| Literature DB >> 26206937 |
Bernice Lo1, Kejian Zhang2, Wei Lu3, Lixin Zheng3, Qian Zhang4, Chrysi Kanellopoulou3, Yu Zhang4, Zhiduo Liu5, Jill M Fritz3, Rebecca Marsh6, Ammar Husami7, Diane Kissell7, Shannon Nortman7, Vijaya Chaturvedi6, Hilary Haines8, Lisa R Young9, Jun Mo10, Alexandra H Filipovich6, Jack J Bleesing6, Peter Mustillo11, Michael Stephens12, Cesar M Rueda13, Claire A Chougnet13, Kasper Hoebe13, Joshua McElwee14, Jason D Hughes14, Elif Karakoc-Aydiner15, Helen F Matthews3, Susan Price3, Helen C Su4, V Koneti Rao3, Michael J Lenardo1, Michael B Jordan16.
Abstract
Mutations in the LRBA gene (encoding the lipopolysaccharide-responsive and beige-like anchor protein) cause a syndrome of autoimmunity, lymphoproliferation, and humoral immune deficiency. The biological role of LRBA in immunologic disease is unknown. We found that patients with LRBA deficiency manifested a dramatic and sustained improvement in response to abatacept, a CTLA4 (cytotoxic T lymphocyte antigen-4)-immunoglobulin fusion drug. Clinical responses and homology of LRBA to proteins controlling intracellular trafficking led us to hypothesize that it regulates CTLA4, a potent inhibitory immune receptor. We found that LRBA colocalized with CTLA4 in endosomal vesicles and that LRBA deficiency or knockdown increased CTLA4 turnover, which resulted in reduced levels of CTLA4 protein in FoxP3(+) regulatory and activated conventional T cells. In LRBA-deficient cells, inhibition of lysosome degradation with chloroquine prevented CTLA4 loss. These findings elucidate a mechanism for CTLA4 trafficking and control of immune responses and suggest therapies for diseases involving the CTLA4 pathway.Entities:
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Year: 2015 PMID: 26206937 DOI: 10.1126/science.aaa1663
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728