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Transcriptional Regulator CTR9 Inhibits Th17 Differentiation via Repression of IL-17 Expression. SCIE SCOPUS

Title
Transcriptional Regulator CTR9 Inhibits Th17 Differentiation via Repression of IL-17 Expression.
Authors
Hyun-Suk YooYongwook ChoiNarae AhnSaseong LeeWan-Uk KimMin Seong JangMyoung Ho JangYon Su KimYoo, JY
Date Issued
2014-02-15
Publisher
Baltimore : Williams & Wilkins, c1950
Abstract
PAF complex is an evolutionarily conserved transcriptional complex that associates with RNA polymerase II in the coding region of actively transcribing genes. Although its transcriptional activity is closely related to diverse cellular processes, such as cell-cycle progression or development in mammals, its role in immune responses has not been addressed yet. In this study, we show that CTR9, a component of PAF complex, functions as a repressor of Th17 differentiation. Both mRNA and protein levels of CTR9 were significantly decreased during the differentiation processes of naive T into Th17 effector cells. When CTR9 was depleted, IL-17 expression was induced and differentiation into Th17 cells enhanced. In naive T cells, CTR9 occupied the coding region of Il17a, but dissociated under Th17 in vitro-polarizing conditions. In contrast, both CDC73 and PAF1 were recruited to the Il17a locus under Th17-differentiation conditions. In the IL-6-stimulated splenocytes, expression of CTR9 was decreased, and chromatin-bound CTR9 disappeared in the coding region of Il17a. IL-6 also directly repressed expression of CTR9 gene, as promoter activity of CTR9 was similarly repressed by IL-6 treatment. Moreover, in mice with collagen-induced arthritis, lentivirus-mediated CTR9 overexpression in the joints ameliorated arthritis severity, decreasing the frequency of CD4(+) IL-17(+) T cells in lymph nodes. In conclusion, our data propose a novel feed-forward loop of IL-17 transcriptional regulatory circuit, via IL-6-mediated repression of CTR9 which is a transcriptional repressor of IL-17.
Keywords
RNA-POLYMERASE-II; COLLAGEN-INDUCED ARTHRITIS; ROR-GAMMA-T; PAF1 COMPLEX; SACCHAROMYCES-CEREVISIAE; STAT3 BETA; HISTONE H3; CELLS; ELONGATION; INTERLEUKIN-17
URI
https://oasis.postech.ac.kr/handle/2014.oak/14948
DOI
10.4049/JIMMUNOL.1201952
ISSN
0022-1767
Article Type
Article
Citation
JOURNAL OF IMMUNOLOGY, vol. 192, no. 4, page. 1440 - 1448, 2014-02-15
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유주연YOO, JOO YEON
Dept of Life Sciences
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