Essential role for the interaction between hnRNP H/F and a G quadruplex in maintaining p53 pre-mRNA 3′-end processing and function during DNA damage

Adrien Decorsière; Anne Cayrel; Stéphan Vagner; Stefania Millevoi

doi:10.1101/gad.607011

Essential role for the interaction between hnRNP H/F and a G quadruplex in maintaining p53 pre-mRNA 3′-end processing and function during DNA damage

Adrien Decorsière
, Anne Cayrel
, Stéphan Vagner
, Stefania Millevoi

Research output: Contribution to journal › Article › peer-review

Abstract

Following DNA damage, mRNA 3′-end formation is inhibited, contributing to repression of mRNA synthesis. Here we investigated how DNA-damaged cells accomplish p53 mRNA 3′-end formation when normal mechanisms of pre-mRNA 3′-end processing regulation are inhibited. The underlying mechanism involves the interaction between a G-quadruplex structure located downstream from the p53 cleavage site and hnRNP H/F. Importantly, this interaction is critical for p53 expression and contributes to p53-mediated apoptosis. Our results uncover the existence of a specific rescue mechanism of 3′-end processing regulation allowing stress-induced p53 accumulation and function in apoptosis.

Original language	English
Pages (from-to)	220-225
Number of pages	6
Journal	Genes and Development
Volume	25
Issue number	3
DOIs	https://doi.org/10.1101/gad.607011
Publication status	Published - 1 Feb 2011
Externally published	Yes

Keywords

DNA damage
Polyadenylation
hnRNP F
hnRNP H
p53 tumor suppressor
pre-mRNA 3′-end processing

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10.1101/gad.607011

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abstract = "Following DNA damage, mRNA 3′-end formation is inhibited, contributing to repression of mRNA synthesis. Here we investigated how DNA-damaged cells accomplish p53 mRNA 3′-end formation when normal mechanisms of pre-mRNA 3′-end processing regulation are inhibited. The underlying mechanism involves the interaction between a G-quadruplex structure located downstream from the p53 cleavage site and hnRNP H/F. Importantly, this interaction is critical for p53 expression and contributes to p53-mediated apoptosis. Our results uncover the existence of a specific rescue mechanism of 3′-end processing regulation allowing stress-induced p53 accumulation and function in apoptosis.",

keywords = "DNA damage, Polyadenylation, hnRNP F, hnRNP H, p53 tumor suppressor, pre-mRNA 3′-end processing",

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AU - Decorsière, Adrien

AU - Cayrel, Anne

AU - Vagner, Stéphan

AU - Millevoi, Stefania

PY - 2011/2/1

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N2 - Following DNA damage, mRNA 3′-end formation is inhibited, contributing to repression of mRNA synthesis. Here we investigated how DNA-damaged cells accomplish p53 mRNA 3′-end formation when normal mechanisms of pre-mRNA 3′-end processing regulation are inhibited. The underlying mechanism involves the interaction between a G-quadruplex structure located downstream from the p53 cleavage site and hnRNP H/F. Importantly, this interaction is critical for p53 expression and contributes to p53-mediated apoptosis. Our results uncover the existence of a specific rescue mechanism of 3′-end processing regulation allowing stress-induced p53 accumulation and function in apoptosis.

AB - Following DNA damage, mRNA 3′-end formation is inhibited, contributing to repression of mRNA synthesis. Here we investigated how DNA-damaged cells accomplish p53 mRNA 3′-end formation when normal mechanisms of pre-mRNA 3′-end processing regulation are inhibited. The underlying mechanism involves the interaction between a G-quadruplex structure located downstream from the p53 cleavage site and hnRNP H/F. Importantly, this interaction is critical for p53 expression and contributes to p53-mediated apoptosis. Our results uncover the existence of a specific rescue mechanism of 3′-end processing regulation allowing stress-induced p53 accumulation and function in apoptosis.

KW - DNA damage

KW - Polyadenylation

KW - hnRNP F

KW - hnRNP H

KW - p53 tumor suppressor

KW - pre-mRNA 3′-end processing

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DO - 10.1101/gad.607011

M3 - Article

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SN - 0890-9369

VL - 25

SP - 220

EP - 225

JO - Genes and Development

JF - Genes and Development

IS - 3

ER -

Essential role for the interaction between hnRNP H/F and a G quadruplex in maintaining p53 pre-mRNA 3′-end processing and function during DNA damage

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Keywords

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