Literature DB >> 31208207

An altered response in macrophage phenotype following damage in aged human skeletal muscle: implications for skeletal muscle repair.

Jacob R Sorensen1,2, Jamie P Kaluhiokalani1, Paul S Hafen1, Michael R Deyhle1, Allen C Parcell1, Robert D Hyldahl1.   

Abstract

The purpose of this study was to test the hypothesis that macrophage polarization is altered in old compared to young skeletal muscle, possibly contributing to the poor satellite cell response observed in older muscle tissue. Muscle biopsies were collected prior to and at 3, 24, and 72 h following a muscle-damaging exercise in young and old individuals. Immunohistochemistry was used to measure i.m. macrophage content and phenotype, and cell culture experiments tested macrophage behavior and influence on primary myoblasts from older individuals. We found that macrophage infiltration was similar between groups at 24 (young: 3712 ± 2407 vs. old: 5035 ± 2978 cells/mm3) and 72 (young: 4326 ± 2622 vs. old: 5287 ± 2248 cells/mm3) hours postdamage, yet the proportion of macrophages that expressed the proinflammatory marker CD11b were markedly lower in the older subjects (young: 74.5 ± 15 vs. old: 52.6 ± 17%). This finding was coupled with a greater overall proportion of CD206+, anti-inflammatory macrophages in the old (group: P = 0.0005). We further demonstrate in vitro that proliferation, and in some cases differentiation, of old primary human myoblasts increase as much as 30% when exposed to a young macrophage-conditioned environment. Collectively, the data suggest that old macrophages appear less capable of adapting and maintaining inflammatory function, which may contribute to poor satellite cell activation and delayed recovery from muscle damage.-Sorensen, J. R., Kaluhiokalani, J. P., Hafen, P. S., Deyhle, M. R., Parcell, A. C., Hyldahl, R. D. An altered response in macrophage phenotype following damage in aged human skeletal muscle: implications for skeletal muscle repair.

Entities:  

Keywords:  immune cells; inflammation; muscle damage; primary myoblasts; satellite cell

Mesh:

Year:  2019        PMID: 31208207     DOI: 10.1096/fj.201900519R

Source DB:  PubMed          Journal:  FASEB J        ISSN: 0892-6638            Impact factor:   5.191


  8 in total

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Review 3.  Aging of the immune system and impaired muscle regeneration: A failure of immunomodulation of adult myogenesis.

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5.  Exosomes derived from inflammatory myoblasts promote M1 polarization and break the balance of myoblast proliferation/differentiation.

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6.  Phytoecdysteroids Accelerate Recovery of Skeletal Muscle Function Following in vivo Eccentric Contraction-Induced Injury in Adult and Old Mice.

Authors:  Kevin A Zwetsloot; R Andrew Shanely; Joshua S Godwin; Charles F Hodgman
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7.  Metabolipidomic profiling reveals an age-related deficiency of skeletal muscle pro-resolving mediators that contributes to maladaptive tissue remodeling.

Authors:  James F Markworth; Lemuel A Brown; Eunice Lim; Jesus A Castor-Macias; Jacqueline Larouche; Peter C D Macpherson; Carol Davis; Carlos A Aguilar; Krishna Rao Maddipati; Susan V Brooks
Journal:  Aging Cell       Date:  2021-06-02       Impact factor: 11.005

8.  Muscle Microbiopsy to Delineate Stem Cell Involvement in Young Patients: A Novel Approach for Children With Cerebral Palsy.

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  8 in total

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