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mRNA 3 '-UTR shortening is a molecular signature of mTORC1 activation

Authors
Chang, Jae-WoongZhang, WeiYeh, Hsin-Sungde Jong, Ebbing P.Jun, SemoKim, Kwan-HyunBae, Sun S.Beckman, KennethHwang, Tae HyunKim, Kye-SeongKim, Do-HyungGriffin, Timothy J.Kuang, RuiYong, Jeongsik
Issue Date
Jun-2015
Publisher
Nature Publishing Group
Citation
Nature Communications, v.6, pp 1 - 9
Pages
9
Indexed
SCI
SCIE
SCOPUS
Journal Title
Nature Communications
Volume
6
Start Page
1
End Page
9
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/157105
DOI
10.1038/ncomms8218
ISSN
2041-1723
2041-1723
Abstract
Mammalian target of rapamycin (mTOR) enhances translation from a subset of messenger RNAs containing distinct 5'-untranslated region (UTR) sequence features. Here we identify 3'-UTR shortening of mRNAs as an additional molecular signature of mTOR activation and show that 3'-UTR shortening enhances the translation of specific mRNAs. Using genetic or chemical modulations of mTOR activity in cells or mouse tissues, we show that cellular mTOR activity is crucial for 3'-UTR shortening. Although long 3'-UTR-containing transcripts minimally contribute to translation, 3-'UTR-shortened transcripts efficiently form polysomes in the mTOR-activated cells, leading to increased protein production. Strikingly, selected E2 and E3 components of ubiquitin ligase complexes are enriched by this mechanism, resulting in elevated levels of protein ubiquitination on mTOR activation. Together, these findings identify a previously uncharacterized role for mTOR in the selective regulation of protein synthesis by modulating 3'-UTR length of mRNAs.
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서울 의생명공학전문대학원 > 서울 의생명과학과 > 1. Journal Articles

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GRADUATE SCHOOL OF BIOMEDICAL SCIENCE AND ENGINEERING (DEPARTMENT OF BIOMEDICAL SCIENCE)
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