MUTATION PROFILE OF BREAST CANCER IN MALAYSIAN PATIENTS

F. Amini, Wong Fu Hou, Edmond Ng Siah Chye, R. Omar, S. Rejab, Izyan Wajiha Mohd Noor, B. M. Hussain
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引用次数: 1

Abstract

Background: Breast cancer (BC) is the most common cancer in women globally. In low- and middle-income countries, the use of appropriate breast cancer genetics services for screening and personalized treatments is severely lacking. This review is aimed to assess and summarize the reported mutation profiles of Malaysian BC patients. Methods: A literature search was performed in PubMed and Google Scholar from 2002 to 2019 using a set of keywords and MESH terms. Results: Data from 14 eligible studies are presented here. A total of 28 genes were studied in Malaysian BC patients in which 445 genetic alterations (229 deleterious, 209 variants with unknown clinical significance (VUC), and seven protective variants) have been reported, with 73 being novel (16% novel). The frequency ranged from 0.2% to 76% for VUC and 2.1 to 15% for deleterious variations. Only BRCA1, BRCA2, PALB2, APOBEC3B, and P53 have been associated with BC risk in Malaysian patients. Nine of these studies were conducted using the overlapped source of patients, which may limit the generalizability of the findings to the whole population of Malaysia. Conclusion: Information on the genetic basis of BC in the Malaysian population is scant. Multidisciplinary efforts with appropriate sample selection techniques and study design with multicenter collaboration are needed to address this issue. Out of thirteen high- and moderated-penetrance pathogenic mutations for BC, only five have been linked to Malaysians’ BC susceptibility. The findings from this review is valuable for decision-makers, researchers, and physicians, to enhance the research plans and utility of genetic services for screening and prevention.
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马来西亚乳腺癌患者的突变谱
背景:癌症是全球女性最常见的癌症。在中低收入国家,严重缺乏使用适当的癌症基因服务进行筛查和个性化治疗。这篇综述旨在评估和总结马来西亚BC患者的突变谱。方法:2002年至2019年,在PubMed和Google Scholar上使用一组关键词和MESH术语进行文献检索。结果:本文提供了14项合格研究的数据。在马来西亚BC患者中共研究了28个基因,其中445个基因改变(229个有害变异,209个临床意义未知的变异(VUC)和7个保护性变异)已被报道,其中73个是新的(16%是新的)。VUC的频率在0.2%至76%之间,有害变化的频率在2.1至15%之间。在马来西亚患者中,只有BRCA1、BRCA2、PALB2、APOBEC3B和P53与BC风险相关。其中9项研究是使用重叠的患者来源进行的,这可能会限制研究结果在马来西亚全体人群中的可推广性。结论:关于马来西亚人群BC基因基础的信息很少。需要通过适当的样本选择技术和多中心合作的研究设计进行多学科的努力来解决这个问题。在13个BC的高外显率和中等外显率致病突变中,只有5个与马来西亚人的BC易感性有关。这篇综述的发现对决策者、研究人员和医生来说很有价值,有助于加强遗传服务在筛查和预防中的研究计划和效用。
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