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Rescooped by Gilbert C FAURE from Cancer Immunotherapy Review and Collection
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Peripheral regulatory T lymphocytes recirculating to the thymus suppress the development of their precursors

Peripheral regulatory T lymphocytes recirculating to the thymus suppress the development of their precursors | Immunology | Scoop.it

Most T lymphocytes, including regulatory T cells (Treg cells), differentiate in the thymus. The age-dependent involution of this organ leads to decreasing production of T cells. Here we found that the output of new Treg cells from the thymus decreased substantially more than that of conventional T cells. Peripheral mouse and human Treg cells recirculated back to the thymus, where they constituted a large proportion of the pool of Treg cells and displayed an activated and differentiated phenotype. In the thymus, the recirculating cells exerted their regulatory function by inhibiting interleukin 2 (IL-2)-dependent de novo differentiation of Treg cells. Thus, Treg cell development is controlled by a negative feedback loop in which mature progeny cells return to the thymus and restrain development of precursors of Treg cells.


Via Krishan Maggon
Krishan Maggon 's curator insight, May 10, 2015 10:10 AM

NATURE IMMUNOLOGY | ARTICLE

Peripheral regulatory T lymphocytes recirculating to the thymus suppress the development of their precursorsNicolas Thiault,Julie Darrigues,Véronique Adoue,Marine Gros,Bénédicte Binet,Corine Perals,Bertrand Leobon,Nicolas Fazilleau,Olivier P Joffre,Ellen A Robey,Joost P M van Meerwijk& Paola RomagnoliAffiliationsContributionsCorresponding authorsNature Immunology (2015) doi:10.1038/ni.3150Received 18 December 2014 Accepted 17 March 2015 Published online 04 May 2015
Rescooped by Gilbert C FAURE from Multiple sclerosis New Drugs Review
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Multiple Sclerosis and T Lymphocytes: An Entangled Story - Online First - Springer

Multiple Sclerosis and T Lymphocytes: An Entangled Story - Online First - Springer | Immunology | Scoop.it

Multiple Sclerosis and T Lymphocytes: An Entangled Story - 

 

Abstract

Multiple sclerosis (MS) is the prototypic inflammatory disease of the central nervous system (CNS) characterized by multifocal areas of demyelination, axonal damage, activation of glial cells, and immune cell infiltration. Despite intensive years of research, the etiology of this neurological disorder remains elusive. Nevertheless, the abundance of immune cells such as T lymphocytes and their products in CNS lesions of MS patients supports the notion that MS is an immune-mediated disorder. An important body of evidence gathered from MS animal models such as experimental autoimmune encephalomyelitis (EAE), points to the central contribution of CD4 T lymphocytes in disease pathogenesis. Both Th1 (producing interferon-γ) and Th17 (producing interleukin 17) CD4 T lymphocytes targeting CNS self-antigens have been implicated in MS and EAE pathobiology. Moreover, several publications suggest that CD8 T lymphocytes also participate in the development of MS lesions. The migration of activated T lymphocytes from the periphery into the CNS has been identified as a crucial step in the formation of MS lesions. Several factors promote such T cell extravasation including: molecules (e.g., cell adhesion molecules) implicated in the T cell-blood brain barrier interaction, and chemokines produced by neural cells. Finally, once in the CNS, T lymphocytes need to be reactivated by local antigen presenting cells prior to enter the parenchyma where they can initiate damage. Further investigations will be necessary to elucidate the impact of environmental factors (e.g., gut microbiota) and CNS intrinsic properties (e.g., microglial activation) on this inflammatory neurological disease.


Via Krishan Maggon
Krishan Maggon 's curator insight, May 7, 2015 1:51 AM
Journal of Neuroimmune PharmacologyMay 2015Date: 07 May 2015Multiple Sclerosis and T Lymphocytes: An Entangled StoryLaurine Legroux, Nathalie Arbour