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Mutational analysis of the human cyclin-dependent kinase inhibitor p27kip1in primary breast carcinomas

机译:原发性乳腺癌中人细胞周期蛋白依赖性激酶抑制剂p27kip1的突变分析

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The human p27kip1gene encodes a cyclin-dependent kinase inhibitor implicated in the negative regulation of the cell cycle. In order to elucidate the possible role of p27 mutations in the development or progression of human breast cancer, we have studied the occurrence of genetic abnormalities in this gene in a series of 30 primary breast carcinomas. Direct sequence analysis of the polymerase chain reaction amplified human p27 gene revealed the occurrence of two sequence variations with respect to the reported sequence; both variants were also present in the lymphocyte DNA from the same patients. First, a silent G to A change at codon 142 (Thr) was detected in a single case. Second, a T to G transversion at codon 109, resulting in a Val to Gly change, was observed in eight tumour DNA samples (26) and in 31 out of 80 unrelated normal individuals (39). This latter change creates aBglI restriction site that might be useful for genetic analysis of human tumours. Despite the occurrence of these polymorphisms, we did not however find any evidence of somatic mutations in the coding region of the p27 gene. On the basis of these results, we suggest that alterations in the integrity of the human p27 gene are not common events in human breast carcinomas.
机译:人 p27kip1 基因编码一种细胞周期蛋白依赖性激酶抑制剂,与细胞周期的负调控有关。为了阐明p27突变在人类乳腺癌发展或进展中的可能作用,我们研究了该基因在30例原发性乳腺癌中遗传异常的发生。对聚合酶链反应扩增的人 p27 基因进行直接序列分析,发现与报告的序列相比,存在两个序列变异;这两种变体也存在于同一患者的淋巴细胞DNA中。首先,在单个病例中检测到密码子 142 (Thr) 处的无声 G 到 A 变化。其次,在 8 个肿瘤 DNA 样本 (26%) 和 80 个无关正常个体中的 31 个 (39%) 中观察到密码子 109 位点 T 到 G 的位移,导致 Val 到 Gly 的变化。后一种变化产生了aBglI限制位点,该位点可能有助于人类肿瘤的遗传分析。尽管发生了这些多态性,但我们没有发现p27基因编码区存在体细胞突变的任何证据。基于这些结果,我们认为人类p27基因完整性的改变在人类乳腺癌中并不常见。

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