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SR proteins collaborate with 7SK and promoter-associated nascent RNA to release paused polymerase.


ABSTRACT: RNAP II is frequently paused near gene promoters in mammals, and its transition to productive elongation requires active recruitment of P-TEFb, a cyclin-dependent kinase for RNAP II and other key transcription elongation factors. A fraction of P-TEFb is sequestered in an inhibitory complex containing the 7SK noncoding RNA, but it has been unclear how P-TEFb is switched from the 7SK complex to RNAP II during transcription activation. We report that SRSF2 (also known as SC35, an SR-splicing factor) is part of the 7SK complex assembled at gene promoters and plays a direct role in transcription pause release. We demonstrate RNA-dependent, coordinated release of SRSF2 and P-TEFb from the 7SK complex and transcription activation via SRSF2 binding to promoter-associated nascent RNA. These findings reveal an unanticipated SR protein function, a role for promoter-proximal nascent RNA in gene activation, and an analogous mechanism to HIV Tat/TAR for activating cellular genes.

SUBMITTER: Ji X 

PROVIDER: S-EPMC4103662 | biostudies-literature | 2013 May

REPOSITORIES: biostudies-literature

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SR proteins collaborate with 7SK and promoter-associated nascent RNA to release paused polymerase.

Ji Xiong X   Zhou Yu Y   Pandit Shatakshi S   Huang Jie J   Li Hairi H   Lin Charles Y CY   Xiao Rui R   Burge Christopher B CB   Fu Xiang-Dong XD  

Cell 20130501 4


RNAP II is frequently paused near gene promoters in mammals, and its transition to productive elongation requires active recruitment of P-TEFb, a cyclin-dependent kinase for RNAP II and other key transcription elongation factors. A fraction of P-TEFb is sequestered in an inhibitory complex containing the 7SK noncoding RNA, but it has been unclear how P-TEFb is switched from the 7SK complex to RNAP II during transcription activation. We report that SRSF2 (also known as SC35, an SR-splicing factor  ...[more]

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