Overexpression of Colligin 2 in Glioma Vasculature is Associated with Overexpression of Heat Shock Factor 2.

Dana A M Mustafa, Anieta M Sieuwerts, Ping Pin Zheng, Johan M Kros
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引用次数: 14

Abstract

In previous studies we found expression of the protein colligin 2 (heat shock protein 47 (HSP47), SERPINH1) in glioma neovasculature while not in normal brain tissue. Generally, the regulation of heat shock gene expression in eukaryotes is mediated by heat shock factors (HSF). In mammals, three heat shock transcription factors, HSF-1, -2, and -4, have been isolated. Here we investigated the relation between the expression of colligin 2 and these heat shock factors at the mRNA level using real-time reverse transcriptase PCR (qRT-PCR) in different grades of astrocytic tumorigenesis, viz., low-grade glioma and glioblastoma. Endometrium samples, representing physiological angiogenesis, were included as controls. Since colligin 2 is a chaperon for collagens, the gene expression of collagen I (COL1A1) was also investigated. The blood vessel density of the samples was monitored by expression of the endothelial marker CD31 (PECAM1). Because NG2-immunopositive pericytic cells are involved in glioma neovascularization, the expression of NG2 (CSPG4) was also measured.We demonstrate overexpression of HSF2 in both stages of glial tumorigenesis (reaching significance only in low-grade glioma) and also minor elevated levels of HSF1 as compared to normal brain. There were no differences in expression of HSF4 between low-grade glioma and normal brain while HSF4 was downregulated in glioblastoma. In the endometrium samples, none of the HSFs were upregulated. In the low-grade gliomas SERPINH appeared to be slightly overexpressed with a parallel 4-fold upregulation of COL1A1, while in glioblastoma there was over 5-fold overexpression of SERPINH1 and more than 150-fold overexpression of COL1A1. In both the lowgrade gliomas and the glioblastomas overexpression of CSPG4 was found and overexpression of PECAM1 was only found in the latter. Our data suggest that the upregulated expression of colligin 2 in glioma is accompanied by upregulation of COL1A1, CSPG4, HSF2 and to a lesser extent, HSF1. Further studies will unravel the association of these factors with colligin 2 expression, possibly leading to keys for therapeutic intervention.

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胶质瘤血管中胶原蛋白2的过度表达与热休克因子2的过度表达有关。
在之前的研究中,我们发现胶原蛋白2(热休克蛋白47 (HSP47), SERPINH1)在胶质瘤新生血管中表达,而在正常脑组织中不表达。一般来说,真核生物热休克基因表达的调控是由热休克因子(heat shock factors, HSF)介导的。在哺乳动物中,已经分离出三种热休克转录因子HSF-1、-2和-4。本研究采用实时逆转录酶PCR (real-time reverse transcriptase PCR, qRT-PCR)技术,在不同级别的星形细胞瘤,即低级别胶质瘤和胶质母细胞瘤中,研究了胶原蛋白2的表达与这些热休克因子在mRNA水平上的关系。代表生理性血管生成的子宫内膜样本作为对照。由于胶原蛋白2是胶原蛋白的伴侣蛋白,我们也研究了胶原蛋白I (COL1A1)的基因表达。通过内皮标志物CD31 (PECAM1)的表达监测样本的血管密度。由于NG2免疫阳性的周细胞参与了胶质瘤新生血管的形成,我们也测量了NG2 (CSPG4)的表达。我们发现HSF2在胶质瘤发生的两个阶段都过表达(仅在低级别胶质瘤中达到显著性),并且与正常大脑相比,HSF2水平也有轻微升高。HSF4在低级别脑胶质瘤和正常脑中表达无差异,而在胶质母细胞瘤中表达下调。在子宫内膜样本中,hsf均未上调。在低级别胶质瘤中,SERPINH出现轻微过表达,COL1A1平行上调4倍,而在胶质母细胞瘤中,SERPINH1过表达超过5倍,COL1A1过表达超过150倍。在低级别胶质瘤和胶质母细胞瘤中均发现CSPG4过表达,而PECAM1仅在后者中过表达。我们的数据表明,胶质瘤中胶原蛋白2的表达上调伴随着COL1A1、CSPG4、HSF2以及HSF1的表达上调。进一步的研究将揭示这些因子与胶原蛋白2表达的关系,可能为治疗干预提供关键。
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