Gene knockdown of CENPA reduces sphere forming ability and stemness of glioblastoma initiating cells

Neuroepigenetics Pub Date : 2016-09-01 DOI:10.1016/j.nepig.2016.08.002

Jinan Behnan , Zanina Grieg , Mrinal Joel , Ingunn Ramsness , Biljana Stangeland

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引用次数: 15

Abstract

CENPA is a centromere-associated variant of histone H3 implicated in numerous malignancies. However, the role of this protein in glioblastoma (GBM) has not been demonstrated. GBM is one of the most aggressive human cancers. GBM initiating cells (GICs), contained within these tumors are deemed to convey characteristics such as invasiveness and resistance to therapy. Therefore, there is a strong rationale for targeting these cells. We investigated the expression of CENPA and other centromeric proteins (CENPs) in GICs, GBM and variety of other cell types and tissues. Bioinformatics analysis identified the gene signature: high_CENP(AEFNM)/low_CENP(BCTQ) whose expression correlated with significantly worse GBM patient survival.

Knockdown of CENPA reduced sphere forming ability, proliferation and cell viability of GICs. We also detected significant reduction in the expression of stemness marker SOX2 and the proliferation marker Ki67. These results indicate that CENPA might represent a promising therapeutic target for GBM treatment.

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基因敲低CENPA可降低胶质母细胞瘤起始细胞的成球能力和干性

CENPA是组蛋白H3的着丝粒相关变体，与许多恶性肿瘤有关。然而，该蛋白在胶质母细胞瘤(GBM)中的作用尚未得到证实。GBM是最具侵袭性的人类癌症之一。这些肿瘤中包含的GBM起始细胞(gic)被认为具有侵袭性和抗治疗性等特征。因此，靶向这些细胞是有充分理由的。我们研究了CENPA和其他着丝粒蛋白(CENPs)在GICs、GBM和其他多种细胞类型和组织中的表达。生物信息学分析确定了基因特征:high_CENP(AEFNM)/low_CENP(BCTQ)，其表达与GBM患者生存率显著降低相关。敲低CENPA可降低GICs的成球能力、增殖能力和细胞活力。我们还检测到干性标记SOX2和增殖标记Ki67的表达显著降低。这些结果表明，CENPA可能是治疗GBM的一个有希望的治疗靶点。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Neuroepigenetics

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