CD8+T Cells Induce Fatal Brainstem Pathology during Cerebral Malaria via Luminal Antigen-Specific Engagement of Brain Vasculature

Nayak, Debasis

Please use this identifier to cite or link to this item: https://dspace.iiti.ac.in/handle/123456789/4051

Title:	CD8+T Cells Induce Fatal Brainstem Pathology during Cerebral Malaria via Luminal Antigen-Specific Engagement of Brain Vasculature
Authors:	Nayak, Debasis
Keywords:	CD31 antigen;CD45 antigen;gamma interferon;intercellular adhesion molecule 1;lymphocyte function associated antigen 1;tight junction protein;vascular cell adhesion molecule 1;very late activation antigen 4;animal tissue;Article;blood brain barrier;bone marrow;brain blood vessel;brain hernia;brain stem;brain water;cause of death;CD4+ T lymphocyte;CD8+ T lymphocyte;cerebral malaria;controlled study;flow cytometry;immunohistochemistry;immunopathogenesis;innate immunity;mouse;nerve cell necrosis;nonhuman;polymerase chain reaction;protein expression;survival rate;animal;blood vessel;brain stem;CD8+ T lymphocyte;cerebral malaria;disease model;immunology;pathology;Plasmodium berghei;transgenic mouse;Animals;Blood Vessels;Blood-Brain Barrier;Brain Stem;CD8-Positive T-Lymphocytes;Disease Models, Animal;Flow Cytometry;Immunohistochemistry;Malaria, Cerebral;Mice;Mice, Transgenic;Plasmodium berghei
Issue Date:	2016
Publisher:	Public Library of Science
Citation:	Swanson, P. A., Hart, G. T., Russo, M. V., Nayak, D., Yazew, T., Peña, M., . . . McGavern, D. B. (2016). CD8+T cells induce fatal brainstem pathology during cerebral malaria via luminal antigen-specific engagement of brain vasculature. PLoS Pathogens, 12(12) doi:10.1371/journal.ppat.1006022
Abstract:	Cerebral malaria (CM) is a severe complication of Plasmodium falciparum infection that results in thousands of deaths each year, mostly in African children. The in vivo mechanisms underlying this fatal condition are not entirely understood. Using the animal model of experimental cerebral malaria (ECM), we sought mechanistic insights into the pathogenesis of CM. Fatal disease was associated with alterations in tight junction proteins, vascular breakdown in the meninges / parenchyma, edema, and ultimately neuronal cell death in the brainstem, which is consistent with cerebral herniation as a cause of death. At the peak of ECM, we revealed using intravital two-photon microscopy that myelomonocytic cells and parasite-specific CD8+T cells associated primarily with the luminal surface of CNS blood vessels. Myelomonocytic cells participated in the removal of parasitized red blood cells (pRBCs) from cerebral blood vessels, but were not required for the disease. Interestingly, the majority of disease-inducing parasite-specific CD8+T cells interacted with the lumen of brain vascular endothelial cells (ECs), where they were observed surveying, dividing, and arresting in a cognate peptide-MHC I dependent manner. These activities were critically dependent on IFN-γ, which was responsible for activating cerebrovascular ECs to upregulate adhesion and antigen-presenting molecules. Importantly, parasite-specific CD8+T cell interactions with cerebral vessels were impaired in chimeric mice rendered unable to present EC antigens on MHC I, and these mice were in turn resistant to fatal brainstem pathology. Moreover, anti-adhesion molecule (LFA-1 / VLA-4) therapy prevented fatal disease by rapidly displacing luminal CD8+T cells from cerebrovascular ECs without affecting extravascular T cells. These in vivo data demonstrate that parasite-specific CD8+T cell-induced fatal vascular breakdown and subsequent neuronal death during ECM is associated with luminal, antigen-dependent interactions with cerebrovasculature. © 2016 Meuris et al.
URI:	https://doi.org/10.1371/journal.ppat.1006022 https://dspace.iiti.ac.in/handle/123456789/4051
ISSN:	1553-7366
Type of Material:	Journal Article
Appears in Collections:	Department of Biosciences and Biomedical Engineering

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