Am. J. Respir. Crit. Care Med., Vol 150, No. 1, 07 1994, 174-178.
Age-related changes in diaphragm muscle contractile properties and myosin heavy chain isoforms [published erratum appears in Am J Respir Crit Care Med 1994 Sep;150(3):879]
LE Gosselin, BD Johnson and GC Sieck
Department of Anesthesiology, Mayo Clinic and Foundation, Rochester, Minnesota 55902.
The present study sought to examine the effects of aging on the isometric
contractile and fatigue properties as well as the myosin heavy chain (MCH)
isoform composition of the rat diaphragm muscle. Male Fischer 344 (F344)
specific pathogen-free rats 6 and 24 mo old were used in the study. Peak
twitch force was approximately 23% lower (p < 0.05) in the senescent
diaphragm compared with the young. Time to peak twitch force and one-half
relaxation time of twitch force did not differ between groups. There was a
significant decrease (15 to 18%, p < 0.05) in the specific force (N/cm2)
of the senescent diaphragm at all stimulation frequencies (10 to 100 Hz)
examined. In addition, the fatigability of the diaphragm did not
significantly differ between the two groups. No significant changes in the
distribution of MHC 1 and 2A isoforms were observed with aging. However,
the contribution of MHC 2X significantly decreased with senescence (young,
37.5%; senescent, 30.5%), whereas the contribution of MHC 2B in the
senescent diaphragm was significantly higher (young, 6.5%; senescent,
15.0%; p < 0.05). We conclude that the age-related decline in diaphragm
muscle specific force is caused by intrinsic factors other than changes in
MHC composition.
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Copyright © 1994 American Thoracic Society
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