Skeletal muscle molecular alterations precede whole-muscle dysfunction in NYHA Class II heart failure patients | Zendy

Michael P. Godard | Zendy; Si Young Song | Zendy; Delafontaine | Zendy; Whitman | Zendy

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Skeletal muscle molecular alterations precede whole-muscle dysfunction in NYHA Class II heart failure patients

Author(s) -

Michael P. Godard,

Si Young Song,

Delafontaine,

Whitman

Publication year - 2012

Publication title -

clinical interventions in aging

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 1.184

H-Index - 76

eISSN - 1178-1998

pISSN - 1176-9092

DOI - 10.2147/cia.s37879

Subject(s) - skeletal muscle , heart failure , medicine , myosin , endocrinology , myh7 , isometric exercise , myocyte , heart disease , muscle hypertrophy , biology , myosin light chain kinase , microbiology and biotechnology

Heart failure (HF), a debilitating disease in a growing number of adults, exerts structural and neurohormonal changes in both cardiac and skeletal muscles. However, these alterations and their affected molecular pathways remain uncharacterized. Disease progression is known to transform skeletal muscle fiber composition by unknown mechanisms. In addition, perturbation of specific hormonal pathways, including those involving skeletal muscle insulin-like growth factor-1 (IGF-1) and insulin-like growth factor-binding protein-5 (IGFB-5) appears to occur, likely affecting muscle metabolism and regeneration. We hypothesized that changes in IGF-1 and IGFB-5 mRNA levels correlate with the transformation of single-skeletal muscle fiber myosin heavy chain isoforms early in disease progression, making these molecules valuable markers of skeletal muscle changes in heart failure.

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