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SOCS1 and regulation of regulatory T cells plasticity
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نویسنده
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takahashi r. ,yoshimura a.
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منبع
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journal of immunology research - 2014 - دوره : 2014 - شماره : 0
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چکیده
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Several reports have suggested that natural regulatory t cells (tregs) lose forkhead box p3 (foxp3) expression and suppression activity under certain inflammatory conditions. treg plasticity has been studied because it may be associated with the pathogenesis of autoimmunity. some studies showed that a minor uncommitted foxp3+ t cell population,which lacks hypomethylation at treg-specific demethylation regions (tsdrs),may convert to effector/helper t cells. suppressor of cytokine signaling 1 (socs1),a negative regulator of cytokine signaling,has been reported to play an important role in treg cell integrity and function by protecting the cells from excessive inflammatory cytokines. in this review,we discuss treg plasticity and maintenance of suppression functions in both physiological and pathological settings. in addition,we discuss molecular mechanisms of maintaining treg plasticity by socs1 and other molecules. such information will be useful for therapy of autoimmune diseases and reinforcement of antitumor immunity. © 2014 reiko takahashi and akihiko yoshimura.
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آدرس
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division of rheumatology,department of internal medicine,national defense medical college,3-2 namiki,tokorozawa,saitama,japan,department of microbiology and immunology,keio university school of medicine,35 shinanomachi,shinjuku-ku,tokyo,japan,japan science and technology agency (jst),crest,chiyoda-ku, Japan, department of microbiology and immunology,keio university school of medicine,35 shinanomachi,shinjuku-ku,tokyo,japan,japan science and technology agency (jst),crest,chiyoda-ku, Japan
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Authors
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