Abnormal Activation of BMP Signaling Causes Myopathy in Fbn2 Null Mice

Fibrillins are large extracellular macromolecules that polymerize to form the backbone structure of connective tissue microfibrils. Mutations in the gene for fibrillin-1 cause the Marfan syndrome, while mutations in the gene for fibrillin-2 cause Congenital Contractural Arachnodactyly. Both are auto...

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Autores principales: Sengle, Gerhard, Carlberg, Valerie, Tufa, Sara F., Charbonneau, Noe L., Smaldone, Silvia, Carlson, Eric J., Ramirez, Francesco, Keene, Douglas R., Sakai, Lynn Y.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4482570/
https://www.ncbi.nlm.nih.gov/pubmed/26114882
http://dx.doi.org/10.1371/journal.pgen.1005340
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author Sengle, Gerhard
Carlberg, Valerie
Tufa, Sara F.
Charbonneau, Noe L.
Smaldone, Silvia
Carlson, Eric J.
Ramirez, Francesco
Keene, Douglas R.
Sakai, Lynn Y.
author_facet Sengle, Gerhard
Carlberg, Valerie
Tufa, Sara F.
Charbonneau, Noe L.
Smaldone, Silvia
Carlson, Eric J.
Ramirez, Francesco
Keene, Douglas R.
Sakai, Lynn Y.
author_sort Sengle, Gerhard
collection PubMed
description Fibrillins are large extracellular macromolecules that polymerize to form the backbone structure of connective tissue microfibrils. Mutations in the gene for fibrillin-1 cause the Marfan syndrome, while mutations in the gene for fibrillin-2 cause Congenital Contractural Arachnodactyly. Both are autosomal dominant disorders, and both disorders affect musculoskeletal tissues. Here we show that Fbn2 null mice (on a 129/Sv background) are born with reduced muscle mass, abnormal muscle histology, and signs of activated BMP signaling in skeletal muscle. A delay in Myosin Heavy Chain 8, a perinatal myosin, was found in Fbn2 null forelimb muscle tissue, consistent with the notion that muscle defects underlie forelimb contractures in these mice. In addition, white fat accumulated in the forelimbs during the early postnatal period. Adult Fbn2 null mice are already known to demonstrate persistent muscle weakness. Here we measured elevated creatine kinase levels in adult Fbn2 null mice, indicating ongoing cycles of muscle injury. On a C57Bl/6 background, Fbn2 null mice showed severe defects in musculature, leading to neonatal death from respiratory failure. These new findings demonstrate that loss of fibrillin-2 results in phenotypes similar to those found in congenital muscular dystrophies and that FBN2 should be considered as a candidate gene for recessive congenital muscular dystrophy. Both in vivo and in vitro evidence associated muscle abnormalities and accumulation of white fat in Fbn2 null mice with abnormally activated BMP signaling. Genetic rescue of reduced muscle mass and accumulation of white fat in Fbn2 null mice was accomplished by deleting a single allele of Bmp7. In contrast to other reports that activated BMP signaling leads to muscle hypertrophy, our findings demonstrate the exquisite sensitivity of BMP signaling to the fibrillin-2 extracellular environment during early postnatal muscle development. New evidence presented here suggests that fibrillin-2 can sequester BMP complexes in a latent state.
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spelling pubmed-44825702015-06-29 Abnormal Activation of BMP Signaling Causes Myopathy in Fbn2 Null Mice Sengle, Gerhard Carlberg, Valerie Tufa, Sara F. Charbonneau, Noe L. Smaldone, Silvia Carlson, Eric J. Ramirez, Francesco Keene, Douglas R. Sakai, Lynn Y. PLoS Genet Research Article Fibrillins are large extracellular macromolecules that polymerize to form the backbone structure of connective tissue microfibrils. Mutations in the gene for fibrillin-1 cause the Marfan syndrome, while mutations in the gene for fibrillin-2 cause Congenital Contractural Arachnodactyly. Both are autosomal dominant disorders, and both disorders affect musculoskeletal tissues. Here we show that Fbn2 null mice (on a 129/Sv background) are born with reduced muscle mass, abnormal muscle histology, and signs of activated BMP signaling in skeletal muscle. A delay in Myosin Heavy Chain 8, a perinatal myosin, was found in Fbn2 null forelimb muscle tissue, consistent with the notion that muscle defects underlie forelimb contractures in these mice. In addition, white fat accumulated in the forelimbs during the early postnatal period. Adult Fbn2 null mice are already known to demonstrate persistent muscle weakness. Here we measured elevated creatine kinase levels in adult Fbn2 null mice, indicating ongoing cycles of muscle injury. On a C57Bl/6 background, Fbn2 null mice showed severe defects in musculature, leading to neonatal death from respiratory failure. These new findings demonstrate that loss of fibrillin-2 results in phenotypes similar to those found in congenital muscular dystrophies and that FBN2 should be considered as a candidate gene for recessive congenital muscular dystrophy. Both in vivo and in vitro evidence associated muscle abnormalities and accumulation of white fat in Fbn2 null mice with abnormally activated BMP signaling. Genetic rescue of reduced muscle mass and accumulation of white fat in Fbn2 null mice was accomplished by deleting a single allele of Bmp7. In contrast to other reports that activated BMP signaling leads to muscle hypertrophy, our findings demonstrate the exquisite sensitivity of BMP signaling to the fibrillin-2 extracellular environment during early postnatal muscle development. New evidence presented here suggests that fibrillin-2 can sequester BMP complexes in a latent state. Public Library of Science 2015-06-26 /pmc/articles/PMC4482570/ /pubmed/26114882 http://dx.doi.org/10.1371/journal.pgen.1005340 Text en © 2015 Sengle et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Sengle, Gerhard
Carlberg, Valerie
Tufa, Sara F.
Charbonneau, Noe L.
Smaldone, Silvia
Carlson, Eric J.
Ramirez, Francesco
Keene, Douglas R.
Sakai, Lynn Y.
Abnormal Activation of BMP Signaling Causes Myopathy in Fbn2 Null Mice
title Abnormal Activation of BMP Signaling Causes Myopathy in Fbn2 Null Mice
title_full Abnormal Activation of BMP Signaling Causes Myopathy in Fbn2 Null Mice
title_fullStr Abnormal Activation of BMP Signaling Causes Myopathy in Fbn2 Null Mice
title_full_unstemmed Abnormal Activation of BMP Signaling Causes Myopathy in Fbn2 Null Mice
title_short Abnormal Activation of BMP Signaling Causes Myopathy in Fbn2 Null Mice
title_sort abnormal activation of bmp signaling causes myopathy in fbn2 null mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4482570/
https://www.ncbi.nlm.nih.gov/pubmed/26114882
http://dx.doi.org/10.1371/journal.pgen.1005340
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