Massive parallel sequencing in individuals with multiple primary tumours reveals the benefit of re-analysis.

IF 2 4区 医学 Q3 ONCOLOGY
Karin Wallander, Håkan Thonberg, Daniel Nilsson, Emma Tham
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Abstract

Multiple primary cancers, defined as three or more primary tumours, are rare, and there are few genetic studies concerning them. There is a need for increased knowledge on the heritability of multiple primary cancers and genotype-phenotype correlations. We have performed whole-genome/exome sequencing (WGS/WES) in ten individuals with three or more primary tumours, with no previous findings on standard clinical genetic investigations. In one individual with a clinical diagnosis of MEN1, a likely pathogenic cryptic splice site variant was detected in the MEN1 gene. The variant (c.654C > A) is synonymous but we showed in a cDNA analysis that it affects splicing and leads to a frameshift, with the theoretical new amino acid sequence p.(Gly219Glufs*13). In one individual with metachronous colorectal cancers, ovarian cancer, endometrial cancer and chronic lymphocytic leukaemia, we found a likely pathogenic variant in the MLH1 gene (c.27G > A), and two risk factor variants in the genes CHEK2 and HOXB13. The MLH1 variant is synonymous but has previously been shown to be associated to constitutional low-grade hypermethylation of the MLH1 promoter, and segregates with disease in families with colorectal and endometrial cancer. No pathogenic single nucleotide or structural variants were detected in the remaining eight individuals in the study. The pathogenic variants found by WGS/WES were in genes already sequenced by Sanger sequencing and WES in the clinic, without any findings. We conclude that, in individuals with an unequivocal clinical diagnosis of a specific hereditary cancer syndrome, where standard clinical testing failed to detect a causative variant, re-analysis may lead to a diagnosis.

Abstract Image

对患有多种原发性肿瘤的个体进行大规模平行测序,揭示了重新分析的益处。
多发性原发性癌症是指三个或三个以上的原发性肿瘤,这种癌症非常罕见,有关这种癌症的遗传学研究也很少。我们需要进一步了解多发性原发性癌症的遗传性以及基因型与表型之间的相关性。我们对 10 名患有 3 个或更多原发性肿瘤,且之前未进行过标准临床基因检测的患者进行了全基因组/外显子组测序(WGS/WES)。在一名临床诊断为 MEN1 的患者中,我们在 MEN1 基因中检测到了一个可能致病的隐性剪接位点变异。该变异(c.654C > A)是同义变异,但我们在 cDNA 分析中发现,该变异会影响剪接并导致帧移位,其理论上的新氨基酸序列为 p.(Gly219Glufs*13)。在一个同时患有结直肠癌、卵巢癌、子宫内膜癌和慢性淋巴细胞白血病的人身上,我们发现了 MLH1 基因中一个可能的致病变体(c.27G > A),以及 CHEK2 和 HOXB13 基因中的两个风险因子变体。MLH1基因变异是同义的,但先前已证明它与MLH1基因启动子的低度低甲基化有关,并在结直肠癌和子宫内膜癌家族中与疾病分离。研究中的其余 8 人未检测到致病性单核苷酸变异或结构变异。通过 WGS/WES 发现的致病变异位于已在临床上通过 Sanger 测序和 WES 测序的基因中,但没有任何发现。我们的结论是,在临床明确诊断为特定遗传性癌症综合征的个体中,如果标准临床检测未能检测到致病变异,重新分析可能会得出诊断结果。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
3.10
自引率
5.90%
发文量
38
审稿时长
>12 weeks
期刊介绍: Hereditary Cancer in Clinical Practice is an open access journal that publishes articles of interest for the cancer genetics community and serves as a discussion forum for the development appropriate healthcare strategies. Cancer genetics encompasses a wide variety of disciplines and knowledge in the field is rapidly growing, especially as the amount of information linking genetic differences to inherited cancer predispositions continues expanding. With the increased knowledge of genetic variability and how this relates to cancer risk there is a growing demand not only to disseminate this information into clinical practice but also to enable competent debate concerning how such information is managed and what it implies for patient care. Topics covered by the journal include but are not limited to: Original research articles on any aspect of inherited predispositions to cancer. Reviews of inherited cancer predispositions. Application of molecular and cytogenetic analysis to clinical decision making. Clinical aspects of the management of hereditary cancers. Genetic counselling issues associated with cancer genetics. The role of registries in improving health care of patients with an inherited predisposition to cancer.
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