Intronic Determinants Coordinate Charme LncRNA Nuclear Activity Through the Interaction with MATR3 and PTBP1

Overview

Journal Cell Rep

Publisher Cell Press

Specialties Biology
Cell Biology
Molecular Biology

Date 2020 Dec 28

PMID 33357424

Citations 21

Authors

Fabio Desideri

Andrea Cipriano

Silvia Petrezselyova

Giulia Buonaiuto

Tiziana Santini

Petr Kasparek

Jan Prochazka

Giacomo Janson

Alessandro Paiardini

Alessandro Calicchio

Alessio Colantoni

Radislav Sedlacek

Irene Bozzoni

Monica Ballarino

Affiliations

Soon will be listed here.

Abstract

Chromatin architect of muscle expression (Charme) is a muscle-restricted long noncoding RNA (lncRNA) that plays an important role in myogenesis. Earlier evidence indicates that the nuclear Charme isoform, named pCharme, acts on the chromatin by assisting the formation of chromatin domains where myogenic transcription occurs. By combining RNA antisense purification (RAP) with mass spectrometry and loss-of-function analyses, we have now identified the proteins that assist these chromatin activities. These proteins-which include a sub-set of splicing regulators, principally PTBP1 and the multifunctional RNA/DNA binding protein MATR3-bind to sequences located within the alternatively spliced intron-1 to form nuclear aggregates. Consistent with the functional importance of pCharme interactome in vivo, a targeted deletion of the intron-1 by a CRISPR-Cas9 approach in mouse causes the release of pCharme from the chromatin and results in cardiac defects similar to what was observed upon knockout of the full-length transcript.

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