Muscle-specific inactivation of the IGF-I receptor induces compensatory hyperplasia in skeletal muscle

Muscle-specific inactivation of the IGF-I receptor induces compensatory hyperplasia in skeletal muscle

During the development of skeletal muscle, myoblasts withdraw from the cell cycle and differentiate into myotubes. The insulin-like growth factors IGF-I and IGF-II, through their cognate tyrosine kinase receptor (IGF-I receptor), are known to play a role in this process. After withdrawal of myoblast...

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Veröffentlicht in:The Journal of clinical investigation 2002-02, Vol.109 (3), p.347-355
Hauptverfasser: Fernández, Ana M., Dupont, Joëlle, Farrar, Roger P., Lee, Sukho, Stannard, Bethel, Le Roith, Derek
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container_end_page 355
container_issue 3
container_start_page 347
container_title The Journal of clinical investigation
container_volume 109
creator Fernández, Ana M.
Dupont, Joëlle
Farrar, Roger P.
Lee, Sukho
Stannard, Bethel
Le Roith, Derek
description During the development of skeletal muscle, myoblasts withdraw from the cell cycle and differentiate into myotubes. The insulin-like growth factors IGF-I and IGF-II, through their cognate tyrosine kinase receptor (IGF-I receptor), are known to play a role in this process. After withdrawal of myoblasts from the cell cycle, IGF-I promotes muscle differentiation by inducing the expression or activity of myogenic regulatory factors (MyoD, myogenin) and effectors (p21). However, little is known about the intracellular mechanisms by which the IGF-I system regulates these factors during the process of myogenesis. Here we show that MKR mice, which express a dominant negative IGF-I receptor specifically in skeletal muscle, have marked muscle hypoplasia from birth to 3 weeks of age. This hypoplasia occurs concomitantly with a decrease in ERK immunoreactivity levels and decreases in MyoD and myogenin expression. BrdU immunocytochemistry showed a compensatory hyperplasia as MKR mice grew to adulthood. Interestingly, hyperplasia occurred concomitantly with an increase in p38, MyoD, myogenin, and p21 immunoreactivity levels, as well as a decrease in Twist levels. These findings suggest that regulation of these cellular elements by IGF-I may play a role in the development and differentiation of skeletal muscle in vivo.
doi_str_mv 10.1172/JCI13503
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title Muscle-specific inactivation of the IGF-I receptor induces compensatory hyperplasia in skeletal muscle
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