| Literature DB >> 30185651 |
Emmanuel Clave1,2, Itauá Leston Araujo1,2, Cécile Alanio3,4,5, Etienne Patin6,7,8, Jacob Bergstedt9, Alejandra Urrutia3,4,5,10, Silvia Lopez-Lastra5,11, Yan Li5,11, Bruno Charbit3, Cameron Ross MacPherson3, Milena Hasan3, Breno Luiz Melo-Lima1,2, Corinne Douay1,2, Noémie Saut12,13, Marine Germain14,15, David-Alexandre Trégouët14,15, Pierre-Emmanuel Morange12,13, Magnus Fontes10,16, Darragh Duffy3,4,5, James P Di Santo5,11, Lluis Quintana-Murci6,7,8, Matthew L Albert17,4,5,10, Antoine Toubert18,2,19.
Abstract
The thymus is the primary lymphoid organ where naïve T cells are generated; however, with the exception of age, the parameters that govern its function in healthy humans remain unknown. We characterized the variability of thymic function among 1000 age- and sex-stratified healthy adults of the Milieu Intérieur cohort, using quantification of T cell receptor excision circles (TRECs) in peripheral blood T cells as a surrogate marker of thymopoiesis. Age and sex were the only nonheritable factors identified that affect thymic function. TREC amounts decreased with age and were higher in women compared to men. In addition, a genome-wide association study revealed a common variant (rs2204985) within the T cell receptor TCRA-TCRD locus, between the DD2 and DD3 gene segments, which associated with TREC amounts. Strikingly, transplantation of human hematopoietic stem cells with the rs2204985 GG genotype into immunodeficient mice led to thymopoiesis with higher TRECs, increased thymocyte counts, and a higher TCR repertoire diversity. Our population immunology approach revealed a genetic locus that influences thymopoiesis in healthy adults, with potentially broad implications in precision medicine.Entities:
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Year: 2018 PMID: 30185651 DOI: 10.1126/scitranslmed.aao2966
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956