期刊
NEURON
卷 67, 期 5, 页码 781-796出版社
CELL PRESS
DOI: 10.1016/j.neuron.2010.08.008
关键词
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资金
- Project ALS
- NIH [R01 NS044385, P01 NS055923, R01 NS062822]
- Alfred P. Sloan Foundation
- Burroughs Welcome Fund
- McKnight Foundation
- NYStem
In the developing spinal cord, regional and combinatorial activities of Hox transcription factors are critical in controlling motor neuron fates along the rostrocaudal axis, exemplified by the precise pattern of limb innervation by more than fifty Hox-dependent motor pools. The mechanisms by which motor neuron diversity is constrained to limb levels are, however, not well understood. We show that a single Hox gene, Hoxc9, has an essential role in organizing the motor system through global repressive activities. Hoxc9 is required for the generation of thoracic motor columns, and in its absence, neurons acquire the fates of limb-innervating populations. Unexpectedly, multiple Hox genes are derepressed in Hoxc9 mutants, leading to motor pool disorganization and alterations in the connections by thoracic and forelimb-level subtypes. Genome-wide analysis of Hoxc9 binding suggests that this mode of repression is mediated by direct interactions with Hox regulatory elements, independent of chromatin marks typically associated with repressed Hox genes.
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