Your search keyword '"Parsons MJ"' showing total 114 results

1. Mutation burden and other molecular markers of prognosis in the QUASAR2 clinical trial of colorectal cancer treated with curative intent

Author

Domingo, E, Camps, C, Kaisaki, PJ, Parsons, MJ, Mouradov, D, Pentony, MM, Makino, S, Palmieri, M, Ward, RL, Hawkins, NJ, Gibbs, P, Askautrud, H, Oukrif, D, Wang, H, Wood, J, Tomlinson, E, Bark, Y, Kaur, K, Johnstone, EC, Palles, CL, Church, DN, Novelli, M, Danielsen, HE, Sherlock, J, Kerr, DJ, Kerr, R, Sieber, O, Taylor, JC, and Tomlinson, I

Subjects

endocrine system diseases, neoplasms, digestive system diseases

Abstract

Background Several relatively large studies have assessed molecular indicators of colorectal cancer (CRC) prognosis, but most analyses have been restricted to a handful of markers. Methods In stage II/III CRCs from the QUASAR2 clinical trial and from an Australian community-based series, we assessed gene panels for somatic driver mutations and overall mutation burden. We determined molecular pathways of tumorigenesis, and analysed associations with treatment response and prognosis. Findings In QUASAR2 (N=511), TP53, KRAS, BRAF and GNAS mutations were independently associated with shorter relapse-free survival, whereas total somatic mutation burden was associated with longer survival, even after excluding mismatch repair-deficient (MSI+) and POLE-mutant tumours. We successfully validated these associations in the Australian sample set (N=296). In an extended analysis of 1,752 QUASAR2 and Australian CRCs for which KRAS, BRAF and MSI status was available, we found that KRAS and BRAF mutations were specifically associated with poor prognosis in MSI- cancers. This association was not present in MSI+ cancers, and MSI+ tumours with KRAS or BRAF mutation actually had better prognosis than MSI- cancers that were wildtype for KRAS or BRAF. New rare molecular pathways were also uncovered: mutations in the genes NF1 and NRAS from the MAP kinase pathway co-occurred, mutations in TP53 and ATM appeared to be alternative ways of inactivating the DNA damage response pathway. Interpretation A multi-gene panel has identified two previously unreported prognostic associations in CRC involving both TP53 mutation and total mutation burden, and confirmed associations with KRAS and BRAF. We conclude that even a modest-sized gene panel can provide important information for use in clinical practice and out-perform MSI-based models.

Published

2018

2. On the genetics of sleep disorders: genome-wide association studies and beyond

Author

Parsons MJ

Subjects

lcsh:Genetics, lcsh:QH426-470

Abstract

Michael J ParsonsMammalian Genetics Unit, MRC Harwell, Harwell, Oxfordshire, UKAbstract: Sleep is an essential behavior, yet much of its underlying functions are still unknown. The disruption of sleep can led to a variety of health consequences. Family and twin studies have together shown that genetic factors underlie variation in sleep characteristics and sleep disorders. Given the importance of sleep to our well-being, understanding its underlying genetic factors is essential to both the prevention and treatment of these disorders. Recently, genome-wide association studies (GWAS) have helped to provide evidence of associations of both known and novel genetic variants with sleep disorders. This review outlines the findings from GWAS for a number of sleep disorders, including insomnia, restless leg syndrome, obstructive sleep apnea, and narcolepsy, and discusses these findings in the context of supporting evidence from independent methodologies. Finally, the limitations of GWAS approaches are outlined, along with the future directions of the genetics of sleep in the post-GWAS era.Keywords: genome-wide association studies, sleep, sleep disorder, insomnia, restless leg syndrome, obstructive sleep apnea, narcolepsy

Published

2015

3. MACROD2 deletions cause impaired PARP1 activity and chromosome instability in colorectal cancer.

Author

Sakthianandeswaren, A, Parsons, MJ, Mouradov, D, Sieber, OM, Sakthianandeswaren, A, Parsons, MJ, Mouradov, D, and Sieber, OM

Published

2018

4. Genetic polymorphisms and their association with brain and behavioural measures in heterogeneous stock mice

Author

Janecka, M, Marzi, SJ, Parsons, MJ, Liu, L, Paya-Cano, JL, Smith, RG, Fernandes, C, and Schalkwyk, LC

Subjects

EXPRESSION, Male, STRATEGIES, Quantitative Trait Loci, Gene Expression, Tryptophan Hydroxylase, Polymorphism, Single Nucleotide, Genetic Heterogeneity, Mice, INBRED MOUSE STRAINS, Animals, GENOME-WIDE ASSOCIATION, MODULATION, NEURODEVELOPMENTAL DISORDERS, Genetic Association Studies, Science & Technology, RECEPTOR, Behavior, Animal, COMPLEX TRAITS, SEROTONIN, QUANTITATIVE TRAIT GENES, Brain, Sp2 Transcription Factor, Multidisciplinary Sciences, Science & Technology - Other Topics, Receptors, Serotonin, 5-HT3, Microtubule-Associated Proteins

Abstract

Although the search for quantitative trait loci for behaviour remains a considerable challenge, the complicated genetic architecture of quantitative traits is beginning to be understood. The current project utilised heterogeneous stock (HS) male mice (n = 580) to investigate the genetic basis for brain weights, activity, anxiety and cognitive phenotypes. We identified 126 single nucleotide polymorphisms (SNPs) in genes involved in regulation of neurotransmitter systems, nerve growth/death and gene expression, and subsequently investigated their associations with changes in behaviour and/or brain weights in our sample. We found significant associations between four SNP-phenotype pairs, after controlling for multiple testing. Specificity protein 2 (Sp2, rs3708840), tryptophan hydroxylase 1 (Tph1, rs262731280) and serotonin receptor 3A (Htr3a, rs50670893) were associated with activity/anxiety behaviours, and microtubule-associated protein 2 (Map2, rs13475902) was associated with cognitive performance. All these genes except for Tph1 were expressed in the brain above the array median, and remained significantly associated with relevant behaviours after controlling for the family structure. Additionally, we found evidence for a correlation between Htr3a expression and activity. We discuss our findings in the light of the advantages and limitations of currently available mouse genetic tools, suggesting further directions for association studies in rodents.

Published

2017

5. Morphology and taxonomy of the Dasyaceae and the Lophothalieae (Rhodomelaceae) of the Rhodophyta

Author

Parsons, MJ

Abstract

To date the knowledge of the family Dasyaceae has been obtained from species known only in the northern hemisphere, yet southern Australia is an important centre of distribution for species of this family. These morphological studies on the Dasyaceae concern four species of Dasya (Dasya clavigera (Womersley) comb. nov. has been transferred from Dasyopsis), five species of Heterosiphonia and two species of Thuretia. Additional comments are made on a further species of Dasya and one of Heterosiphonia. New descriptions of the genera are given. Several features reported in the literature as being characteristic of the Dasyaceae are found to be inconsistent and it is shown that the development of the fusion cell, and the sympodial growth of the thallus, are good family characters. Three genera of the tribe Lophothalieae (Rhodomelaceae) are studied because of their superficial similarity with species in the Dasyaceae. The type species of Lophothalia, Doxodasya and Haplodasya, and one other species of Doxodasya and Haplodasya (H. tomentosa sp. nov.) are studied in detail to provide an understanding of the tribe Lophothalieae. Haplodasya, once placed in the Dasyaceae, is removed to the Lophothalieae. Comparisons of the Lophothalieae with Brongniartella (as described in the literature) are made and the differences require the formation of a new tribe, the Brongniartelleae, to take Brongniartella and similar genera once placed close to Lophothalia. It would appear that the Lophothalieae and the Dasyaceae are examples of parallel evolution of thallus form and are not closely related. Two species of Dasya and two of Heterosiphonia were used in an attempt to culture these plants completely through their life cycle in the laboratory. Dasya clavigera has been successfully taken through its life cycle for two generations of sexual plants and one of tetrasporangial plants. No other species grew to reproductive maturity.

Published

1975

6. Polyhalogenated Monoterpenes of the New Zealand Marine Red Alga Plocamium cartilagineum

Author

Blunt, JW, Bowman, NJ, Munro, HG, Parsons, MJ, Wright, GJ, and Yeow, Kok Kon.

Abstract

A series of polyhalogenated monoterpenes have been isolated from the New Zealand marine red alga Plocamium cartilagineum (L.) Dixon. These findings are in contrast to the previously reported finding of a hydroxy bisnor monoterpene from a morphologically similar sample of P. cartilagineum collected from the same area.

Published

1985

7. Generation and application of endogenously floxed alleles for cell-specific knockout in zebrafish.

Author

Shin M, Yin HM, Shih YH, Nozaki T, Portman D, Toles B, Kolb A, Luk K, Isogai S, Ishida K, Hanasaka T, Parsons MJ, Wolfe SA, Burns CE, Burns CG, and Lawson ND

Subjects

Mice, Animals, Mice, Knockout, Alleles, Gene Knockout Techniques, Zebrafish genetics, Integrases genetics

Abstract

The zebrafish is amenable to a variety of genetic approaches. However, lack of conditional deletion alleles limits stage- or cell-specific gene knockout. Here, we applied an existing protocol to establish a floxed allele for gata2a but failed to do so due to off-target integration and incomplete knockin. To address these problems, we applied simultaneous co-targeting with Cas12a to insert loxP sites in cis, together with transgenic counterscreening and comprehensive molecular analysis, to identify off-target insertions and confirm targeted knockins. We subsequently used our approach to establish endogenously floxed alleles of foxc1a, rasa1a, and ruvbl1, each in a single generation. We demonstrate the utility of these alleles by verifying Cre-dependent deletion, which yielded expected phenotypes in each case. Finally, we used the floxed gata2a allele to demonstrate an endothelial autonomous requirement in lymphatic valve development. Together, our results provide a framework for routine generation and application of endogenously floxed alleles in zebrafish., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published

2023

8. Habitat type drives the spatial distribution of Australian fish chorus diversitya).

Author

Hawkins LA, Saunders BJ, Landero Figueroa MM, McCauley RD, Parnum IM, Parsons MJ, and Erbe C

Subjects

Animals, Australia, Biodiversity, Acoustics, Ecosystem, Fishes

Abstract

Fish vocalize in association with life functions with many species calling en masse to produce choruses. Monitoring the distribution and behavior of fish choruses provides high-resolution data on fish distribution, habitat use, spawning behavior, and in some circumstances, local abundance. The purpose of this study was to use long-term passive acoustic recordings to obtain a greater understanding of the patterns and drivers of Australian fish chorus diversity at a national scale. This study detected 133 fish choruses from year-long recordings taken at 29 Australian locations with the highest fish chorus diversity identified at a site in the country's northern, tropical waters. A linear model fitted with a generalized least squares regression identified geomorphic feature type, benthic substrate type, and northness (of slope) as explanatory variables of fish chorus diversity. Geomorphic feature type was identified as the significant driver of fish chorus diversity. These results align with broad-scale patterns reported previously in fish biodiversity, fish assemblages, and fish acoustic diversity. This study has highlighted that passive acoustic monitoring of fish chorus diversity has the potential to be used as an indicator of fish biodiversity and to highlight habitats of ecological importance., (© 2023 Author(s). All article content, except where otherwise noted, is licensed under a Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).)

Published

2023

9. An inducible model of chronic hyperglycemia.

Author

Tucker TR, Knitter CA, Khoury DM, Eshghi S, Tran S, Sharrock AV, Wiles TJ, Ackerley DF, Mumm JS, and Parsons MJ

Subjects

Animals, Zebrafish metabolism, Metronidazole pharmacology, Metronidazole therapeutic use, Nitroreductases metabolism, Animals, Genetically Modified, Hyperglycemia complications, Diabetes Mellitus

Abstract

Transgene driven expression of Escherichia coli nitroreductase (NTR1.0) renders animal cells susceptible to the antibiotic metronidazole (MTZ). Many NTR1.0/MTZ ablation tools have been reported in zebrafish, which have significantly impacted regeneration studies. However, NTR1.0-based tools are not appropriate for modeling chronic cell loss as prolonged application of the required MTZ dose (10 mM) is deleterious to zebrafish health. We established that this dose corresponds to the median lethal dose (LD50) of MTZ in larval and adult zebrafish and that it induced intestinal pathology. NTR2.0 is a more active nitroreductase engineered from Vibrio vulnificus NfsB that requires substantially less MTZ to induce cell ablation. Here, we report on the generation of two new NTR2.0-based zebrafish lines in which acute β-cell ablation can be achieved without MTZ-associated intestinal pathology. For the first time, we were able to sustain β-cell loss and maintain elevated glucose levels (chronic hyperglycemia) in larvae and adults. Adult fish showed significant weight loss, consistent with the induction of a diabetic state, indicating that this paradigm will allow the modeling of diabetes and associated pathologies., Competing Interests: Competing interests J.S.M. has been awarded patents for the creation (US patent no. 7,514,595) and use of zebrafish expressing NTR enzymes for gene (US patent no. 8,071,838) and drug discovery (US patent no. 8,431,768) applications. J.S.M. serves as a consultant at Luminomics, a biotechnology start-up that offers phenotypic drug-based screening services. The remaining authors declare no competing interests., (© 2023. Published by The Company of Biologists Ltd.)

Published

2023

10. Patterns of care and outcomes of early stage I-II Hodgkin lymphoma treated with or without radiation therapy.

Author

Weil CR, Parsons MJ, Hutten RJ, Lew FH, Johnson SB, Gaffney DK, and Tao R

Subjects

Humans, Combined Modality Therapy, Retrospective Studies, Neoplasm Staging, Antineoplastic Combined Chemotherapy Protocols adverse effects, Hodgkin Disease diagnosis, Hodgkin Disease drug therapy

Abstract

Omission of radiotherapy in the upfront management of early-stage classic Hodgkin lymphoma (cHL) has become more common with time. We report patterns of care and outcomes of stage I-II cHL treated with chemotherapy (CT) only versus CT and radiotherapy (combined modality therapy, CMT). From the National Cancer Database, we identified 28,327 early-stage cHL patients treated with CT ( n  = 15,798) or CMT ( n  = 12,529) from 2004 to 2018. CMT utilization declined over the period from 58% to 34%. With median follow-up of 6.2 years, the 5- and 10-year overall survival for CT versus CMT was 93.3% versus 96.9% ( p  < 0.001) and 88.7% versus 93.5% ( p  < 0.001), respectively. On multivariable analysis, uninsured (OR 0.75, p  < 0.001) and Black patients (OR 0.86, p  = 0.02) were less likely to receive CMT, and treatment with CT was predictive of death (OR 2.0, p  < 0.001). This report highlights real-world outcomes in early-stage cHL, with worse survival with CT and notable disparities in CMT utilization.

Published

2022

11. Correction: Caspase-2 regulates S-phase cell cycle events to protect from DNA damage accumulation independent of apoptosis.

Author

Boice AG, Lopez KE, Pandita RK, Parsons MJ, Charendoff CI, Charaka V, Carisey AF, Pandita TK, and Bouchier-Hayes L

Published

2022

12. Caspase-2 regulates S-phase cell cycle events to protect from DNA damage accumulation independent of apoptosis.

Author

Boice AG, Lopez KE, Pandita RK, Parsons MJ, Charendoff CI, Charaka V, Carisey AF, Pandita TK, and Bouchier-Hayes L

Subjects

Animals, Apoptosis, Humans, Mice, Caspase 2 genetics, Cell Cycle genetics, DNA Damage genetics

Abstract

In addition to its classical role in apoptosis, accumulating evidence suggests that caspase-2 has non-apoptotic functions, including regulation of cell division. Loss of caspase-2 is known to increase proliferation rates but how caspase-2 is regulating this process is currently unclear. We show that caspase-2 is activated in dividing cells in G1-phase of the cell cycle. In the absence of caspase-2, cells exhibit numerous S-phase defects including delayed exit from S-phase, defects in repair of chromosomal aberrations during S-phase, and increased DNA damage following S-phase arrest. In addition, caspase-2-deficient cells have a higher frequency of stalled replication forks, decreased DNA fiber length, and impeded progression of DNA replication tracts. This indicates that caspase-2 protects from replication stress and promotes replication fork protection to maintain genomic stability. These functions are independent of the pro-apoptotic function of caspase-2 because blocking caspase-2-induced cell death had no effect on cell division, DNA damage-induced cell cycle arrest, or DNA damage. Thus, our data supports a model where caspase-2 regulates cell cycle and DNA repair events to protect from the accumulation of DNA damage independently of its pro-apoptotic function., (© 2021. The Author(s), under exclusive licence to Springer Nature Limited.)

Published

2022

13. WNT as a Driver and Dependency in Cancer.

Author

Parsons MJ, Tammela T, and Dow LE

Subjects

Carcinogenesis, Humans, Tumor Microenvironment, Neoplasms genetics, Wnt Signaling Pathway genetics

Abstract

The WNT signaling pathway is a critical regulator of development and adult tissue homeostasis and becomes dysregulated in many cancer types. Although hyperactivation of WNT signaling is common, the type and frequency of genetic WNT pathway alterations can vary dramatically between different cancers, highlighting possible cancer-specific mechanisms for WNT-driven disease. In this review, we discuss how WNT pathway disruption contributes to tumorigenesis in different organs and how WNT affects the tumor cell and immune microenvironment. Finally, we describe recent and ongoing efforts to target oncogenic WNT signaling as a therapeutic strategy. SIGNIFICANCE: WNT signaling is a fundamental regulator of tissue homeostasis and oncogenic driver in many cancer types. In this review, we highlight recent advances in our understanding of WNT signaling in cancer, particularly the complexities of WNT activation in distinct cancer types, its role in immune evasion, and the challenge of targeting the WNT pathway as a therapeutic strategy., (©2021 American Association for Cancer Research.)

Published

2021

14. SOX9 modulates cancer biomarker and cilia genes in pancreatic cancer.

Author

Edelman HE, McClymont SA, Tucker TR, Pineda S, Beer RL, McCallion AS, and Parsons MJ

Subjects

Animals, Biomarkers, Tumor genetics, Carcinoma, Pancreatic Ductal genetics, Carcinoma, Pancreatic Ductal metabolism, Cell Movement, Cell Proliferation, Cilia metabolism, Epithelial Cell Adhesion Molecule genetics, Humans, Pancreatic Neoplasms genetics, Pancreatic Neoplasms metabolism, SOX9 Transcription Factor genetics, Signal Transduction, Zebrafish, Biomarkers, Tumor metabolism, Carcinoma, Pancreatic Ductal pathology, Cilia genetics, Epithelial Cell Adhesion Molecule metabolism, Pancreatic Neoplasms pathology, SOX9 Transcription Factor metabolism

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is an aggressive form of cancer with high mortality. The cellular origins of PDAC are largely unknown; however, ductal cells, especially centroacinar cells (CACs), have several characteristics in common with PDAC, such as expression of SOX9 and components of the Notch-signaling pathway. Mutations in KRAS and alterations to Notch signaling are common in PDAC, and both these pathways regulate the transcription factor SOX9. To identify genes regulated by SOX9, we performed siRNA knockdown of SOX9 followed by RNA-seq in PANC-1s, a human PDAC cell line. We report 93 differentially expressed (DE) genes, with convergence on alterations to Notch-signaling pathways and ciliogenesis. These results point to SOX9 and Notch activity being in a positive feedback loop and SOX9 regulating cilia production in PDAC. We additionally performed ChIP-seq in PANC-1s to identify direct targets of SOX9 binding and integrated these results with our DE gene list. Nine of the top 10 downregulated genes have evidence of direct SOX9 binding at their promoter regions. One of these targets was the cancer stem cell marker EpCAM. Using whole-mount in situ hybridization to detect epcam transcript in zebrafish larvae, we demonstrated that epcam is a CAC marker and that Sox9 regulation of epcam expression is conserved in zebrafish. Additionally, we generated an epcam null mutant and observed pronounced defects in ciliogenesis during development. Our results provide a link between SOX9, EpCAM and ciliary repression that can be exploited in improving our understanding of the cellular origins and mechanisms of PDAC., (© The Author(s) 2021. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2021

15. Report on the 22nd International Mammalian Genome Conference.

Author

Quwailid MM, Parsons MJ, and Denny P

Subjects

Animals, Humans, Genome, Genomics methods, Mammals genetics

Published

2021

16. Attenuating the Epidermal Growth Factor Receptor-Extracellular Signal-Regulated Kinase-Sex-Determining Region Y-Box 9 Axis Promotes Liver Progenitor Cell-Mediated Liver Regeneration in Zebrafish.

Author

So J, Kim M, Lee SH, Ko S, Lee DA, Park H, Azuma M, Parsons MJ, Prober D, and Shin D

Subjects

Animals, Animals, Genetically Modified, Butadienes pharmacology, Cell Differentiation drug effects, Enzyme Inhibitors pharmacology, ErbB Receptors antagonists & inhibitors, Extracellular Signal-Regulated MAP Kinases antagonists & inhibitors, Hepatocytes cytology, Nitriles pharmacology, Quinazolines pharmacology, Stem Cells cytology, Tyrphostins pharmacology, ErbB Receptors metabolism, Extracellular Signal-Regulated MAP Kinases metabolism, Liver Regeneration drug effects, MAP Kinase Signaling System drug effects, SOX9 Transcription Factor metabolism, Stem Cells metabolism, Zebrafish metabolism

Abstract

Background and Aims: The liver is a highly regenerative organ, but its regenerative capacity is compromised in severe liver injury settings. In chronic liver diseases, the number of liver progenitor cells (LPCs) correlates proportionally to disease severity, implying that their inefficient differentiation into hepatocytes exacerbates the disease. Moreover, LPCs secrete proinflammatory cytokines; thus, their prolonged presence worsens inflammation and induces fibrosis. Promoting LPC-to-hepatocyte differentiation in patients with advanced liver disease, for whom liver transplantation is currently the only therapeutic option, may be a feasible clinical approach because such promotion generates more functional hepatocytes and concomitantly reduces inflammation and fibrosis., Approach and Results: Here, using zebrafish models of LPC-mediated liver regeneration, we present a proof of principle of such therapeutics by demonstrating a role for the epidermal growth factor receptor (EGFR) signaling pathway in differentiation of LPCs into hepatocytes. We found that suppression of EGFR signaling promoted LPC-to-hepatocyte differentiation through the mitogen-activated ERK kinase (MEK)-extracellular signal-regulated kinase (ERK)-sex-determining region Y-box 9 (SOX9) cascade. Pharmacological inhibition of EGFR or MEK/ERK promoted LPC-to-hepatocyte differentiation as well as genetic suppression of the EGFR-ERK-SOX9 axis. Moreover, Sox9b overexpression in LPCs blocked their differentiation into hepatocytes. In the zebrafish liver injury model, both hepatocytes and biliary epithelial cells contributed to LPCs. EGFR inhibition promoted the differentiation of LPCs regardless of their origin. Notably, short-term treatment with EGFR inhibitors resulted in better liver recovery over the long term., Conclusions: The EGFR-ERK-SOX9 axis suppresses LPC-to-hepatocyte differentiation during LPC-mediated liver regeneration. We suggest EGFR inhibitors as a proregenerative therapeutic drug for patients with advanced liver disease., (© 2020 by the American Association for the Study of Liver Diseases.)

Published

2021

17. An In Vivo Kras Allelic Series Reveals Distinct Phenotypes of Common Oncogenic Variants.

Author

Zafra MP, Parsons MJ, Kim J, Alonso-Curbelo D, Goswami S, Schatoff EM, Han T, Katti A, Fernandez MTC, Wilkinson JE, Piskounova E, and Dow LE

Subjects

Cell Line, Tumor, Humans, Phenotype, Alleles, Oncogenes genetics, Proto-Oncogene Proteins p21(ras) genetics

Abstract

KRAS is the most frequently mutated oncogene in cancer, yet there is little understanding of how specific KRAS amino acid changes affect tumor initiation, progression, or therapy response. Using high-fidelity CRISPR-based engineering, we created an allelic series of new LSL-Kras mutant mice, reflecting codon 12 and 13 mutations that are highly prevalent in lung (KRAS G12C ), pancreas (KRAS G12R ), and colon (KRAS G13D ) cancers. Induction of each allele in either the murine colon or pancreas revealed striking quantitative and qualitative differences between KRAS mutants in driving the early stages of transformation. Furthermore, using pancreatic organoid models, we show that KRAS G13D mutants are sensitive to EGFR inhibition, whereas KRAS G12C -mutant organoids are selectively responsive to covalent G12C inhibitors only when EGFR is suppressed. Together, these new mouse strains provide an ideal platform for investigating KRAS biology in vivo and for developing preclinical precision oncology models of KRAS-mutant pancreas, colon, and lung cancers. SIGNIFICANCE: KRAS is the most frequently mutated oncogene. Here, we describe new preclinical models that mimic tissue-selective KRAS mutations and show that each mutation has distinct cellular consequences in vivo and carries differential sensitivity to targeted therapeutic agents. See related commentary by Kostyrko and Sweet-Cordero, p. 1626 . This article is highlighted in the In This Issue feature, p. 1611 ., (©2020 American Association for Cancer Research.)

Published

2020

18. Objective assessment of stored blood quality by deep learning.

Author

Doan M, Sebastian JA, Caicedo JC, Siegert S, Roch A, Turner TR, Mykhailova O, Pinto RN, McQuin C, Goodman A, Parsons MJ, Wolkenhauer O, Hennig H, Singh S, Wilson A, Acker JP, Rees P, Kolios MC, and Carpenter AE

Subjects

Humans, Blood Banks, Deep Learning, Erythrocytes cytology

Abstract

Stored red blood cells (RBCs) are needed for life-saving blood transfusions, but they undergo continuous degradation. RBC storage lesions are often assessed by microscopic examination or biochemical and biophysical assays, which are complex, time-consuming, and destructive to fragile cells. Here we demonstrate the use of label-free imaging flow cytometry and deep learning to characterize RBC lesions. Using brightfield images, a trained neural network achieved 76.7% agreement with experts in classifying seven clinically relevant RBC morphologies associated with storage lesions, comparable to 82.5% agreement between different experts. Given that human observation and classification may not optimally discern RBC quality, we went further and eliminated subjective human annotation in the training step by training a weakly supervised neural network using only storage duration times. The feature space extracted by this network revealed a chronological progression of morphological changes that better predicted blood quality, as measured by physiological hemolytic assay readouts, than the conventional expert-assessed morphology classification system. With further training and clinical testing across multiple sites, protocols, and instruments, deep learning and label-free imaging flow cytometry might be used to routinely and objectively assess RBC storage lesions. This would automate a complex protocol, minimize laboratory sample handling and preparation, and reduce the impact of procedural errors and discrepancies between facilities and blood donors. The chronology-based machine-learning approach may also improve upon humans' assessment of morphological changes in other biomedically important progressions, such as differentiation and metastasis., Competing Interests: The authors declare no competing interest., (Copyright © 2020 the Author(s). Published by PNAS.)

Published

2020

19. Platelet activating factor receptor acts to limit colitis-induced liver inflammation.

Author

Liu G, Baird AW, Parsons MJ, Fan K, Skerrett-Byrne DA, Nair PM, Makanyengo S, Chen J, Neal R, Goggins BJ, Tay H, Mathe A, Soh WS, Minahan K, Hansbro PM, Nixon B, McCaughan GW, Holtmann G, Colgan SP, and Keely S

Subjects

Animals, Caspase 1 metabolism, Cells, Cultured, Colitis chemically induced, Colon metabolism, Colon pathology, Dextran Sulfate pharmacology, Hepatocytes drug effects, Hepatocytes metabolism, Hepatocytes pathology, Humans, Inflammasomes metabolism, Inflammation chemically induced, Inflammatory Bowel Diseases metabolism, Inflammatory Bowel Diseases pathology, Interleukin-1beta metabolism, Kupffer Cells metabolism, Kupffer Cells pathology, Liver drug effects, Liver pathology, Male, Mice, Mice, Inbred C57BL, NLR Family, Pyrin Domain-Containing 3 Protein metabolism, Toll-Like Receptor 4 metabolism, Colitis metabolism, Colitis pathology, Inflammation metabolism, Inflammation pathology, Liver metabolism, Platelet Membrane Glycoproteins metabolism, Receptors, G-Protein-Coupled metabolism

Abstract

Liver inflammation is a common extraintestinal manifestation in inflammatory bowel disease (IBD), yet, the mechanisms driving gut-liver axis inflammation remain poorly understood. IBD leads to a breakdown in the integrity of the intestinal barrier causing an increase in portal and systemic gut-derived antigens, which challenge the liver. Here, we examined the role of platelet activating factor receptor (PAFR) in colitis-associated liver damage using dextran sulfate sodium (DSS) and anti-CD40-induced colitis models. Both DSS and anti-CD40 models exhibited liver inflammation associated with colitis. Colitis reduced global PAFR protein expression in mouse livers causing an exclusive re-localization of PAFR to the portal triad. The global decrease in liver PAFR was associated with increased sirtuin 1 while relocalized PAFR expression was limited to Kupffer cells (KCs) and co-localized with toll-like receptor 4. DSS activated the NLRP3-inflammasome and increased interleukin (IL)-1β in the liver. Antagonism of PAFR amplified the inflammasome response by increasing NLRP3, caspase-1, and IL-1β protein levels in the liver. LPS also increased NLRP3 response in human hepatocytes, however, overexpression of PAFR restored the levels of NLPR3 and caspase-1 proteins. Interestingly, KCs depletion also increased IL-1β protein in mouse liver after DSS challenge. These data suggest a protective role for PAFR-expressing KCs during colitis and that regulation of PAFR is important for gut-liver axis homeostasis., (© 2020 Federation of American Societies for Experimental Biology.)

Published

2020

20. Methamphetamine increases dopamine release in the nucleus accumbens through calcium-dependent processes.

Author

Yorgason JT, Hedges DM, Obray JD, Jang EY, Bills KB, Woodbury M, Williams B, Parsons MJ, Andres MA, and Steffensen SC

Subjects

Animals, Dopamine Plasma Membrane Transport Proteins metabolism, Humans, Male, Mice, Mice, Inbred C57BL, Nucleus Accumbens drug effects, Rats, Rats, Sprague-Dawley, Stem Cells drug effects, Stem Cells metabolism, Calcium metabolism, Dopamine metabolism, Dopamine Uptake Inhibitors pharmacology, Methamphetamine pharmacology, Nucleus Accumbens metabolism

Abstract

Rationale: Methamphetamine (METH) enhances exocytotic dopamine (DA) signals and induces DA transporter (DAT)-mediated efflux in brain striatal regions such as the nucleus accumbens (NAc). Blocking sigma receptors prevents METH-induced DA increases. Sigma receptor activation induces Ca 2+ release from intracellular stores, which may be responsible for METH-induced DA increases., Objectives: The role of intracellular and extracellular Ca 2+ in METH-induced DA increases and associated behavior was tested., Methods: METH-induced Ca 2+ release was measured in hNPC-derived DA cells using ratiometric Ca 2+ imaging. In mouse brain slices, fast-scan cyclic voltammetry was used to measure METH effects on two measures of dopamine: electrically stimulated and DAT-mediated efflux. Intracellular and extracellular Ca 2+ was removed through pharmacological blockade of Ca 2+ permeable channels (Cd 2+ and IP3 sensitive channels), intracellular Ca 2+ chelation (BAPTA-AM), or non-inclusion (zero Ca 2+ ). Lastly, METH effects on dopamine-mediated locomotor behavior were tested in rats. Rats received intra-NAc injections of ACSF or 2-aminoethoxydiphenyl borate (2-APB; IP3 receptor blocker) and intraperitoneal METH (5 mg/kg) to test the role of intracellular Ca 2+ release in DA-mediated behaviors., Results: Reducing Ca 2+ extracellular levels and Ca 2+ release from intracellular stores prevented intracellular Ca 2+ release. Intracellular Ca 2+ chelation and blocking intracellular Ca 2+ release reduced METH effects on voltammetric measures of dopamine. Blocking intracellular Ca 2+ release via 2-APB resulted in increased METH-induced circling behavior., Conclusions: METH induces NAc DA release through intracellular Ca 2+ activity. Blocking intracellular Ca 2+ release prevents METH effects on DA signals and related behavior.

Published

2020

21. Dissociable effects of visual crowding on the perception of color and motion.

Author

Greenwood JA and Parsons MJ

Subjects

Attention physiology, Color, Female, Humans, Male, Photic Stimulation methods, Color Vision physiology, Crowding, Models, Neurological, Motion, Visual Perception physiology

Abstract

Our ability to recognize objects in peripheral vision is fundamentally limited by crowding, the deleterious effect of clutter that disrupts the recognition of features ranging from orientation and color to motion and depth. Previous research is equivocal on whether this reflects a singular process that disrupts all features simultaneously or multiple processes that affect each independently. We examined crowding for motion and color, two features that allow a strong test of feature independence. "Cowhide" stimuli were presented 15° in peripheral vision, either in isolation or surrounded by flankers to give crowding. Observers reported either the target direction (clockwise/counterclockwise from upward) or its hue (blue/purple). We first established that both features show systematic crowded errors (biased predominantly toward the flanker identities) and selectivity for target-flanker similarity (with reduced crowding for dissimilar target/flanker elements). The multiplicity of crowding was then tested with observers identifying both features. Here, a singular object-selective mechanism predicts that when crowding is weak for one feature and strong for the other that crowding should be all-or-none for both. In contrast, when crowding was weak for color and strong for motion, errors were reduced for color but remained for motion, and vice versa with weak motion and strong color crowding. This double dissociation reveals that crowding disrupts certain combinations of visual features in a feature-specific manner, ruling out a singular object-selective mechanism. Thus, the ability to recognize one aspect of a cluttered scene, like color, offers no guarantees for the correct recognition of other aspects, like motion., Competing Interests: The authors declare no competing interest.

Published

2020

22. Label-Free Analysis of Red Blood Cell Storage Lesions Using Imaging Flow Cytometry.

Author

Pinto RN, Sebastian JA, Parsons MJ, Chang TC, Turner TR, Acker JP, and Kolios MC

Subjects

Erythrocyte Deformability, Humans, Image Cytometry methods, Image Processing, Computer-Assisted, Microscopy, Blood Preservation, Erythrocytes cytology, Flow Cytometry methods

Abstract

Deleterious changes, collectively termed as storage lesions, alter the characteristics of red blood cell (RBC) morphology during in vitro storage. Due to gradual loss of cellular membrane, RBCs lose their original biconcave disk shape and begin a process of spherical deformation that is characterized by well-defined morphological criteria. At the spheroechinocyte stage, the structure of RBC is irreversibly damaged and lacks the elasticity necessary to efficiently deliver oxygen. Quantifying the prevalence of spheroechinocytes could provide an important morphological measure of the quality of stored blood products. Unlike the conventional RBC morphology characterization assay involving light microscopy, we introduce a label-free assay using imaging flow cytometry (IFC). The technique captures 100,000 images of a sample and calculates a relative measure of spheroechinocyte population in a fraction of the time required by the conventional method. A comparative method study, measuring a morphological index for 11 RCC units through storage, found that the two techniques measured similar trends with IFC reporting the metric at an average of 3.9% higher. We monitored 18 RCC units between Weeks 1 and 6 of storage and found that the spheroechinocyte population increased by an average of 26.2%. The large (3.5-64.1%) variation between the units' spheroechinocyte population percentage at Week 1 suggests a possible dependence of blood product quality on donor characteristics. Given our method's ability to rapidly monitor large samples and refine morphological characterization beyond conventional methods, we believe our technique offers good potential for studying the underlying relationships between RBC morphology and blood storage lesions. © 2019 International Society for Advancement of Cytometry., (© 2019 International Society for Advancement of Cytometry.)

Published

2019

23. Lymphocytic response to tumour and deficient DNA mismatch repair identify subtypes of stage II/III colorectal cancer associated with patient outcomes.

Author

Williams DS, Mouradov D, Jorissen RN, Newman MR, Amini E, Nickless DK, Teague JA, Fang CG, Palmieri M, Parsons MJ, Sakthianandeswaren A, Li S, Ward RL, Hawkins NJ, Faragher I, Jones IT, Gibbs P, and Sieber OM

Subjects

Adenocarcinoma genetics, Adenocarcinoma pathology, Aged, Aged, 80 and over, Colorectal Neoplasms genetics, Colorectal Neoplasms pathology, Female, Genomics, Humans, Kaplan-Meier Estimate, Lymphocyte Count, Male, Middle Aged, Neoplasm Staging, Prognosis, Prospective Studies, Reproducibility of Results, Transcriptome, Adenocarcinoma immunology, Colorectal Neoplasms immunology, DNA Mismatch Repair, Lymphocytes, Tumor-Infiltrating immunology

Abstract

Objective: Tumour-infiltrating lymphocyte (TIL) response and deficient DNA mismatch repair (dMMR) are determinants of prognosis in colorectal cancer. Although highly correlated, evidence suggests that these are independent predictors of outcome. However, the prognostic significance of combined TIL/MMR classification and how this compares to the major genomic and transcriptomic subtypes remain unclear., Design: A prospective cohort of 1265 patients with stage II/III cancer was examined for TIL/MMR status and BRAF / KRAS mutations. Consensus molecular subtype (CMS) status was determined for 142 cases. Associations with 5-year disease-free survival (DFS) were evaluated and validated in an independent cohort of 602 patients., Results: Tumours were categorised into four subtypes based on TIL and MMR status: TIL-low/proficient-MMR (pMMR) (61.3% of cases), TIL-high/pMMR (14.8%), TIL-low/dMMR (8.6%) and TIL-high/dMMR (15.2%). Compared with TIL-high/dMMR tumours with the most favourable prognosis, both TIL-low/dMMR (HR=3.53; 95% CI=1.88 to 6.64; P multivariate <0.001) and TIL-low/pMMR tumours (HR=2.67; 95% CI=1.47 to 4.84; P multivariate =0.001) showed poor DFS. Outcomes of patients with TIL-low/dMMR and TIL-low/pMMR tumours were similar. TIL-high/pMMR tumours showed intermediate survival rates. These findings were validated in an independent cohort. TIL/MMR status was a more significant predictor of prognosis than National Comprehensive Cancer Network high-risk features and was a superior predictor of prognosis compared with genomic (dMMR, pMMR/ BRAF wt / KRAS wt , pMMR/ BRAF mut / KRAS wt , pMMR/ BRAF wt / KRAS mut ) and transcriptomic (CMS 1-4) subtypes., Conclusion: TIL/MMR classification identified subtypes of stage II/III colorectal cancer associated with different outcomes. Although dMMR status is generally considered a marker of good prognosis, we found this to be dependent on the presence of TILs. Prognostication based on TIL/MMR subtypes was superior compared with histopathological, genomic and transcriptomic subtypes., Competing Interests: Competing interests: None declared., (© Article author(s) (or their employer(s) unless otherwise stated in the text of the article) 2019. All rights reserved. No commercial use is permitted unless otherwise expressly granted.)

Published

2019

24. FOXO3 Loss Drives Inflammation-Associated CRC: The Consequences of Being (Knock)Out-FOX'd.

Author

Parsons MJ and Keely S

Subjects

Forkhead Box Protein O3 genetics, Gene Expression Profiling, Humans, Colonic Neoplasms, Inflammation immunology

Published

2019

25. Identification of the influence of distal inputs on mercury loading across the mid Great Lakes region using chemical sediment chronologies.

Author

Ruhala SS, Long DT, Vannier RG, Parsons MJ, and Giesy JP

Subjects

Great Lakes Region, Humans, Mercury analysis, Water Pollutants, Chemical analysis, Environmental Monitoring methods, Geologic Sediments chemistry, Mercury chemistry, Water Pollutants, Chemical chemistry

Abstract

Sediment cores from 47 inland lakes in Michigan, USA were used to assess spatial and temporal trends in loadings of mercury (Hg). Focusing/background corrected accumulation rates and inventories and peak concentrations were used to examine: 1) responses of loadings to post-1990 reductions in emissions, 2) if spatial trends are consistent with modeled Hg deposition and 3) evidence for local and distal inputs. Results showed that decreases in concentrations and anthropogenic accumulation rates of Hg were consistent with recent reductions in emissions of Hg. Most lakes exhibiting a decreasing trend were located within an area with the most emission sources. Not all lakes showed the decreasing trend with some showing increases or no change. These lakes tended to be in the northern portion of the state. In all lakes, current concentrations of Hg remain greater than long-term, historical, background concentrations. Sub-regional mean inventories and mean decadal accumulation rates exhibited a south to north gradient, consistent with previously modeled spatial trends. However, individual lake inventories and rates of accumulation compared at shorter times scales varied among lakes. Evidence for event deposition (e.g., volcanic eruptions, manufacturing) was also variable among lakes. These results suggest influence of more distal inputs of Hg, perhaps driven by well-mixed, global sources. Cause(s) of variability on shorter time scales (e.g., events) needs further work. Finally, the results reveal that understanding risks to humans and ecosystems due to exposure to Hg and developing effective abatement policy is challenging., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

26. MACROD2 deletions cause impaired PARP1 activity and chromosome instability in colorectal cancer.

Author

Sakthianandeswaren A, Parsons MJ, Mouradov D, and Sieber OM

Published

2018

27. Mutation burden and other molecular markers of prognosis in colorectal cancer treated with curative intent: results from the QUASAR 2 clinical trial and an Australian community-based series.

Author

Domingo E, Camps C, Kaisaki PJ, Parsons MJ, Mouradov D, Pentony MM, Makino S, Palmieri M, Ward RL, Hawkins NJ, Gibbs P, Askautrud H, Oukrif D, Wang H, Wood J, Tomlinson E, Bark Y, Kaur K, Johnstone EC, Palles C, Church DN, Novelli M, Danielsen HE, Sherlock J, Kerr D, Kerr R, Sieber O, Taylor JC, and Tomlinson I

Subjects

Australia, Colorectal Neoplasms pathology, Colorectal Neoplasms therapy, Gene Drive Technology, Humans, Neoplasm Staging, Prognosis, Sequence Analysis, DNA, Biomarkers, Tumor, Colorectal Neoplasms genetics, Mutation

Abstract

Background: Molecular indicators of colorectal cancer prognosis have been assessed in several studies, but most analyses have been restricted to a handful of markers. We aimed to identify prognostic biomarkers for colorectal cancer by sequencing panels of multiple driver genes., Methods: In stage II or III colorectal cancers from the QUASAR 2 open-label randomised phase 3 clinical trial and an Australian community-based series, we used targeted next-generation sequencing of 82 and 113 genes, respectively, including the main colorectal cancer drivers. We investigated molecular pathways of tumorigenesis, and analysed individual driver gene mutations, combinations of mutations, or global measures such as microsatellite instability (MSI) and mutation burden (total number of non-synonymous mutations and coding indels) for associations with relapse-free survival in univariable and multivariable models, principally Cox proportional hazards models., Findings: In QUASAR 2 (511 tumours), TP53, KRAS, BRAF, and GNAS mutations were independently associated with shorter relapse-free survival (p<0·035 in all cases), and total somatic mutation burden with longer survival (hazard ratio [HR] 0·81 [95% CI 0·68-0·96]; p=0·014). MSI was not independently associated with survival (HR 1·12 [95% CI 0·57-2·19]; p=0·75). We successfully validated these associations in the Australian sample set (296 tumours). In a combined analysis of both the QUASAR 2 and the Australian sample sets, mutation burden was also associated with longer survival (HR 0·84 [95% CI 0·74-0·94]; p=0·004) after exclusion of MSI-positive and POLE mutant tumours. In an extended analysis of 1732 QUASAR 2 and Australian colorectal cancers for which KRAS, BRAF, and MSI status were available, KRAS and BRAF mutations were specifically associated with poor prognosis in MSI-negative cancers. MSI-positive cancers with KRAS or BRAF mutations had better prognosis than MSI-negative cancers that were wild-type for KRAS or BRAF. Mutations in the genes NF1 and NRAS from the MAPK pathway co-occurred, and mutations in the DNA damage-response genes TP53 and ATM were mutually exclusive. We compared a prognostic model based on the gold standard of clinicopathological variables and MSI with our new model incorporating clinicopathological variables, mutation burden, and driver mutations in KRAS, BRAF, and TP53. In both QUASAR 2 and the Australian cohort, our new model was significantly better (p=0·00004 and p=0·0057, respectively, based on a likelihood ratio test)., Interpretation: Multigene panels identified two previously unreported prognostic associations in colorectal cancer involving TP53 mutation and total mutation burden, and confirmed associations with KRAS and BRAF. Even a modest-sized gene panel can provide important information for use in clinical practice and outperform MSI-based prognostic models., Funding: UK Technology Strategy Board, National Institute for Health Research Oxford Biomedical Research Centre, Cancer Australia Project, Cancer Council Victoria, Ludwig Institute for Cancer Research, Victorian Government., (Copyright © 2018 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license. Published by Elsevier Ltd.. All rights reserved.)

Published

2018

28. MACROD2 Haploinsufficiency Impairs Catalytic Activity of PARP1 and Promotes Chromosome Instability and Growth of Intestinal Tumors.

Author

Sakthianandeswaren A, Parsons MJ, Mouradov D, MacKinnon RN, Catimel B, Liu S, Palmieri M, Love C, Jorissen RN, Li S, Whitehead L, Putoczki TL, Preaudet A, Tsui C, Nowell CJ, Ward RL, Hawkins NJ, Desai J, Gibbs P, Ernst M, Street I, Buchert M, and Sieber OM

Subjects

Animals, Cell Line, Tumor, Cell Proliferation, Colorectal Neoplasms genetics, Colorectal Neoplasms metabolism, Colorectal Neoplasms pathology, DNA Damage, DNA Repair Enzymes chemistry, Down-Regulation, Gene Expression Regulation, Neoplastic, HCT116 Cells, Humans, Hydrolases chemistry, Intestinal Neoplasms genetics, Intestinal Neoplasms metabolism, Mice, Neoplasm Staging, Neoplasm Transplantation, DNA Repair Enzymes genetics, Genomic Instability, Haploinsufficiency, Hydrolases genetics, Intestinal Neoplasms pathology, Poly (ADP-Ribose) Polymerase-1 metabolism

Abstract

ADP-ribosylation is an important posttranslational protein modification that regulates diverse biological processes, controlled by dedicated transferases and hydrolases. Here, we show that frequent deletions (∼30%) of the MACROD2 mono-ADP-ribosylhydrolase locus in human colorectal cancer cause impaired PARP1 transferase activity in a gene dosage-dependent manner. MACROD2 haploinsufficiency alters DNA repair and sensitivity to DNA damage and results in chromosome instability. Heterozygous and homozygous depletion of Macrod2 enhances intestinal tumorigenesis in Apc Min/+ mice and the growth of human colorectal cancer xenografts. MACROD2 deletion in sporadic colorectal cancer is associated with the extent of chromosome instability, independent of clinical parameters and other known genetic drivers. We conclude that MACROD2 acts as a haploinsufficient tumor suppressor, with loss of function promoting chromosome instability, thereby driving cancer evolution. Significance: Chromosome instability (CIN) is a hallmark of cancer. We identify MACROD2 deletion as a cause of CIN in human colorectal cancer. MACROD2 loss causes repression of PARP1 activity, impairing DNA repair. MACROD2 haploinsufficiency promotes CIN and intestinal tumor growth. Our results reveal MACROD2 as a major caretaker tumor suppressor gene. Cancer Discov; 8(8); 988-1005. ©2018 AACR. See related commentary by Jin and Burkard, p. 921 This article is highlighted in the In This Issue feature, p. 899 ., (©2018 American Association for Cancer Research.)

Published

2018

29. Endoderm Jagged induces liver and pancreas duct lineage in zebrafish.

Author

Zhang D, Gates KP, Barske L, Wang G, Lancman JJ, Zeng XI, Groff M, Wang K, Parsons MJ, Crump JG, and Dong PDS

Subjects

Alagille Syndrome genetics, Animals, Cell Lineage, Endoderm cytology, Zebrafish, Bile Ducts, Intrahepatic embryology, Calcium-Binding Proteins genetics, Endoderm metabolism, Gene Expression Regulation, Developmental, Jagged-2 Protein genetics, Pancreatic Ducts embryology, Zebrafish Proteins genetics

Abstract

Liver duct paucity is characteristic of children born with Alagille Syndrome (ALGS), a disease associated with JAGGED1 mutations. Here, we report that zebrafish embryos with compound homozygous mutations in two Notch ligand genes, jagged1b (jag1b) and jagged2b (jag2b) exhibit a complete loss of canonical Notch activity and duct cells within the liver and exocrine pancreas, whereas hepatocyte and acinar pancreas development is not affected. Further, animal chimera studies demonstrate that wild-type endoderm cells within the liver and pancreas can rescue Notch activity and duct lineage specification in adjacent cells lacking jag1b and jag2b expression. We conclude that these two Notch ligands are directly and solely responsible for all duct lineage specification in these organs in zebrafish. Our study uncovers genes required for lineage specification of the intrahepatopancreatic duct cells, challenges the role of duct cells as progenitors, and suggests a genetic mechanism for ALGS ductal paucity.The hepatopancreatic duct cells connect liver hepatocytes and pancreatic acinar cells to the intestine, but the mechanism for their lineage specification is unclear. Here, the authors reveal that Notch ligands Jagged1b and Jagged2b induce duct cell lineage in the liver and pancreas of the zebrafish.

Published

2017

30. Inducible Knockout of Mouse Zfhx3 Emphasizes Its Key Role in Setting the Pace and Amplitude of the Adult Circadian Clock.

Author

Wilcox AG, Vizor L, Parsons MJ, Banks G, and Nolan PM

Subjects

Age Factors, Animals, Gene Expression Regulation, Mice, Mice, Knockout, Mutation, Period Circadian Proteins genetics, Period Circadian Proteins metabolism, Photoperiod, Suprachiasmatic Nucleus physiology, Tamoxifen pharmacology, Circadian Clocks drug effects, Circadian Clocks genetics, Circadian Rhythm genetics, Homeodomain Proteins genetics, Homeodomain Proteins physiology

Abstract

The transcription factor zinc finger homeobox 3 (ZFHX3) plays a key role in coupling intracellular transcriptional-translational oscillations with intercellular synchrony in mouse suprachiasmatic nucleus (SCN). However, like many key players in central nervous system function, ZFHX3 serves an important role in neurulation and neuronal terminal differentiation while retaining discrete additional functions in the adult SCN. Recently, using a dominant missense mutation in mouse Zfhx3, we established that this gene can modify circadian period and sleep in adult animals. Nevertheless, we were still concerned that the neurodevelopmental consequences of ZFHX3 dysfunction in this mutant may interfere with, or confound, its critical adult-specific roles in SCN circadian function. To circumvent the developmental consequences of Zfhx3 deletion, we crossed a conditional null Zfhx3 mutant to an inducible, ubiquitously expressed Cre line (B6.Cg-Tg(UBC-cre/ERT2)1Ejb/J). This enabled us to assess circadian behavior in the same adult animals both before and after Cre-mediated excision of the critical Zfhx3 exons using tamoxifen treatment. Remarkably, we found a strong and significant alteration in circadian behavior in tamoxifen-treated homozygous animals with no phenotypic changes in heterozygous or control animals. Cre-mediated excision of Zfhx3 critical exons in adult animals resulted in shortening of the period of wheel-running in constant darkness by more than 1 h in the majority of homozygotes while, in 30% of animals, excision resulted in complete behavioral arrhythmicity. In addition, we found that homozygous animals reentrain almost immediately to 6-h phase advances in the light-dark cycle. No additional overt phenotypic changes were evident in treated homozygous animals. These findings confirm a sustained and significant role for ZFHX3 in maintaining rhythmicity in the adult mammalian circadian system.

Published

2017

31. NPM1 directs PIDDosome-dependent caspase-2 activation in the nucleolus.

Author

Ando K, Parsons MJ, Shah RB, Charendoff CI, Paris SL, Liu PH, Fassio SR, Rohrman BA, Thompson R, Oberst A, Sidi S, and Bouchier-Hayes L

Subjects

Animals, CRADD Signaling Adaptor Protein metabolism, Caspase 2 genetics, Cysteine Endopeptidases genetics, Death Domain Receptor Signaling Adaptor Proteins genetics, Enzyme Activation, Genotype, HEK293 Cells, HeLa Cells, Humans, Mice, Knockout, Microscopy, Confocal, Microscopy, Fluorescence, Microscopy, Video, Multiprotein Complexes, Nuclear Proteins genetics, Nucleophosmin, Phenotype, Protein Binding, RNA Interference, Signal Transduction, Transfection, Zebrafish genetics, Zebrafish metabolism, Zebrafish Proteins genetics, Zebrafish Proteins metabolism, Apoptosis, Caspase 2 metabolism, Cell Nucleolus enzymology, Cysteine Endopeptidases metabolism, DNA Damage, Death Domain Receptor Signaling Adaptor Proteins metabolism, Nuclear Proteins metabolism

Abstract

The PIDDosome (PIDD-RAIDD-caspase-2 complex) is considered to be the primary signaling platform for caspase-2 activation in response to genotoxic stress. Yet studies of PIDD-deficient mice show that caspase-2 activation can proceed in the absence of PIDD. Here we show that DNA damage induces the assembly of at least two distinct activation platforms for caspase-2: a cytoplasmic platform that is RAIDD dependent but PIDD independent, and a nucleolar platform that requires both PIDD and RAIDD. Furthermore, the nucleolar phosphoprotein nucleophosmin (NPM1) acts as a scaffold for PIDD and is essential for PIDDosome assembly in the nucleolus after DNA damage. Inhibition of NPM1 impairs caspase-2 processing, apoptosis, and caspase-2-dependent inhibition of cell growth, demonstrating that the NPM1-dependent nucleolar PIDDosome is a key initiator of the caspase-2 activation cascade. Thus we have identified the nucleolus as a novel site for caspase-2 activation and function., (© 2017 Ando et al.)

Published

2017

32. Genetic polymorphisms and their association with brain and behavioural measures in heterogeneous stock mice.

Author

Janecka M, Marzi SJ, Parsons MJ, Liu L, Paya-Cano JL, Smith RG, Fernandes C, and Schalkwyk LC

Subjects

Animals, Gene Expression, Genetic Heterogeneity, Male, Mice, Microtubule-Associated Proteins genetics, Receptors, Serotonin, 5-HT3 genetics, Sp2 Transcription Factor genetics, Tryptophan Hydroxylase genetics, Behavior, Animal, Brain metabolism, Genetic Association Studies methods, Polymorphism, Single Nucleotide, Quantitative Trait Loci

Abstract

Although the search for quantitative trait loci for behaviour remains a considerable challenge, the complicated genetic architecture of quantitative traits is beginning to be understood. The current project utilised heterogeneous stock (HS) male mice (n = 580) to investigate the genetic basis for brain weights, activity, anxiety and cognitive phenotypes. We identified 126 single nucleotide polymorphisms (SNPs) in genes involved in regulation of neurotransmitter systems, nerve growth/death and gene expression, and subsequently investigated their associations with changes in behaviour and/or brain weights in our sample. We found significant associations between four SNP-phenotype pairs, after controlling for multiple testing. Specificity protein 2 (Sp2, rs3708840), tryptophan hydroxylase 1 (Tph1, rs262731280) and serotonin receptor 3A (Htr3a, rs50670893) were associated with activity/anxiety behaviours, and microtubule-associated protein 2 (Map2, rs13475902) was associated with cognitive performance. All these genes except for Tph1 were expressed in the brain above the array median, and remained significantly associated with relevant behaviours after controlling for the family structure. Additionally, we found evidence for a correlation between Htr3a expression and activity. We discuss our findings in the light of the advantages and limitations of currently available mouse genetic tools, suggesting further directions for association studies in rodents., Competing Interests: The authors declare no competing financial interests.

Published

2017

33. Sox9b is a mediator of retinoic acid signaling restricting endocrine progenitor differentiation.

Author

Huang W, Beer RL, Delaspre F, Wang G, Edelman HE, Park H, Azuma M, and Parsons MJ

Subjects

Alleles, Animals, Blood Glucose genetics, Cell Differentiation physiology, Cell Movement genetics, Cell Movement physiology, Larva growth & development, Receptors, Notch metabolism, Regeneration genetics, SOX9 Transcription Factor metabolism, Signal Transduction, Zebrafish Proteins metabolism, Cell Differentiation genetics, Insulin-Secreting Cells cytology, Pancreas embryology, SOX9 Transcription Factor genetics, Tretinoin metabolism, Zebrafish embryology, Zebrafish Proteins genetics

Abstract

Centroacinar cells (CACs) are ductal Notch-responsive progenitors that in the larval zebrafish pancreas differentiate to form new islets and ultimately contribute to the majority of the adult endocrine mass. Uncovering the mechanisms regulating CAC differentiation will facilitate understanding how insulin-producing β cells are formed. Previously we reported retinoic acid (RA) signaling and Notch signaling both regulate larval CAC differentiation, suggesting a shared downstream intermediate. Sox9b is a transcription factor important for islet formation whose expression is upregulated by Notch signaling in larval CACs. Here we report that sox9b expression in larval CACs is also regulated by RA signaling. Therefore, we hypothesized that Sox9b is an intermediate between both RA- and Notch-signaling pathways. In order to study the role of Sox9b in larval CACs, we generated two cre/lox based transgenic tools, which allowed us to express full-length or truncated Sox9b in larval CACs. In this way we were able to perform spatiotemporal-controlled Sox9b gain- and loss-of-function studies and observe the subsequent effect on progenitor differentiation. Our results are consistent with Sox9b regulating CAC differentiation by being a downstream intermediate of both RA- and Notch-signaling pathways. We also demonstrate that adult zebrafish with only one functional allele of sox9b undergo accelerated β-cell regeneration, an observation consistent with sox9b regulating CAC differentiation in adults., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

34. The Zfhx3-Mediated Axis Regulates Sleep and Interval Timing in Mice.

Author

Balzani E, Lassi G, Maggi S, Sethi S, Parsons MJ, Simon M, Nolan PM, and Tucci V

Subjects

Animals, Homeostasis physiology, Male, Mice, Mice, Inbred C57BL, Neuropeptides metabolism, Protein Interaction Maps physiology, Suprachiasmatic Nucleus metabolism, Suprachiasmatic Nucleus physiology, Circadian Clocks physiology, Circadian Rhythm physiology, Homeodomain Proteins metabolism, Sleep physiology

Abstract

An AT motif-dependent axis, modulated by the transcription factor Zfhx3, influences the circadian clock in mice. In particular, gain of function of Zfhx3 significantly shortens circadian rhythms and alters the transcriptional activity of an important class of neuropeptides that controls intercellular signaling in the suprachiasmatic nucleus (SCN) of the hypothalamus. The ZFHX3/AT axis revealed an important, largely cell-nonautonomous control of the circadian clock. Here, by studying the recently identified circadian mouse mutant Zfhx3(Sci/+), we identify significant effects on sleep homeostasis, a phenomenon that is outside the canonical circadian clock system and that is modulated by the activity of those neuropeptides at a circuit level. We show that the Zfhx3(Sci/+) mutation accelerates the circadian clock at both the hourly scale (i.e., advancing circadian rhythms) and the seconds-to-minutes scale (i.e., anticipating behavioral responses) in mice. The in vivo results are accompanied by a significant presence of sleep targets among protein-protein interactions of the Zfhx3(Sci/+)-dependent network., (Copyright © 2016 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2016

35. Gfap-positive radial glial cells are an essential progenitor population for later-born neurons and glia in the zebrafish spinal cord.

Author

Johnson K, Barragan J, Bashiruddin S, Smith CJ, Tyrrell C, Parsons MJ, Doris R, Kucenas S, Downes GB, Velez CM, Schneider C, Sakai C, Pathak N, Anderson K, Stein R, Devoto SH, Mumm JS, and Barresi MJ

Subjects

Age Factors, Animals, Animals, Genetically Modified, Apoptosis genetics, Cell Differentiation, Cell Proliferation genetics, Embryo, Nonmammalian, Embryonic Development genetics, Glial Fibrillary Acidic Protein genetics, Green Fluorescent Proteins genetics, Green Fluorescent Proteins metabolism, Locomotion genetics, Luminescent Proteins genetics, Luminescent Proteins metabolism, Mice, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Spinal Cord embryology, Time Factors, Zebrafish, Zebrafish Proteins genetics, Zebrafish Proteins metabolism, Red Fluorescent Protein, Glial Fibrillary Acidic Protein metabolism, Neurogenesis physiology, Neurons physiology, Spinal Cord cytology

Abstract

Radial glial cells are presumptive neural stem cells (NSCs) in the developing nervous system. The direct requirement of radial glia for the generation of a diverse array of neuronal and glial subtypes, however, has not been tested. We employed two novel transgenic zebrafish lines and endogenous markers of NSCs and radial glia to show for the first time that radial glia are essential for neurogenesis during development. By using the gfap promoter to drive expression of nuclear localized mCherry we discerned two distinct radial glial-derived cell types: a major nestin+/Sox2+ subtype with strong gfap promoter activity and a minor Sox2+ subtype lacking this activity. Fate mapping studies in this line indicate that gfap+ radial glia generate later-born CoSA interneurons, secondary motorneurons, and oligodendroglia. In another transgenic line using the gfap promoter-driven expression of the nitroreductase enzyme, we induced cell autonomous ablation of gfap+ radial glia and observed a reduction in their specific derived lineages, but not Blbp+ and Sox2+/gfap-negative NSCs, which were retained and expanded at later larval stages. Moreover, we provide evidence supporting classical roles of radial glial in axon patterning, blood-brain barrier formation, and locomotion. Our results suggest that gfap+ radial glia represent the major NSC during late neurogenesis for specific lineages, and possess diverse roles to sustain the structure and function of the spinal cord. These new tools will both corroborate the predicted roles of astroglia and reveal novel roles related to development, physiology, and regeneration in the vertebrate nervous system. GLIA 2016;64:1170-1189., (© 2016 Wiley Periodicals, Inc.)

Published

2016

36. Centroacinar cells: At the center of pancreas regeneration.

Author

Beer RL, Parsons MJ, and Rovira M

Subjects

Animals, Cell Differentiation, Cell Lineage, Cell Proliferation, Endocrine Cells cytology, Homeostasis, Humans, Insulin-Secreting Cells cytology, Insulin-Secreting Cells metabolism, Mammals, Mice, Pancreas cytology, Signal Transduction, Stem Cells cytology, Zebrafish, Pancreas embryology, Pancreas physiology, Pancreatic Ducts cytology, Regeneration

Abstract

The process of regeneration serves to heal injury by replacing missing cells. Understanding regeneration can help us replace cell populations lost during disease, such as the insulin-producing β cells lost in diabetic patients. Centroacinar cells (CACs) are a specialized ductal pancreatic cell type that act as progenitors to replace β cells in the zebrafish. However, whether CACs contribute to β-cell regeneration in adult mammals remains controversial. Here we review the current understanding of the role of CACs as endocrine progenitors during regeneration in zebrafish and mammals., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

37. BOK Is a Non-canonical BCL-2 Family Effector of Apoptosis Regulated by ER-Associated Degradation.

Author

Llambi F, Wang YM, Victor B, Yang M, Schneider DM, Gingras S, Parsons MJ, Zheng JH, Brown SA, Pelletier S, Moldoveanu T, Chen T, and Green DR

Subjects

Animals, Embryo, Mammalian cytology, Embryo, Mammalian metabolism, Endoplasmic Reticulum metabolism, Fibroblasts metabolism, Humans, Mice, Permeability, Proteasome Endopeptidase Complex metabolism, Proto-Oncogene Proteins c-bcl-2 genetics, Apoptosis, Endoplasmic Reticulum-Associated Degradation, Mitochondrial Membranes metabolism, Proto-Oncogene Proteins c-bcl-2 metabolism

Abstract

The mitochondrial pathway of apoptosis is initiated by mitochondrial outer membrane permeabilization (MOMP). The BCL-2 family effectors BAX and BAK are thought to be absolutely required for this process. Here, we report that BCL-2 ovarian killer (BOK) is a bona fide yet unconventional effector of MOMP that can trigger apoptosis in the absence of both BAX and BAK. However, unlike the canonical effectors, BOK appears to be constitutively active and unresponsive to antagonistic effects of the antiapoptotic BCL-2 proteins. Rather, BOK is controlled at the level of protein stability by components of the endoplasmic reticulum (ER)-associated degradation pathway. BOK is ubiquitylated by the AMFR/gp78 E3 ubiquitin ligase complex and targeted for proteasomal degradation in a VCP/p97-dependent manner, which allows survival of the cell. When proteasome function, VCP, or gp78 activity is compromised, BOK is stabilized to induce MOMP and apoptosis independently of other BCL-2 proteins., Competing Interests: The authors declare no conflict of interest., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

38. Early doors (Edo) mutant mouse reveals the importance of period 2 (PER2) PAS domain structure for circadian pacemaking.

Author

Militi S, Maywood ES, Sandate CR, Chesham JE, Barnard AR, Parsons MJ, Vibert JL, Joynson GM, Partch CL, Hastings MH, and Nolan PM

Subjects

Amino Acid Sequence, Animals, Blotting, Western, COS Cells, Casein Kinase 1 epsilon genetics, Casein Kinase 1 epsilon metabolism, Chlorocebus aethiops, Circadian Clocks physiology, Circadian Rhythm physiology, Female, HEK293 Cells, Humans, Male, Mice, Inbred BALB C, Mice, Inbred C3H, Mice, Inbred C57BL, Mice, Knockout, Models, Molecular, Molecular Sequence Data, Motor Activity genetics, Motor Activity physiology, Period Circadian Proteins chemistry, Period Circadian Proteins metabolism, Protein Multimerization, Protein Structure, Tertiary, Sequence Homology, Amino Acid, Suprachiasmatic Nucleus metabolism, Suprachiasmatic Nucleus physiopathology, Circadian Clocks genetics, Circadian Rhythm genetics, Mutation, Missense, Period Circadian Proteins genetics

Abstract

The suprachiasmatic nucleus (SCN) defines 24 h of time via a transcriptional/posttranslational feedback loop in which transactivation of Per (period) and Cry (cryptochrome) genes by BMAL1-CLOCK complexes is suppressed by PER-CRY complexes. The molecular/structural basis of how circadian protein complexes function is poorly understood. We describe a novel N-ethyl-N-nitrosourea (ENU)-induced mutation, early doors (Edo), in the PER-ARNT-SIM (PAS) domain dimerization region of period 2 (PER2) (I324N) that accelerates the circadian clock of Per2(Edo/Edo) mice by 1.5 h. Structural and biophysical analyses revealed that Edo alters the packing of the highly conserved interdomain linker of the PER2 PAS core such that, although PER2(Edo) complexes with clock proteins, its vulnerability to degradation mediated by casein kinase 1ε (CSNK1E) is increased. The functional relevance of this mutation is revealed by the ultrashort (<19 h) but robust circadian rhythms in Per2(Edo/Edo); Csnk1e(Tau/Tau) mice and the SCN. These periods are unprecedented in mice. Thus, Per2(Edo) reveals a direct causal link between the molecular structure of the PER2 PAS core and the pace of SCN circadian timekeeping.

Published

2016

39. Detection of Initiator Caspase Induced Proximity in Single Cells by Caspase Bimolecular Fluorescence Complementation.

Author

Parsons MJ, Fassio SR, and Bouchier-Hayes L

Subjects

HeLa Cells, Humans, Microscopy, Confocal methods, Plasmids, Time-Lapse Imaging methods, Apoptosis, Bacterial Proteins metabolism, Caspases metabolism, Luminescent Proteins metabolism, Microscopy, Fluorescence methods, Optical Imaging methods, Single-Cell Analysis methods

Abstract

The caspase family of proteases includes key regulators of apoptosis and inflammation. The caspases can be divided into two groups, the initiator caspases and the executioner caspases. Initiator caspases include caspase-2, caspase-8, and caspase-9 and are activated by proximity-induced dimerization upon recruitment to large molecular weight protein complexes called activation platforms. This protocol describes an imaging-based technique called caspase Bimolecular Fluorescence Complementation (BiFC) that measures induced proximity of initiator caspases. This method uses nonfluorescent fragments of the fluorescent protein Venus fused to initiator caspase monomers. When the caspase is recruited to its activation platform, the resulting induced proximity of the caspase monomers facilitates refolding of the Venus fragments into the full molecule, reconstituting its fluorescence. Thus, the assembly of initiator caspase activation platforms can be followed in single cells in real time. Induced proximity is the most apical step in the activation of initiator caspases, and therefore, caspase BiFC is a robust and specific method to measure initiator caspase activation.

Published

2016

40. Epigenome-Wide DNA Methylation Analysis of Monozygotic Twins Discordant for Diurnal Preference.

Author

Wong CC, Parsons MJ, Lester KJ, Burrage J, Eley TC, Mill J, Dempster EL, and Gregory AM

Subjects

Adolescent, Female, Genome-Wide Association Study, Humans, Male, Young Adult, Circadian Rhythm genetics, DNA Methylation, Epigenesis, Genetic, Twins, Monozygotic genetics

Abstract

Diurnal preference is an individual's preference for daily activities and sleep timing and is strongly correlated with the underlying circadian clock and the sleep-wake cycle validating its use as an indirect circadian measure in humans. Recent research has implicated DNA methylation as a mechanism involved in the regulation of the circadian clock system in humans and other mammals. In order to evaluate the extent of epigenetic differences associated with diurnal preference, we examined genome-wide patterns of DNA methylation in DNA from monozygotic (MZ) twin-pairs discordant for diurnal preference. MZ twins were selected from a longitudinal twin study designed to investigate the interplay of genetic and environmental factors in the development of emotional and behavioral difficulties. Fifteen pairs of MZ twins were identified in which one member scored considerably higher on the Horne-Ostberg Morningness-Eveningness Questionnaire (MEQ) than the other. Genome-wide DNA methylation patterns were assessed in twins' buccal cell DNA using the Illumina Infinium HumanMethylation450 BeadChips. Quality control and data pre-processing was undertaken using the wateRmelon package. Differentially methylated probes (DMPs) were identified using an analysis strategy taking into account both the significance and the magnitude of DNA methylation differences. Our data indicate that DNA methylation differences are detectable in MZ twins discordant for diurnal preference. Moreover, downstream gene ontology (GO) enrichment analysis on the top-ranked diurnal preference associated DMPs revealed significant enrichment of pathways that have been previously associated with circadian rhythm regulation, including cell adhesion processes and calcium ion binding.

Published

2015

41. Centroacinar Cells Are Progenitors That Contribute to Endocrine Pancreas Regeneration.

Author

Delaspre F, Beer RL, Rovira M, Huang W, Wang G, Gee S, Vitery Mdel C, Wheelan SJ, and Parsons MJ

Subjects

Acinar Cells cytology, Animals, Animals, Genetically Modified, Larva physiology, Pancreatectomy, RNA genetics, RNA metabolism, Receptors, Notch genetics, Receptors, Notch metabolism, Stem Cells cytology, Transcriptome, Zebrafish, Acinar Cells physiology, Gene Expression Regulation physiology, Islets of Langerhans physiology, Regeneration physiology, Stem Cells physiology

Abstract

Diabetes is associated with a paucity of insulin-producing β-cells. With the goal of finding therapeutic routes to treat diabetes, we aim to find molecular and cellular mechanisms involved in β-cell neogenesis and regeneration. To facilitate discovery of such mechanisms, we use a vertebrate organism where pancreatic cells readily regenerate. The larval zebrafish pancreas contains Notch-responsive progenitors that during development give rise to adult ductal, endocrine, and centroacinar cells (CACs). Adult CACs are also Notch responsive and are morphologically similar to their larval predecessors. To test our hypothesis that adult CACs are also progenitors, we took two complementary approaches: 1) We established the transcriptome for adult CACs. Using gene ontology, transgenic lines, and in situ hybridization, we found that the CAC transcriptome is enriched for progenitor markers. 2) Using lineage tracing, we demonstrated that CACs do form new endocrine cells after β-cell ablation or partial pancreatectomy. We concluded that CACs and their larval predecessors are the same cell type and represent an opportune model to study both β-cell neogenesis and β-cell regeneration. Furthermore, we show that in cftr loss-of-function mutants, there is a deficiency of larval CACs, providing a possible explanation for pancreatic complications associated with cystic fibrosis., (© 2015 by the American Diabetes Association. Readers may use this article as long as the work is properly cited, the use is educational and not for profit, and the work is not altered.)

Published

2015

42. A twin and molecular genetics study of sleep paralysis and associated factors.

Author

Denis D, French CC, Rowe R, Zavos HM, Nolan PM, Parsons MJ, and Gregory AM

Subjects

Adult, Anxiety genetics, Circadian Rhythm genetics, Female, Homeostasis genetics, Humans, Male, Models, Genetic, Period Circadian Proteins genetics, Polymorphism, Single Nucleotide genetics, Risk Factors, Siblings, Sleep genetics, Sleep Paralysis epidemiology, United Kingdom epidemiology, Young Adult, Sleep Paralysis genetics, Twins, Dizygotic genetics, Twins, Monozygotic genetics

Abstract

Sleep paralysis is a relatively common but under-researched phenomenon. In this paper we examine prevalence in a UK sample and associations with candidate risk factors. This is the first study to investigate the heritability of sleep paralysis in a twin sample and to explore genetic associations between sleep paralysis and a number of circadian expressed single nucleotide polymorphisms. Analyses are based on data from the Genesis1219 twin/sibling study, a community sample of twins/siblings from England and Wales. In total, data from 862 participants aged 22-32 years (34% male) were used in the study. This sample consisted of monozygotic and dizygotic twins and siblings. It was found that self-reports of general sleep quality, anxiety symptoms and exposure to threatening events were all associated independently with sleep paralysis. There was moderate genetic influence on sleep paralysis (53%). Polymorphisms in the PER2 gene were associated with sleep paralysis in additive and dominant models of inheritance-although significance was not reached once a Bonferroni correction was applied. It is concluded that factors associated with disrupted sleep cycles appear to be associated with sleep paralysis. In this sample of young adults, sleep paralysis was moderately heritable. Future work should examine specific polymorphisms associated with differences in circadian rhythms and sleep homeostasis further in association with sleep paralysis., (© 2015 The Authors. Journal of Sleep Research published by John Wiley & Sons Ltd on behalf of European Sleep Research Society.)

Published

2015

43. The Regulatory Factor ZFHX3 Modifies Circadian Function in SCN via an AT Motif-Driven Axis.

Author

Parsons MJ, Brancaccio M, Sethi S, Maywood ES, Satija R, Edwards JK, Jagannath A, Couch Y, Finelli MJ, Smyllie NJ, Esapa C, Butler R, Barnard AR, Chesham JE, Saito S, Joynson G, Wells S, Foster RG, Oliver PL, Simon MM, Mallon AM, Hastings MH, and Nolan PM

Subjects

Amino Acid Sequence, Animals, Down-Regulation, Homeodomain Proteins chemistry, Homeodomain Proteins genetics, In Vitro Techniques, Mice, Mice, Inbred C57BL, Molecular Sequence Data, Mutation, Nucleotide Motifs, Promoter Regions, Genetic, Sequence Alignment, Transcription, Genetic, Circadian Rhythm, Gene Expression Regulation, Homeodomain Proteins metabolism, Neuropeptides genetics, Suprachiasmatic Nucleus metabolism

Abstract

We identified a dominant missense mutation in the SCN transcription factor Zfhx3, termed short circuit (Zfhx3(Sci)), which accelerates circadian locomotor rhythms in mice. ZFHX3 regulates transcription via direct interaction with predicted AT motifs in target genes. The mutant protein has a decreased ability to activate consensus AT motifs in vitro. Using RNA sequencing, we found minimal effects on core clock genes in Zfhx3(Sci/+) SCN, whereas the expression of neuropeptides critical for SCN intercellular signaling was significantly disturbed. Moreover, mutant ZFHX3 had a decreased ability to activate AT motifs in the promoters of these neuropeptide genes. Lentiviral transduction of SCN slices showed that the ZFHX3-mediated activation of AT motifs is circadian, with decreased amplitude and robustness of these oscillations in Zfhx3(Sci/+) SCN slices. In conclusion, by cloning Zfhx3(Sci), we have uncovered a circadian transcriptional axis that determines the period and robustness of behavioral and SCN molecular rhythms., (Copyright © 2015 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2015

44. First quantitative high-throughput screen in zebrafish identifies novel pathways for increasing pancreatic β-cell mass.

Author

Wang G, Rajpurohit SK, Delaspre F, Walker SL, White DT, Ceasrine A, Kuruvilla R, Li RJ, Shim JS, Liu JO, Parsons MJ, and Mumm JS

Subjects

Animals, Automation, Laboratory methods, Insulin-Secreting Cells drug effects, Cell Differentiation drug effects, Cell Proliferation drug effects, Drug Discovery methods, High-Throughput Screening Assays methods, Insulin-Secreting Cells physiology, Zebrafish physiology

Abstract

Whole-organism chemical screening can circumvent bottlenecks that impede drug discovery. However, in vivo screens have not attained throughput capacities possible with in vitro assays. We therefore developed a method enabling in vivo high-throughput screening (HTS) in zebrafish, termed automated reporter quantification in vivo (ARQiv). In this study, ARQiv was combined with robotics to fully actualize whole-organism HTS (ARQiv-HTS). In a primary screen, this platform quantified cell-specific fluorescent reporters in &gt;500,000 transgenic zebrafish larvae to identify FDA-approved (Federal Drug Administration) drugs that increased the number of insulin-producing β cells in the pancreas. 24 drugs were confirmed as inducers of endocrine differentiation and/or stimulators of β-cell proliferation. Further, we discovered novel roles for NF-κB signaling in regulating endocrine differentiation and for serotonergic signaling in selectively stimulating β-cell proliferation. These studies demonstrate the power of ARQiv-HTS for drug discovery and provide unique insights into signaling pathways controlling β-cell mass, potential therapeutic targets for treating diabetes.

Published

2015

45. Single-cell imaging of inflammatory caspase dimerization reveals differential recruitment to inflammasomes.

Author

Sanders MG, Parsons MJ, Howard AG, Liu J, Fassio SR, Martinez JA, and Bouchier-Hayes L

Subjects

Adaptor Proteins, Signal Transducing metabolism, Apoptosis immunology, Apoptosis Regulatory Proteins metabolism, CARD Signaling Adaptor Proteins, Caspase 1 chemistry, Caspase 1 isolation & purification, Caspase 12 chemistry, Caspase 12 isolation & purification, Caspase 12 metabolism, Caspases chemistry, Caspases isolation & purification, Caspases, Initiator, Cholera Toxin pharmacology, Cytoskeletal Proteins metabolism, Humans, Immunity, Innate genetics, Inflammasomes chemistry, Inflammasomes metabolism, Inflammation pathology, Macrophages enzymology, Molecular Imaging methods, NLR Proteins, Protein Multimerization, Caspase 1 metabolism, Caspases metabolism, Inflammation enzymology, Single-Cell Analysis methods

Abstract

The human inflammatory caspases, including caspase-1, -4, -5 and -12, are considered as key regulators of innate immunity protecting from sepsis and numerous inflammatory diseases. Caspase-1 is activated by proximity-induced dimerization following recruitment to inflammasomes but the roles of the remaining inflammatory caspases in inflammasome assembly are unclear. Here, we use caspase bimolecular fluorescence complementation to visualize the assembly of inflammasomes and dimerization of inflammatory caspases in single cells. We observed caspase-1 dimerization induced by the coexpression of a range of inflammasome proteins and by lipospolysaccharide (LPS) treatment in primary macrophages. Caspase-4 and -5 were only dimerized by select inflammasome proteins, whereas caspase-12 dimerization was not detected by any investigated treatment. Strikingly, we determined that certain inflammasome proteins could induce heterodimerization of caspase-1 with caspase-4 or -5. Caspase-5 homodimerization and caspase-1/-5 heterodimerization was also detected in LPS-primed primary macrophages in response to cholera toxin subunit B. The subcellular localization and organization of the inflammasome complexes varied markedly depending on the upstream trigger and on which caspase or combination of caspases were recruited. Three-dimensional imaging of the ASC (apoptosis-associated speck-like protein containing a caspase recruitment domain)/caspase-1 complexes revealed a large spherical complex of ASC with caspase-1 dimerized on the outer surface. In contrast, NALP1 (NACHT leucine-rich repeat protein 1)/caspase-1 complexes formed large filamentous structures. These results argue that caspase-1, -4 or -5 can be recruited to inflammasomes under specific circumstances, often leading to distinctly organized and localized complexes that may impact the functions of these proteases.

Published

2015

46. Involvement of the HCK and FGR src-family kinases in FCRL4-mediated immune regulation.

Author

Liu Y, Bezverbnaya K, Zhao T, Parsons MJ, Shi M, Treanor B, and Ehrhardt GR

Subjects

Cell Line, Gene Expression, Genes, Reporter, Humans, Immunoglobulin A immunology, Immunoglobulin A metabolism, Interferon-gamma genetics, Interferon-gamma metabolism, Interleukin-10 genetics, Interleukin-10 metabolism, Mutation, NF-kappa B metabolism, Phosphorylation, Protein Binding immunology, Protein Interaction Domains and Motifs, Protein Processing, Post-Translational, Receptors, Antigen, B-Cell metabolism, Receptors, Fc chemistry, Receptors, Fc genetics, ets-Domain Protein Elk-1 metabolism, Immunomodulation genetics, Proto-Oncogene Proteins metabolism, Proto-Oncogene Proteins c-hck metabolism, Receptors, Fc metabolism, src-Family Kinases metabolism

Abstract

FCRL4 is an immunoregulatory receptor expressed by a subpopulation of memory B cells. These tissue-based cells express increased levels of the src-family kinases HCK and FGR. In this study, we investigate the roles of these src-family kinases in FCRL4-mediated immunoregulation of B cells in the context of previously unrecognized palmitoylation of the receptor. We observed enhanced phosphorylation of FCRL4 on tyrosine residues in the presence of the HCK p59 or FGR. This phosphorylation was markedly reduced in assays using a palmitoylation-defective mutant of FCRL4. In reporter gene studies, we observe that FCRL4 expression enhances CpG-mediated activation of NF-κB signaling. Surprisingly, using a reporter gene linked to activation of the MAPK substrate Elk-1 in response to Ag receptor ligation, we find that FCRL4 has inhibitory activity in cells coexpressing FGR but an activating function in cells coexpressing HCK p59. We provide evidence that in primary memory B cells, expression of FCRL4 leads to increased expression of IL-10 in the presence of FGR or HCK p59 in response to CpG, but increased levels of IFN-γ only in the context of coexpression of FGR. Our study supports the specific requirement of HCK p59 and FGR src-family kinases for FCRL4-mediated immunomodulatory activity and indicates that palmitoylation serves as an additional level of regulatory control of FCRL4., (Copyright © 2015 by The American Association of Immunologists, Inc.)

Published

2015

47. Fate mapping of ptf1a-expressing cells during pancreatic organogenesis and regeneration in zebrafish.

Author

Wang YJ, Park JT, Parsons MJ, and Leach SD

Subjects

Acinar Cells cytology, Animals, Animals, Genetically Modified, Cell Lineage, Chromosomes, Artificial, Bacterial, Gallbladder cytology, Gene Dosage, Genotype, Islets of Langerhans cytology, Islets of Langerhans embryology, Islets of Langerhans growth & development, Organ Specificity, Pancreas cytology, Pancreas growth & development, Pancreas physiology, Pancreas, Exocrine cytology, Pancreas, Exocrine embryology, Pancreas, Exocrine growth & development, Receptors, Notch physiology, Recombination, Genetic, Regeneration, Stem Cells cytology, Transcription Factors deficiency, Transcription Factors genetics, Zebrafish genetics, Zebrafish growth & development, Pancreas embryology, Transcription Factors physiology, Zebrafish embryology

Abstract

Background: Pancreas development in zebrafish shares many features with mammals, including the participation of epithelial progenitor cells expressing pancreas transcription factor 1a (ptf1a). However, to date it has remained unclear whether, as in mammals, ptf1a-expressing zebrafish pancreatic progenitors are able to contribute to multiple exocrine and endocrine lineages. To delineate the lineage potential of ptf1a-expressing cells, we generated ptf1a:creER(T2) transgenic fish and performed genetic-inducible lineage tracing in developmental, regenerating, and ptf1a-deficient zebrafish pancreas., Results: In addition to their contribution to the acinar cell lineage, ptf1a-expressing cells give rise to both pancreatic Notch-responsive-cells (PNCs) as well as small numbers of endocrine cells during pancreatic development. In fish with ptf1a haploinsufficiency, a higher proportion of ptf1a lineage-labeled cells are traced into the PNC and endocrine compartments. Further reduction of ptf1a gene dosage converts pancreatic progenitor cells to gall bladder and other non-pancreatic cell fates., Conclusions: Our results confirm the presence of multipotent ptf1a-expressing progenitor cells in developing zebrafish pancreas, with reduced ptf1a dosage promoting greater contributions towards non-acinar lineages. As in mammals, loss of ptf1a results in conversion of nascent pancreatic progenitor cells to non-pancreatic cell fates, underscoring the central role of ptf1a in foregut tissue specification., (© 2015 Wiley Periodicals, Inc.)

Published

2015

48. Differential in vivo tumorigenicity of diverse KRAS mutations in vertebrate pancreas: A comprehensive survey.

Author

Park JT, Johnson N, Liu S, Levesque M, Wang YJ, Ho H, Huso D, Maitra A, Parsons MJ, Prescott JD, and Leach SD

Subjects

Animals, Cell Transformation, Neoplastic pathology, Epithelium pathology, Gene Expression Regulation, Neoplastic genetics, Humans, Mitogen-Activated Protein Kinase Kinases genetics, Pancreatic Neoplasms genetics, Pancreatic Neoplasms pathology, Proto-Oncogene Mas, Proto-Oncogene Proteins p21(ras), Zebrafish genetics, Cell Transformation, Neoplastic genetics, Mutation genetics, Pancreas pathology, Proto-Oncogene Proteins genetics, Vertebrates genetics, ras Proteins genetics

Abstract

Somatic activation of the KRAS proto-oncogene is evident in almost all pancreatic cancers, and appears to represent an initiating event. These mutations occur primarily at codon 12 and less frequently at codons 13 and 61. Although some studies have suggested that different KRAS mutations may have variable oncogenic properties, to date there has been no comprehensive functional comparison of multiple KRAS mutations in an in vivo vertebrate tumorigenesis system. We generated a Gal4/UAS-based zebrafish model of pancreatic tumorigenesis in which the pancreatic expression of UAS-regulated oncogenes is driven by a ptf1a:Gal4-VP16 driver line. This system allowed us to rapidly compare the ability of 12 different KRAS mutations (G12A, G12C, G12D, G12F, G12R, G12S, G12V, G13C, G13D, Q61L, Q61R and A146T) to drive pancreatic tumorigenesis in vivo. Among fish injected with one of five KRAS mutations reported in other tumor types but not in human pancreatic cancer, 2/79 (2.5%) developed pancreatic tumors, with both tumors arising in fish injected with A146T. In contrast, among fish injected with one of seven KRAS mutations known to occur in human pancreatic cancer, 22/106 (20.8%) developed pancreatic cancer. All eight tumorigenic KRAS mutations were associated with downstream MAPK/ERK pathway activation in preneoplastic pancreatic epithelium, whereas nontumorigenic mutations were not. These results suggest that the spectrum of KRAS mutations observed in human pancreatic cancer reflects selection based on variable tumorigenic capacities, including the ability to activate MAPK/ERK signaling.

Published

2015

49. Social jetlag, obesity and metabolic disorder: investigation in a cohort study.

Author

Parsons MJ, Moffitt TE, Gregory AM, Goldman-Mellor S, Nolan PM, Poulton R, and Caspi A

Subjects

Adult, Body Mass Index, Circadian Rhythm, Female, Health Surveys, Humans, Longitudinal Studies, Male, Metabolic Diseases epidemiology, New Zealand epidemiology, Obesity prevention & control, Risk Factors, Sleep, Sleep Disorders, Circadian Rhythm complications, Sleep Disorders, Circadian Rhythm epidemiology, Work Schedule Tolerance, Metabolic Diseases etiology, Metabolic Diseases prevention & control, Obesity etiology, Obesity metabolism, Sleep Disorders, Circadian Rhythm metabolism

Abstract

Background: Obesity is one of the leading causes of preventable death worldwide. Circadian rhythms are known to control both sleep timing and energy homeostasis, and disruptions in circadian rhythms have been linked with metabolic dysfunction and obesity-associated disease. In previous research, social jetlag, a measure of chronic circadian disruption caused by the discrepancy between our internal versus social clocks, was associated with elevated self-reported body mass index, possibly indicative of a more generalized association with obesity and metabolic dysfunction., Methods: We studied participants from the population-representative Dunedin Longitudinal Study (N=1037) to determine whether social jetlag was associated with clinically assessed measurements of metabolic phenotypes and disease indicators for obesity-related disease, specifically, indicators of inflammation and diabetes., Results: Our analysis was restricted to N=815 non-shift workers in our cohort. Among these participants, we found that social jetlag was associated with numerous clinically assessed measures of metabolic dysfunction and obesity. We distinguished between obese individuals who were metabolically healthy versus unhealthy, and found higher social jetlag levels in metabolically unhealthy obese individuals. Among metabolically unhealthy obese individuals, social jetlag was additionally associated with elevated glycated hemoglobin and an indicator of inflammation., Conclusions: The findings are consistent with the possibility that 'living against our internal clock' may contribute to metabolic dysfunction and its consequences. Further research aimed at understanding that the physiology and social features of social jetlag may inform obesity prevention and have ramifications for policies and practices that contribute to increased social jetlag, such as work schedules and daylight savings time.

Published

2015

50. Telecare for diabetes, CHF or COPD: effect on quality of life, hospital use and costs. A randomised controlled trial and qualitative evaluation.

Author

Kenealy TW, Parsons MJ, Rouse AP, Doughty RN, Sheridan NF, Hindmarsh JK, Masson SC, and Rea HH

Subjects

Aged, Aged, 80 and over, Australia, Diabetes Mellitus parasitology, Female, Heart Failure parasitology, Hospitals, Humans, Male, Middle Aged, New Zealand, Patient Satisfaction, Pulmonary Disease, Chronic Obstructive parasitology, Quality of Life, Self Care psychology, Surveys and Questionnaires, Telemedicine economics, Diabetes Mellitus therapy, Heart Failure therapy, Pulmonary Disease, Chronic Obstructive therapy, Self Care methods, Telemedicine methods

Abstract

Objectives: To assess the effect of telecare on health related quality of life, self-care, hospital use, costs and the experiences of patients, informal carers and health care professionals., Methods: Patients were randomly assigned either to usual care or to additionally entering their data into a commercially-available electronic device that uploaded data once a day to a nurse-led monitoring station. Patients had congestive heart failure (Site A), chronic obstructive pulmonary disease (Site B), or any long-term condition, mostly diabetes (Site C). Site C contributed only intervention patients - they considered a usual care option to be unethical. The study took place in New Zealand between September 2010 and February 2012, and lasted 3 to 6 months for each patient. The primary outcome was health-related quality of life (SF36). Data on experiences were collected by individual and group interviews and by questionnaire., Results: There were 171 patients (98 intervention, 73 control). Quality of life, self-efficacy and disease-specific measures did not change significantly, while anxiety and depression both decreased significantly with the intervention. Hospital admissions, days in hospital, emergency department visits, outpatient visits and costs did not differ significantly between the groups. Patients at all sites were universally positive. Many felt safer and more cared-for, and said that they and their family had learned more about managing their condition. Staff could all see potential benefits of telecare, and, after some initial technical problems, many staff felt that telecare enabled them to effectively monitor more patients., Conclusions: Strongly positive patient and staff experiences and attitudes complement and contrast with small or non-significant quantitative changes. Telecare led to patients and families taking a more active role in self-management. It is likely that subgroups of patients benefitted in ways that were not measured or visible within the quantitative data, especially feelings of safety and being cared-for., Trial Registration: Australian New Zealand Clinical Trials Registry ACTRN12610000269033.

Published

2015