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端粒酶逆转录酶是否诱导人内皮细胞功能去分化?

Does telomerase reverse transcriptase induce functional de-differentiation of human endothelial cells?

机构信息

NMI, Natural and Medical Sciences Institute at the University of Tübingen, Reutlingen, Germany.

出版信息

Cell Mol Life Sci. 2010 Jul;67(14):2451-65. doi: 10.1007/s00018-010-0349-z. Epub 2010 Mar 30.

Abstract

By counteracting the shortening of chromosome telomeres, telomerase reverse transcriptase (hTERT) prevents senescence and age-related cell death. Embryonic cells display a high telomerase activity that declines rapidly with cell differentiation. Conversely, de-differentiated tumor cells tend to re-express telomerase. In view of the controversial data on the reciprocal correlation between cell proliferation and differentiation, we questioned whether telomerase overexpression and the resulting immortalization would affect the functional phenotype of human endothelial cells. Our comparative analysis addressed (1) distinct cell adhesion to different ECM-proteins analyzed on miniaturized multisubstrate arrays (MSA), (2) protein expression of diverse markers, (3) the uptake of DiI-Ac-LDL, (4) the inflammatory response based on upregulation of ICAM-1, (5) tube formation, and (6) the barrier properties of cell monolayers in transfilter cultures. Our results, based on some 40 data sets, demonstrate that immortalization of primary endothelial cells by hTERT maintains the typical endothelial characteristics without any sign of functional de-differentiation.

摘要

通过抵消染色体端粒的缩短,端粒酶逆转录酶(hTERT)可以防止衰老和与年龄相关的细胞死亡。胚胎细胞显示出高的端粒酶活性,随着细胞分化迅速下降。相反,去分化的肿瘤细胞往往重新表达端粒酶。鉴于细胞增殖和分化之间相互关联的争议数据,我们质疑端粒酶的过表达和由此导致的永生化是否会影响人内皮细胞的功能表型。我们的比较分析解决了以下问题:(1)在微型多底物阵列(MSA)上分析的不同细胞对不同 ECM-蛋白的黏附;(2)不同标记物的蛋白表达;(3)DiI-Ac-LDL 的摄取;(4)基于 ICAM-1 上调的炎症反应;(5)管状形成;以及(6)细胞单层在跨膜培养中的屏障特性。我们的结果基于大约 40 个数据集,表明通过 hTERT 永生化原代内皮细胞可以维持典型的内皮特征,而没有任何功能去分化的迹象。

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