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Defective brain development in mice lacking the Hif-1alpha gene in neural cells
Authors:Tomita Shuhei  Ueno Masaki  Sakamoto Masami  Kitahama Yuki  Ueki Masaaki  Maekawa Nobuhiro  Sakamoto Haruhiko  Gassmann Max  Kageyama Ryoichiro  Ueda Natsuo  Gonzalez Frank J  Takahama Yousuke
Affiliation:Department of Immune System Development, RIKEN Research Center for Allergy and Immunology, Tokushima 770-8503, Japan. tomita@genome.tokushima-u.ac.jp
Abstract:Hypoxia-inducible factor 1alpha (HIF-1alpha) is essential for vascular development during embryogenesis and pathogenesis. However, little is known about its role in brain development. To investigate the function of HIF-1alpha in the central nervous system, a conditional knockout mouse was made with the Cre/LoxP system with a nestin promoter-driven Cre. Neural cell-specific HIF-1alpha-deficient mice exhibit hydrocephalus accompanied by a reduction in neural cells and an impairment of spatial memory. Apoptosis of neural cells coincided with vascular regression in the telencephalon of mutant embryos, and these embryonic defects were successfully restored by in vivo gene delivery of HIF-1alpha to the embryos. These results showed that expression of HIF-1alpha in neural cells was essential for normal development of the brain and established a mouse model that would be useful for the evaluation of therapeutic strategies for ischemia, including hypoxia-mediated hydrocephalus.
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