Your search keyword '"Michael Bramhall"' showing total 30 results

1. CD4+ T cells display a spectrum of recall dynamics during re-infection with malaria parasites

Author

Hyun Jae Lee, Marcela L. Moreira, Shihan Li, Takahiro Asatsuma, Cameron G. Williams, Oliver P. Skinner, Saba Asad, Michael Bramhall, Zhe Jiang, Zihan Liu, Ashlyn S. Kerr, Jessica A. Engel, Megan S. F. Soon, Jasmin Straube, Irving Barrera, Evan Murray, Fei Chen, Jason Nideffer, Prasanna Jagannathan, and Ashraful Haque

Subjects

Science

Abstract

Abstract Children in malaria-endemic regions can experience repeated Plasmodium infections over short periods of time. Effects of re-infection on multiple co-existing CD4+ T cell subsets remain unresolved. Here, we examine antigen-experienced CD4+ T cells during re-infection in mice, using scRNA-seq/TCR-seq and spatial transcriptomics. TCR transgenic TEM cells initiate rapid Th1/Tr1 recall responses prior to proliferating, while GC Tfh counterparts are refractory, with TCM/Tfh-like cells exhibiting modest non-proliferative responses. Th1-recall is a partial facsimile of primary Th1-responses, with no upregulated effector-associated genes being unique to recall. Polyclonal, TCR-diverse, CD4+ T cells exhibit similar recall dynamics, with individual clones giving rise to multiple effectors including highly proliferative Th1/Tr1 cells, as well as GC Tfh and Tfh-like cells lacking proliferative capacity. Thus, we show substantial diversity in recall responses mounted by multiple co-existing CD4+ T cell subsets in the spleen, and present graphical user interfaces for studying gene expression dynamics and clonal relationships during re-infection.

Published

2024

2. Francisella tularensis induces Th1 like MAIT cells conferring protection against systemic and local infection

Author

Zhe Zhao, Huimeng Wang, Mai Shi, Tianyuan Zhu, Troi Pediongco, Xin Yi Lim, Bronwyn S. Meehan, Adam G. Nelson, David P. Fairlie, Jeffrey Y. W. Mak, Sidonia B. G. Eckle, Marcela de Lima Moreira, Carolin Tumpach, Michael Bramhall, Cameron G. Williams, Hyun Jae Lee, Ashraful Haque, Maximilien Evrard, Jamie Rossjohn, James McCluskey, Alexandra J. Corbett, and Zhenjun Chen

Subjects

Science

Abstract

Mucosal-Associated Invariant T (MAIT) cells are associated with established functions during bacterial infection. Here the authors show inoculation with Francisella tularensis results in induction of MAIT cells associated with prototypic Th1 immunity and confer protection to systemic and local infection.

Published

2021

3. The Methyltransferase DOT1L Controls Activation and Lineage Integrity in CD4+ T Cells during Infection and Inflammation

Author

Sebastian Scheer, Jessica Runting, Michael Bramhall, Brendan Russ, Aidil Zaini, Jessie Ellemor, Grace Rodrigues, Judy Ng, and Colby Zaph

Subjects

DOT1L, CD4 T cells, Th1, Th2, IFN-γ, Trichuris muris, Biology (General), QH301-705.5

Abstract

Summary: CD4+ T helper (Th) cell differentiation is controlled by lineage-specific expression of transcription factors and effector proteins, as well as silencing of lineage-promiscuous genes. Lysine methyltransferases (KMTs) comprise a major class of epigenetic enzymes that are emerging as important regulators of Th cell biology. Here, we show that the KMT DOT1L regulates Th cell function and lineage integrity. DOT1L-dependent dimethylation of lysine 79 of histone H3 (H3K79me2) is associated with lineage-specific gene expression. However, DOT1L-deficient Th cells overproduce IFN-γ under lineage-specific and lineage-promiscuous conditions. Consistent with the increased IFN-γ response, mice with a T-cell-specific deletion of DOT1L are susceptible to infection with the helminth parasite Trichuris muris and are resistant to the development of allergic lung inflammation. These results identify a central role for DOT1L in Th2 cell lineage commitment and stability and suggest that inhibition of DOT1L may provide a therapeutic strategy to limit type 2 immune responses.

Published

2020

4. HIC1 links retinoic acid signalling to group 3 innate lymphoid cell-dependent regulation of intestinal immunity and homeostasis.

Author

Kyle Burrows, Frann Antignano, Alistair Chenery, Michael Bramhall, Vladimir Korinek, T Michael Underhill, and Colby Zaph

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

The intestinal immune system must be able to respond to a wide variety of infectious organisms while maintaining tolerance to non-pathogenic microbes and food antigens. The Vitamin A metabolite all-trans-retinoic acid (atRA) has been implicated in the regulation of this balance, partially by regulating innate lymphoid cell (ILC) responses in the intestine. However, the molecular mechanisms of atRA-dependent intestinal immunity and homeostasis remain elusive. Here we define a role for the transcriptional repressor Hypermethylated in cancer 1 (HIC1, ZBTB29) in the regulation of ILC responses in the intestine. Intestinal ILCs express HIC1 in a vitamin A-dependent manner. In the absence of HIC1, group 3 ILCs (ILC3s) that produce IL-22 are lost, resulting in increased susceptibility to infection with the bacterial pathogen Citrobacter rodentium. Thus, atRA-dependent expression of HIC1 in ILC3s regulates intestinal homeostasis and protective immunity.

Published

2018

5. Bias in the reporting of sex and age in biomedical research on mouse models

Author

Oscar Flórez-Vargas, Andy Brass, George Karystianis, Michael Bramhall, Robert Stevens, Sheena Cruickshank, and Goran Nenadic

Subjects

text-mining, sex, age, reporting, bias, Medicine, Science, Biology (General), QH301-705.5

Abstract

In animal-based biomedical research, both the sex and the age of the animals studied affect disease phenotypes by modifying their susceptibility, presentation and response to treatment. The accurate reporting of experimental methods and materials, including the sex and age of animals, is essential so that other researchers can build on the results of such studies. Here we use text mining to study 15,311 research papers in which mice were the focus of the study. We find that the percentage of papers reporting the sex and age of mice has increased over the past two decades: however, only about 50% of the papers published in 2014 reported these two variables. We also compared the quality of reporting in six preclinical research areas and found evidence for different levels of sex-bias in these areas: the strongest male-bias was observed in cardiovascular disease models and the strongest female-bias was found in infectious disease models. These results demonstrate the ability of text mining to contribute to the ongoing debate about the reproducibility of research, and confirm the need to continue efforts to improve the reporting of experimental methods and materials.

Published

2016

6. The quality of methods reporting in parasitology experiments.

Author

Oscar Flórez-Vargas, Michael Bramhall, Harry Noyes, Sheena Cruickshank, Robert Stevens, and Andy Brass

Subjects

Medicine, Science

Abstract

There is a growing concern both inside and outside the scientific community over the lack of reproducibility of experiments. The depth and detail of reported methods are critical to the reproducibility of findings, but also for making it possible to compare and integrate data from different studies. In this study, we evaluated in detail the methods reporting in a comprehensive set of trypanosomiasis experiments that should enable valid reproduction, integration and comparison of research findings. We evaluated a subset of other parasitic (Leishmania, Toxoplasma, Plasmodium, Trichuris and Schistosoma) and non-parasitic (Mycobacterium) experimental infections in order to compare the quality of method reporting more generally. A systematic review using PubMed (2000-2012) of all publications describing gene expression in cells and animals infected with Trypanosoma spp was undertaken based on PRISMA guidelines; 23 papers were identified and included. We defined a checklist of essential parameters that should be reported and have scored the number of those parameters that are reported for each publication. Bibliometric parameters (impact factor, citations and h-index) were used to look for association between Journal and Author status and the quality of method reporting. Trichuriasis experiments achieved the highest scores and included the only paper to score 100% in all criteria. The mean of scores achieved by Trypanosoma articles through the checklist was 65.5% (range 32-90%). Bibliometric parameters were not correlated with the quality of method reporting (Spearman's rank correlation coefficient 0.05). Our results indicate that the quality of methods reporting in experimental parasitology is a cause for concern and it has not improved over time, despite there being evidence that most of the assessed parameters do influence the results. We propose that our set of parameters be used as guidelines to improve the quality of the reporting of experimental infection models as a pre-requisite for integrating and comparing sets of data.

Published

2014

7. CD4+T cells display a spectrum of recall dynamics during re-infection with malaria parasites

Author

Hyun Jae Lee, Marcela L. Moreira, Shihan Li, Cameron G. Williams, Oliver P. Skinner, Saba Asad, Takahiro Asatsuma, Michael Bramhall, Zhe Jiang, Jessica A. Engel, Megan S. F. Soon, Jasmin Straube, Irving Barrera, Evan Murray, Fei Chen, Jason Nideffer, Prasanna Jagannathan, and Ashraful Haque

Abstract

Children in malaria-endemic regions can experience multiplePlasmodiuminfections over a short period of time, within vitroCD4+T cell recall responses becoming more regulatory with increasing age and exposure. This suggests that repeated infection qualitatively changes CD4+T cells, although the heterogeneity and dynamics of these responses await systematic analysisin vivo. Here, we examined TCR transgenic PbTII and polyclonal CD4+T cells duringPlasmodiumre-infection in mice, in conjunction with scRNA-seq/TCR-seq and spatial transcriptomics at near single-cell resolution. PbTII cells gave rise to multiple antigen-experienced states in different areas of the spleen after primary infection and antimalarial treatment, including ongoing GC responses and T-cell zone memory. Upon re-infection, Th1-memory PbTII cells initiated a rapid effector response prior to proliferating, while GC Tfh cells of the same antigen specificity were entirely refractory within the same organ. Transcriptome dynamic modelling and network analysis of Th1 recall revealed a biphasic wave of RNA processing that firstly preceded immune effector transcription, and later accompanied cellular proliferation. Importantly, Th1 recall constituted a partial facsimile of primary Th1 responses, with no unique genes amongst the small subset of those upregulated upon re-infection. Finally, we noted a similar spectrum of antigen-experienced states and recall dynamics by polyclonal CD4+T cells with diverse TCRs. Therefore, during re-infection withPlasmodium, persisting GC Tfh cells remained unaltered transcriptionally, Tcm/Tfh-like cells exhibited minimal proliferation, and Th1-memory cells displayed a rapid, proliferating IL-10-producing Tr1 response consistent with a shift towards immune-regulation. These data highlight a broad spectrum of simultaneous CD4+T cell responses that occur in the spleen during re-infection with malaria parasites.HighlightsSplenic TCR transgenic CD4+T cells are highly heterogeneous prior to re-infection.Persisting GC Tfh cells are refractory to re-activation during re-infection.Th1-memory cells rapidly upregulate RNA processing prior to effector function and proliferation.Th1-recall is an imperfect but faithful facsimile of primary Th1 responses.A spectrum of recall states is observed in polyclonal CD4+T cells with diverse TCRs.

Published

2023

8. Memory CD4+ T cells that co-express PD1 and CTLA4 have reduced response to activating stimuli facilitating HIV latency

Author

Thomas A. Rasmussen, Jennifer M. Zerbato, Ajantha Rhodes, Carolin Tumpach, Ashanti Dantanarayana, James H. McMahon, Jillian S.Y. Lau, J. Judy Chang, Celine Gubser, Wendy Brown, Rebecca Hoh, Melissa Krone, Rachel Pascoe, Chris Y. Chiu, Michael Bramhall, Hyun Jae Lee, Ashraful Haque, Rèmi Fromentin, Nicolas Chomont, Jeffrey Milush, Renee M. Van der Sluis, Sarah Palmer, Steven G. Deeks, Paul U. Cameron, Vanessa Evans, and Sharon R. Lewin

Subjects

CTLA4, PD1, T cell exhaustion, HIV cure, HIV reservoirs, HIV, HIV persistence, immune checkpoints, HIV latency, General Biochemistry, Genetics and Molecular Biology

Abstract

Programmed cell death 1 (PD1) and cytotoxic T lymphocyte-associated protein 4 (CTLA4) suppress CD4 + T cell activation and may promote latent HIV infection. By performing leukapheresis (n = 21) and lymph node biopsies (n = 8) in people with HIV on antiretroviral therapy (ART) and sorting memory CD4 + T cells into subsets based on PD1/CTLA4 expression, we investigate the role of PD1 and CTLA 4 in HIV persistence. We show that double-positive (PD1 +CTLA4 +) cells in blood contain more HIV DNA compared with double-negative (PD1 -CTLA4 -) cells but still have a lower proportion of cells producing multiply spliced HIV RNA after stimulation as well as reduced upregulation of T cell activation and proliferation markers. Transcriptomics analyses identify differential expression of key genes regulating T cell activation and proliferation with MAF, KLRB1, and TIGIT being upregulated in double-positive compared with double-negative cells, whereas FOS is downregulated. We conclude that, in addition to being enriched for HIV DNA, double-positive cells are characterized by negative signaling and a reduced capacity to respond to stimulation, favoring HIV latency.

Published

2022

9. Differential Expression of Soluble Receptor for Advanced Glycation End-products in Mice Susceptible or Resistant to Chronic Colitis

Author

Andy Brass, Kevin Rich, Michael Bramhall, Sheena M. Cruickshank, Ajanta Chakraborty, James Wilson, Larisa Logunova, Namshik Han, and John McLaughlin

Subjects

Male, colitis, Receptor for Advanced Glycation End Products, Inflammation, Inflammatory bowel disease, Trichuris muris, Immunophenotyping, RAGE (receptor), Mice, Mice, Inbred AKR, Immune system, Antigens, Neoplasm, Glycation, Immune Tolerance, medicine, Animals, Humans, Immunology and Allergy, RNA, Messenger, Trichuriasis, Intestinal Diseases, Parasitic, Colitis, Basic Science Review, mouse, Irritable bowel syndrome, Mice, Inbred BALB C, biology, business.industry, Gene Expression Profiling, Gastroenterology, T-Lymphocytes, Helper-Inducer, biology.organism_classification, medicine.disease, Trichuris, Chronic Disease, Immunology, Disease Susceptibility, Inflammation Mediators, Mitogen-Activated Protein Kinases, medicine.symptom, business, Biomarkers, sRAGE

Abstract

Background Identifying the factors that contribute to chronicity in inflamed colitic tissue is not trivial. However, in mouse models of colitis, we can investigate at preclinical timepoints. We sought to validate murine Trichuris muris infection as a model for identification of factors that promote development of chronic colitis. Methods We compared preclinical changes in mice with a resolving immune response to T. muris (resistant) vs mice that fail to expel the worms and develop chronic colitis (susceptible). Findings were then validated in healthy controls and patients with suspected or confirmed IBD. Results The receptor for advanced glycation end products (RAGE) was highly dysregulated between resistant and susceptible mice before the onset of any pathological signs. Increased soluble RAGE (sRAGE) in the serum and feces of resistant mice correlated with reduced colitis scores. Mouse model findings were validated in a preliminary clinical study: fecal sRAGE was differentially expressed in patients with active IBD compared with IBD in remission, patients with IBD excluded, or healthy controls. Conclusions Preclinical changes in mouse models can identify early pathways in the development of chronic inflammation that human studies cannot. We identified the decoy receptor sRAGE as a potential mechanism for protection against chronic inflammation in colitis in mice and humans. We propose that the RAGE pathway is clinically relevant in the onset of chronic colitis and that further study of sRAGE in IBD may provide a novel diagnostic and therapeutic target.

Published

2019

10. Memory CD4

Author

Thomas A, Rasmussen, Jennifer M, Zerbato, Ajantha, Rhodes, Carolin, Tumpach, Ashanti, Dantanarayana, James H, McMahon, Jillian S Y, Lau, J Judy, Chang, Celine, Gubser, Wendy, Brown, Rebecca, Hoh, Melissa, Krone, Rachel, Pascoe, Chris Y, Chiu, Michael, Bramhall, Hyun Jae, Lee, Ashraful, Haque, Rèmi, Fromentin, Nicolas, Chomont, Jeffrey, Milush, Renee M, Van der Sluis, Sarah, Palmer, Steven G, Deeks, Paul U, Cameron, Vanessa, Evans, and Sharon R, Lewin

Subjects

CD4-Positive T-Lymphocytes, T-Lymphocytes, Programmed Cell Death 1 Receptor, Humans, RNA, CTLA-4 Antigen, HIV Infections, Receptors, Immunologic

Abstract

Programmed cell death 1 (PD1) and cytotoxic T lymphocyte-associated protein 4 (CTLA4) suppress CD4

Published

2021

11. Heterogeneous Tfh cell populations that develop during enteric helminth infection predict the quality of type 2 protective response

Author

Kim L. Good-Jacobson, Aidil Zaini, Lauren Hailes, Daniel Thiele, Judy Ng, Amania A. Sheikh, Colby Zaph, Michael Bramhall, Lennard Dalit, Joanna R Groom, Sebastian Scheer, Grace Rodrigues, Yan Zhang, and Jessica Runting

Subjects

Chronic infection, medicine.anatomical_structure, Immune system, biology, Humoral immunity, Cell, Immunology, medicine, Epigenetics, biology.organism_classification, Trichuris muris, B cell, Chromatin

Abstract

T follicular helper (Tfh) cells are an important component of the germinal centre (GC)-mediated humoral immunity. Yet, how regulation of Tfh- GC responses impacts on effective responses to helminth infection are poorly understood. Here we show that chronic helminth Trichuris muris infection fails to induce Tfh-GC B cell responses, with Tfh cells expressing T-bet and IFN-γ. In contrast, Tfh cells that express GATA-3 and IL-4 dominate responses to an acute, resolving infection. Accordingly, heightened expression and increased chromatin accessibility of Th1- and Th2 cell-associated genes is observed in chronic and acute induced Tfh cells, respectively. However, both acute and chronic Tfh cell populations retained the capacity to produce IL-21 in spite of the Th-biased response. Blockade of Tfh-GC interactions impaired type 2 immunity, highlighting the protective role of GC-dependent Th2-like Tfh cell responses against helminths. Collectively, these results provide new insights into the protective roles of Tfh-GC responses and identify distinct transcriptional and epigenetic features of Tfh cells that emerge during resolving or chronic helminth infections.Author summaryAbout a quarter of the world population is afflicted with parasitic worm infection. Although deworming drugs can reduce the levels of the infection, they fail to prevent reinfections. Therefore, the most sustainable goal is to develop vaccines against human helminth parasites, which has been extremely challenging due to the lack of understanding of host-parasite interactions. While the protective roles of T helper 2 (Th2) cells are well established, the regulation of T follicular helper (Tfh) cells and their roles during helminth infection remain poorly defined. In this study, we describe the differential regulation of Tfh cell responses during chronic non-protective vs acute protective responses during helminth infection. We show that Tfh cells during chronic infection are rare and have strikingly different characteristics to acute-induced Tfh cells, which appear to be more like Th2 cells. Specifically, we show that blockade of Th2-like Tfh cell response during acute infection results in the host failing to expel the worms. Our study identifies that Tfh cell populations that emerge during chronic and acute infection are strikingly heterogeneous and critically important in mediating protective immune responses against helminths.

Published

2021

12. The Methyltransferase DOT1L Controls Activation and Lineage Integrity in CD4+ T Cells during Infection and Inflammation

Author

Aidil Zaini, Judy Ng, Jessica Runting, Brendan Russ, Jessie Ellemor, Colby Zaph, Michael Bramhall, Sebastian Scheer, and Grace Rodrigues

Subjects

0301 basic medicine, Methyltransferase, biology, Effector, Cellular differentiation, CD4 T cells, DOT1L, biology.organism_classification, General Biochemistry, Genetics and Molecular Biology, Trichuris muris, Cell biology, Th1, 03 medical and health sciences, Histone H3, Th2, 030104 developmental biology, 0302 clinical medicine, Immune system, lcsh:Biology (General), Epigenetics, IFN-γ, lcsh:QH301-705.5, 030217 neurology & neurosurgery

Abstract

Summary: CD4+ T helper (Th) cell differentiation is controlled by lineage-specific expression of transcription factors and effector proteins, as well as silencing of lineage-promiscuous genes. Lysine methyltransferases (KMTs) comprise a major class of epigenetic enzymes that are emerging as important regulators of Th cell biology. Here, we show that the KMT DOT1L regulates Th cell function and lineage integrity. DOT1L-dependent dimethylation of lysine 79 of histone H3 (H3K79me2) is associated with lineage-specific gene expression. However, DOT1L-deficient Th cells overproduce IFN-γ under lineage-specific and lineage-promiscuous conditions. Consistent with the increased IFN-γ response, mice with a T-cell-specific deletion of DOT1L are susceptible to infection with the helminth parasite Trichuris muris and are resistant to the development of allergic lung inflammation. These results identify a central role for DOT1L in Th2 cell lineage commitment and stability and suggest that inhibition of DOT1L may provide a therapeutic strategy to limit type 2 immune responses.

Published

2020

13. Engineering Education: The Uk Challenge

Author

Ian Robinson, Michael Bramhall, and John Rowe

Published

2020

14. Business And Management In The Engineering Curriculum

Author

Michael Bramhall, Steve Lawson, and Ian Robinson

Published

2020

15. Communication Apprehension In U.K. Engineering Students: A Comparative Study

Author

Trevor Hassall, Jose Arquero, John Joyce, Ian Robinson, and Michael Bramhall

Published

2020

16. Promoting Learner Autonomy In Engineering

Author

Michael Bramhall and Keith Radley

Published

2020

17. Transcriptome dynamics of CD4

Author

Megan S F, Soon, Hyun Jae, Lee, Jessica A, Engel, Jasmin, Straube, Bryce S, Thomas, Clara P S, Pernold, Lachlan S, Clarke, Pawat, Laohamonthonkul, Rohit N, Haldar, Cameron G, Williams, Lianne I M, Lansink, Marcela L, Moreira, Michael, Bramhall, Lambros T, Koufariotis, Scott, Wood, Xi, Chen, Kylie R, James, Tapio, Lönnberg, Steven W, Lane, Gabrielle T, Belz, Christian R, Engwerda, David S, Khoury, Miles P, Davenport, Valentine, Svensson, Sarah A, Teichmann, and Ashraful, Haque

Subjects

CD4-Positive T-Lymphocytes, Plasmodium, Gene Expression Profiling, Adoptive Transfer, Chromatin, Malaria, Antimalarials, Disease Models, Animal, Mice, Animals, Humans, Transcriptome, Immunologic Memory, Biomarkers

Abstract

The dynamics of CD4

Published

2020

18. Transcriptome dynamics of CD4+ T cells during malaria maps gradual transit from effector to memory

Author

Ashraful Haque, Lachlan S. Clarke, Scott Wood, Kylie R. James, Xi Chen, Jessica A. Engel, Lianne I. M. Lansink, David S. Khoury, Valentine Svensson, Megan S. F. Soon, Pawat Laohamonthonkul, Clara P. S. Pernold, Steven W. Lane, Hyun Jae Lee, Bryce S. Thomas, Tapio Lönnberg, Jasmin Straube, Marcela de Lima Moreira, Gabrielle T. Belz, Rohit N. Haldar, Christian R. Engwerda, Cameron G. Williams, Michael Bramhall, Miles P. Davenport, Lambros T. Koufariotis, and Sarah A. Teichmann

Subjects

0301 basic medicine, Adoptive cell transfer, Recall, Effector, T cell, Immunology, Biology, 3. Good health, Cell biology, Gene expression profiling, Transcriptome, 03 medical and health sciences, Memory development, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, medicine, Immunology and Allergy, 030215 immunology, Epigenomics

Abstract

The dynamics of CD4⁺ T cell memory development remain to be examined at genome scale. In malaria-endemic regions, antimalarial chemoprevention protects long after its cessation and associates with effects on CD4⁺ T cells. We applied single-cell RNA sequencing and computational modelling to track memory development during Plasmodium infection and treatment. In the absence of central memory precursors, two trajectories developed as T helper 1 (T_H1) and follicular helper T (T_(FH)) transcriptomes contracted and partially coalesced over three weeks. Progeny of single clones populated T_H1 and T_(FH) trajectories, and fate-mapping suggested that there was minimal lineage plasticity. Relationships between T_(FH) and central memory were revealed, with antimalarials modulating these responses and boosting T_H1 recall. Finally, single-cell epigenomics confirmed that heterogeneity among effectors was partially reset in memory. Thus, the effector-to-memory transition in CD4⁺ T cells is gradual during malaria and is modulated by antiparasitic drugs. Graphical user interfaces are presented for examining gene-expression dynamics and gene–gene correlations (http://haquelab.mdhs.unimelb.edu.au/cd4_memory/).

Published

2020

19. The Methyltransferase DOT1L Limits Activation and the Th1 Program in CD4+ T Cells During Infection and Inflammation

Author

Grace Rodrigues, Judy Ng, Sebastian Scheer, Colby Zaph, Michael Bramhall, Jessie Ellemor, Brendan E. Russ, Jessica Runting, and Aidil Zaini

Subjects

Histone H3, Immune system, Methyltransferase, Effector, Cellular differentiation, Epigenetics, DOT1L, Biology, biology.organism_classification, Trichuris muris, Cell biology

Abstract

CD4 + T helper (Th) cell differentiation is controlled by lineage-specific expression of transcription factors and effector proteins, as well as silencing of lineage-promiscuous genes. Lysine methyltransferases (KMTs) comprise a major class of epigenetic enzymes that are emerging as important regulators of Th cell biology. Here, we show that the KMT DOT1L regulates Th cell function and lineage integrity. DOT1L-dependent dimethylation of lysine 79 of histone H3 (H3K79me2) is associated with lineage-specific gene expression. However, DOT1L-deficient Th cells overproduce IFN-γ under lineage-specific and lineage-promiscuous conditions. Consistent with the increased IFN-γ response, mice with a T cell-specific deletion of DOT1L are susceptible to infection with the helminth parasite Trichuris muris and resistant to the development of allergic lung inflammation. These results identify a central role for DOT1L in Th cell lineage commitment and stability, and suggest that inhibition of DOT1L may provide a novel therapeutic strategy to limit type 2 immune responses.

Published

2020

20. The methyltransferase DOT1L limits activation and the Th1 program in CD4+ T cells during infection and inflammation

Author

Jessie Ellemor, Jessica Runting, Colby Zaph, Michael Bramhall, Grace Rodrigues, Aidil Zaini, Sebastian Scheer, Brendan E. Russ, and Judy Ng

Subjects

0303 health sciences, Methyltransferase, Effector, Cellular differentiation, DOT1L, Biology, biology.organism_classification, Trichuris muris, 3. Good health, Cell biology, 03 medical and health sciences, Histone H3, 0302 clinical medicine, Immune system, Epigenetics, 030304 developmental biology, 030215 immunology

Abstract

CD4+ T helper (Th) cell differentiation is controlled by lineage-specific expression of transcription factors and effector proteins, as well as silencing of lineage-promiscuous genes. Lysine methyltransferases (KMTs) comprise a major class of epigenetic enzymes that are emerging as important regulators of Th cell biology. Here, we show that the KMT DOT1L regulates Th cell function and lineage integrity. DOT1L-dependent dimethylation of lysine 79 of histone H3 (H3K79me2) is associated with lineage-specific gene expression. However, DOT1L-deficient Th cells overproduce IFN-γ under lineage-specific and lineage-promiscuous conditions. Consistent with the increased IFN-γ response, mice with a T cell-specific deletion of DOT1L are susceptible to infection with the helminth parasite Trichuris muris and resistant to the development of allergic lung inflammation. These results identify a central role for DOT1L in Th cell lineage commitment and stability, and suggest that inhibition of DOT1L may provide a novel therapeutic strategy to limit type 2 immune responses.

Published

2019

21. Differential expression of soluble receptor for advanced glycation end-products (sRAGE) in mice susceptible or resistant to chronic colitis

Author

Sheena M. Cruickshank, John McLaughlin, James Wilson, Ajanta Chakraborty, Larisa Logunova, Namshik Han, Catherine Booth, Michael Bramhall, Andy Brass, and Kevin Rich

Subjects

biology, business.industry, Inflammation, medicine.disease, biology.organism_classification, Trichuris muris, RAGE (receptor), Immune system, Glycation, Immunology, medicine, Colitis, medicine.symptom, Receptor, business, Pathological

Abstract

AimsIdentifying the factors that contribute to chronicity in inflamed colitic tissue is not trivial. However, in mouse models of colitis, we can investigate at preclinical timepoints. We sought to validate murine Trichuris muris infection as a model for identification of factors that promote development of chronic colitis.MethodsWe compared preclinical changes in mice with a resolving immune response to T. muris (resistant) versus mice that fail to expel the worms and develop chronic colitis (susceptible). Findings were then validated in healthy controls and patients with suspected or confirmed IBD.ResultsThe Receptor for Advanced Glycation End Products (Rage) was highly dysregulated between resistant and susceptible mice prior to the onset of any pathological signs. Increased soluble RAGE (sRAGE) in the serum and faeces of resistant mice correlated with reduced colitis scores. Mouse model findings were validated in a preliminary clinical study: faecal sRAGE was differentially expressed in patients with active IBD compared with IBD in remission, patients with IBD excluded or healthy controls.ConclusionPre-clinical changes in mouse models can identify early pathways in the development of chronic inflammation that human studies cannot. We identified the decoy receptor sRAGE as a potential mechanism for protection against chronic inflammation in colitis in mice and humans. We propose that the RAGE pathway is clinically relevant in the onset of chronic colitis, and that further study of sRAGE in IBD may provide a novel diagnostic and therapeutic target.

Published

2019

22. Mastering gut permeability: New roles for old friends

Author

Colby Zaph and Michael Bramhall

Subjects

0301 basic medicine, medicine.medical_treatment, Immunology, Context (language use), Friends, Biology, Permeability, 03 medical and health sciences, Chymases, Intestinal mucosa, medicine, Immunology and Allergy, Compartment (development), Helminths, Humans, Mast Cells, Intestinal Mucosa, Innate immune system, Protease, Intestinal permeability, medicine.disease, Mast cell, Intestines, 030104 developmental biology, medicine.anatomical_structure, Mastocytosis

Abstract

Mast cells are innate immune cells that respond rapidly to infection in barrier tissues such as the skin and intestinal mucosa. Expulsion of parasitic worms in the gut involves a robust type 2 host response, and an acute mastocytosis is often generated at the site of infection. However, the role of mast cells in resistance to worm infections appears to be parasite specific. Mast cells are also involved in tissue repair, but the long-term contribution of mast cell activation after worm expulsion has not been definitively studied. In this issue of European Journal of Immunology, Sorobetea et al. [Eur. J. Immunol. 2017. 47: 257-268] demonstrate that activated mast cells persist in the large intestinal lamina propria and intraepithelial compartment long after worm expulsion, resulting in continued local and systemic presence of the mast cell protease mast cell protease 1 (MCPt-1) and enhanced intestinal permeability. In this commentary, we discuss these findings in the wider context of mast cell function in health and disease.

Published

2016

23. The transcriptional repressor HIC1 regulates intestinal immune homeostasis

Author

Kyle Burrows, T. Michael Underhill, Sebastian Scheer, Vladimir Korinek, Colby Zaph, Michael Bramhall, Frann Antignano, and Alistair Chenery

Subjects

0301 basic medicine, T-Lymphocytes, T cell, Immunology, Kruppel-Like Transcription Factors, Retinoic acid, Mice, Transgenic, Tretinoin, Inflammation, Biology, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Immune system, Antigen, Immunity, medicine, Animals, Homeostasis, Immunology and Allergy, Transcription factor, Cells, Cultured, 030304 developmental biology, Regulation of gene expression, 0303 health sciences, Mucous Membrane, Interleukin-17, 3. Good health, Cell biology, Intestines, Repressor Proteins, 030104 developmental biology, medicine.anatomical_structure, Gene Expression Regulation, chemistry, 030220 oncology & carcinogenesis, Interleukin 17, medicine.symptom

Abstract

The intestine is a unique immune environment that must respond to infectious organisms but remain tolerant to commensal microbes and food antigens. However, the molecular mechanisms that regulate immune cell function in the intestine remain unclear. Here we identify the POK/ZBTB family transcription factor Hypermethylated in cancer 1 (HIC1, ZBTB29) as a central component of immunity and inflammation in the intestine. HIC1 is specifically expressed in immune cells in the intestinal lamina propria (LP) in the steady state and mice with a T cell-specific deletion of HIC1 have reduced numbers of T cells in the LP. HIC1 expression is regulated by the Vitamin A metabolite retinoic acid, as mice raised on a Vitamin A-deficient diet lack HIC1-positive cells in the intestine. HIC1-deficient T cells overproduce IL-17A in vitro and in vivo, and fail to induce intestinal inflammation, identifying a critical role for HIC1 in the regulation of T cell function in the intestinal microenvironment under both homeostatic and inflammatory conditions.

Published

2016

24. Author response: Bias in the reporting of sex and age in biomedical research on mouse models

Author

Goran Nenadic, Andy Brass, Oscar Florez-Vargas, Sheena M. Cruickshank, Michael Bramhall, George Karystianis, and Robert Stevens

Subjects

Response bias, Psychology, Clinical psychology

Published

2016

25. HIC1 links retinoic acid signalling to group 3 innate lymphoid cell-dependent regulation of intestinal immunity and homeostasis

Author

Alistair Chenery, Kyle Burrows, Frann Antignano, Colby Zaph, Michael Bramhall, T. Michael Underhill, and Vladimir Korinek

Subjects

Bacterial Diseases, 0301 basic medicine, Physiology, Retinoic acid, Cell-Mediated Immunity, White Blood Cells, Mice, chemistry.chemical_compound, 0302 clinical medicine, Animal Cells, Medicine and Health Sciences, Homeostasis, Lymphocytes, Biology (General), Regulation of gene expression, T Cells, Innate lymphoid cell, Enterobacteriaceae Infections, Infectious Disease Immunology, 3. Good health, Cell biology, Intestines, Infectious Diseases, 030220 oncology & carcinogenesis, Anatomy, Cellular Types, Signal transduction, medicine.symptom, Research Article, Signal Transduction, Colon, QH301-705.5, Immune Cells, Immunology, Kruppel-Like Transcription Factors, Mice, Transgenic, Tretinoin, Inflammation, Biology, Microbiology, 03 medical and health sciences, Immune system, Immunity, Virology, Genetics, medicine, Animals, Molecular Biology, Nutrition, Blood Cells, Biology and Life Sciences, Cell Biology, RC581-607, Immunity, Innate, Diet, Gastrointestinal Tract, Mice, Inbred C57BL, 030104 developmental biology, Gene Expression Regulation, chemistry, Citrobacter rodentium, Clinical Immunology, Parasitology, Clinical Medicine, Immunologic diseases. Allergy, Physiological Processes, Digestive System

Abstract

The intestinal immune system must be able to respond to a wide variety of infectious organisms while maintaining tolerance to non-pathogenic microbes and food antigens. The Vitamin A metabolite all-trans-retinoic acid (atRA) has been implicated in the regulation of this balance, partially by regulating innate lymphoid cell (ILC) responses in the intestine. However, the molecular mechanisms of atRA-dependent intestinal immunity and homeostasis remain elusive. Here we define a role for the transcriptional repressor Hypermethylated in cancer 1 (HIC1, ZBTB29) in the regulation of ILC responses in the intestine. Intestinal ILCs express HIC1 in a vitamin A-dependent manner. In the absence of HIC1, group 3 ILCs (ILC3s) that produce IL-22 are lost, resulting in increased susceptibility to infection with the bacterial pathogen Citrobacter rodentium. Thus, atRA-dependent expression of HIC1 in ILC3s regulates intestinal homeostasis and protective immunity., Author summary Innate lymphoid cells (ILCs) are emerging as important regulators of immune responses at barrier sites such as the intestine. However, the molecular mechanisms that control this are not well described. In the intestine, the Vitamin A metabolite all-trans-retinoic acid (atRA) has been shown to be an important component of the homeostatic mechanisms. In this manuscript, we show that the atRA-dependent transcription factor Hypermethylated in cancer 1 (HIC1, ZBTB29) is required for ILC homeostasis and function in the steady state as well as following infection with the bacterial pathogen Citrobacter rodentium. Thus, HIC1 links RA signalling to intestinal immune responses. Further, our results identify HIC1 as a potential target to modulate ILC responses in vivo in health and disease.

Published

2018

26. Quality of methods reporting in animal models of colitis

Author

Michael, Bramhall, Oscar, Flórez-Vargas, Robert, Stevens, Andy, Brass, and Sheena, Cruickshank

Subjects

colitis, Dextran Sulfate, IBD, Original Basic Science Articles, Inflammatory Bowel Diseases, animal models, Checklist, Interleukin-10, methods, Disease Models, Animal, Trinitrobenzenesulfonic Acid, Research Design, Animals, Humans, Leukocyte Common Antigens

Abstract

Article first published online 29 April 2015. Supplemental Digital Content is Available in the Text., Background: Current understanding of the onset of inflammatory bowel diseases relies heavily on data derived from animal models of colitis. However, the omission of information concerning the method used makes the interpretation of studies difficult or impossible. We assessed the current quality of methods reporting in 4 animal models of colitis that are used to inform clinical research into inflammatory bowel disease: dextran sulfate sodium, interleukin-10−/−, CD45RBhigh T cell transfer, and 2,4,6-trinitrobenzene sulfonic acid (TNBS). Methods: We performed a systematic review based on PRISMA guidelines, using a PubMed search (2000–2014) to obtain publications that used a microarray to describe gene expression in colitic tissue. Methods reporting quality was scored against a checklist of essential and desirable criteria. Results: Fifty-eight articles were identified and included in this review (29 dextran sulfate sodium, 15 interleukin-10−/−, 5 T cell transfer, and 16 TNBS; some articles use more than 1 colitis model). A mean of 81.7% (SD = ±7.038) of criteria were reported across all models. Only 1 of the 58 articles reported all essential criteria on our checklist. Animal age, gender, housing conditions, and mortality/morbidity were all poorly reported. Conclusions: Failure to include all essential criteria is a cause for concern; this failure can have large impact on the quality and replicability of published colitis experiments. We recommend adoption of our checklist as a requirement for publication to improve the quality, comparability, and standardization of colitis studies and will make interpretation and translation of data to human disease more reliable.

Published

2015

27. The Quality of Methods Reporting in Parasitology Experiments

Author

Michael Bramhall, Sheena M. Cruickshank, Harry Noyes, Oscar Florez-Vargas, Andy Brass, and Robert Stevens

Subjects

Proteomics, Microbiological Techniques, medicine.medical_specialty, Veterinary medicine, media_common.quotation_subject, Science, Immunology, Population Modeling, Biology, Bibliometrics, Biochemistry, Microbiology, medicine, Genetics, Medicine and Health Sciences, Parasitic Diseases, Animals, Medical physics, Quality (business), Differential expression, media_common, Rank correlation, Medicine(all), Infectious Disease Medicine, Multidisciplinary, Agricultural and Biological Sciences(all), Impact factor, Biochemistry, Genetics and Molecular Biology(all), Biology and Life Sciences, Computational Biology, Reproducibility of Results, Genomics, Research findings, Tropical Diseases, Checklist, Infectious Diseases, Parasitology, Medicine, Periodicals as Topic, Infectious Disease Modeling, Research Article, Neglected Tropical Diseases

Abstract

There is a growing concern both inside and outside the scientific community over the lack of reproducibility of experiments. The depth and detail of reported methods are critical to the reproducibility of findings, but also for making it possible to compare and integrate data from different studies. In this study, we evaluated in detail the methods reporting in a comprehensive set of trypanosomiasis experiments that should enable valid reproduction, integration and comparison of research findings. We evaluated a subset of other parasitic (Leishmania, Toxoplasma, Plasmodium, Trichuris and Schistosoma) and non-parasitic (Mycobacterium) experimental infections in order to compare the quality of method reporting more generally. A systematic review using PubMed (2000-2012) of all publications describing gene expression in cells and animals infected with Trypanosoma spp was undertaken based on PRISMA guidelines; 23 papers were identified and included. We defined a checklist of essential parameters that should be reported and have scored the number of those parameters that are reported for each publication. Bibliometric parameters (impact factor, citations and h-index) were used to look for association between Journal and Author status and the quality of method reporting. Trichuriasis experiments achieved the highest scores and included the only paper to score 100% in all criteria. The mean of scores achieved by Trypanosoma articles through the checklist was 65.5% (range 32-90%). Bibliometric parameters were not correlated with the quality of method reporting (Spearman's rank correlation coefficient 0.05). Our results indicate that the quality of methods reporting in experimental parasitology is a cause for concern and it has not improved over time, despite there being evidence that most of the assessed parameters do influence the results. We propose that our set of parameters be used as guidelines to improve the quality of the reporting of experimental infection models as a pre-requisite for integrating and comparing sets of data. © 2014 Flórez-Vargas et al.

Published

2014

28. The Quality of Methods Reporting in Parasitology Experiments

Author

Oscar Flo´ rez-Vargas, Michael Bramhall, Harry Noyes, Sheena Cruickshank, Robert Stevens, Andy Brass

Abstract

There is a growing concern both inside and outside the scientific community over the lack of reproducibility of experiments. The depth and detail of reported methods are critical to the reproducibility of findings, but also for making it possible to compare and integrate data from different studies. In this study, we evaluated in detail the methods reporting in a comprehensive set of trypanosomiasis experiments that should enable valid reproduction, integration and comparison of research findings. We evaluated a subset of other parasitic (Leishmania, Toxoplasma, Plasmodium, Trichuris and Schistosoma) and non-parasitic (Mycobacterium) experimental infections in order to compare the quality of method reporting more generally. A systematic review using PubMed (2000–2012) of all publications describing gene expression in cells and animals infected with Trypanosoma spp was undertaken based on PRISMA guidelines; 23 papers were identified and included. We defined a checklist of essential parameters that should be reported and have scored the number of those parameters that are reported for each publication. Bibliometric parameters (impact factor, citations and h-index) were used to look for association between Journal and Author status and the quality of method reporting. Trichuriasis experiments achieved the highest scores and included the only paper to score 100% in all criteria. The mean of scores achieved by Trypanosoma articles through the checklist was 65.5% (range 32–90%). Bibliometric parameters were not correlated with the quality of method reporting (Spearman’s rank correlation coefficient ,20.5; p.0.05). Our results indicate that the quality of methods reporting in experimental parasitology is a cause for concern and it has not improved over time, despite there being evidence that most of the assessed parameters do influence the results. We propose that our set of parameters be used as guidelines to improve the quality of the reporting of experimental infection models as a pre-requisite for integrating and comparing sets of data.

Published

2014

29. LB-006 Quality Of Methods Reporting In Colitis Experiments And The Subsequent Impact On The Development Of A Gut Knowledge Base

Author

Sheena M. Cruickshank, James M. Wilson, Oscar Florez-Vargas, Robert Stevens, Andy Brass, and Michael Bramhall

Subjects

Annotation, Knowledge base, business.industry, Gene ontology, media_common.quotation_subject, Gastroenterology, Medicine, Domain knowledge, Quality (business), business, Data science, Checklist, media_common

Abstract

Introduction Current gastroenterological research generates vast quantities of clinical or animal model-derived data that is necessary to the study of IBD, yet much of it lies unused in repositories after publication. There is a growing need to develop more appropriate, structured storage systems that can be used by researchers to query this wealth of information with emerging questions. A domain-specific knowledge base combining clinical and laboratory datasets, annotated and connected via ontological terms, would be a valuable tool for gastroenterologists. However, development of a gut domain knowledge base may be severely impeded by incomplete methods reporting in the literature. This is further compounded by two factors. Firstly, non-domain experts, who may not be well suited to identifying missing methods, usually undertake construction of a knowledge base. Secondly, variations in experimental protocols may make it difficult for investigators to compare results from similar, but not identical, experiments. Methods In order to address these issues we have systematically collated published papers that employed the widely used DSS colitis model. The papers were assessed against a checklist of essential parameters that should be reported for the experiment to be accurately described to allow for correct annotation and entry into a knowledge base. Results We provide a comprehensive review of the quality of methods reporting in experiments using the DSS colitis model. We also report on the heterogeneity of the DSS colitis model currently in use. Conclusion We provide a number of recommendations in order for researchers to standardise their methods and ensure that all relevant factors are reported during the publication of their research. Building from this, we will use what we have learnt to better inform the construction of a gut domain knowledge base. Disclosure of Interest M. Bramhall Grant/research support from: Epistem Ltd., O. Florez-Vargas: None Declared, R. Stevens: None Declared, J. Wilson: None Declared, S. Cruickshank: None Declared, A. Brass: None Declared.

Published

2014

30. PWE-098 Mechanisms the Underlying Development of Chronic Inflammation in Inflammatory Bowel Disease: Defining the Role of the Rage Pathway Using Computational and Biological Analysis Strategies

Author

James M. Wilson, R Haggart, Namshik Han, Sheena M. Cruickshank, Andy Brass, and Michael Bramhall

Subjects

business.industry, Microarray analysis techniques, Gastroenterology, Inflammation, Disease, Dendritic cell, medicine.disease, Inflammatory bowel disease, RAGE (receptor), Immune system, Immunology, Medicine, medicine.symptom, Colitis, business

Abstract

Introduction Inflammatory bowel disease (IBD) is a chronic inflammatory disease with an estimated annual cost to the NHS of £720 million. Patients typically present with established disease and this makes it difficult to determine the underlying aetiology: knowledge that would aid early diagnosis and treatment. Methods To better define factors underlying the development of IBD that might be used as diagnostic aids for treatment/prevention of IBD we have analysed the early immune response in mice that will develop colitis using a validated infection model of colitis. Microarray analyses of colon tissue were conducted using the Puma and Tigre packages for Bioconductor to determine gene expression and investigate the transcription factor pathways involved. Results Microarray analysis identified an early and rapid increase in expression of the receptor for advanced glycation end-products (RAGE) in colitic prone (susceptible) mice. In contrast, mice that clear the infection (resistant mice) had no increase in RAGE. In addition, the transcription factor analysis revealed a downregulation of colitic protective factors in the RAGE signalling pathway. Immunohistochemistry data showed high RAGE expression in the gut epithelium prior to the onset of colitis. Previous work from our group has shown that epithelial cells promote dendritic cell recruitment associated with resistance and clearance of parasite infection. In the colitis model, infection also induced the rapid recruitment of macrophages and dendritic cells (DC) into the gut and lymph nodes in resistant mice but not susceptible mice. By day 31 post-infection, resistant mice had resolved the infection and inflammation whereas susceptible mice had significantly higher immune cell accumulation and colitis. Current work is addressing the expression of RAGE blocking ligands and the regulation of RAGE in the guts of resistant and susceptible mice. Conclusion RAGE has been associated with chronic IBD in patients however our data implicates RAGE in the development and propagation of IBD. We propose that the RAGE pathway is an early indicator of IBD and may be useful therapeutically and in determining efficacy of IBD therapy. Disclosure of Interest M. Bramhall Grant/Research Support from: Epistem Ltd., N. Han: None Declared, R. Haggart: None Declared, J. Wilson: None Declared, A. Brass: None Declared, S. Cruickshank: None Declared.

Published

2013