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Long noncoding RNA LIRIL2R modulates FOXP3 levels and suppressive function of human CD4 regulatory T cells by regulating IL2RA

Proc Natl Acad Sci U S A. 2024-05; 
Syed Bilal Ahmad Andrabi, Ubaid Ullah Kalim, Senthil Palani, Mohd Moin Khan, Meraj Hasan Khan, Jimmy Fagersund, Julius Orpana, Niklas Paulin, Kedar Batkulwar, Sini Junttila, Tanja Buchacher, Toni Grönroos, Lea Toikka, Tea Ammunet, Partho Sen, Matej Orešič, Venla Kumpulainen, Johanna E E Tuomisto, Rahul Sinha, Alexander Marson, Omid Rasool, Laura L Elo, Riitta Lahesmaa
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摘要

Regulatory T cells (Tregs) are central in controlling immune responses, and dysregulation of their function can lead to autoimmune disorders or cancer. Despite extensive studies on Tregs, the basis of epigenetic regulation of human Treg development and function is incompletely understood. Long intergenic noncoding RNAs (lincRNA)s are important for shaping and maintaining the epigenetic landscape in different cell types. In this study, we identified a gene on the chromosome 6p25.3 locus, encoding a lincRNA, that was up-regulated during early differentiation of human Tregs. The lincRNA regulated the expression of interleukin-2 receptor alpha (IL2RA), and we named it the lincRNA regulator of IL2RA (LIRIL2R). Throu... More

关键词

FOXP3, IL2RA, LIRIL2R, long noncoding RNA, regulatory T cells