Nesprin-1 and -2 Are Involved in the Pathogenesis of Emery Dreifuss Muscular Dystrophy and Are Critical for Nuclear Envelope Integrity

Overview

Journal Hum Mol Genet

Specialties Genetics
Molecular Biology

Date 2007 Sep 1

PMID 17761684

Citations 279

Authors

Qiuping Zhang

Cornelia Bethmann

Nathalie F Worth

John D Davies

Christina Wasner

Anja Feuer

Cassandra D Ragnauth

Qijian Yi

Jason A Mellad

Derek T Warren

Matthew A Wheeler

Juliet A Ellis

Jeremy N Skepper

Matthias Vorgerd

Beate Schlotter-Weigel

Peter L Weissberg

Roland G Roberts

Manfred Wehnert

Catherine M Shanahan

Affiliations

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Abstract

Emery-Dreifuss muscular dystrophy (EDMD) is a heterogeneous late-onset disease involving skeletal muscle wasting and heart defects caused, in a minority of cases, by mutations in either of two genes encoding the inner nuclear membrane (INM) proteins, emerin and lamins A/C. Nesprin-1 and -2 are multi-isomeric, spectrin-repeat proteins that bind both emerin and lamins A/C and form a network in muscle linking the nucleoskeleton to the INM, the outer nuclear membrane, membraneous organelles, the sarcomere and the actin cytoskeleton. Thus, disruptions in nesprin/lamin/emerin interactions might play a role in the muscle-specific pathogenesis of EDMD. Screening for DNA variations in the genes encoding nesprin-1 (SYNE1) and nesprin-2 (SYNE2) in 190 probands with EDMD or EDMD-like phenotypes identified four heterozygous missense mutations. Fibroblasts from these patients exhibited nuclear morphology defects and specific patterns of emerin and SUN2 mislocalization. In addition, diminished nuclear envelope localization of nesprins and impaired nesprin/emerin/lamin binding interactions were common features of all EDMD patient fibroblasts. siRNA knockdown of nesprin-1 or -2 in normal fibroblasts reproduced the nuclear morphological changes and mislocalization of emerin and SUN2 observed in patient fibroblasts. Taken together, these data suggest that EDMD may be caused, in part, by uncoupling of the nucleoskeleton and cytoskeleton because of perturbed nesprin/emerin/lamin interactions.

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