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KISS1 甲基化和表达作为膀胱癌患者肿瘤分层生物标志物和临床预后预测因子。

KISS1 methylation and expression as tumor stratification biomarkers and clinical outcome prognosticators for bladder cancer patients.

机构信息

Tumor Markers Group, Molecular Pathology Program, Spanish National Cancer Center, Madrid, Spain.

出版信息

Am J Pathol. 2011 Aug;179(2):540-6. doi: 10.1016/j.ajpath.2011.05.009. Epub 2011 Jun 17.

DOI:10.1016/j.ajpath.2011.05.009
PMID:21683672
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3157173/
Abstract

KISS1 is a metastasis suppressor gene that is lost in several malignancies, including bladder cancer. We tested the epigenetic silencing hypothesis and evaluated the biological influence of KISS1 methylation on its expression and clinical relevance in bladder cancer. KISS1 hypermethylation was frequent in bladder cancer cells analyzed by methylation-specific PCR and bisulfite sequencing and was associated with low gene expression, being restored in vitro by demethylating azacytidine. Hypermethylation was also frequently observed in a large series of bladder tumors (83.1%, n = 804). KISS1 methylation was associated with increasing stage (P = 0.001) and tumor grade (P = 0.010). KISS1 methylation was associated with low KISS1 transcript expression by quantitative RT-PCR (P = 0.037). KISS1 transcript expression was also associated with histopathological tumor stage (P < 0.0005). Low transcript expression alone (P = 0.003) or combined with methylation (P = 0.019) was associated with poor disease-specific survival (n = 205). KISS1 transcript expression remained an independent prognosticator in multivariate analyses (P = 0.017). KISS1 hypermethylation was identified in bladder cancer, providing a potential mechanistic explanation (epigenetic silencing) for the observed loss of KISS1 in uroepithelial malignancies. Associations of KISS1 methylation and its expression with histopathological variables and poor survival suggest the utility of incorporating KISS1 measurement using paraffin-embedded material for tumor stratification and clinical outcome prognosis of patients with uroepithelial neoplasias.

摘要

KISS1 是一种转移抑制基因,在包括膀胱癌在内的几种恶性肿瘤中丢失。我们测试了表观遗传沉默假说,并评估了 KISS1 甲基化对其表达的生物学影响及其在膀胱癌中的临床相关性。通过甲基化特异性 PCR 和亚硫酸氢盐测序分析,发现膀胱癌细胞中存在 KISS1 高甲基化,且与低基因表达相关,阿扎胞苷去甲基化可在体外恢复其表达。在一系列大型膀胱癌肿瘤中也频繁观察到高甲基化(83.1%,n=804)。KISS1 甲基化与肿瘤分期(P=0.001)和肿瘤分级(P=0.010)增加相关。通过定量 RT-PCR 发现 KISS1 甲基化与 KISS1 转录物表达降低相关(P=0.037)。KISS1 转录物表达也与组织病理学肿瘤分期相关(P<0.0005)。单独低转录物表达(P=0.003)或与甲基化相结合(P=0.019)与不良疾病特异性生存相关(n=205)。KISS1 转录物表达在多变量分析中仍然是独立的预后指标(P=0.017)。在膀胱癌中鉴定出 KISS1 高甲基化,为观察到的尿路上皮恶性肿瘤中 KISS1 的缺失提供了潜在的机制解释(表观遗传沉默)。KISS1 甲基化及其表达与组织病理学变量和不良生存相关,表明使用石蜡包埋材料进行 KISS1 测量可用于肿瘤分层和预测尿路上皮肿瘤患者的临床预后。

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