首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Regulation of TrkA and ChAT expression in developing rat basal forebrain: evidence that both exogenous and endogenous NGF regulate differentiation of cholinergic neurons.
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Regulation of TrkA and ChAT expression in developing rat basal forebrain: evidence that both exogenous and endogenous NGF regulate differentiation of cholinergic neurons.

机译:发育中大鼠基底前脑中TrkA和ChAT表达的调节:证据表明外源性和内源性NGF均可调节胆碱能神经元的分化。

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TrkA is a receptor tyrosine kinase whose activation transduces NGF signaling. TrkA expression has been demonstrated in NGF-responsive adult basal forebrain cholinergic neurons (BFCNs). Several lines of evidence have suggested that endogenous NGF plays a role in the development and differentiation of these neurons. We examined TrkA expression during development. TrkA mRNA and protein were present in basal forebrain neurons during the entire postnatal period; the distribution of neurons bearing these markers was identical to that for those containing choline acetyltransferase (ChAT) mRNA, suggesting that, as in the adult, TrkA gene expression is localized to BFCNs. The expression of TrkA and ChAT followed a very similar temporal pattern, suggesting regulation by the same factor(s). We discovered that NGF administration in vivo activated TrkA receptors, and increased both TrkA and ChAT mRNA; conversely, anti-NGF infusions suppressed expression of both genes. These results suggest that endogenous NGF regulates expression of TrkA and ChAT. Finally, while NGF infusion increased the size of developing BFCNs, NGF antibodies inhibited the normal developmental increase. The results are evidence that endogenous NGF acts on developing BFCNs to enhance gene expression and cellular differentiation.
机译:TrkA是一种受体酪氨酸激酶,其激活可转导NGF信号传导。 TrkA表达已在NGF响应​​的成人基底前脑胆碱能神经元(BFCNs)中得到证实。几条证据表明内源性NGF在这些神经元的发育和分化中起作用。我们在开发过程中检查了TrkA表达。在整个产后期间,TrkA mRNA和蛋白存在于基底前脑神经元中。带有这些标记的神经元的分布与含有胆碱乙酰基转移酶(ChAT)mRNA的神经元的分布相同,这表明与成年人一样,TrkA基因的表达也定位于BFCN。 TrkA和ChAT的表达遵循非常相似的时间模式,表明受到相同因素的调控。我们发现在体内施用NGF激活了TrkA受体,并增加了TrkA和ChAT mRNA。相反,抗NGF输注抑制了两个基因的表达。这些结果表明内源性NGF调节TrkA和ChAT的表达。最后,尽管NGF注入增加了发育中的BFCN的大小,但NGF抗体抑制了正常发育的增长。结果证明内源性NGF作用于发育中的BFCN,以增强基因表达和细胞分化。

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