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LRRC3B 基因在几种上皮性恶性肿瘤中经常被表观遗传失活,抑制细胞生长和复制。

LRRC3B gene is frequently epigenetically inactivated in several epithelial malignancies and inhibits cell growth and replication.

机构信息

Department of Microbiology, Tumor and Cell Biology, Karolinska Institute, Stockholm, Sweden.

出版信息

Biochimie. 2012 May;94(5):1151-7. doi: 10.1016/j.biochi.2012.01.019. Epub 2012 Feb 2.

Abstract

Chromosome 3 specific NotI microarrays containing 180 NotI linking clones associated with 188 genes were hybridized to NotI representation probes prepared using matched tumor/normal samples from major epithelial cancers: breast (47 pairs), lung (40 pairs) cervical (43 pairs), kidney (34 pairs of clear cell renal cell carcinoma), colon (24 pairs), ovarian (25 pairs) and prostate (18 pairs). In all tested primary tumors (compared to normal controls) methylation and/or deletions was found. For the first time we showed that the gene LRRC3B was frequently methylated and/or deleted in breast carcinoma - 32% of samples, cervical - 35%, lung - 40%, renal - 35%, ovarian - 28%, colon - 33% and prostate cancer - 44%. To check these results bisulfite sequencing using cloned PCR products with representative two breast, one cervical, two renal, two ovarian and two colon cancer samples was performed. In all cases methylation was confirmed. Expression analysis using RT-qPCR showed that LRRC3B is strongly down-regulated at the latest stages of RCC and ovarian cancers. In addition we showed that LRRC3B exhibit strong cell growth inhibiting activity (more than 95%) in colony formation experiments in vitro in KRC/Y renal cell carcinoma line. All these data suggest that LRRC3B gene could be involved in the process of carcinogenesis as a tumor suppressor gene.

摘要

使用来自主要上皮癌的匹配肿瘤/正常样本(乳腺[47 对]、肺[40 对]、宫颈[43 对]、肾[34 对透明细胞肾细胞癌]、结肠[24 对]、卵巢[25 对]和前列腺[18 对])制备的 NotI 代表性探针与包含与 188 个基因相关的 180 个 NotI 连接克隆的 3 号染色体特异性 NotI 微阵列杂交。在所有测试的原发性肿瘤(与正常对照相比)中发现了甲基化和/或缺失。我们首次表明,LRRC3B 基因在乳腺癌中频繁发生甲基化和/或缺失 - 32%的样本,宫颈癌 - 35%,肺癌 - 40%,肾癌 - 35%,卵巢癌 - 28%,结肠癌 - 33%和前列腺癌 - 44%。为了检查这些结果,使用来自代表性的两个乳腺癌、一个宫颈癌、两个肾癌、两个卵巢癌和两个结肠癌样本的克隆 PCR 产物进行了亚硫酸氢盐测序。在所有情况下均确认了甲基化。使用 RT-qPCR 进行的表达分析显示,LRRC3B 在 RCC 和卵巢癌的晚期表达强烈下调。此外,我们还表明,LRRC3B 在 KRC/Y 肾细胞癌细胞系的体外集落形成实验中表现出强烈的细胞生长抑制活性(超过 95%)。所有这些数据表明,LRRC3B 基因可能作为肿瘤抑制基因参与致癌过程。

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