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在携带5-氨基酮戊酸诱导的卟啉荧光的胶质瘤和转移组织中的水通道蛋白4

Aquaporin-4 in glioma and metastatic tissues harboring 5-aminolevulinic acid-induced porphyrin fluorescence.

作者信息

Suero Molina Eric Jose, Ardon Hilko, Schroeteler Juliane, Klingenhöfer Mark, Holling Markus, Wölfer Johannes, Fischer Bernhard, Stummer Walter, Ewelt Christian

机构信息

Department of Neurosurgery, University Hospital of Münster, Münster, Germany.

出版信息

Clin Neurol Neurosurg. 2013 Oct;115(10):2075-81. doi: 10.1016/j.clineuro.2013.07.016. Epub 2013 Jul 31.

Abstract

INTRODUCTION

Aquaporin channels (AQPs) are a group of integral membrane proteins that regulate the transport of water through cell membranes. Previous studies have shown that up-regulation of AQP1 and AQP4, two of the predominant AQPs in the human brain, in high grade glial tumors contribute to cerebral edema. Others link AQPs to the regulation of human glioma cell migration and invasion. The aim of this study was to determine AQPs expression in tumor tissue harboring 5-aminolevulinic acid (ALA)-induced porphyrin fluorescence with flow cytometry and compare it to the expression in normal brain tissue.

METHODS

Tissue samples were obtained from fluorescing brain tumors of 26 patients treated with ALA prior to surgery (20 mg/kg b.w.). Expression levels of aquaporin channels were measured in primary tissue cultures using a FACS CANTO I flow cytometer. A control group consisted of four non-fluorescing tissue samples, the C6 and the U87 cell line.

RESULTS

Nineteen gliomas (14 high grade, 5 low grade) and 7 metastases were analyzed. On the 4th post-operative day, expression levels of AQP4 channels, but not of AQP1 channels, were significantly increased in samples from fluorescing tissue compared to non-fluorescing tissue. In addition we could see how ALA induces fluorescence in metastases.

CONCLUSION

Flow cytometry appears to be an auspicious method for the analysis of porphyrins and AQPs in primary brain cell tumor cultures. ALA fluorescing tissue showed higher AQP4 expression compared to normal brain tissue. The demonstrated expression in a context with ALA could open a targeted therapeutic spectrum, for example to selectively target AQP4.

摘要

引言

水通道蛋白通道(AQPs)是一组整合膜蛋白,可调节水通过细胞膜的运输。先前的研究表明,人类大脑中两种主要的水通道蛋白AQP1和AQP4在高级别胶质瘤中上调会导致脑水肿。其他研究将水通道蛋白与人类胶质瘤细胞的迁移和侵袭调节联系起来。本研究的目的是通过流式细胞术确定携带5-氨基乙酰丙酸(ALA)诱导的卟啉荧光的肿瘤组织中水通道蛋白的表达,并将其与正常脑组织中的表达进行比较。

方法

组织样本取自26例术前接受ALA治疗(20mg/kg体重)的荧光脑肿瘤患者。使用FACS CANTO I流式细胞仪在原代组织培养物中测量水通道蛋白通道的表达水平。对照组由四个非荧光组织样本、C6和U87细胞系组成。

结果

分析了19例胶质瘤(14例高级别,5例低级别)和7例转移瘤。术后第4天,与非荧光组织相比,荧光组织样本中AQP4通道的表达水平显著增加,而AQP1通道的表达水平未显著增加。此外,我们可以看到ALA如何在转移瘤中诱导荧光。

结论

流式细胞术似乎是分析原发性脑细胞肿瘤培养物中卟啉和水通道蛋白的一种有前景的方法。与正常脑组织相比,ALA荧光组织显示出更高的AQP4表达。在ALA背景下证实的表达可能会开启一个靶向治疗谱,例如选择性靶向AQP4。

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