Rutter Joni L, Goldstein Alisa M, Dávila Michael R, Tucker Margaret A, Struewing Jeffery P
Laboratory of Population Genetics, Center for Cancer Research, National Cancer Institute, National Institutes of Health, DHHS, Bethesda, MD, USA.
Oncogene. 2003 Jul 10;22(28):4444-8. doi: 10.1038/sj.onc.1206564.
The CDKN2A gene, which encodes the proteins p16(INK4a) and p14(ARF), is located on chromosome 9p21. Germline mutations at this locus increase susceptibility to cutaneous malignant melanoma (CMM). In general, missense and nonsense mutations are primarily responsible for defective p16(INK4a) and possibly p14(ARF) protein function and account for approximately 20% of inherited CMM cases. We report a G>T transversion mutation in the last nucleotide of exon 2, affecting the aspartic acid residue at position 153 of CDKN2A-p16(INK4a) in a proband with melanoma. If splicing were unaffected, this mutation would change Asp to Tyr. RT-PCR analysis, however, revealed that this mutation, which we have termed D153spl(c.457G>T), and a previously described mutation at the next nucleotide, IVS2+1G>T, result in identical aberrant splicing affecting both p16(INK4a) and p14(ARF). The two main alternate splice products for each of the two normal transcripts includes a 74 bp deletion in exon 2, revealing a cryptic splice site, and the complete skipping of exon 2. The dual inactivation of p16(INK4a) and p14(ARF) may contribute to the CMM in these families.
编码蛋白质p16(INK4a)和p14(ARF)的CDKN2A基因位于9号染色体的p21区域。该位点的种系突变会增加患皮肤恶性黑色素瘤(CMM)的易感性。一般来说,错义突变和无义突变主要导致p16(INK4a)功能缺陷,可能还有p14(ARF)蛋白功能缺陷,约占遗传性CMM病例的20%。我们报告了一名黑色素瘤先证者中,外显子2最后一个核苷酸发生G>T颠换突变,影响CDKN2A-p16(INK4a)第153位的天冬氨酸残基。如果剪接不受影响,该突变会将天冬氨酸变为酪氨酸。然而,逆转录聚合酶链反应(RT-PCR)分析显示,我们称之为D153spl(c.457G>T)的这一突变,以及下一个核苷酸处先前描述的IVS2+1G>T突变,导致相同的异常剪接,影响p16(INK4a)和p14(ARF)。两种正常转录本各自的两种主要可变剪接产物包括外显子2中74 bp的缺失,揭示了一个隐蔽剪接位点,以及外显子2的完全跳跃。p16(INK4a)和p14(ARF)的双重失活可能导致这些家族发生CMM。
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