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封闭蛋白在人肿瘤性和非肿瘤性脑微血管中的表达

Occludin expression in microvessels of neoplastic and non-neoplastic human brain.

作者信息

Papadopoulos M C, Saadoun S, Woodrow C J, Davies D C, Costa-Martins P, Moss R F, Krishna S, Bell B A

机构信息

Department of Neurosurgery, Atkinson Morley's Hospital, London SW20 0NE, UK.

出版信息

Neuropathol Appl Neurobiol. 2001 Oct;27(5):384-95. doi: 10.1046/j.0305-1846.2001.00341.x.

Abstract

The tight junction protein occludin 'glues' normal, adjacent brain microvessel endothelial cells together. Malignant brain tumours cause cerebral oedema because they have leaky endothelial tight junctions, which allow plasma fluid to enter the brain from the microvessel lumen. In order to identify molecular abnormalities in tumour endothelial tight junctions, we investigated occludin expression in microvessels from adult human non-neoplastic brain tissue using immunohistochemistry and immunoblotting. The proportions of microvessels immunolabelling for occludin were >2/3 in 5/5 non-neoplastic brain tissue samples, >1/3 in 5/5 low grade (Daumas-Duport I or II) astrocytomas and <1/3 in 5/5 high grade (III or IV) astrocytomas and 6/6 metastatic adenocarcinomas. Six non-neoplastic brain tissue immunoblots gave a 55-kDa occludin band, three low-grade astrocytomas gave 55-kDa and 60-kDa bands, 13 high-grade astrocytomas gave 60-kDa or no band and four adenocarcinomas did not give an occludin band. Expression of 55-kDa occludin inversely correlated with the presence of contrast enhancement on computed tomograms (P < 0.001). Electron microscopy showed open endothelial tight junctions in 0/2 non-neoplastic human brain specimens and 2/2 high-grade astrocytomas. We suggest that loss of 55-kDa occludin expression in human brain tumours may contribute to endothelial tight junction opening. Characterizing the molecular pathology of brain endothelial tight junctions may facilitate the design of novel drugs against cerebral oedema.

摘要

紧密连接蛋白闭合蛋白将正常相邻的脑微血管内皮细胞“黏合”在一起。恶性脑肿瘤会导致脑水肿,因为它们的内皮紧密连接有渗漏,使得血浆液体能够从微血管腔进入脑内。为了确定肿瘤内皮紧密连接中的分子异常,我们使用免疫组织化学和免疫印迹法研究了成人非肿瘤性脑组织微血管中闭合蛋白的表达。在5份非肿瘤性脑组织样本中,免疫标记闭合蛋白的微血管比例>2/3;在5份低级别(达马-迪波尔I级或II级)星形细胞瘤中,该比例>1/3;而在5份高级别(III级或IV级)星形细胞瘤和6份转移性腺癌中,该比例<1/3。6份非肿瘤性脑组织的免疫印迹显示有一条55 kDa的闭合蛋白条带,3份低级别星形细胞瘤显示有55 kDa和60 kDa的条带,13份高级别星形细胞瘤显示有60 kDa的条带或无条带,4份腺癌未显示闭合蛋白条带。55 kDa闭合蛋白的表达与计算机断层扫描上的对比增强呈负相关(P<0.001)。电子显微镜检查显示,2份非肿瘤性人脑标本中有0份、2份高级别星形细胞瘤中有2份存在开放的内皮紧密连接。我们认为,人脑肿瘤中55 kDa闭合蛋白表达的缺失可能导致内皮紧密连接开放。了解脑内皮紧密连接的分子病理学特征可能有助于设计抗脑水肿的新型药物。

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