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Literature DB >> 25575120

MED26 regulates the transcription of snRNA genes through the recruitment of little elongation complex.

Hidehisa Takahashi¹, Ichigaku Takigawa², Masashi Watanabe¹, Delnur Anwar¹, Mio Shibata¹, Chieri Tomomori-Sato³, Shigeo Sato³, Amol Ranjan³, Chris W Seidel³, Tadasuke Tsukiyama¹, Wataru Mizushima¹, Masayasu Hayashi⁴, Yasuyuki Ohkawa⁴, Joan W Conaway⁵, Ronald C Conaway⁵, Shigetsugu Hatakeyama¹.

Abstract

Regulation of transcription elongation by RNA polymerase II (Pol II) is a key regulatory step in gene transcription. Recently, the little elongation complex (LEC)-which contains the transcription elongation factor ELL/EAF-was found to be required for the transcription of Pol II-dependent small nuclear RNA (snRNA) genes. Here we show that the human Mediator subunit MED26 plays a role in the recruitment of LEC to a subset of snRNA genes through direct interaction of EAF and the N-terminal domain (NTD) of MED26. Loss of MED26 in cells decreases the occupancy of LEC at a subset of snRNA genes and results in a reduction in their transcription. Our results suggest that the MED26-NTD functions as a molecular switch in the exchange of TBP-associated factor 7 (TAF7) for LEC to facilitate the transition from initiation to elongation during transcription of a subset of snRNA genes.

Entities: CellLine Chemical Disease Gene Mutation Species

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Year: 2015 PMID： 25575120 PMCID： PMC4646223 DOI： 10.1038/ncomms6941

Source DB: PubMed Journal: Nat Commun ISSN： 2041-1723 Impact factor: 14.919

47 in total

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3. HIV-1 Tat assembles a multifunctional transcription elongation complex and stably associates with the 7SK snRNP.

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4. HIV-1 Tat and host AFF4 recruit two transcription elongation factors into a bifunctional complex for coordinated activation of HIV-1 transcription.

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5. Identification of SNAPc subunit domains that interact with specific nucleotide positions in the U1 and U6 gene promoters.

Authors: Mun Kyoung Kim; Yoon Soon Kang; Hsien-Tsung Lai; Nermeen H Barakat; Deodato Magante; William E Stumph
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6. Human mediator subunit MED26 functions as a docking site for transcription elongation factors.

Authors: Hidehisa Takahashi; Tari J Parmely; Shigeo Sato; Chieri Tomomori-Sato; Charles A S Banks; Stephanie E Kong; Henrietta Szutorisz; Selene K Swanson; Skylar Martin-Brown; Michael P Washburn; Laurence Florens; Chris W Seidel; Chengqi Lin; Edwin R Smith; Ali Shilatifard; Ronald C Conaway; Joan W Conaway
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7. The structure of an Iws1/Spt6 complex reveals an interaction domain conserved in TFIIS, Elongin A and Med26.

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9. Multivalent Role of Human TFIID in Recruiting Elongation Components at the Promoter-Proximal Region for Transcriptional Control.

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10. Oxidative stress induces Ser 2 dephosphorylation of the RNA polymerase II CTD and premature transcription termination.

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