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转基因小鼠表皮中神经生长因子的过表达导致外周神经系统肥大。

Overexpression of nerve growth factor in epidermis of transgenic mice causes hypertrophy of the peripheral nervous system.

作者信息

Albers K M, Wright D E, Davis B M

机构信息

Department of Pathology, University of Kentucky College of Medicine, Lexington 40536.

出版信息

J Neurosci. 1994 Mar;14(3 Pt 2):1422-32. doi: 10.1523/JNEUROSCI.14-03-01422.1994.

DOI:10.1523/JNEUROSCI.14-03-01422.1994
PMID:8126547
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6577586/
Abstract

Survival of developing neurons is dependent on access to a limited supply of target-derived neurotrophic factors. NGF is the most extensively characterized of these molecules and during development is synthesized by neuronal and nonneuronal target tissues such as the skin. To investigate how target-derived NGF affects neuron survival and development of the PNS, we used an epidermal-specific gene promoter to produce transgenic mice that overexpress the mouse NGF cDNA in skin. Analysis of transgenic skin mRNA synthesis by Northern and in situ hybridizations showed increased levels of transgene-derived mRNA in the epidermis and associated hair follicles. The increase in NGF mRNA correlated with a hypertrophy of peripheral sensory and sympathetic nerves. Immunological analysis of skin using an anti-150 kDa neurofilament antibody showed numerous large nerve bundles and fibers coursing throughout the dermis. Increased numbers of nerve processes in the transgenic skin had immunoreactivity for calcitonin gene-related peptide and tyrosine hydroxylase, indicating that both the sensory and sympathetic systems were hypertrophied. The trigeminal and superior cervical ganglia were greatly enlarged. Cell counts of trigeminal ganglia of control and transgenic mice showed a 26-117% increase in the number of neurons in the transgenics, indicating a reduction or total prevention of the program of naturally occurring cell death. These results demonstrate that NGF production by the epidermal target tissue controls neuronal survival, and in so doing, establishes the level of innervation.

摘要

发育中神经元的存活依赖于获取有限的靶源性神经营养因子。神经生长因子(NGF)是这些分子中特征描述最为广泛的,在发育过程中由神经元和非神经元靶组织如皮肤合成。为了研究靶源性NGF如何影响周围神经系统(PNS)神经元的存活和发育,我们使用表皮特异性基因启动子制备了在皮肤中过表达小鼠NGF cDNA的转基因小鼠。通过Northern杂交和原位杂交对转基因皮肤mRNA合成进行分析,结果显示表皮和相关毛囊中转基因衍生的mRNA水平升高。NGF mRNA的增加与外周感觉神经和交感神经的肥大相关。使用抗150 kDa神经丝抗体对皮肤进行免疫分析,结果显示真皮中有大量粗大的神经束和神经纤维。转基因皮肤中神经突起数量增加,对降钙素基因相关肽和酪氨酸羟化酶具有免疫反应性,表明感觉和交感神经系统均肥大。三叉神经节和颈上神经节显著增大。对对照小鼠和转基因小鼠的三叉神经节进行细胞计数,结果显示转基因小鼠中神经元数量增加了26%-117%,表明自然发生的细胞死亡程序减少或完全被阻止。这些结果表明,表皮靶组织产生的NGF控制着神经元的存活,并以此确定神经支配水平。

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