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来自胚胎或新生大鼠的星形胶质细胞培养物中,125I-博尔顿·亨特P物质结合以及P物质诱导的磷脂酶C激活存在显著的区域异质性。

Marked regional heterogeneity of 125I-Bolton Hunter substance P binding and substance P-induced activation of phospholipase C in astrocyte cultures from the embryonic or newborn rat.

作者信息

Beaujouan J C, Daguet de Montety M C, Torrens Y, Saffroy M, Dietl M, Glowinski J

机构信息

Collège de France, INSERM U 114, Paris.

出版信息

J Neurochem. 1990 Feb;54(2):669-75. doi: 10.1111/j.1471-4159.1990.tb01923.x.

DOI:10.1111/j.1471-4159.1990.tb01923.x
PMID:1688922
Abstract

The specific binding of 125I-Bolton Hunter substance P (125I-BHSP) was estimated on 4- to 5-week-old primary cultures of astrocytes from several brain structures and the spinal cord of 16-day-old embryonic or newborn rats. In both cases, high levels of binding of 125I-BHSP were found on intact astrocytes from the brainstem, but this binding was low or negligible on cells from the cerebral cortex, striatum, hypothalamus, and mesencephalon. In addition, hippocampal astrocytes from newborn rats were also devoid of 125I-BHSP binding sites, while a binding of 125I-BHSP (half that of brainstem cells) was observed on astrocytes from the cerebellum and spinal cord. It was also shown that this regional heterogeneity in 125I-BHSP binding was not linked to differences in the inactivation of the ligand, cell plating density. or eventual cell contaminants. Five-day-old cultures from 16-day-old embryos were used to estimate 125I-BHSP binding on neuron-enriched cultures. Specific 125I-BHSP binding was found on cells from the brainstem, mesencephalon, and hypothalamus, but neurons from the cerebral cortex or the striatum contained low or negligible amounts of 125I-BHSP binding sites. Competition studies using tachykinins and SP analogues indicated that 125I-BHSP binding sites on brainstem astrocytes (16-day-old embryos) have the pharmacological profile expected for NK1 binding sites. SP (1 microM) stimulated phosphoinositide breakdown in cells rich in 125I-BHSP binding sites (brainstem) but not in those devoid of 125I-BHSP binding (striatum).(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在来自16日龄胚胎或新生大鼠的几种脑结构及脊髓的4至5周龄原代星形胶质细胞培养物上,对125I - 博尔顿·亨特P物质(125I - BHSP)的特异性结合进行了评估。在这两种情况下,均发现来自脑干的完整星形胶质细胞上125I - BHSP的结合水平很高,但来自大脑皮质、纹状体、下丘脑和中脑的细胞上这种结合水平很低或可忽略不计。此外,新生大鼠海马星形胶质细胞也没有125I - BHSP结合位点,而在来自小脑和脊髓的星形胶质细胞上观察到125I - BHSP的结合(为脑干细胞结合的一半)。还表明,125I - BHSP结合的这种区域异质性与配体失活、细胞接种密度或最终的细胞污染物差异无关。使用来自16日龄胚胎的5日龄培养物来评估125I - BHSP在富含神经元的培养物上的结合。在来自脑干、中脑和下丘脑的细胞上发现了特异性的125I - BHSP结合,但来自大脑皮质或纹状体的神经元含有少量或可忽略不计的125I - BHSP结合位点。使用速激肽和P物质类似物的竞争研究表明,脑干星形胶质细胞(16日龄胚胎)上的125I - BHSP结合位点具有NK1结合位点预期的药理学特征。P物质(1微摩尔)刺激了富含125I - BHSP结合位点的细胞(脑干)中的磷酸肌醇分解,但未刺激缺乏125I - BHSP结合的细胞(纹状体)中的磷酸肌醇分解。(摘要截短于250字)

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