Olf/Ebf transcription factors have been implicated in numerous developmental processes, ranging from B-cell development to neuronal differentiation. We describe mice that carry a targeted deletion within the Ebf2 (O/E3) gene. In Ebf2-null mutants, because of defective migration of gonadotropin releasing hormone-synthesizing neurons, formation of the neuroendocrine axis (which is essential for pubertal development) is impaired, leading to secondary hypogonadism. In addition, Ebf2(-/-) peripheral nerves feature defective axon sorting, hypomyelination, segmental dysmyelination and axonal damage, accompanied by a sharp decrease in motor nerve conduction velocity. Ebf2-null mice reveal a novel genetic cause of hypogonadotropic hypogonadism and peripheral neuropathy in the mouse, disclosing an important role for Ebf2 in neuronal migration and nerve development.

Hypogonadotropic hypogonadism and peripheral neuropathy in Ebf2-null mice / A. Corradi, L. Croci, V. Broccoli, S. Zecchini, S. Previtali, W. Wurst, S. Amadio, R. Maggi, A. Quattrini, G.G. Consalez. - In: DEVELOPMENT. - ISSN 0950-1991. - 130:2(2003 Jan), pp. 401-410.

Hypogonadotropic hypogonadism and peripheral neuropathy in Ebf2-null mice

S. Zecchini;R. Maggi;
2003

Abstract

Olf/Ebf transcription factors have been implicated in numerous developmental processes, ranging from B-cell development to neuronal differentiation. We describe mice that carry a targeted deletion within the Ebf2 (O/E3) gene. In Ebf2-null mutants, because of defective migration of gonadotropin releasing hormone-synthesizing neurons, formation of the neuroendocrine axis (which is essential for pubertal development) is impaired, leading to secondary hypogonadism. In addition, Ebf2(-/-) peripheral nerves feature defective axon sorting, hypomyelination, segmental dysmyelination and axonal damage, accompanied by a sharp decrease in motor nerve conduction velocity. Ebf2-null mice reveal a novel genetic cause of hypogonadotropic hypogonadism and peripheral neuropathy in the mouse, disclosing an important role for Ebf2 in neuronal migration and nerve development.
COE2; Dysmyelination; Gene targeting; GnRH neurons; Homologous recombination; Knockout; Neural development; Neuroendocrine; Neurogenesis; Neuronal migration; O/E3; Olf/Ebf genes; Peripheral nerve; Peripheral neuropathy; Targeted inactivation
Settore BIO/09 - Fisiologia
gen-2003
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/175329
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