Congenital muscular dystrophy with laminin α2 chain-deficiency. Initiation of disease and development of treatment

Körner, Zandra

Congenital muscular dystrophy with laminin α2 chain-deficiency. Initiation of disease and development of treatment

Mark

Körner, Zandra ^LU (2016)

Abstract: Congenital muscle dystrophy type 1A (MDC1A) is a muscle disease caused by
mutations in the LAMA2 gene, encoding the basement membrane protein laminin
α2 chain. MDC1A patients exhibit neonatal onset of muscle weakness, progressive
muscle wasting and hypotonia, joint contractures that mostly affect elbows, hips,
knees and ankles along with scoliosis and delayed motor milestones. Currently,
there is no cure for MDC1A and respiratory failure is the main cause of death.
Patients with complete laminin α2 chain-deficiency have an early onset and also a
more severe muscle phenotype whereas patients with partial loss usually have a
milder disease course. The same genotype-phenotype correlations can be seen in
the... (More); Congenital muscle dystrophy type 1A (MDC1A) is a muscle disease caused by
mutations in the LAMA2 gene, encoding the basement membrane protein laminin
α2 chain. MDC1A patients exhibit neonatal onset of muscle weakness, progressive
muscle wasting and hypotonia, joint contractures that mostly affect elbows, hips,
knees and ankles along with scoliosis and delayed motor milestones. Currently,
there is no cure for MDC1A and respiratory failure is the main cause of death.
Patients with complete laminin α2 chain-deficiency have an early onset and also a
more severe muscle phenotype whereas patients with partial loss usually have a
milder disease course. The same genotype-phenotype correlations can be seen in
the mouse models of MDC1A. The dy3K/dy3K knock-out model exhibits a much
more severe phenotype than the dy2J/dy2Jmouse model, which expresses a
truncated laminin α2 chain. However, we have not before this thesis known how
early the pathogenesis in the skeletal muscle starts. Here, we demonstrated that
changes in skeletal muscle start with apoptosis already at day one after birth and
inflammation at day four in dy3K/dy3K mice.
Previously, it was demonstrated that the ubiquitin-proteasome system is
upregulated in the dy3K/dy3K mouse muscle. Moreover, by inhibiting the
proteasome by using a lab-bench drug, dy3K/dy3Kmice exhibited reduced muscular
dystrophy. This led us to testing an approved FDA drug, bortezomib, which also
inhibits the proteasome. By using bortezomib we could partially ameliorate the
disease in the dy3K/dy3Kmice with an increased lifespan and improved muscle
function. However, this could not be recapitulated in the dy2J/dy2J mice.
Furthermore, in this thesis we also showed that another pathway for cellular
degradation, the autophagy-lysosome pathway, is upregulated in the
dy3K/dy3Kmouse muscle. By inhibiting the autophagy pathway, dy3K/dy3K mice
exhibited improved muscle morphology and increased lifespan. In summary, I
have shown that there is enhanced proteasome and autophagy activity in MDC1A
muscle and that proteasome and autophagy inhibitors, respectively, can be used to
reduce disease in mice. I hope that our studies can form the basis for the
development of clinically relevant autophagy inhibitors. It may also be worth
testing bortezomib as a possible supportive therapy for MDC1A. Furthermore, our
data suggest that treatment should be initiated as early as possible given that we
detected disease changes already one to four days after birth in mice. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/2610e14d-b29e-4c7d-8285-5c14a32b1e18

author

Körner, Zandra ^LU

supervisor

Madeleine Durbeej-Hjalt ^LU
Anna Hultgårdh ^LU

opponent

professor Pedrosa-Domellöf, Fatima, Umeå University

organization

Muscle Biology (research group)

alternative title

Kongenital muskeldystrofi med lamininbrist : Sjukdomsinitiering och utveckling av behandling

publishing date

2016

type

Thesis

publication status

published

subject

Cell and Molecular Biology

keywords

muskeldystrofi, Muscular dystrophy, Autophagy, proteasome, Laminin, MDC1A

pages

118 pages

publisher

Lund University: Faculty of Medicine

defense location

Belfragesalen, BMC D15, Klinikgatan 32, Lund

defense date

2016-09-03 10:00:00

ISBN

978-91-7619-312-9

language

English

LU publication?

yes

additional info

ISSN: 1652-8220 Lund University, Faculty of Medicine Doctoral Dissertation Series 2016:86

id

2610e14d-b29e-4c7d-8285-5c14a32b1e18

date added to LUP

2016-07-29 14:38:48

date last changed

2019-11-19 13:49:11

@phdthesis{2610e14d-b29e-4c7d-8285-5c14a32b1e18,
  abstract     = {{Congenital muscle dystrophy type 1A (MDC1A) is a muscle disease caused by<br/>mutations in the LAMA2 gene, encoding the basement membrane protein laminin<br/>α2 chain. MDC1A patients exhibit neonatal onset of muscle weakness, progressive<br/>muscle wasting and hypotonia, joint contractures that mostly affect elbows, hips,<br/>knees and ankles along with scoliosis and delayed motor milestones. Currently,<br/>there is no cure for MDC1A and respiratory failure is the main cause of death.<br/>Patients with complete laminin α2 chain-deficiency have an early onset and also a<br/>more severe muscle phenotype whereas patients with partial loss usually have a<br/>milder disease course. The same genotype-phenotype correlations can be seen in<br/>the mouse models of MDC1A. The dy3K/dy3K knock-out model exhibits a much<br/>more severe phenotype than the dy2J/dy2Jmouse model, which expresses a<br/>truncated laminin α2 chain. However, we have not before this thesis known how<br/>early the pathogenesis in the skeletal muscle starts. Here, we demonstrated that<br/>changes in skeletal muscle start with apoptosis already at day one after birth and<br/>inflammation at day four in dy3K/dy3K mice.<br/>Previously, it was demonstrated that the ubiquitin-proteasome system is<br/>upregulated in the dy3K/dy3K mouse muscle. Moreover, by inhibiting the<br/>proteasome by using a lab-bench drug, dy3K/dy3Kmice exhibited reduced muscular<br/>dystrophy. This led us to testing an approved FDA drug, bortezomib, which also<br/>inhibits the proteasome. By using bortezomib we could partially ameliorate the<br/>disease in the dy3K/dy3Kmice with an increased lifespan and improved muscle<br/>function. However, this could not be recapitulated in the dy2J/dy2J mice.<br/>Furthermore, in this thesis we also showed that another pathway for cellular<br/>degradation, the autophagy-lysosome pathway, is upregulated in the<br/>dy3K/dy3Kmouse muscle. By inhibiting the autophagy pathway, dy3K/dy3K mice<br/>exhibited improved muscle morphology and increased lifespan. In summary, I<br/>have shown that there is enhanced proteasome and autophagy activity in MDC1A<br/>muscle and that proteasome and autophagy inhibitors, respectively, can be used to<br/>reduce disease in mice. I hope that our studies can form the basis for the<br/>development of clinically relevant autophagy inhibitors. It may also be worth<br/>testing bortezomib as a possible supportive therapy for MDC1A. Furthermore, our<br/>data suggest that treatment should be initiated as early as possible given that we<br/>detected disease changes already one to four days after birth in mice.}},
  author       = {{Körner, Zandra}},
  isbn         = {{978-91-7619-312-9}},
  keywords     = {{muskeldystrofi; Muscular dystrophy; Autophagy; proteasome; Laminin; MDC1A}},
  language     = {{eng}},
  publisher    = {{Lund University: Faculty of Medicine}},
  school       = {{Lund University}},
  title        = {{Congenital muscular dystrophy with laminin α2 chain-deficiency. Initiation of disease and development of treatment}},
  url          = {{https://lup.lub.lu.se/search/files/10296340/e_spik_Zandra_.pdf}},
  year         = {{2016}},
}

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Congenital muscular dystrophy with laminin α2 chain-deficiency. Initiation of disease and development of treatment