be used for multiple genome-wide CRISPR screens in a variety of hPSC-induced cell types. As proof of concept, we performed three screens for regulators of properties fundamental to hPSCs: their ability to self-renew and/or survive (fitness), their inability to survive as single-cell clones, and their capacity to differentiate. We identified the majority of known genes and pathways involved in these processes, as well as a plethora of genes with unidentified roles. This resource will increase the understanding of human development and genetics. This approach will be a powerful tool to identify disease-modifying genes and pathways. : Ihry et al. develop a CRISPR/Cas9 genetic screening platform for hPSCs that enables unbiased genome-scale genetic screening. The platform exhibits high performance and accurately detects the dropout of essential genes. Furthermore, proof-of-concept screens exploit hPSC-specific phenotypes to identify regulators of fitness, survival after single-cell dissociation, and pluripotency. Keywords: CRISPR genome-wide screening, human pluripotent stem cells, iPSC, hESC, PAWR, PMAIP1, DDR

Published

2019

47. Structure of the germline genome of Tetrahymena thermophila and relationship to the massively rearranged somatic genome

Author

Jie Xiong, Riza M. Daza, Robert S. Coyne, Nikhat Zafar, Tomoko Noto, Lin Fan, Eduardo Orias, Eileen P. Hamilton, Cédric Feschotte, Donna Cassidy-Hanley, Jennifer R. Wortman, Michalis Hadjithomas, Piroska Huvos, Wei Miao, Joshua Z. Levin, Jonathan H. Badger, Romeo Papazyan, Jainy Thomas, Vivek Krishnakumar, Clayton M. Carey, Sharvari Gujja, Sarah Young, Qiandong Zeng, Ryan Hegarty, Paul H. Dear, Terrance Shea, Elisabet Caler, Aurélie Kapusta, Chad Nusbaum, Ellen J. Pritham, Haibao Tang, Shelby L. Bidwell, Kazufumi Mochizuki, Bruce W. Birren, Sean D. Taverna, and Carsten Russ

Subjects

0301 basic medicine, Genome evolution, QH301-705.5, Science, Genomics, Genome, General Biochemistry, Genetics and Molecular Biology, Tetrahymena thermophila, 03 medical and health sciences, Biology (General), Genetics, genome rearrangement, General Immunology and Microbiology, biology, General Neuroscience, Tetrahymena, General Medicine, Genome project, Gene rearrangement, transposable element, biology.organism_classification, intermal eliminated sequence, 030104 developmental biology, centromere, chromosome breakage, Medicine, Programmed DNA elimination, Chromosome breakage

Abstract

The germline genome of the binucleated ciliate Tetrahymena thermophila undergoes programmed chromosome breakage and massive DNA elimination to generate the somatic genome. Here, we present a complete sequence assembly of the germline genome and analyze multiple features of its structure and its relationship to the somatic genome, shedding light on the mechanisms of genome rearrangement as well as the evolutionary history of this remarkable germline/soma differentiation. Our results strengthen the notion that a complex, dynamic, and ongoing interplay between mobile DNA elements and the host genome have shaped Tetrahymena chromosome structure, locally and globally. Non-standard outcomes of rearrangement events, including the generation of short-lived somatic chromosomes and excision of DNA interrupting protein-coding regions, may represent novel forms of developmental gene regulation. We also compare Tetrahymena’s germline/soma differentiation to that of other characterized ciliates, illustrating the wide diversity of adaptations that have occurred within this phylum.

Published

2016

48. Author response: Structure of the germline genome of Tetrahymena thermophila and relationship to the massively rearranged somatic genome

Author

Eduardo Orias, Robert S. Coyne, Vivek Krishnakumar, Piroska Huvos, Elisabet Caler, Kazufumi Mochizuki, Eileen P. Hamilton, Jainy Thomas, Haibao Tang, Shelby L. Bidwell, Aurélie Kapusta, Terrance Shea, Sean D. Taverna, Sharvari Gujja, Michalis Hadjithomas, Jie Xiong, Chad Nusbaum, Clayton M. Carey, Ellen J. Pritham, Wei Miao, Carsten Russ, Nikhat Zafar, Donna Cassidy-Hanley, Cédric Feschotte, Jonathan H. Badger, Bruce W. Birren, Ryan Hegarty, Paul H. Dear, Sarah Young, Romeo Papazyan, Joshua Z. Levin, Tomoko Noto, Riza M. Daza, Lin Fan, Qiandong Zeng, and Jennifer R. Wortman

Subjects

Genetics, Somatic cell, Tetrahymena, Biology, biology.organism_classification, Genome, Germline

Published

2016

49. Genome Sequence of Spizellomyces punctatus

Author

Zehua Chen, Chad Nusbaum, B. Franz Lang, Terrance Shea, Christina A. Cuomo, Qiandong Zeng, Carsten Russ, Sarah Young, and Sharvari Gujja

Subjects

0301 basic medicine, Whole genome sequencing, Chytridiomycota, Spizellomyces punctatus, Spizellomyces, biology, Phylum, Eukaryotes, fungi, Fungus, 030108 mycology & parasitology, 15. Life on land, biology.organism_classification, complex mixtures, 03 medical and health sciences, 030104 developmental biology, Evolutionary biology, Genetics, Terrestrial ecosystem, Molecular Biology

Abstract

Spizellomyces punctatus is a basally branching chytrid fungus that is found in the Chytridiomycota phylum. Spizellomyces species are common in soil and of importance in terrestrial ecosystems. Here, we report the genome sequence of S. punctatus , which will facilitate the study of this group of early diverging fungi.

Published

2016

50. Author response: Functional CRISPR screening identifies the ufmylation pathway as a regulator of SQSTM1/p62

Author

Zuncai Wang, Walter Carbone, Jennifer Kelliher, Rowena DeJesus, Guglielmo Roma, John S. Reece-Hoyes, Aylwin Ng, Francesca Moretti, Craig Mickanin, Phil Bergman, Alicia Lindeman, Shanming Liu, Gregory R. Hoffman, John Alford, Martin Beibel, Beat Nyfeler, Leon Murphy, Carsten Russ, John A. Tallarico, Gregory McAllister, Judith Knehr, Ramnik J. Xavier, Elizabeth Frias, and Jeffery A. Porter

Subjects

Regulator, CRISPR, Computational biology, Biology

Published

2016