PP2B and PP1α cooperatively disrupt 7SK snRNP to release P-TEFb for transcription in response to Ca<sup>2+</sup> signaling

Chen, Ruichuan; Liu, Min; Li, Huan; Xue, Yuhua; Ramey, Wanichaya N.; He, Nanhai; Ai, Nanping; Luo, Haohong; Zhu, Ying; Zhou, Nan; Zhou, Qiang

doi:10.1101/gad.1636008

Cited by 163 publications

(262 citation statements)

References 38 publications

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“…We also found that HMBA, SAHA, and JQ1 share a common mechanism of transcriptional activation (16,17,34). SAHA also affects histone acetylation, and JQ1 affects the "readout" of these marks by BRD4.…”

Section: Discussionmentioning

confidence: 53%

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Bromodomain and Extra-terminal (BET) Bromodomain Inhibition Activate Transcription via Transient Release of Positive Transcription Elongation Factor b (P-TEFb) from 7SK Small Nuclear Ribonucleoprotein

Bartholomeeusen

Xiang

Fujinaga

et al. 2012

Journal of Biological Chemistry

180

162

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Background: P-TEFb regulates transcription elongation, cell growth, and proliferation. Results: BET bromodomain inhibition by JQ1 transiently releases free P-TEFb from the inactive 7SK snRNP, thus activating HEXIM1 and HIV transcription. Conclusion: JQ1 affects the P-TEFb equilibrium. Significance: P-TEFb release from and reassembly into 7SK snRNP by JQ1 inhibits tumor cell growth and reactivates latent HIV.

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Section: Discussionmentioning

confidence: 53%

“…JQ1, HMBA, and SAHA Have Comparable Effects on HIV Transcription-This and previous studies suggested that HMBA, SAHA, and JQ1 share a common mechanism of transcriptional activation (16,17,34). To this end, we treated J⌬K cells with HMBA or SAHA alone or in combination with JQ1 for 24 h and measured the production of HIV by p24 capsid ELISA.…”

Section: Jq1mentioning

confidence: 92%

Bromodomain and Extra-terminal (BET) Bromodomain Inhibition Activate Transcription via Transient Release of Positive Transcription Elongation Factor b (P-TEFb) from 7SK Small Nuclear Ribonucleoprotein

Bartholomeeusen

Xiang

Fujinaga

et al. 2012

Journal of Biological Chemistry

180

162

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“…Such contact between Hexim1 and the Cdk9 activation segment accounts for its inhibition. Importantly, phosphorylation of S175 and T186 in the "T-loop" is required for P-TEFb assembly with Hexim1 and 7SK RNA (21,48,49). Like Hexim1, the HIV viral protein Tat interacts mainly with cyclin T1 and is known to compete with Hexim1 for association with P-TEFb (5,22).…”

Section: Discussionmentioning

confidence: 99%

An evolutionary conserved Hexim1 peptide binds to the Cdk9 catalytic site to inhibit P-TEFb

Kobbi

Demey-Thomas

Brayé

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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The positive transcription elongation factor (P-TEFb) is required for the transcription of most genes by RNA polymerase II. Hexim proteins associated with 7SK RNA bind to P-TEFb and reversibly inhibit its activity. P-TEFb comprises the Cdk9 cyclin-dependent kinase and a cyclin T. Hexim proteins have been shown to bind the cyclin T subunit of P-TEFb. How this binding leads to inhibition of the kinase activity of Cdk9 has remained elusive, however. Using a photoreactive amino acid incorporated into proteins, we show that in live cells, cell extracts, and in vitro reconstituted complexes, Hexim1 cross-links and thus contacts Cdk9. Notably, replacement of a phenylalanine, F208, belonging to an evolutionary conserved Hexim1 peptide ( 202 PYNTTQFLM 210 ) known as the "PYNT" sequence, cross-links a peptide within the activation segment that controls access to the Cdk9 catalytic cleft. Reciprocally, Hexim1 is cross-linked by a photoreactive amino acid replacing Cdk9 W193, a tryptophan within this activation segment. These findings provide evidence of a direct interaction between Cdk9 and its inhibitor, Hexim1. Based on similarities with Cdk2 3D structure, the Cdk9 peptide cross-linked by Hexim1 corresponds to the substrate bindingsite. Accordingly, the Hexim1 PYNT sequence is proposed to interfere with substrate binding to Cdk9 and thereby to inhibit its kinase activity.cyclin-dependent kinase inhibition | transcription factor regulation | regulatory noncoding RNA | benzoyl phenylalanine | protein-protein cross-linking

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“…However, the outcome of the slow polymerase was an even greater decrease in miRNA synthesis. It is therefore anticipated that under certain physiological conditions in which PolII processivity is altered 40,41 or transcription re-initiation rate is regulated, 42 the effect on miRNA expression would be differential.…”

Section: Discussionmentioning

confidence: 99%

Disparity between microRNA levels and promoter strength is associated with initiation rate and Pol II pausing

et al. 2013

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MicroRNAs are transcribed by RNA polymerase II but the transcriptional features influencing their synthesis are poorly defined. Here we report that a TATA box in microRNA and proteincoding genes is associated with increased sensitivity to slow RNA polymerase II. Promoters driven by TATA box or NF-kB elicit high re-initiation rates, but paradoxically lower microRNA levels. MicroRNA synthesis becomes more productive by decreasing the initiation rate, but less productive when the re-initiation rate increases. This phenomenon is associated with a delay in miR-146a induction by NF-kB. Finally, we demonstrate that microRNAs are remarkably strong pause sites. Our findings suggest that lower efficiency of microRNA synthesis directed by TATA box or NF-kB is a consequence of frequent transcription initiations that lead to RNA polymerase II crowding at pause sites, thereby increasing the chance of collision and premature termination. These findings highlight the importance of the transcription initiation mechanism for microRNA synthesis, and have implications for TATA-box promoters in general.

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PP2B and PP1α cooperatively disrupt 7SK snRNP to release P-TEFb for transcription in response to Ca²⁺ signaling

Cited by 163 publications

References 38 publications

Bromodomain and Extra-terminal (BET) Bromodomain Inhibition Activate Transcription via Transient Release of Positive Transcription Elongation Factor b (P-TEFb) from 7SK Small Nuclear Ribonucleoprotein

Bromodomain and Extra-terminal (BET) Bromodomain Inhibition Activate Transcription via Transient Release of Positive Transcription Elongation Factor b (P-TEFb) from 7SK Small Nuclear Ribonucleoprotein

An evolutionary conserved Hexim1 peptide binds to the Cdk9 catalytic site to inhibit P-TEFb

Disparity between microRNA levels and promoter strength is associated with initiation rate and Pol II pausing

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PP2B and PP1α cooperatively disrupt 7SK snRNP to release P-TEFb for transcription in response to Ca2+ signaling

Cited by 163 publications

References 38 publications

Bromodomain and Extra-terminal (BET) Bromodomain Inhibition Activate Transcription via Transient Release of Positive Transcription Elongation Factor b (P-TEFb) from 7SK Small Nuclear Ribonucleoprotein

Bromodomain and Extra-terminal (BET) Bromodomain Inhibition Activate Transcription via Transient Release of Positive Transcription Elongation Factor b (P-TEFb) from 7SK Small Nuclear Ribonucleoprotein

An evolutionary conserved Hexim1 peptide binds to the Cdk9 catalytic site to inhibit P-TEFb

Disparity between microRNA levels and promoter strength is associated with initiation rate and Pol II pausing

Contact Info

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PP2B and PP1α cooperatively disrupt 7SK snRNP to release P-TEFb for transcription in response to Ca²⁺ signaling