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大鼠胶质瘤中的血管分化与葡萄糖转运蛋白表达:类固醇的作用

Vascular differentiation and glucose transporter expression in rat gliomas: effects of steroids.

作者信息

Guerin C, Wolff J E, Laterra J, Drewes L R, Brem H, Goldstein G W

机构信息

Department of Neurosurgery, Johns Hopkins University School of Medicine, Baltimore, MD 21205.

出版信息

Ann Neurol. 1992 May;31(5):481-7. doi: 10.1002/ana.410310504.

DOI:10.1002/ana.410310504
PMID:1596083
Abstract

The GLUT1 isoform of the glucose transporter is normally expressed at high levels in differentiated brain vessels that also express a permeability barrier. In contrast, malignant brain neoplasms have relatively undifferentiated vessels that are highly permeable, proliferate to high vascular densities, and often lose GLUT1 expression. Using the rat intracerebral 9L glioma model, we investigated whether dexamethasone-induced changes in permeability are associated with the appearance of other differentiated vascular properties. The percentage of vessels expressing immunohistochemically detectable GLUT1 (74.2 +/- 6.1%) and the tumor vessel density as assessed by laminin immunostaining (282 +/- 37 vessels/mm2) did not vary with control tumor size. Dexamethasone treatment resulted in an 83% reduction of vascular permeability to intravenous Evans blue, an increased percentage of vessels expressing GLUT1 (106.4 +/- 10.5%), lower vascular density (102 +/- 64 vessels/mm2), and smaller tumor size (control cross-sectional area, 17.0 +/- 3.4 mm2; treated, 4.6 +/- 1.0 mm2). Essentially all vessels became GLUT1-positive after dexamethasone treatment. Increased GLUT1 expression by glioma vessels in association with the appearance of other signs of differentiation (low vascular density, slow tumor growth) suggests that immunostaining for GLUT1 may identify neoplasms that are biologically less aggressive.

摘要

葡萄糖转运蛋白的GLUT1亚型通常在分化的脑血管中高水平表达,这些脑血管也具有通透性屏障。相比之下,恶性脑肿瘤的血管相对未分化,具有高通透性,增殖至高血管密度,且常失去GLUT1表达。利用大鼠脑内9L胶质瘤模型,我们研究了地塞米松诱导的通透性变化是否与其他分化血管特性的出现相关。免疫组化检测到表达GLUT1的血管百分比(74.2±6.1%)以及通过层粘连蛋白免疫染色评估的肿瘤血管密度(282±37个血管/mm²)与对照肿瘤大小无关。地塞米松治疗导致静脉注射伊文思蓝后的血管通透性降低83%,表达GLUT1的血管百分比增加(106.4±10.5%),血管密度降低(102±64个血管/mm²),肿瘤大小减小(对照横截面积,17.0±3.4mm²;治疗后,4.6±1.0mm²)。地塞米松治疗后,基本上所有血管都变为GLUT1阳性。胶质瘤血管中GLUT1表达增加并伴有其他分化迹象(低血管密度、肿瘤生长缓慢)表明,GLUT1免疫染色可能识别出生物学上侵袭性较小的肿瘤。

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