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发育中大鼠脑内少突胶质前体细胞上NG2蛋白聚糖与血小板源性生长因子α受体的共定位

Co-localization of NG2 proteoglycan and PDGF alpha-receptor on O2A progenitor cells in the developing rat brain.

作者信息

Nishiyama A, Lin X H, Giese N, Heldin C H, Stallcup W B

机构信息

La Jolla Cancer Research Foundation, California, USA.

出版信息

J Neurosci Res. 1996 Feb 1;43(3):299-314. doi: 10.1002/(SICI)1097-4547(19960201)43:3<299::AID-JNR5>3.0.CO;2-E.

Abstract

A detailed comparison in the developing rat central nervous system between the distribution of the NG2 proteoglycan and the alpha-receptor for platelet-derived growth factor (PDGF) shows that these two molecules are co-expressed by glial progenitor cells of the O2A lineage and can serve as reliable markers for identification of O2A cells in vivo. Our mapping experiments indicate that NG2-positive, PDGF alpha-receptor positive O2A cells are abundant throughout the developing central nervous system in both white and gray matter. The earliest cells immunoreactive for either of the two markers are found adjacent to the central canal of the embryonic day 15 (E15) spinal cord. These cells express only PDGF alpha-receptor and not NG2. By E17, process-bearing cells expressing both NG2 and PDGF alpha-receptor in a highly co-localized fashion are found throughout the central nervous system. The first postnatal week marks the peak in the number of NG2 and PDGF alpha-receptor immunoreactive cells, as well as the peak in the level of expression and the extent of co-localization of the two molecules. After the first week, the level of expression of both NG2 and PDGF alpha-receptor declines, although both molecules continue to be expressed in the adult brain. On O2A cells in the mature brain, NG2 and PDGF alpha-receptor are not as well co-localized at the subcellular level as they are on O2A cells in the younger brain. The functional consequences of co-localization and subsequent dissociation of NG2 and PDGF alpha-receptor on maturing O2A progenitors are investigated in the accompanying paper (Nishiyama et al.: J Neurosci Res 43:315-330, 1996).

摘要

在发育中的大鼠中枢神经系统中,对神经胶质2蛋白聚糖(NG2)和血小板衍生生长因子(PDGF)α受体的分布进行详细比较后发现,这两种分子由O2A谱系的神经胶质祖细胞共同表达,并且可作为在体内识别O2A细胞的可靠标志物。我们的定位实验表明,NG2阳性、PDGF α受体阳性的O2A细胞在整个发育中的中枢神经系统的白质和灰质中都很丰富。最早对这两种标志物中的任何一种呈免疫反应的细胞出现在胚胎第15天(E15)脊髓中央管附近。这些细胞仅表达PDGF α受体,而不表达NG2。到E17时,在整个中枢神经系统中都能发现以高度共定位方式同时表达NG2和PDGF α受体的有突起的细胞。出生后的第一周是NG2和PDGF α受体免疫反应性细胞数量的峰值,也是这两种分子表达水平和共定位程度的峰值。第一周之后,NG2和PDGF α受体的表达水平均下降,不过这两种分子在成年大脑中仍继续表达。在成熟大脑的O2A细胞上,NG2和PDGF α受体在亚细胞水平上的共定位情况不如在较年轻大脑的O2A细胞上那样好。随附论文(西山等人:《神经科学研究杂志》43:315 - 330,1996年)对成熟的O2A祖细胞上NG2和PDGF α受体的共定位及随后的解离所产生的功能后果进行了研究。

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