Please use this identifier to cite or link to this item: http://hdl.handle.net/123456789/638
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dc.contributor.authorRath, Satyajit-
dc.date.accessioned2015-08-20T10:30:51Z-
dc.date.available2015-08-20T10:30:51Z-
dc.date.issued2012-08-
dc.identifier.urihttp://hdl.handle.net/123456789/638-
dc.description.abstractApoptosis-inducing factor (Aif) is a mitochondrial flavoprotein that regulates cell metabolism and survival in many tissues. We report that aif-hypomorphic harlequin (Hq) mice show thymic hypocellularity and a cell-autonomous thymocyte developmental block associated with apoptosis at the β-selection stage, independent of T cell receptor β recombination. No abnormalities are observed in the B cell lineage. Transgenes encoding wild-type or DNA-binding-deficient mutant Aif rectify the thymic defect, but a transgene encoding oxidoreductase activity-deficient mutant Aif does not. The Hq thymic block is reversed in vivo by antioxidant treatment, and Hq T but not B lineage cells show enhanced oxidative stress. Thus, Aif, a ubiquitous protein, serves a lineage-specific nonredundant antiapoptotic role in the T cell lineage by regulating reactive oxygen species during thymic β-selection.en_US
dc.publisherThe Rockefeller University Pressen_US
dc.titleA role for apoptosis-inducing factor in T cell developmenten_US
dc.contributor.coauthorBanerjee, Hridesh-
dc.contributor.coauthorDas, Abhishek-
dc.contributor.coauthorSrivastava, Smita-
dc.contributor.coauthorMattoo, Hamid R-
dc.contributor.coauthorThyagarajan, Krishnamurthy-
dc.contributor.coauthorKhalsa, Jasneet Kaur-
dc.contributor.coauthorTanwar, Shalini-
dc.contributor.coauthorDas, Deepika Sharma-
dc.contributor.coauthorMajumdar, Subeer S-
dc.contributor.coauthorGeorge, Anna-
dc.contributor.coauthorBal, Vineeta-
dc.contributor.coauthorDurdik, Jeannine M-
dc.journalJournal of Experimental Medicineen_US
dc.volumeno209en_US
dc.issueno9en_US
dc.pages1641-1653en_US
Appears in Collections:Cellular Endocrinology, Publications

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