Overexpression of Hypermethylated Homeobox A11 (HOXA11) Inhibits Tumor Cell Growth and Induces Apoptosis in Cervical Cancer.

Development & reproduction Pub Date : 2024-06-01 Epub Date: 2024-06-30 DOI:10.12717/DR.2024.28.2.37
Seung-Yul Lee, Tae Jeong Oh, Sungwhan An, Seung-Hoon Lee
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Abstract

This study aimed to elucidate the potential of Homeobox A11 (HOXA11) as a therapeutic target and a diagnostic methylation marker for cervical cancer. Gene expression analysis using cDNA microarray in cervical cancer cell lines revealed significantly reduced expression of the HOXA11 gene. Subsequent investigation of HOXA11 promoter methylation in samples from normal individuals and invasive cervical cancer patients showed over 53.2% higher methylation in cancer scrapes compared to normal scrapes. Furthermore, overexpression of HOXA11, which is downregulated in cervical cancer, strongly suppressed cell growth in cervical cancer cell lines, HeLa and HT3. Additionally, we performed transferase dUTP nick end labeling assay and confirmed that the inhibition of cervical cancer cell proliferation occurred via apoptosis. Mechanistically, overexpression of HOXA11 led to mitochondrial apoptosis characterized by PARP cleavage due to increased c-Myc and enhanced cytochrome C secretion into the cytoplasm. These findings suggest that HOXA11 could potentially serve as a methylation marker for diagnosing cervical cancer and as a novel therapeutic target for its treatment.

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宫颈癌中过表达的高甲基化Homeobox A11(HOXA11)可抑制肿瘤细胞生长并诱导其凋亡
本研究旨在阐明Homeobox A11(HOXA11)作为宫颈癌治疗靶点和诊断甲基化标记物的潜力。利用 cDNA 微阵列对宫颈癌细胞系进行基因表达分析,发现 HOXA11 基因的表达明显降低。随后对正常人和浸润性宫颈癌患者样本中的 HOXA11 启动子甲基化进行了调查,结果显示,与正常人的刮痕相比,癌症刮痕的甲基化程度要高出 53.2%。此外,在宫颈癌中下调的 HOXA11 的过表达能强烈抑制宫颈癌细胞株 HeLa 和 HT3 的细胞生长。此外,我们还进行了转移酶 dUTP 缺口标记实验,证实了宫颈癌细胞增殖抑制是通过细胞凋亡实现的。从机理上讲,HOXA11的过表达会导致线粒体凋亡,其特点是c-Myc增加导致PARP裂解,细胞色素C分泌到细胞质中的能力增强。这些研究结果表明,HOXA11 有可能成为诊断宫颈癌的甲基化标记物和治疗宫颈癌的新靶点。
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