中国人群尖锐湿疣黑色素瘤中 CDK4 基因拷贝数的增加和同时发生的基因变化。

IF 3.6 3区 医学 Q1 PATHOLOGY
Leyuan Yang, Yan Liu, Ruiping Guo, Juan Du, Lingchao Liu, Xiaolong Liu, Jianfang Zhao, Fang Shi, Xin Zhang, Jing Su
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引用次数: 0

摘要

口腔黑色素瘤(AM)是亚洲人群中最常见的黑色素瘤亚型。p16-细胞周期蛋白D1-CDK4信号通路的异常在AM的发生和发展中起着至关重要的作用。然而,关于AM中CDK4拷贝数变异(CNVs)的报道却很少。在本研究中,我们调查了中国AM患者队列中CDK4基因拷贝数和同时发生的分子变化,以探讨CDK4 CNVs及其在AM中的意义。我们用荧光原位杂交(FISH)技术检测了31例AM患者的CDK4 CNV。我们还通过新一代测序技术检测了6例CDK4高水平拷贝数增加的患者,以发现并发的分子变化。通过FISH,12例(12/31,38.7%)患者出现CDK4拷贝数增加,其中6例(6/31,19.4%)为低水平拷贝数增加,6例(6/31,19.4%)为高水平拷贝数增加。六例 CDK4 低水平拷贝数增加病例中有五例伴有 12 号染色体多体,一例没有。六例 CDK4 高拷贝数增加病例中有两例伴有 12 号染色体多体,四例没有。CDK4 拷贝数的增加与患者的年龄明显相关。在6例CDK4高拷贝数增加病例中,1例伴有NRAS突变,1例伴有HER2突变,1例伴有BCL2L11突变,1例伴有BRAF、HER2和BCL2L11突变。我们的研究证实,AM病例中存在CDK4拷贝数增加。通过FISH检测CDK4拷贝数增加对AM的诊断是可靠的。有些CDK4拷贝数增加是12号染色体多倍体的结果。CDK4高拷贝数增加与AM的其他致病突变共存。CDK4似乎是治疗AM的一个有希望的靶点,有望与其他靶向疗法相结合。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
CDK4 gene copy number increase and concurrent genetic changes in acral melanoma of a Chinese cohort.

Acral melanoma (AM) is the most common subtype of melanoma in the Asian population. Abnormalities in the p16-cyclin D1-CDK4 signalling pathway play a crucial role in the development and progression of AM. However, the CDK4 copy number variations (CNVs) in AM are under-reported. In this study, we investigated CDK4 gene copy number and concurrent molecular changes in a Chinese cohort with AM, to explore CDK4 CNVs and their significance in AM. We examined CDK4 CNVs with fluorescence in situ hybridisation (FISH) in 31 patients with AM. Six patients with CDK4 high-level copy number increase were examined by next-generation sequencing to detect concurrent molecular changes. Using FISH, 12 (12/31, 38.7%) cases showed CDK4 copy number increase, with six (6/31, 19.4%) low-level copy number increase and six (6/31, 19.4%) high-level copy number increase. Five of six CDK4 low-level copy number increase cases were accompanied by polysomy of chromosome 12, while one case was not. Two of six CDK4 high-level copy number increase cases were accompanied by polysomy of chromosome 12, while four cases were not. CDK4 copy number increase was significantly correlated with younger patient age. In six CDK4 high-level copy number increase cases, one case was found to be accompanied by NRAS mutation, one case was accompanied by HER2 mutation, one case was accompanied by BCL2L11 mutation ​and one case was accompanied by BRAF, HER2 and BCL2L11 mutations. Our study confirmed the presence of CDK4 copy number increase in AM cases. Detecting CDK4 copy number increase by FISH can be reliable in the diagnosis of AM. Some CDK4 copy number increases are the results of polysomy of chromosome 12. CDK4 high-level copy number increase coexists with other pathogenic mutations in AM. CDK4 appears to be a promising target for AM treatment and is expected to be combined with other targeted therapies.

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来源期刊
Pathology
Pathology 医学-病理学
CiteScore
6.50
自引率
2.20%
发文量
459
审稿时长
54 days
期刊介绍: Published by Elsevier from 2016 Pathology is the official journal of the Royal College of Pathologists of Australasia (RCPA). It is committed to publishing peer-reviewed, original articles related to the science of pathology in its broadest sense, including anatomical pathology, chemical pathology and biochemistry, cytopathology, experimental pathology, forensic pathology and morbid anatomy, genetics, haematology, immunology and immunopathology, microbiology and molecular pathology.
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