Proteasome Inhibition Improves the Muscle of Laminin {alpha}2 Chain Deficient Mice.

Carmignac, Virginie; Quere, Ronan; Durbeej-Hjalt, Madeleine

Proteasome Inhibition Improves the Muscle of Laminin {alpha}2 Chain Deficient Mice.

Mark

Carmignac, Virginie ^LU ; Quere, Ronan ^LU and Durbeej-Hjalt, Madeleine ^LU (2011) In Human Molecular Genetics 20(3). p.541-552

Abstract: Muscle atrophy, a significant characteristic of congenital muscular dystrophy with laminin α2 chain deficiency (also known as MDC1A), occurs by a change in the normal balance between protein synthesis and protein degradation. The ubiquitin-proteasome system plays a key role in protein degradation in skeletal muscle cells. In order to identify new targets for drug therapy against MDC1A, we have investigated whether increased proteasomal degradation is a feature of MDC1A. Using the generated dy(3K)/dy(3K) mutant mouse model of MDC1A, we studied the expression of members of the ubiquitin-proteasome pathway in laminin α2 chain deficient muscle and we treated dy(3K)/dy(3K) mice with the proteasome inhibitor MG-132. We show that members of the... (More); Muscle atrophy, a significant characteristic of congenital muscular dystrophy with laminin α2 chain deficiency (also known as MDC1A), occurs by a change in the normal balance between protein synthesis and protein degradation. The ubiquitin-proteasome system plays a key role in protein degradation in skeletal muscle cells. In order to identify new targets for drug therapy against MDC1A, we have investigated whether increased proteasomal degradation is a feature of MDC1A. Using the generated dy(3K)/dy(3K) mutant mouse model of MDC1A, we studied the expression of members of the ubiquitin-proteasome pathway in laminin α2 chain deficient muscle and we treated dy(3K)/dy(3K) mice with the proteasome inhibitor MG-132. We show that members of the ubiquitin-proteasome system are upregulated and that the global ubiquitination of proteins is raised in dystrophic limb muscles. Also, phosphorylation of Akt is diminished in diseased muscles. Importantly, proteasome inhibition significantly improves the dystrophic dy(3K)/dy(3K) phenotype. Specifically, treatment with MG-132 increases lifespan, enhances locomotive activity, enlarges muscle fiber diameter, reduces fibrosis, restores Akt phosphorylation and decreases apoptosis. These studies promote better understanding of the disease process in mice and could lead to a drug therapy for MDC1A patients. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/1731851

author

Carmignac, Virginie ^LU ; Quere, Ronan ^LU and Durbeej-Hjalt, Madeleine ^LU

organization

publishing date

2011

type

Contribution to journal

publication status

published

subject

Medical Genetics

in

Human Molecular Genetics

volume

20

issue

3

pages

541 - 552

publisher

Oxford University Press

external identifiers

wos:000286006300012
pmid:21084425
scopus:78651076693

ISSN

0964-6906

DOI

10.1093/hmg/ddq499

language

English

LU publication?

yes

id

99e50975-5937-443b-a398-649a478caa17 (old id 1731851)

alternative location

http://www.ncbi.nlm.nih.gov/pubmed/21084425?dopt=Abstract

date added to LUP

2016-04-01 09:51:17

date last changed

2022-04-19 20:13:50

@article{99e50975-5937-443b-a398-649a478caa17,
  abstract     = {{Muscle atrophy, a significant characteristic of congenital muscular dystrophy with laminin α2 chain deficiency (also known as MDC1A), occurs by a change in the normal balance between protein synthesis and protein degradation. The ubiquitin-proteasome system plays a key role in protein degradation in skeletal muscle cells. In order to identify new targets for drug therapy against MDC1A, we have investigated whether increased proteasomal degradation is a feature of MDC1A. Using the generated dy(3K)/dy(3K) mutant mouse model of MDC1A, we studied the expression of members of the ubiquitin-proteasome pathway in laminin α2 chain deficient muscle and we treated dy(3K)/dy(3K) mice with the proteasome inhibitor MG-132. We show that members of the ubiquitin-proteasome system are upregulated and that the global ubiquitination of proteins is raised in dystrophic limb muscles. Also, phosphorylation of Akt is diminished in diseased muscles. Importantly, proteasome inhibition significantly improves the dystrophic dy(3K)/dy(3K) phenotype. Specifically, treatment with MG-132 increases lifespan, enhances locomotive activity, enlarges muscle fiber diameter, reduces fibrosis, restores Akt phosphorylation and decreases apoptosis. These studies promote better understanding of the disease process in mice and could lead to a drug therapy for MDC1A patients.}},
  author       = {{Carmignac, Virginie and Quere, Ronan and Durbeej-Hjalt, Madeleine}},
  issn         = {{0964-6906}},
  language     = {{eng}},
  number       = {{3}},
  pages        = {{541--552}},
  publisher    = {{Oxford University Press}},
  series       = {{Human Molecular Genetics}},
  title        = {{Proteasome Inhibition Improves the Muscle of Laminin {alpha}2 Chain Deficient Mice.}},
  url          = {{http://dx.doi.org/10.1093/hmg/ddq499}},
  doi          = {{10.1093/hmg/ddq499}},
  volume       = {{20}},
  year         = {{2011}},
}

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Proteasome Inhibition Improves the Muscle of Laminin {alpha}2 Chain Deficient Mice.