宫颈癌发病过程中分泌型 Frizzled-Related 蛋白 2 的频繁失活:易感等位基因的鉴定及其临床意义

Sudip Samadder, Debolina Pal, A. Roychowdhury, Arindam Dutta, Mukta Basu, Sankhadeep Dutta, A. Roy, R. Mandal, S. Roychoudhury, C. Panda
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引用次数: 0

摘要

摘要 本研究评估了 wnt 干细胞更新通路拮抗剂 SFRP2 在宫颈癌(CACX)发病中的重要性,分析了 SFRP2 在不同临床阶段的原发性宫颈病变中的变化(表达/甲基化/缺失),以及它们与不同临床病理参数的相关性。然后,通过病例对照研究和体外验证确定了 SFRP2 的易感等位基因。 SFRP2 的 mRNA 表达随着 CACX 的进展而逐渐减少。在免疫组化中,SFRP2膜表达主要存在于正常宫颈上皮的棘层,其蛋白表达在CACX样本中的减少与mRNA表达一致。SFRP2的频繁缺失/甲基化与宫颈癌的发生有关。SFRP2 的甲基化主要与早期浸润性病变(I/II 期)有关,而缺失则与晚期浸润性病变(III/IV 期)有关。从恶性前CIN到I/II期样本,SFRP2的总体改变(缺失/甲基化)明显增加,随后与下一阶段(III/IV期)样本的变化相当。此外,SFRP2 的缺失和/或甲基化与患者的不良预后有关。在一项病例对照研究中,发现在七个微卫星等位基因中,不常见的 SFRP_CA15/16 等位基因和常见的 SFRP_CA17 等位基因与 CACX 的发生有关。在肿瘤邻近的正常宫颈上皮细胞中,SFRP2 的表达(mRNA/蛋白质)相对于其他等位基因有所降低。这一点在体外荧光素酶启动子活性测定中得到了进一步验证,SFRP_CA16 重复序列比其他重复序列显示出较高的活性降低,其次是 SFRP_CA15 重复序列。 因此,我们的数据表明,不常见的易感等位基因的存在以及缺失/甲基化可能会在 CACX 的发展过程中对 SFRP2 的频繁失活产生协同效应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Frequent Inactivation of Secreted Frizzled-Related Protein 2 during the Development of Cervical Carcinoma: Identification of Susceptible Alleles and Clinical Implications
ABSTRACT In this study, importance of SFRP2, wnt stem cell renewal pathway antagonist, in the development of cervical cancer (CACX) was evaluated Alterations (expression/ methylation/ deletion) of SFRP2 were analysed in primary cervical lesions of different clinical stages followed by their correlation with different clinicopathological parameters. Then, susceptible allele(s) of SFRP2 was identified through case control study followed by and in vitro validation. The mRNA expression of SFRP2 was gradually reduced with progression of CACX. In immunohistochemistry, SFRP2 membrane expression was mainly present in the spinous layers of normal cervical epithelium and its reduced protein expression in CACX samples showed concordance with mRNA expression. Frequent deletion/ methylation of SFRP2 were seen to be associated with development of cervical cancer. Methylation of SFRP2 was prevalently associated with early invasive lesions (stage I/II) while, deletion with late invasive lesions (stage III/IV). Overall alterations (deletion/ methylation) of SFRP2 were significantly increased from premalignant CIN to stage-I/II samples followed by comparable change to the next stage (stage III/IV) samples. Moreover, deletion and/or methylation of SFRP2 were associated with poor prognosis of the patients. In a case control study, out of its seven microsatellite alleles infrequent SFRP_CA15/16 alleles along with frequent SFRP_CA17 allelewere found to be associated with CACX development. Comparatively reduced expression (mRNA/ protein) of SFRP2 was seen in the tumor adjacent normal cervical epithelium having SFRP_CA15/16 alleles than the other alleles. This has been further validated in in vitro luciferase promoter activity assay where SFRP_CA16 repeat showed high reduced activity followed by SFRP_CA15 repeat than the other repeats. Thus, our data showed that presence of the infrequent susceptible alleles along with deletion/methylation might have synergistic effect on frequent inactivation of SFRP2 during development of CACX.
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