Tankyrase-1 Regulates RBP-mediated MRNA Turnover to Promote Muscle Fiber Formation

Overview

Journal Nucleic Acids Res

Publisher Oxford University Press

Specialty Biochemistry

Date 2024 Feb 7

PMID 38321934

Authors

Souad Mubaid

Brenda Janice Sanchez

Rinad A Algehani

Viktoriia Skopenkova

Pauline Adjibade

Derek T Hall

Sandrine Busque

Xian Jin Lian

Kholoud Ashour

Anne-Marie K Tremblay

Graeme Carlile

Jean-Philippe Gagne

Andrea Diaz-Gaxiola

Shahryar Khattak

Sergio Di Marco

David Y Thomas

Guy G Poirier

Imed-Eddine Gallouzi

Affiliations

Soon will be listed here.

Abstract

Poly(ADP-ribosylation) (PARylation) is a post-translational modification mediated by a subset of ADP-ribosyl transferases (ARTs). Although PARylation-inhibition based therapies are considered as an avenue to combat debilitating diseases such as cancer and myopathies, the role of this modification in physiological processes such as cell differentiation remains unclear. Here, we show that Tankyrase1 (TNKS1), a PARylating ART, plays a major role in myogenesis, a vital process known to drive muscle fiber formation and regeneration. Although all bona fide PARPs are expressed in muscle cells, experiments using siRNA-mediated knockdown or pharmacological inhibition show that TNKS1 is the enzyme responsible of catalyzing PARylation during myogenesis. Via this activity, TNKS1 controls the turnover of mRNAs encoding myogenic regulatory factors such as nucleophosmin (NPM) and myogenin. TNKS1 mediates these effects by targeting RNA-binding proteins such as Human Antigen R (HuR). HuR harbors a conserved TNKS-binding motif (TBM), the mutation of which not only prevents the association of HuR with TNKS1 and its PARylation, but also precludes HuR from regulating the turnover of NPM and myogenin mRNAs as well as from promoting myogenesis. Therefore, our data uncover a new role for TNKS1 as a key modulator of RBP-mediated post-transcriptional events required for vital processes such as myogenesis.

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