Actin and hnRNP U cooperate for productive transcription by RNA polymerase II

Kukalev, Alexander; Nord, Ylva; Palmberg, Carina; Bergman, Tomas; Percipalle, Piergiorgio

doi:10.1038/nsmb904

Cited by 212 publications

(224 citation statements)

References 45 publications

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“…hnRNPU-B23 interaction is mediated by histone-binding domain of B23 and RNA-binding domain of hnRNPU Both B23 and hnRNPU were known to contain functional domains, which account for their distinctive biochemical functions (Hingorani et al, 2000;Kukalev Figure 1 B23 interacts with hnRNPA1 and hnRNPU in the cytosol on ActD treatment. (a) HeLa cells stably expressing GFP were treated with the 0.1% DMSO vehicle, CHX (25 mg/ml) and ActD (1 mg/ml), respectively, followed by immunostaining with anti-B23 antibody (red).…”

Section: B23 Binds To Hnrnpu and Hnrnpa1 In The Cytosol In Response Tmentioning

confidence: 99%

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B23 acts as a nucleolar stress sensor and promotes cell survival through its dynamic interaction with hnRNPU and hnRNPA1

et al. 2010

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Section: B23 Binds To Hnrnpu and Hnrnpa1 In The Cytosol In Response Tmentioning

confidence: 99%

“…Protein hnRNPU, another hnRNPs family member, is able to stabilize specific mRNAs by binding to their 3 0 -untranslated regions (UTRs) (Yugami et al, 2007). Moreover, hnRNPU has a regulatory function during the initial phases of transcription activation by affecting the activity of RNA Pol II (Kukalev et al, 2005).…”

mentioning

confidence: 99%

B23 acts as a nucleolar stress sensor and promotes cell survival through its dynamic interaction with hnRNPU and hnRNPA1

et al. 2010

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“…Nuclear ␤-actin associates with components of the ATP-dependent chromatin-remodeling complexes (Olave et al, 2002;Bettinger et al, 2004), with RNP particles (Percipalle and Visa, 2006), and with the three RNA polymerases in the eukaryotic cell nucleus, both in vitro and in vivo (Hu et al, 2004;Philimonenko et al, 2004;Kukalev et al, 2005;Wu et al, 2006). The above studies have shown that nuclear actin is a component of large protein complexes that include RNA polymerases, transcription elongation factors, and accessory splicing factors that can be recruited to the RNAPII carboxy terminal domain and hence to promoters.…”

Section: Introductionmentioning

confidence: 99%

Induction of HoxB Transcription by Retinoic Acid Requires Actin Polymerization

Ferrai

Naum-Onganía

Longobardi

et al. 2009

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We have analyzed the role of actin polymerization in retinoic acid (RA)-induced HoxB transcription, which is mediated by the HoxB regulator Prep1. RA induction of the HoxB genes can be prevented by the inhibition of actin polymerization. Importantly, inhibition of actin polymerization specifically affects the transcription of inducible Hox genes, but not that of their transcriptional regulators, the RARs, nor of constitutively expressed, nor of actively transcribed Hox genes. RA treatment induces the recruitment to the HoxB2 gene enhancer of a complex composed of "elongating" RNAPII, Prep1, ␤-actin, and N-WASP as well as the accessory splicing components p54Nrb and PSF. We show that inhibition of actin polymerization prevents such recruitment. We conclude that inducible Hox genes are selectively sensitive to the inhibition of actin polymerization and that actin polymerization is required for the assembly of a transcription complex on the regulatory region of the Hox genes.

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“…The endogenous proteins physically interact via the zinc-fingers of WT1 and the middle domain of hnRNP-U, the interaction is direct and hnRNP-U can inhibit WT1-mediated transcriptional activation. hnRNP-U has been shown to regulate splicing and RNA transport as well as transcription (Kanai et al, 2004;Kukalev et al, 2005). Similar roles have been proposed for WT1 (Davies et al, 1998;Ladomery et al, 1999;Niksic et al, 2004), so the interaction with hnRNP-U could potentially regulate any of these processes.…”

Section: Antibody (C Es Cells; D M15 Cells) (E)mentioning

confidence: 87%

“…This transcriptional inhibition by hnRNP-U was shown to involve the middle domain of hnRNP-U, the same domain that associates with WT1, suggesting that the hnRNP-U:WT1 interaction may mediate transcriptional inhibition by bringing hnRNP-U into the proximity of RNA polymerase II via WT1-binding sites in the promoters of target genes. In addition, a search for novel actin-binding proteins associated with RNA polymerase II identified hnRNP-U (Kukalev et al, 2005) and showed that both actin and hnRNP-U associate with the phosphorylated form of RNA polymerase II and are implicated in the initial phases of transcription. In the present study, we also detected a protein that matched either g-or b-actin in the MS-FIT database as immunoprecipitating with WT1 (Table 2.1).…”

mentioning

confidence: 99%

hnRNP-U directly interacts with WT1 and modulates WT1 transcriptional activation

et al. 2006

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The Wilms' tumour suppressor gene, WT1, encodes a zinc-finger protein that is mutated in Wilms' tumours and highly expressed in a wide variety of other malignancies. WT1 is a transcription factor that is likely to have additional, post-transcriptional, regulatory roles, although the molecular mechanisms by which WT1 acts remain poorly understood. We have combined genetic and biochemical approaches to show, that endogenous WT1 binds to heterogeneous nuclear ribonuclear protein U (hnRNP-U), that this interaction does not require any other proteins or nucleic acids, involves the zinc-fingers of WT1 and the middle domain of hnRNP-U, and that hnRNP-U can modulate WT1 transcriptional activation of a bona fide WT1 target gene. These findings increase our knowledge of how WT1 exerts its transcriptional regulatory role and suggests that hnRNP-U may be a candidate Wilms' tumour gene at 1q44.

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Actin and hnRNP U cooperate for productive transcription by RNA polymerase II

Cited by 212 publications

References 45 publications

B23 acts as a nucleolar stress sensor and promotes cell survival through its dynamic interaction with hnRNPU and hnRNPA1

B23 acts as a nucleolar stress sensor and promotes cell survival through its dynamic interaction with hnRNPU and hnRNPA1

Induction of HoxB Transcription by Retinoic Acid Requires Actin Polymerization

hnRNP-U directly interacts with WT1 and modulates WT1 transcriptional activation

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