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Expression of two developmentally regulated brain-specific proteins is correlated with late outgrowth of the pyramidal tract

机译:两种发育受调节的大脑特异性蛋白的表达与锥体束的晚期生长相关

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摘要

The regulation of axon outgrowth is not well understood. In previous studies, however, axon elongation has been well correlated with expression of a small number of growth-associated proteins (GAPs). To identify other proteins whose expression could be correlated with axon outgrowth during development of CNS pathways, monoclonal antibodies were raised against growth cone particles isolated from neonatal hamster brains. Two of these antibodies recognized a brain-specific 33 kDa protein associated with intracellular membranes of axons and growth cones. Immunoblotting demonstrated a sharp developmental decline in levels of the protein in hamster brain during the first postnatal week and a more gradual decline thereafter. Immunocytochemical studies with the antibodies revealed ubiquitous staining of the neuropil during the first several days, which by the end of the first week became restricted to a few later-maturing pathways. Staining was most intense in the pyramidal tract and was well correlated with axon outgrowth, which continues until 14 d in this pathway. These results suggest that the 33 kDa protein may, like previously identified GAPs, play a role in axon elongation. Late outgrowth of the hamster pyramidal tract is also correlated with expression of another developmentally regulated protein, the high-molecular-weight neurofilament subunit (NF-H). Immunostaining with a monoclonal antibody that recognized phosphorylated NF-H demonstrated that this subunit does not begin to appear in the late-maturing pyramidal tract fibers until several weeks after birth, in striking contrast to intense immunoreactivity of other spinal cord pathways from postnatal day 1. This finding suggests that specific pathways may have a highly idiosyncratic time course for expression of neurofilament subunits.
机译:轴突生长的调控尚不十分清楚。但是,在以前的研究中,轴突伸长与少量的生长相关蛋白(GAP)的表达高度相关。为了鉴定在中枢神经系统通路发育过程中其表达可能与轴突生长相关的其他蛋白质,提出了针对从新生仓鼠脑中分离的生长锥颗粒的单克隆抗体。这些抗体中的两种可识别与轴突和生长锥的细胞内膜相关的大脑特异性33 kDa蛋白。免疫印迹显示,在产后的第一个星期内,仓鼠大脑中蛋白质的水平急剧下降,此后逐渐下降。用抗体进行的免疫细胞化学研究表明,神经纤维蛋白在头几天内普遍存在染色,到第一周结束时,其染色仅限于一些较晚的成熟途径。染色在锥体束中最强烈,并且与轴突生长密切相关,轴突生长一直持续到该途径的14 d。这些结果表明33 kDa的蛋白质可能像以前确定的GAP一样,在轴突伸长中起作用。仓鼠锥体束的较晚生长也与另一种发育受调节的蛋白,高分子量神经丝亚基(NF-H)的表达有关。用识别磷酸化NF-H的单克隆抗体进行的免疫染色表明,该亚基直到出生后几周才开始在成熟的锥体束纤维中出现,这与出生后第一天其他脊髓途径的强烈免疫反应性形成鲜明对比。该发现表明特定的途径对于神经丝亚单位的表达可能具有高度的特异时间过程。

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