Literature DB >> 21277300

Sparing of extraocular muscle in aging and muscular dystrophies: a myogenic precursor cell hypothesis.

Kristen M Kallestad1, Sadie L Hebert, Abby A McDonald, Mark L Daniel, Sharon R Cu, Linda K McLoon.   

Abstract

The extraocular muscles (EOM) are spared from pathology in aging and many forms of muscular dystrophy. Despite many studies, this sparing remains an enigma. The EOM have a distinct embryonic lineage compared to somite-derived muscles, and we have shown that they continuously remodel throughout life, maintaining a population of activated satellite cells even in aging. These data suggested the hypothesis that there is a population of myogenic precursor cells (mpcs) in EOM that is different from those in limb, with either elevated numbers of stem cells and/or mpcs with superior proliferative capacity compared to mpcs in limb. Using flow cytometry, EOM and limb muscle mononuclear cells were compared, and a number of differences were seen. Using two different cell isolation methods, EOM have significantly more mpcs per mg muscle than limb skeletal muscle. One specific subpopulation significantly increased in EOM compared to limb was positive for CD34 and negative for Sca-1, M-cadherin, CD31, and CD45. We named these the EOMCD34 cells. Similar percentages of EOMCD34 cells were present in both newborn EOM and limb muscle. They were retained in aged EOM, whereas the population decreased significantly in adult limb muscle and were extremely scarce in aged limb muscle. Most importantly, the percentage of EOMCD34 cells was elevated in the EOM from both the mdx and the mdx/utrophin(-/-) (DKO) mouse models of DMD and extremely scarce in the limb muscles of these mice. In vitro, the EOMCD34 cells had myogenic potential, forming myotubes in differentiation media. After determining a media better able to induce proliferation in these cells, a fusion index was calculated. The cells isolated from EOM had a 40% higher fusion index compared to the same cells isolated from limb muscle. The EOMCD34 cells were resistant to both oxidative stress and mechanical injury. These data support our hypothesis that the EOM may be spared in aging and in muscular dystrophies due to a subpopulation of mpcs, the EOMCD34 cells, that are retained in significantly higher percentages in normal, mdx and DKO mice EOM, appear to be resistant to elevated levels of oxidative stress and toxins, and actively proliferate throughout life. Current studies are focused on further defining the EOMCD34 cell subtype molecularly, with the hopes that this may shed light on a cell type with potential therapeutic use in patients with sarcopenia, cachexia, or muscular dystrophy.
Copyright © 2011 Elsevier Inc. All rights reserved.

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Year:  2011        PMID: 21277300      PMCID: PMC3072110          DOI: 10.1016/j.yexcr.2011.01.018

Source DB:  PubMed          Journal:  Exp Cell Res        ISSN: 0014-4827            Impact factor:   3.905


  69 in total

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9.  Activated satellite cells are present in uninjured extraocular muscles of mature mice.

Authors:  Linda K McLoon; Jonathan Wirtschafter
Journal:  Trans Am Ophthalmol Soc       Date:  2002

10.  Co-expression of multiple myosin heavy chain genes, in addition to a tissue-specific one, in extraocular musculature.

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3.  Pharyngeal Satellite Cells Undergo Myogenesis Under Basal Conditions and Are Required for Pharyngeal Muscle Maintenance.

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Review 5.  Stem cell therapy. Use of differentiated pluripotent stem cells as replacement therapy for treating disease.

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7.  RhoA/ROCK inhibition improves the beneficial effects of glucocorticoid treatment in dystrophic muscle: implications for stem cell depletion.

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9.  Effects of retinoic acid signaling on extraocular muscle myogenic precursor cells in vitro.

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10.  Mouse Extraocular Muscles and the Musculotopic Organization of Their Innervation.

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