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胶质瘤细胞的弥漫性脑侵袭需要β1整合素。

Diffuse brain invasion of glioma cells requires beta 1 integrins.

作者信息

Paulus W, Baur I, Beutler A S, Reeves S A

机构信息

Division of Neuropathology, University of Erlangen Medical School, Germany.

出版信息

Lab Invest. 1996 Dec;75(6):819-26.

PMID:8973477
Abstract

Diffuse invasion of brain tissue by single tumor cells is a characteristic feature of gliomas and a major reason why these tumors cannot be completely resected. The molecular basis of brain invasion is poorly understood. We regulated the expression of beta 1 integrins, the major group of extracellular matrix receptors, in astrocytic tumor cells by using a tetracycline-dependent transcription control system. Rat C6 glioma cells were stably transfected with (a) the tetracycline-controlled transactivator (tTA) gene, (b) antisense beta 1 cDNA under the control of a tTA/tetracycline-responsive promoter, and (c) the beta-galactosidase (lacZ) gene for histochemical identification. In one clone, C6TL beta, beta 1 protein levels were unaffected in the presence of tetracycline, but they were reduced by 60% in the absence of tetracycline because of production of antisense mRNA. C6TL beta cells were transplanted into the striatum of nude mice. After 14 days in the presence of tetracycline in the drinking water, tumors showed diffuse brain invasion, mainly along vascular basement membranes. In the absence of tetracycline, however, tumor cells were compact and generally well delineated from the surrounding brain tissue. These data, ie, blocking of brain invasion by antisense beta 1 mRNA, either because of disturbed interaction of beta 1 with brain extracellular matrix components or interference with beta 1-dependent signaling pathways, strongly suggest that beta 1 integrins are required for diffuse brain invasion of gliomas.

摘要

单个肿瘤细胞对脑组织的弥漫性浸润是胶质瘤的一个特征性表现,也是这些肿瘤无法完全切除的主要原因。脑浸润的分子基础目前了解甚少。我们通过使用四环素依赖性转录控制系统来调节星形细胞瘤细胞中β1整合素(细胞外基质受体的主要类别)的表达。将大鼠C6胶质瘤细胞稳定转染(a)四环素调控反式激活因子(tTA)基因、(b)在tTA/四环素反应性启动子控制下的反义β1 cDNA以及(c)用于组织化学鉴定的β-半乳糖苷酶(lacZ)基因。在一个克隆C6TLβ中,在有四环素存在时β1蛋白水平未受影响,但在无四环素时,由于反义mRNA的产生,β1蛋白水平降低了60%。将C6TLβ细胞移植到裸鼠的纹状体中。在饮用水中加入四环素14天后,肿瘤呈现弥漫性脑浸润,主要沿血管基底膜浸润。然而,在无四环素时,肿瘤细胞紧密聚集,通常与周围脑组织界限清晰。这些数据,即反义β1 mRNA阻断脑浸润,要么是因为β1与脑外基质成分的相互作用受到干扰,要么是因为干扰了β1依赖性信号通路,强烈提示β1整合素是胶质瘤弥漫性脑浸润所必需的。

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