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酶性血脑屏障的研究:微血管壁中多巴脱羧酶的定量测定及其与不同中枢神经系统区域实质的关系。

Studies on the enzymatic blood-brain barrier: quantitative measurements of DOPA decarboxylase in the wall of microvessels as related to the parenchyma in various CNS regions.

作者信息

Hardebo J E, Falck B, Owman C, Rosengren E

出版信息

Acta Physiol Scand. 1979 Apr;105(4):453-60. doi: 10.1111/j.1748-1716.1979.tb00110.x.

Abstract

The presence of DOPA decarboxylase in cerebral microvessels (capillaries and venules) impedes the passage of circulating amine precursors into the brain. The relative amount of DOPA decarboxylase in this trapping mechanism as compared to the parenchyma per se was estimated in various CNS regions, measuring the formation of dopamine from L-DOPA in vitro or in vivo in two experimental models on rats and rabbits: (1) On the basis of the treatment with a peripheral decarboxylase inhibitor (carbidopa, which inhibits also microvascular DOPA decarboxylase in the CNS) it could be calculated that the enzyme in the microvessels of the caudate nucleus (rich in catecholamine nerve terminals), cerebellum (poor in catecholamine nerves), and spinal cord comprised 25, 91 and 79 per cent, respectively, of the total enzyme activity. (2) Measurement of dopamine formation in the spinal cord following transection at the midthoracic level (which causes degeneration of the catecholamine neurons caudal to the lesion since they are all descending) indicated that a similar fraction as found in the carbidopa model, 71%, of the total tissue decarboxylase activity resided in the microvessel walls. The results show that a considerable portion of tissue decarboxylase in the CNS is present in the microvessel walls, where it represents part of an enzymatic blood-brain barrier mechanism.

摘要

脑微血管(毛细血管和小静脉)中多巴脱羧酶的存在阻碍了循环中的胺前体进入大脑。在大鼠和兔子的两种实验模型中,通过体外或体内测量左旋多巴转化为多巴胺的量,估算了在这种捕获机制中多巴脱羧酶与脑实质本身相比的相对含量。实验涉及中枢神经系统的各个区域:(1)根据外周脱羧酶抑制剂(卡比多巴,它也抑制中枢神经系统中的微血管多巴脱羧酶)的处理,可以计算出尾状核(富含儿茶酚胺神经末梢)、小脑(儿茶酚胺神经较少)和脊髓微血管中的酶分别占总酶活性的25%、91%和79%。(2)在胸段中部横断脊髓(这会导致损伤尾侧的儿茶酚胺神经元变性,因为它们都是下行的)后测量脊髓中多巴胺的形成,结果表明,与卡比多巴模型中发现的相似比例,即71%的总组织脱羧酶活性存在于微血管壁中。结果表明,中枢神经系统中相当一部分组织脱羧酶存在于微血管壁中,它是酶性血脑屏障机制的一部分。

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