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Identification of common polymorphisms in the coding sequence of the human MSH receptor (MCIR) with possible biological effects.鉴定人类促黑素细胞激素受体(MC1R)编码序列中可能具有生物学效应的常见多态性。
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The Asp84Glu variant of the melanocortin 1 receptor (MC1R) is associated with melanoma.黑皮质素1受体(MC1R)的Asp84Glu变体与黑色素瘤相关。
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人类先天性黑素细胞痣中N-ras、p53、p16INK4a、CDK4和MC1R基因的突变分析

Mutational analysis of the N-ras, p53, p16INK4a, CDK4, and MC1R genes in human congenital melanocytic naevi.

作者信息

Papp T, Pemsel H, Zimmermann R, Bastrop R, Weiss D G, Schiffmann D

机构信息

University of Rostock, Department of Biology, Germany.

出版信息

J Med Genet. 1999 Aug;36(8):610-4.

PMID:10465111
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1762982/
Abstract

Eighteen human congenital melanocytic naevi (CMN) from 17 patients were screened for activating point mutations in the oncogenes N-ras and CDK4 and for sequence variants in the MC1R gene by combined RFLP-PCR/SSCP analysis. In addition, all lesions were screened for deletions and point mutations in the tumour suppressor genes p53 and p16INK4a (CDKN2A) by combined multiplex PCR/SSCP analysis. Positive screening data were specified by sequencing of the corresponding PCR product. Activating point mutations in the N-ras gene (nine CAA (Gln) to AAA (Lys) transversions and one CAA (Gln) to CGA (Arg) transition at codon 61) were detected at high frequency (56%). Furthermore, three missense mutations (V92M) and two silent mutations (CGA (Arg) to CGG (Arg), codon 213, exon 6) were found in the MC1R and p53 genes, respectively. No mutations were found in p16 or CDK4. The activated N-ras oncogene, which is also found in human cutaneous melanomas, may constitute a potential risk factor for melanoma formation within CMN.

摘要

通过联合RFLP-PCR/SSCP分析,对来自17例患者的18个人类先天性黑素细胞痣(CMN)进行筛查,以检测癌基因N-ras和CDK4中的激活点突变以及MC1R基因中的序列变异。此外,通过联合多重PCR/SSCP分析,对所有病变进行肿瘤抑制基因p53和p16INK4a(CDKN2A)中的缺失和点突变筛查。通过对相应PCR产物进行测序来确定阳性筛查数据。在N-ras基因中检测到高频(56%)的激活点突变(9个密码子61处的CAA(Gln)到AAA(Lys)的颠换和1个CAA(Gln)到CGA(Arg)的转换)。此外,在MC1R和p53基因中分别发现了3个错义突变(V92M)和2个沉默突变(密码子213、外显子6处的CGA(Arg)到CGG(Arg))。在p16或CDK4中未发现突变。在人类皮肤黑色素瘤中也发现的激活的N-ras癌基因可能构成CMN内黑色素瘤形成的潜在危险因素。