| Literature DB >> 25583492 |
Samia Afzal1, Zhenyue Hao2, Momoe Itsumi3, Yasser Abouelkheer2, Dirk Brenner4, Yunfei Gao2, Andrew Wakeham2, Claire Hong2, Wanda Y Li2, Jennifer Sylvester2, Syed O Gilani2, Anne Brüstle5, Jillian Haight2, Annick J You-Ten2, Gloria H Y Lin2, Satoshi Inoue2, Tak W Mak6.
Abstract
UV radiation resistance-associated gene (UVRAG) encodes a tumor suppressor with putative roles in autophagy, endocytic trafficking, and DNA damage repair but its in vivo role in T cells is unknown. Because conditional homozygous deletion of Uvrag in mice results in early embryonic lethality, we generated T-cell-specific UVRAG-deficient mice that lacked UVRAG expression specifically in T cells. This loss of UVRAG led to defects in peripheral homeostasis that could not be explained by the increased sensitivity to cell death and impaired proliferation observed for other autophagy-related gene knockout mice. Instead, UVRAG-deficient T-cells exhibited normal mitochondrial clearance and activation-induced autophagy, suggesting that UVRAG has an autophagy-independent role that is critical for peripheral naive T-cell homeostatic proliferation. In vivo, T-cell-specific loss of UVRAG dampened CD8(+) T-cell responses to LCMV infection in mice, delayed viral clearance, and impaired memory T-cell generation. Our data provide novel insights into the control of autophagy in T cells and identify UVRAG as a new regulator of naïve peripheral T-cell homeostasis.Entities:
Keywords: T-cell homeostasis; UVRAG-deficient mice; autophagy; embryonic lethality
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Year: 2015 PMID: 25583492 PMCID: PMC4313859 DOI: 10.1073/pnas.1423588112
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205