Abstract
Muscle spindles are skeletal muscle sensory organs that provide axial and limb position information (proprioception) to the central nervous system. Spindles consist of encapsulated muscle fibers (intrafusal fibers) that are innervated by specialized motor and sensory axons. Although the molecular mechanisms involved in spindle ontogeny are poorly understood, the innervation of a subset of developing myotubes (type I) by peripheral sensory afferents (group la) is a critical event for inducing intrafusal fiber differentiation and subsequent spindle formation. The Egr family of zinc- finger transcription factors, whose members include Egr1 (NGFI-A), Egr2 (Krox-20), Egr3 and Egr4 (NGFIC), are thought to regulate critical genetic programs involved in cellular growth and differentiation (refs 4-8, and W.G.T. et al., manuscript submitted). Mice deficient in Egr3 were generated by gene targeting and had gait ataxia, increased frequency of perinatal mortality, scoliosis, resting tremors and ptosis. Although extrafusal skeletal muscle fibers appeared normal, Egr3-deficient animals lacked muscle spindles, a finding that is consistent with their profound gait ataxia. Egr3 was highly expressed in developing muscle spindles, but not in la afferent neurons or their terminals during developmental periods that coincided with the induction of spindle morphogenesis by sensory afferent axons. These results indicate that type 1 myotubes are dependent upon Egr3-mediated transcription for proper spindle development.
Original language | English (US) |
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Pages (from-to) | 87-91 |
Number of pages | 5 |
Journal | Nature Genetics |
Volume | 20 |
Issue number | 1 |
DOIs | |
State | Published - 1998 |
Funding
We greatly appreciate technical assistance from L. Cabalka Tourtellotte, G. Gavrilina, T. Gorodinsky, C. Bollinger and L. Roberts. We thank E. Johnson, J. Lichtman, J. Sanes and B. Snider for their comments and suggestions during the preparation of this manuscript. The antibodies to Parvalbumin (R301), slow-tonic myosin heavy chain (S46) and Egr3 were generous gifts from K. Baimbridge, F. Stockdale and J. Baraban, respectively. A. Pestronk generously provided the ATPase histochemistry protocols. This work was supported by MH1426 (W.G.T.) and CA13730 (J.M.).
ASJC Scopus subject areas
- Genetics