Your search keyword '"Tovah N, Shaw"' showing total 18 results

1. Memory CD8 + T cells exhibit tissue imprinting and non‐stable exposure‐dependent reactivation characteristics following blood‐stage Plasmodium berghei ANKA infections

Author

Leo A. H. Zeef, Jenna J Godfrey, Antonn J Cheeseman, Ana Villegas-Mendez, Michael J. Haley, Rebecca S. Dookie, Patrick Strangward, Kevin N. Couper, and Tovah N. Shaw

Subjects

Effector, brain, CD69, Immunology, Spleen, Biology, biology.organism_classification, immune memory, Phenotype, Cell biology, medicine.anatomical_structure, CD8 T cell, parasitic diseases, medicine, biology.protein, Immunology and Allergy, Cytotoxic T cell, cerebral malaria, Plasmodium berghei, Antibody, CD8

Abstract

Experimental cerebral malaria (ECM) is a severe complication of Plasmodium berghei ANKA (PbA) infection in mice, characterized by CD8+ T-cell accumulation within the brain. Whilst the dynamics of CD8+ T-cell activation and migration during extant primary PbA infection have been extensively researched, the fate of the parasite-specific CD8+ T cells upon resolution of ECM is not understood. In this study, we show that memory OT-I cells persist systemically within the spleen, lung and brain following recovery from ECM after primary PbA-OVA infection. Whereas memory OT-I cells within the spleen and lung exhibited canonical central memory (Tcm) and effector memory (Tem) phenotypes, respectively, memory OT-I cells within the brain post-PbA-OVA infection displayed an enriched CD69+CD103− profile and expressed low levels of T-bet. OT-I cells within the brain were excluded from short-term intravascular antibody labelling but were targeted effectively by longer-term systemically administered antibodies. Thus, the memory OT-I cells were extravascular within the brain post-ECM but were potentially not resident memory cells. Importantly, whilst memory OT-I cells exhibited strong reactivation during secondary PbA-OVA infection, preventing activation of new primary effector T cells, they had dampened reactivation during a fourth PbA-OVA infection. Overall, our results demonstrate that memory CD8+ T cells are systemically distributed but exhibit a unique phenotype within the brain post-ECM, and that their reactivation characteristics are shaped by infection history. Our results raise important questions regarding the role of distinct memory CD8+ T-cell populations within the brain and other tissues during repeat Plasmodium infections.

Published

2021

2. Alterations in T and B cell function persist in convalescent COVID-19 patients

Author

Halima A. Shuwa, Tovah N. Shaw, Sean B. Knight, Kelly Wemyss, Flora A. McClure, Laurence Pearmain, Ian Prise, Christopher Jagger, David J. Morgan, Saba Khan, Oliver Brand, Elizabeth R. Mann, Andrew Ustianowski, Nawar Diar Bakerly, Paul Dark, Christopher E. Brightling, Seema Brij, Timothy Felton, Angela Simpson, John R. Grainger, Tracy Hussell, Joanne E. Konkel, Madhvi Menon, Rohan Ahmed, Miriam Avery, Katharine Birchall, Evelyn Charsley, Alistair Chenery, Christine Chew, Richard Clark, Emma Connolly, Karen Connolly, Simon Dawson, Laura Durrans, Hannah Durrington, Jasmine Egan, Kara Filbey, Claire Fox, Helen Francis, Miriam Franklin, Susannah Glasgow, Nicola Godfrey, Kathryn J. Gray, Seamus Grundy, Jacinta Guerin, Pamela Hackney, Chantelle Hayes, Emma Hardy, Jade Harris, Anu John, Bethany Jolly, Verena Kästele, Gina Kerry, Sylvia Lui, Lijing Lin, Alex G. Mathioudakis, Joanne Mitchell, Clare Moizer, Katrina Moore, Stuart Moss, Syed Murtuza Baker, Rob Oliver, Grace Padden, Christina Parkinson, Michael Phuycharoen, Ananya Saha, Barbora Salcman, Nicholas A. Scott, Seema Sharma, Jane Shaw, Joanne Shaw, Elizabeth Shepley, Lara Smith, Simon Stephan, Ruth Stephens, Gael Tavernier, Rhys Tudge, Louis Wareing, Roanna Warren, Thomas Williams, Lisa Willmore, and Mehwish Younas

Subjects

media_common.quotation_subject, Lymphocyte, medicine.medical_treatment, Translation to patients, T cells, Disease, CD8-Positive T-Lymphocytes, Immune system, medicine, Cytotoxic T cell, Humans, long COVID, B cell, media_common, B cells, business.industry, Interleukin-6, SARS-CoV-2, Convalescence, COVID-19, General Medicine, Clinical and Translational Report, Interleukin-10, medicine.anatomical_structure, Cytokine, Immunology, Cytokines, viral infection, convalescent patients, business, CD8

Abstract

Background Emerging studies indicate that some COVID-19 patients suffer from persistent symptoms including breathlessness and chronic fatigue; however the long-term immune response in these patients presently remains ill-defined. Methods Here we describe the phenotypic and functional characteristics of B and T cells in hospitalised COVID-19 patients during acute disease and at 3-6 months of convalescence. Findings We report that the alterations in B cell subsets observed in acute COVID-19 patients were largely recovered in convalescent patients. In contrast, T cells from convalescent patients displayed continued alterations with persistence of a cytotoxic programme evident in CD8+ T cells as well as elevated production of type-1 cytokines and IL-17. Interestingly, B cells from patients with acute COVID-19 displayed an IL-6/IL-10 cytokine imbalance in response to toll-like receptor activation, skewed towards a pro-inflammatory phenotype. Whereas the frequency of IL-6+ B cells was restored in convalescent patients irrespective of clinical outcome, recovery of IL-10+ B cells was associated with resolution of lung pathology. Conclusions Our data detail lymphocyte alterations in previously hospitalized COVID-19 patients up to 6 months following hospital discharge and identify 3 subgroups of convalescent patients based on distinct lymphocyte phenotypes, with one subgroup associated with poorer clinical outcome. We propose that alterations in B and T cell function following hospitalisation with COVID-19 could impact longer term immunity and contribute to some persistent symptoms observed in convalescent COVID-19 patients. Funding Provided by UKRI, Lister Institute of Preventative Medicine, The Wellcome Trust, The Kennedy Trust for Rheumatology Research and 3M Global Giving., Graphical Abstract, Shuwa et al examine lymphocyte characteristics in acute and convalescent COVID-19 patients, detailing persistent alterations in lymphocyte phenotype up to 6 months following hospital discharge. In this report they identify 3 subgroups of convalescent patients based on distinct lymphocyte signatures, with one subgroup associated with poorer clinical outcome.

Published

2021

3. Hematopoietic stem and progenitor cells are present in healthy gingiva tissue

Author

Hayley M Bridgeman, Tovah N. Shaw, Conor O'Boyle, Joanne E. Konkel, Kelly Wemyss, John R. Grainger, Siddharth Krishnan, Flora A McClure, and Ian E Prise

Subjects

Male, Myeloid, Immunology, Population, Gingiva, Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, stomatognathic system, Bone Marrow, medicine, Animals, Immunology and Allergy, RNA-Seq, Progenitor cell, education, Myeloid Progenitor Cells, 030304 developmental biology, 0303 health sciences, education.field_of_study, Innate immune system, Monocyte, Mouth Mucosa, Brief Definitive Report, Mucosal Immunology, Hematopoiesis, 3. Good health, Mice, Inbred C57BL, stomatognathic diseases, Haematopoiesis, medicine.anatomical_structure, Female, Bone marrow, Single-Cell Analysis, Stem cell, 030215 immunology

Abstract

Krishnan et al. outline a novel pathway of myeloid cell development in healthy gingiva. They identify HSPCs in noninflamed gingiva tissue, which support the generation of a proportion of the innate immune cells that police this barrier site., Hematopoietic stem cells reside in the bone marrow, where they generate the effector cells that drive immune responses. However, in response to inflammation, some hematopoietic stem and progenitor cells (HSPCs) are recruited to tissue sites and undergo extramedullary hematopoiesis. Contrasting with this paradigm, here we show residence and differentiation of HSPCs in healthy gingiva, a key oral barrier in the absence of overt inflammation. We initially defined a population of gingiva monocytes that could be locally maintained; we subsequently identified not only monocyte progenitors but also diverse HSPCs within the gingiva that could give rise to multiple myeloid lineages. Gingiva HSPCs possessed similar differentiation potentials, reconstitution capabilities, and heterogeneity to bone marrow HSPCs. However, gingival HSPCs responded differently to inflammatory insults, responding to oral but not systemic inflammation. Combined, we highlight a novel pathway of myeloid cell development at a healthy barrier, defining a gingiva-specific HSPC network that supports generation of a proportion of the innate immune cells that police this barrier., Graphical Abstract

Published

2021

4. P058 Persistence of neutrophil abnormalities in COVID-19 convalescence

Author

John R. Grainger, Verena Kästele, Tracy Hussell, Andrew Ustianowski, Alex Horsley, Nawar Diar Bakerly, Tovah N. Shaw, Graham M. Lord, Joanne E. Konkel, Magnus Rattray, Christopher Jagger, Paul Dark, Ling-Pei Ho, Ian N. Bruce, Madhvi Menon, Coronavirus Immune Response, Marc Feldmann, Sean B. Knight, Elizabeth R. Mann, Laurence Pearmain, Thomas O Williams, Ian Prise, Angela Simpson, Timothy Felton, and Saba Khan

Subjects

COVID-19 science, Lung, Coronavirus disease 2019 (COVID-19), business.industry, Convalescence, media_common.quotation_subject, Phenotype determination, Inflammation, Persistence (computer science), medicine.anatomical_structure, Immune system, Rheumatology, Intensive care, EPOSTERS, Immunology, Medicine, Pharmacology (medical), medicine.symptom, business, AcademicSubjects/MED00360, media_common

Abstract

Background/Aims Patients infected with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) may develop acute respiratory inflammation, due to an exaggerated immune response and some develop chronic complications. Neutrophils play a major role in the pathology of inflammatory diseases and have been shown to contribute to lung and vascular damage in COVID-19. Our aim was to establish a relationship between neutrophil phenotype and disease severity and to determine whether neutrophil abnormalities persist in convalescent patients. Methods Peripheral blood samples were obtained from acute COVID-19 patients (n = 74), follow-up (FU) patients discharged following inpatient admission (n = 56), a median of 87 days after discharge, and healthy controls (HCs, n = 22). Patients were stratified by disease severity based on inspired oxygen (FiO2) and admission to intensive care (ICU). Neutrophils were isolated from whole blood by negative selection for phenotyping and functional analysis. PBMC Isolation Tubes were used to quantify and phenotype low density neutrophils (LDNs) within the PBMC fraction. For quantification of reactive oxygen species (ROS) production, isolated neutrophils were incubated with a ROS reactive dye, DHR-123 and stimulated with PMA. All samples were stained and fixed prior to analysis by flow cytometry. Results There was a marked increase in neutrophils expressing the activation and degranulation markers, CD64 (P < 0.0001) and CD63 (P < 0.0001) and a reduction in neutrophils expressing the maturity markers, CD10 (P < 0.0005) and CD101 (P < 0.0005) in patients with acute COVID-19 compared to HCs. Increased frequency of neutrophils expressing CD64 (P < 0.005), CD63 (P < 0.01) and expressing decreased CD101 (P < 0.0001) were also detected in FU patients compared to HCs. Notably, 42.3 ± 4.4% of neutrophils were CD101lo in FU patients, compared to 29.0 ± 3.7% in acute patients and 9.6 ± 4.1% in HCs. These changes were most apparent in FU patients recovering from severe COVID-19 compared to mild or moderate disease. The frequency of LDNs in PBMCs from acute patients was significantly higher than HCs (P < 0.0001), and correlated with disease severity. Similarly, the frequency of LDNs in FU patients was significantly higher than in HCs (P < 0.0005). We found a trend towards higher basal ROS production in acute and FU patients, but a blunted response to PMA stimulated ROS production in neutrophils from acute patients versus HCs (P < 0.0001). Impaired ROS production persisted in FU patients compared to HCs (P < 0.01). Conclusion Circulating neutrophils in acute COVID-19 have an altered phenotype and comprise immature and activated cells. This altered phenotype persisted in convalescence and may contribute to the persistence of symptoms and an increased susceptibility to subsequent infections. Future work will aim to investigate the functional implications of these findings. Disclosure T.O. Williams: None. V. Kästele: None. E.R. Mann: None. S.B. Knight: None. M. Menon: None. C. Jagger: None. S. Khan: None. J.E. Konkel: None. T.N. Shaw: None. M. Rattray: Consultancies; M.R. has a paid consultancy with AstraZeneca. L. Pearmain: None. A. Horsley: None. A. Ustianowski: None. I. Prise: None. N.D. Bakerly: None. P.M. Dark: None. G.M. Lord: Corporate appointments; G.M.L. is cofounder and scientific advisory board member of Gritstone Oncology Inc., which is a public company that develops therapeutic vaccines (primarily for the treatment of cancer). A. Simpson: None. T. Felton: None. L. Ho: None. M. Feldmann: None. I. Bruce: None. J.R. Grainger: None. T. Hussell: None.

Published

2021

5. Rate of replenishment and microenvironment contribute to the sexually dimorphic phenotype and function of peritoneal macrophages

Author

Pieter A Louwe, Philippa Saunders, Rebecca Gentek, Katarina Boufea, Sarah R. Walmsley, David H. Dockrell, Nicholas J Steers, Víctor González-Huici, Stephen J. Jenkins, Calum C. Bain, Marlene Magalhaes-Pinto, Cécile Bénézech, Nizar N. Batada, Tovah N. Shaw, Marc Bajénoff, Douglas A Gibson, Catherine J. Doherty, University of Edinburgh, Columbia University Irving Medical Center (CUIMC), Columbia University [New York], Centre d'Immunologie de Marseille - Luminy (CIML), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), The Lydia Becker Institute of Immunology and Inflammation [Manchester, UK] (Faculty of Biology, Medicine and Health), University of Manchester [Manchester]-Manchester Academic Health Sciences Centre [Manchester, UK], Manchester Collaborative Centre for Inflammation Research, University of Manchester [Manchester], Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Aix Marseille Université (AMU), and DUMENIL, Anita

Subjects

Male, 0301 basic medicine, History, Pathology, CCR2, [SDV]Life Sciences [q-bio], STREPTOCOCCUS-PNEUMONIAE, PATHWAY, Mice, 0302 clinical medicine, Homeostasis, Mice, Knockout, Mice, Inbred BALB C, Sex Characteristics, education.field_of_study, Microglia, Cell Differentiation, General Medicine, Phenotype, Computer Science Applications, 3. Good health, [SDV] Life Sciences [q-bio], medicine.anatomical_structure, Differentiation, 030220 oncology & carcinogenesis, Female, Single-Cell Analysis, Infection, Sex characteristics, EXPRESSION, medicine.medical_specialty, SEX-DIFFERENCES, BONE-MARROW, Immunology, Population, Peritonitis, Biology, Article, Education, MICROGLIA, Mice, Congenic, 03 medical and health sciences, Sex Factors, medicine, Humans, Animals, education, business.industry, Sequence Analysis, RNA, Dendritic Cells, medicine.disease, TISSUE-RESIDENT MACROPHAGES, Mice, Inbred C57BL, Sexual dimorphism, 030104 developmental biology, Macrophages, Peritoneal, RNA, Bone marrow, business, 030215 immunology

Abstract

Macrophages reside in the body cavities where they maintain serosal homeostasis and provide immune surveillance. Peritoneal macrophages are implicated in the etiology of pathologies including peritonitis, endometriosis and metastatic cancer thus understanding the factors that govern their behavior is vital. Using a combination of fate mapping techniques, we have investigated the impact of sex and age on murine peritoneal macrophage differentiation, turnover and function. We demonstrate that the sexually dimorphic replenishment of peritoneal macrophages from the bone marrow, which is high in males and very low in females, is driven by changes in the local microenvironment that arise upon sexual maturation. Population and single cell RNAseq revealed striking dimorphisms in gene expression between male and female peritoneal macrophages that was in part explained by differences in composition of these populations. By estimating the time of residency of different subsets within the cavity and assessing development of dimorphisms with age and in monocytopenic Ccr2–/– mice, we demonstrate that key sex-dependent features of peritoneal macrophages are a function of the differential rate of replenishment from the bone marrow while others are reliant on local microenvironment signals. Importantly, we demonstrate that the dimorphic turnover of peritoneal macrophages contributes to differences in the ability to protect against pneumococcal peritonitis between the sexes. These data highlight the importance of considering both sex and age in susceptibility to inflammatory and infectious diseases.

Published

2020

6. Ongoing exposure to peritoneal dialysis fluid alters resident peritoneal macrophage phenotype and activation propensity

Author

Tara E. Sutherland, Tovah N. Shaw, Rachel Lennon, Sarah E. Herrick, and Dominik Rückerl

Subjects

0301 basic medicine, Male, medicine.medical_treatment, Cell Plasticity, Immunology, 030232 urology & nephrology, Peritonitis, Inflammation, macrophage, Immunophenotyping, Peritoneal dialysis, Mice, 03 medical and health sciences, 0302 clinical medicine, Fibrosis, Dialysis Solutions, medicine, Immunology and Allergy, Animals, Macrophage, tissue resident, Original Research, 030304 developmental biology, 0303 health sciences, business.industry, fibrosis, RC581-607, Macrophage Activation, medicine.disease, glucose degradation product, Phenotype, 3. Good health, 030104 developmental biology, Glucose, peritoneal dialysis, inflammation, 030220 oncology & carcinogenesis, Macrophages, Peritoneal, Female, Immunologic diseases. Allergy, medicine.symptom, business, Homeostasis, Kidney disease

Abstract

Peritoneal dialysis (PD) is a more continuous alternative to haemodialysis, for patients with chronic kidney disease, with considerable initial benefits for survival, patient independence and healthcare costs. However, longterm PD is associated with significant pathology, negating the positive effects over haemodialysis. Importantly, peritonitis and activation of macrophages is closely associated with disease progression and treatment failure. However, recent advances in macrophage biology suggest opposite functions for macrophages of different cellular origins. While monocyte-derived macrophages promote disease progression in some models of fibrosis, tissue resident macrophages have rather been associated with protective roles. Thus, we aimed to identify the relative contribution of tissue resident macrophages to PD induced inflammation in mice. Unexpectedly, we found an incremental loss of homeostatic characteristics, anti-inflammatory and efferocytic functionality in peritoneal resident macrophages, accompanied by enhanced inflammatory responses to external stimuli. Moreover, presence of glucose degradation products within the dialysis fluid led to markedly enhanced inflammation and almost complete disappearance of tissue resident cells. Thus, alterations in tissue resident macrophages may render longterm PD patients sensitive to developing peritonitis and consequently fibrosis/sclerosis.

Published

2020

7. Long-Lasting Alterations in T and B Cell Function in Convalescent COVID-19 Patients

Author

Halima Ali Shuwa, Tovah N. Shaw, S. B. Knight, Flora A. McClure, Kelly Wemyss, Ian Prise, Laurence Permain, Christopher Jagger, D. J. Morgan, S. Khan, O. Brand, E. R. Mann, Andrew Ustianowski, Nawar Diar Bakerly, Paul Dark, Christopher Brightling, Seema Brij, CIRCO Study, T. Felton, A. Simpson, John R. Grainger, Tracy Hussell, Joanne E. Konkel, and Madhvi Menon

Subjects

medicine.medical_specialty, business.industry, T cell, Lymphocyte, Convalescence, media_common.quotation_subject, Respiratory infection, Clinical research, medicine.anatomical_structure, Internal medicine, medicine, Cytotoxic T cell, business, B cell, CD8, media_common

Abstract

Emerging studies indicate that some COVID-19 patients suffer from persistent symptoms including breathlessness and chronic fatigue; however the long-term immune response in these patients presently remains ill-defined. Here we describe the phenotypic and functional characteristics of B and T cells in healthy individuals and individuals with acute or convalescent COVID-19. We report that the alterations in B cell subsets observed in acute COVID-19 patients were largely recovered in convalescent patients. In contrast, T cells from convalescent patients displayed long-term alterations with persistence of a cytotoxic programme evident in CD8+ T cells as well as elevated production of type-1 cytokines and IL-17. Interestingly, B cells from patients with acute COVID-19 displayed an IL-6/ IL-10 cytokine imbalance in response to toll-like receptor activation, skewed towards a pro-inflammatory phenotype. Whereas the frequency of IL-10+ B cells was restored in a subset of convalescent patients, IL-6 production remained elevated. Our data are the first to define long-term alterations in the lymphocyte compartment of previously hospitalized COVID-19 patients, at up to 19 weeks of convalescence, and identify 3 subgroups of convalescent patients based on distinct lymphocyte phenotypes. We propose that alterations in B and T cell function following hospitalisation with COVID-19 could impact long-term immunity and contribute to some persistent symptoms observed in convalescent COVID-19 patients. Funding: This study was funded by the BBSRC (BB/M025977/1 to JEK, BB/S01103X/1 to TNS), by the Lister Institute (Prize Fellowship to JEK), by PTDF (SHS/1327/18 to HAS), The Wellcome Trust (202865/Z/16/Z to TH), The Kennedy Trust for Rheumatology Research (Rapid Response Award to JRG) and Versus Arthritis (FAM and JEK studentship). This report is independent research supported by the North West Lung Centre Charity and the NIHR Manchester Clinical Research Facility at Wythenshawe Hospital. We acknowledge the Manchester Allergy, Respiratory and Thoracic Surgery Biobank for supporting this project and thank the study participants for their contribution. Ethical Approval: Ethical approval obtained from the National Research Ethics Service (REC reference 15/NW/0409 for ManARTS and 18/WA/0368 for NCARC). Informed consent was obtained from each patient, clinical information was extracted from written/electronic medical records including demographic data, presenting symptoms, comorbidities, radiographic findings, vital signs, and laboratory data. Declaration of Interest: None to declare.

Published

2020

8. Infection-Induced Resistance to Experimental Cerebral Malaria Is Dependent Upon Secreted Antibody-Mediated Inhibition of Pathogenic CD8+ T Cell Responses

Author

Tovah N. Shaw, Colette A. Inkson, Ana Villegas-Mendez, David J. Pattinson, Patrick Strangward, Kathryn J. Else, Simon J. Draper, Leo A. H. Zeef, and Kevin N. Couper

Subjects

0301 basic medicine, lcsh:Immunologic diseases. Allergy, T cell, brain, Immunology, T cells, 03 medical and health sciences, 0302 clinical medicine, antibody, parasitic diseases, medicine, Immunology and Allergy, Cytotoxic T cell, Plasmodium berghei, B cell, B cells, biology, biology.organism_classification, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, Immunoglobulin class switching, Cerebral Malaria, biology.protein, cerebral malaria, spleen, Antibody, lcsh:RC581-607, CD8, 030215 immunology

Abstract

Cerebral malaria (CM) is one of the most severe complications of Plasmodium falciparum infection. There is evidence that repeated parasite exposure promotes resistance against CM. However, the immunological basis of this infection-induced resistance remains poorly understood. Here, utilizing the Plasmodium berghei ANKA (PbA) model of experimental cerebral malaria (ECM), we show that three rounds of infection and drug-cure protects against the development of ECM during a subsequent fourth (4X) infection. Exposure-induced resistance was associated with specific suppression of CD8+ T cell activation and CTL-related pathways, which corresponded with the development of heterogeneous atypical B cell populations as well as the gradual infection-induced generation and maintenance of high levels of anti-parasite IgG. Mechanistically, transfer of high-titer anti-parasite IgG did not protect 1X infected mice against ECM and depletion of atypical and regulatory B cells during 4X infection failed to abrogate infection-induced resistance to ECM. However, IgMi mice that were unable to produce secreted antibody, or undergo class switching, during the repeated rounds of infection failed to develop resistance against ECM. The failure of infection-induced protection in IgMi mice was associated with impaired development of atypical B cell populations and the inability to suppress pathogenic CD8+ T cell responses. Our results, therefore, suggest the importance of anti-parasite antibody responses, gradually acquired, and maintained through repeated Plasmodium infections, for modulating the B cell compartment and eventually suppressing memory CD8+ T cell reactivation to establish infection-induced resistance to ECM.

Published

2019

9. Antibiotics induce sustained dysregulation of intestinal T cell immunity by perturbing macrophage homeostasis

Author

Anna Andrusaite, Simon Milling, Xuhang Li, Shabhonam Caim, Lindsay J. Hall, Nicholas A. Scott, Allison J. Bancroft, James P. R. Connolly, Gwénaëlle Le Gall, Charlotte Leclaire, Carolyn A. Thomson, Cristina Alcon-Giner, Elizabeth R. Mann, Hannah M. Wessel, Daniel A. Peterson, Ping Wang, Melissa A. E. Lawson, Mark A. Travis, Tovah N. Shaw, Alberto Bravo-Blas, Peter Andersen, Verena Kästele, Andrew J. Roe, Allan McI. Mowat, and Richard K. Grencis

Subjects

0301 basic medicine, biology, business.industry, T cell, Inflammation, General Medicine, Gut flora, medicine.disease, biology.organism_classification, Inflammatory bowel disease, digestive system, 3. Good health, Proinflammatory cytokine, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Immunology, medicine, Macrophage, medicine.symptom, business, Macrophage homeostasis, Dysbiosis

Abstract

Macrophages in the healthy intestine are highly specialized and usually respond to the gut microbiota without provoking an inflammatory response. A breakdown in this tolerance leads to inflammatory bowel disease (IBD), but the mechanisms by which intestinal macrophages normally become conditioned to promote microbial tolerance are unclear. Strong epidemiological evidence linking disruption of the gut microbiota by antibiotic use early in life to IBD indicates an important role for the gut microbiota in modulating intestinal immunity. Here, we show that antibiotic use causes intestinal macrophages to become hyperresponsive to bacterial stimulation, producing excess inflammatory cytokines. Re-exposure of antibiotic-treated mice to conventional microbiota induced a long-term, macrophage-dependent increase in inflammatory T helper 1 (TH1) responses in the colon and sustained dysbiosis. The consequences of this dysregulated macrophage activity for T cell function were demonstrated by increased susceptibility to infections requiring TH17 and TH2 responses for clearance (bacterial Citrobacter rodentium and helminth Trichuris muris infections), corresponding with increased inflammation. Short-chain fatty acids (SCFAs) were depleted during antibiotic administration; supplementation of antibiotics with the SCFA butyrate restored the characteristic hyporesponsiveness of intestinal macrophages and prevented T cell dysfunction. Butyrate altered the metabolic behavior of macrophages to increase oxidative phosphorylation and also promoted alternative macrophage activation. In summary, the gut microbiota is essential to maintain macrophage-dependent intestinal immune homeostasis, mediated by SCFA-dependent pathways. Oral antibiotics disrupt this process to promote sustained T cell-mediated dysfunction and increased susceptibility to infections, highlighting important implications of repeated broad-spectrum antibiotic use.

Published

2018

10. Targeting the IL33–NLRP3 axis improves therapy for experimental cerebral malaria

Author

Sheena M. Cruickshank, Emma Winter, Foo Y. Liew, Alister Craig, Tovah N. Shaw, Stuart M. Allan, Kevin N. Couper, Jack Barrington, Douglas T. Golenbock, Syed Murtuza Baker, Manuel Garcia Albornoz, Michael J. Haley, Te-Chen Tzeng, Rebecca Dookie, Leo Zeef, David Brough, and Patrick Strangward

Subjects

0301 basic medicine, Male, medicine.medical_treatment, Interleukin-1beta, Pharmacology, Mice, Drug Delivery Systems, Malaria, Falciparum, media_common, Multidisciplinary, Microglia, biology, Hemozoin, Brain, Inflammasome, Biological Sciences, medicine.anatomical_structure, Manchester Institute for Collaborative Research on Ageing, Cerebral Malaria, IL33, Female, medicine.drug, Drug, Hemeproteins, ResearchInstitutes_Networks_Beacons/MICRA, qw_568, media_common.quotation_subject, Plasmodium falciparum, malaria, Malaria, Cerebral, 03 medical and health sciences, Antimalarials, NLRP3, inflammasome, NLR Family, Pyrin Domain-Containing 3 Protein, medicine, Animals, Neuroinflammation, qu_107, Chemotherapy, business.industry, Gene Expression Profiling, Macrophages, biology.organism_classification, Interleukin-33, wc_750, Disease Models, Animal, 030104 developmental biology, inflammation, business, Transcriptome

Abstract

Cerebral malaria (CM) is a serious neurological complication caused by Plasmodium falciparum infection. Currently, the only treatment for CM is the provision of antimalarial drugs; however, such treatment by itself often fails to prevent death or development of neurological sequelae. To identify potential improved treatments for CM, we performed a nonbiased whole-brain transcriptomic time-course analysis of antimalarial drug chemotherapy of murine experimental CM (ECM). Bioinformatics analyses revealed IL33 as a critical regulator of neuroinflammation and cerebral pathology that is down-regulated in the brain during fatal ECM and in the acute period following treatment of ECM. Consistent with this, administration of IL33 alongside antimalarial drugs significantly improved the treatment success of established ECM. Mechanistically, IL33 treatment reduced inflammasome activation and IL1β production in microglia and intracerebral monocytes in the acute recovery period following treatment of ECM. Moreover, treatment with the NLRP3-inflammasome inhibitor MCC950 alongside antimalarial drugs phenocopied the protective effect of IL33 therapy in improving the recovery from established ECM. We further showed that IL1β release from macrophages was stimulated by hemozoin and antimalarial drugs and that this was inhibited by MCC950. Our results therefore demonstrate that manipulation of the IL33–NLRP3 axis may be an effective therapy to suppress neuroinflammation and improve the efficacy of antimalarial drug treatment of CM.

Published

2018

11. Parasite-Specific CD4 + IFN-γ + IL-10 + T Cells Distribute within Both Lymphoid and Nonlymphoid Compartments and Are Controlled Systemically by Interleukin-27 and ICOS during Blood-Stage Malaria Infection

Author

Colette A. Inkson, J. Brian de Souza, Ana Villegas-Mendez, Kevin N. Couper, Patrick Strangward, and Tovah N. Shaw

Subjects

0301 basic medicine, Adoptive cell transfer, biology, T cell, Immunology, Priming (immunology), biology.organism_classification, Microbiology, Virology, 3. Good health, Green fluorescent protein, Cell biology, 03 medical and health sciences, Interleukin 10, 030104 developmental biology, 0302 clinical medicine, Infectious Diseases, Immune system, medicine.anatomical_structure, medicine, Parasitology, Interferon gamma, Plasmodium yoelii, 030215 immunology, medicine.drug

Abstract

Immune-mediated pathology in interleukin-10 (IL-10)-deficient mice during blood-stage malaria infection typically manifests in nonlymphoid organs, such as the liver and lung. Thus, it is critical to define the cellular sources of IL-10 in these sensitive nonlymphoid compartments during infection. Moreover, it is important to determine if IL-10 production is controlled through conserved or disparate molecular programs in distinct anatomical locations during malaria infection, as this may enable spatiotemporal tuning of the regulatory immune response. In this study, using dual gamma interferon (IFN-γ)–yellow fluorescent protein (YFP) and IL-10–green fluorescent protein (GFP) reporter mice, we show that CD4 + YFP + T cells are the major source of IL-10 in both lymphoid and nonlymphoid compartments throughout the course of blood-stage Plasmodium yoelii infection. Mature splenic CD4 + YFP + GFP + T cells, which preferentially expressed high levels of CCR5, were capable of migrating to and seeding the nonlymphoid tissues, indicating that the systemically distributed host-protective cells have a common developmental history. Despite exhibiting comparable phenotypes, CD4 + YFP + GFP + T cells from the liver and lung produced significantly larger quantities of IL-10 than their splenic counterparts, showing that the CD4 + YFP + GFP + T cells exert graded functions in distinct tissue locations during infection. Unexpectedly, given the unique environmental conditions within discrete nonlymphoid and lymphoid organs, we show that IL-10 production by CD4 + YFP + T cells is controlled systemically during malaria infection through IL-27 receptor signaling that is supported after CD4 + T cell priming by ICOS signaling. The results in this study substantially improve our understanding of the systemic IL-10 response to malaria infection, particularly within sensitive nonlymphoid organs.

Published

2016

12. IFN-γ–Producing CD4+ T Cells Promote Experimental Cerebral Malaria by Modulating CD8+ T Cell Accumulation within the Brain

Author

Julius C. R. Hafalla, Emily Gwyer Findlay, Ana Villegas-Mendez, Kevin N. Couper, Eleanor M. Riley, J. Brian de Souza, Tovah N. Shaw, Rachel Greig, Daniel G. Blount, Jason S. Stumhofer, and Christopher A. Hunter

Subjects

CD4-Positive T-Lymphocytes, Male, Adoptive cell transfer, Plasmodium berghei, T cell, Immunology, Malaria, Cerebral, CD8-Positive T-Lymphocytes, Biology, Article, Interferon-gamma, Mice, Interleukin 21, Cell Movement, parasitic diseases, medicine, Animals, Immunology and Allergy, CXCL10, Cytotoxic T cell, Genetic Predisposition to Disease, Interferon gamma, Mice, Knockout, Brain, biology.organism_classification, Adoptive Transfer, Immunity, Innate, Cell biology, Mice, Inbred C57BL, Disease Models, Animal, medicine.anatomical_structure, Female, CD8, medicine.drug

Abstract

It is well established that IFN-γ is required for the development of experimental cerebral malaria (ECM) during Plasmodium berghei ANKA infection of C57BL/6 mice. However, the temporal and tissue-specific cellular sources of IFN-γ during P. berghei ANKA infection have not been investigated, and it is not known whether IFN-γ production by a single cell type in isolation can induce cerebral pathology. In this study, using IFN-γ reporter mice, we show that NK cells dominate the IFN-γ response during the early stages of infection in the brain, but not in the spleen, before being replaced by CD4+ and CD8+ T cells. Importantly, we demonstrate that IFN-γ–producing CD4+ T cells, but not innate or CD8+ T cells, can promote the development of ECM in normally resistant IFN-γ−/− mice infected with P. berghei ANKA. Adoptively transferred wild-type CD4+ T cells accumulate within the spleen, lung, and brain of IFN-γ−/− mice and induce ECM through active IFN-γ secretion, which increases the accumulation of endogenous IFN-γ−/− CD8+ T cells within the brain. Depletion of endogenous IFN-γ−/− CD8+ T cells abrogates the ability of wild-type CD4+ T cells to promote ECM. Finally, we show that IFN-γ production, specifically by CD4+ T cells, is sufficient to induce expression of CXCL9 and CXCL10 within the brain, providing a mechanistic basis for the enhanced CD8+ T cell accumulation. To our knowledge, these observations demonstrate, for the first time, the importance of and pathways by which IFN-γ–producing CD4+ T cells promote the development of ECM during P. berghei ANKA infection.

Published

2012

13. CD27 expression discriminates between regulatory and non-regulatory cells after expansion of human peripheral blood CD4+ CD25+cells

Author

J. S. Hill Gaston, Richard C. Duggleby, Lorna B. Jarvis, Tovah N. Shaw, and Gurman Kaur

Subjects

education.field_of_study, medicine.diagnostic_test, Cell growth, Immunology, Population, FOXP3, hemic and immune systems, chemical and pharmacologic phenomena, Biology, medicine.disease_cause, Flow cytometry, Autoimmunity, Cell biology, Immunophenotyping, Cell culture, medicine, Immunology and Allergy, IL-2 receptor, education

Abstract

It is clear that regulatory T cells (Treg) have an important role in preventing autoimmunity and modulating responses to pathogens. Full characterization of Treg cell function in human patients would be greatly facilitated by practical methods for expanding Treg in vitro. Methods for expansion have been reported but whether expression of surface and intracellular markers associated with freshly isolated Treg following expansion correlates with the maintenance of function is unclear. Our aim was to investigate the various methods of expansion and to correlate regulatory activity with expression of these markers. We show that, of the markers associated with freshly isolated Treg, only CD27 expression correlated with regulatory activity and could be used to isolate cells with regulatory activity from lines expanded from CD4+ CD25+ cells. Also, cells expressing high levels of the transcription factor forkhead box P3 (Foxp3) were confined to the CD27+ population within these lines. Expression of CD27 by cells in lines expanded from CD4+ CD25- cells varied depending on the stimulus used for expansion, but these lines did not have significant regulatory activity even when the CD27+ cells were tested. Analysis of synovial CD4+ CD25+ cells from reactive arthritis patients revealed that they were predominantly CD27 positive. This also applied to CD25(high) and CD25(intermediate) CD4+ cells, despite their reported different abilities to regulate. We conclude that, whilst CD27 is useful for identifying Treg in the cell lines obtained after expansion of CD4+ CD25+ cells, its expression may not reliably identify the Treg cell population in other T-cell populations such as those found in joints.

Published

2007

14. The subcellular location of ovalbumin in Plasmodium berghei blood stages influences the magnitude of T-cell responses

Author

Kevin N. Couper, Hans Kroeze, Shahid M. Khan, Severine Chevalley-Maurel, Chris J. Janse, Jing-wen Lin, Pascale Bouchier, Takeshi Annoura, Aurélie Fougère, Tovah N. Shaw, and Blandine Franke-Fayard

Subjects

Ovalbumin, Plasmodium berghei, T cell, T-Lymphocytes, Immunology, Spleen, Microbiology, Mice, Antigen, medicine, Animals, Regulation of gene expression, Host Response and Inflammation, biology, Organisms, Genetically Modified, respiratory system, biology.organism_classification, Cell biology, Malaria, Protein Transport, Infectious Diseases, medicine.anatomical_structure, Gene Expression Regulation, biology.protein, Parasitology, Female, mCherry, CD8

Abstract

Model antigens are frequently introduced into pathogens to study determinants that influence T-cell responses to infections. To address whether an antigen's subcellular location influences the nature and magnitude of antigen-specific T-cell responses, we generated Plasmodium berghei parasites expressing the model antigen ovalbumin (OVA) either in the parasite cytoplasm or on the parasitophorous vacuole membrane (PVM). For cytosolic expression, OVA alone or conjugated to mCherry was expressed from a strong constitutive promoter ( OVA hsp70 or OVA :: mCherry hsp70 ); for PVM expression, OVA was fused to HEP17/EXP1 ( OVA :: Hep17 hep17 ). Unexpectedly, OVA expression in OVA hsp70 parasites was very low, but when OVA was fused to mCherry ( OVA :: mCherry hsp70 ), it was highly expressed. OVA expression in OVA :: Hep17 hep17 parasites was strong but significantly less than that in OVA :: mCherry hsp70 parasites. These transgenic parasites were used to examine the effects of antigen subcellular location and expression level on the development of T-cell responses during blood-stage infections. While all OVA-expressing parasites induced activation and proliferation of OVA-specific CD8 + T cells (OT-I) and CD4 + T cells (OT-II), the level of activation varied: OVA :: Hep17 hep17 parasites induced significantly stronger splenic and intracerebral OT-I and OT-II responses than those of OVA :: mCherry hsp70 parasites, but OVA :: mCherry hsp70 parasites promoted stronger OT-I and OT-II responses than those of OVA hsp70 parasites. Despite lower OVA expression levels, OVA :: Hep17 hep17 parasites induced stronger T-cell responses than those of OVA :: mCherry hsp70 parasites. These results indicate that unconjugated cytosolic OVA is not stably expressed in Plasmodium parasites and, importantly, that its cellular location and expression level influence both the induction and magnitude of parasite-specific T-cell responses. These parasites represent useful tools for studying the development and function of antigen-specific T-cell responses during malaria infection.

Published

2014

15. Intracellular Staining for Phosphorylated STAT4 and STAT5 in Mouse Splenocytes

Author

Eleanor M. Riley, Seen-Wai Lavelle, J. Brian de Souza, Emily Gwyer Findlay, Christopher A. Hunter, Ana Villegas-Mendez, Christiaan J. M. Saris, Kevin N. Couper, and Tovah N. Shaw

Subjects

biology, medicine.diagnostic_test, Chemistry, Strategy and Management, Mechanical Engineering, Metals and Alloys, Molecular biology, Industrial and Manufacturing Engineering, Flow cytometry, Intracellular staining, biology.protein, medicine, Splenocyte, Phosphorylation, STAT4, Immunostaining, STAT5

Published

2014

16. IL-27 receptor signalling regulates CD4+ T cell chemotactic responses during infection

Author

Colette A. Inkson, Eleanor M. Riley, Emily Gwyer Findlay, J. Brian de Souza, Christopher A. Hunter, Tovah N. Shaw, Christiaan J. M. Saris, Ana Villegas-Mendez, and Kevin N. Couper

Subjects

CD4-Positive T-Lymphocytes, Receptors, CCR5, Plasmodium berghei, T cell, Immunology, CCL5, Article, Interleukin 21, Mice, parasitic diseases, medicine, Immunology and Allergy, Cytotoxic T cell, Animals, Receptors, Interleukin-10, IL-2 receptor, Receptors, Cytokine, Antigen-presenting cell, Chemokine CCL4, Chemokine CCL5, Inflammation, Chemistry, Interleukin-12 Subunit p40, ZAP70, Interleukins, T cell chemotaxis, Receptors, Interleukin, Th1 Cells, Cell biology, Malaria, Mice, Inbred C57BL, medicine.anatomical_structure, Interleukin-2, Signal Transduction

Abstract

IL-27 exerts pleiotropic suppressive effects on naive and effector T cell populations during infection and inflammation. Surprisingly, however, the role of IL-27 in restricting or shaping effector CD4+ T cell chemotactic responses, as a mechanism to reduce T cell–dependent tissue inflammation, is unknown. In this study, using Plasmodium berghei NK65 as a model of a systemic, proinflammatory infection, we demonstrate that IL-27R signaling represses chemotaxis of infection-derived splenic CD4+ T cells in response to the CCR5 ligands, CCL4 and CCL5. Consistent with these observations, CCR5 was expressed on significantly higher frequencies of splenic CD4+ T cells from malaria-infected, IL-27R–deficient (WSX-1−/−) mice than from infected wild-type mice. We find that IL-27 signaling suppresses splenic CD4+ T cell CCR5-dependent chemotactic responses during infection by restricting CCR5 expression on CD4+ T cell subtypes, including Th1 cells, and also by controlling the overall composition of the CD4+ T cell compartment. Diminution of the Th1 response in infected WSX-1−/− mice in vivo by neutralization of IL-12p40 attenuated CCR5 expression by infection-derived CD4+ T cells and also reduced splenic CD4+ T cell chemotaxis toward CCL4 and CCL5. These data reveal a previously unappreciated role for IL-27 in modulating CD4+ T cell chemotactic pathways during infection, which is related to its capacity to repress Th1 effector cell development. Thus, IL-27 appears to be a key cytokine that limits the CCR5-CCL4/CCL5 axis during inflammatory settings.

Published

2013

17. IL-27 receptor signalling restricts the formation of pathogenic, terminally differentiated Th1 cells during malaria infection by repressing IL-12 dependent signals

Author

Seen Wai Lavelle, Tovah N. Shaw, Eleanor M. Riley, Nico van Rooijen, Ana Villegas-Mendez, Christiaan J. M. Saris, Christopher A. Hunter, J. Brian de Souza, Kevin N. Couper, Emily Gwyer Findlay, Molecular cell biology and Immunology, and CCA - Immuno-pathogenesis

Subjects

Interleukin-27, Cellular differentiation, Interleukin-10 Receptor alpha Subunit, Apoptosis, Pathogenesis, Protozoology, Mice, 0302 clinical medicine, Biology (General), Malaria, Falciparum, Receptors, Immunologic, Immune Response, Mice, Knockout, 0303 health sciences, Effector, FOXP3, Cell Differentiation, Forkhead Transcription Factors, Interleukin-12, Interleukin-10, 3. Good health, Cell biology, Host-Pathogen Interaction, Interleukin 10, medicine.anatomical_structure, Interleukin 12, Signal Transduction, Research Article, medicine.drug, Interleukin 2, QH301-705.5, Cell Survival, Immune Cells, T cell, Plasmodium falciparum, Immunology, Immunopathology, Biology, Microbiology, Protozoan Classification, Interferon-gamma, 03 medical and health sciences, Virology, Genetics, medicine, Animals, Lectins, C-Type, Receptors, Cytokine, Molecular Biology, Cell Proliferation, 030304 developmental biology, Inflammation, Cell growth, Immunity, Immunoregulation, Immune Defense, Receptors, Interleukin, RC581-607, Th1 Cells, Mice, Inbred C57BL, Interleukin-2, Parasitology, Immunologic diseases. Allergy, T-Box Domain Proteins, Interleukin-1, 030215 immunology

Abstract

The IL-27R, WSX-1, is required to limit IFN-γ production by effector CD4+ T cells in a number of different inflammatory conditions but the molecular basis of WSX-1-mediated regulation of Th1 responses in vivo during infection has not been investigated in detail. In this study we demonstrate that WSX-1 signalling suppresses the development of pathogenic, terminally differentiated (KLRG-1+) Th1 cells during malaria infection and establishes a restrictive threshold to constrain the emergent Th1 response. Importantly, we show that WSX-1 regulates cell-intrinsic responsiveness to IL-12 and IL-2, but the fate of the effector CD4+ T cell pool during malaria infection is controlled primarily through IL-12 dependent signals. Finally, we show that WSX-1 regulates Th1 cell terminal differentiation during malaria infection through IL-10 and Foxp3 independent mechanisms; the kinetics and magnitude of the Th1 response, and the degree of Th1 cell terminal differentiation, were comparable in WT, IL-10R1−/− and IL-10−/− mice and the numbers and phenotype of Foxp3+ cells were largely unaltered in WSX-1−/− mice during infection. As expected, depletion of Foxp3+ cells did not enhance Th1 cell polarisation or terminal differentiation during malaria infection. Our results significantly expand our understanding of how IL-27 regulates Th1 responses in vivo during inflammatory conditions and establishes WSX-1 as a critical and non-redundant regulator of the emergent Th1 effector response during malaria infection., Author Summary The cytokine interleukin 27 (IL-27), a member of the IL-12 family, is produced by cells of the innate immune system and has been shown to exert mainly suppressive effects during a wide range of inflammatory conditions, including malaria infection, where it suppresses the development of CD4+ T cell-dependent immunopathology. In this study we show that IL-27 suppresses the production of IFN-gamma by CD4+ T cells during blood stage malaria infection by preventing the development of terminally differentiated Th1 cells. We investigated the molecular mechanisms by which IL-27 inhibits the formation of terminally differentiated Th1 cells and found that it does so specifically by restricting IL-12 signals. Importantly, we demonstrate that IL-27 mediates its regulatory effects on the Th1 response through IL-10 and Foxp3+ regulatory T cell independent mechanisms. Thus, we have identified a new pathway though which IL-27 signalling regulates the size and quality of the Th1 response during malaria infection, which we believe will have relevance to many other pro-inflammatory conditions. Manipulation of the IL-27 pathway may therefore represent an amenable therapeutic approach during chronic inflammatory disorders.

Published

2013

18. Heterogeneous and tissue-specific regulation of effector T cell responses by IFN-gamma during Plasmodium berghei ANKA infection

Author

Eleanor M. Riley, Tovah N. Shaw, Kevin N. Couper, Rachel Greig, Linda Murungi, J. Brian de Souza, Julius C. R. Hafalla, and Ana Villegas-Mendez

Subjects

CD4-Positive T-Lymphocytes, Contraction (grammar), Plasmodium berghei, T cell, Immunology, Cell Separation, CD8-Positive T-Lymphocytes, Lymphocyte Activation, Article, Interleukin 21, Interferon-gamma, Mice, Cell Movement, parasitic diseases, medicine, Immunology and Allergy, Cytotoxic T cell, Animals, Mice, Knockout, Lung, biology, Effector, Reverse Transcriptase Polymerase Chain Reaction, biology.organism_classification, Flow Cytometry, Cell biology, Malaria, Mice, Inbred C57BL, medicine.anatomical_structure, CD8

Abstract

IFN-γ and T cells are both required for the development of experimental cerebral malaria during Plasmodium berghei ANKA infection. Surprisingly, however, the role of IFN-γ in shaping the effector CD4+ and CD8+ T cell response during this infection has not been examined in detail. To address this, we have compared the effector T cell responses in wild-type and IFN-γ−/− mice during P. berghei ANKA infection. The expansion of splenic CD4+ and CD8+ T cells during P. berghei ANKA infection was unaffected by the absence of IFN-γ, but the contraction phase of the T cell response was significantly attenuated. Splenic T cell activation and effector function were essentially normal in IFN-γ−/− mice; however, the migration to, and accumulation of, effector CD4+ and CD8+ T cells in the lung, liver, and brain was altered in IFN-γ−/− mice. Interestingly, activation and accumulation of T cells in various nonlymphoid organs was differently affected by lack of IFN-γ, suggesting that IFN-γ influences T cell effector function to varying levels in different anatomical locations. Importantly, control of splenic T cell numbers during P. berghei ANKA infection depended on active IFN-γ–dependent environmental signals—leading to T cell apoptosis—rather than upon intrinsic alterations in T cell programming. To our knowledge, this is the first study to fully investigate the role of IFN-γ in modulating T cell function during P. berghei ANKA infection and reveals that IFN-γ is required for efficient contraction of the pool of activated T cells.

Published

2011