Department of Oncology, St. Jude Children's Research Hospital, Memphis, TN, 38105, USA.
Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, TX, 77030, USA.
Genome Med. 2020 May 29;12(1):51. doi: 10.1186/s13073-020-00744-3.
Distinct prevalence of inherited genetic predisposition may partially explain the difference of cancer risks across ancestries. Ancestry-specific analyses of germline genomes are required to inform cancer genetic risk and prognosis of diverse populations.
We conducted analyses using germline and somatic sequencing data generated by The Cancer Genome Atlas. Collapsing pathogenic and likely pathogenic variants to cancer predisposition genes (CPG), we analyzed the association between CPGs and cancer types within ancestral groups. We also identified the predisposition-associated two-hit events and gene expression effects in tumors.
Genetic ancestry analysis classified the cohort of 9899 cancer cases into individuals of primarily European (N = 8184, 82.7%), African (N = 966, 9.8%), East Asian (N = 649, 6.6%), South Asian (N = 48, 0.5%), Native/Latin American (N = 41, 0.4%), and admixed (N = 11, 0.1%) ancestries. In the African ancestry, we discovered a potentially novel association of BRCA2 in lung squamous cell carcinoma (OR = 41.4 [95% CI, 6.1-275.6]; FDR = 0.002) previously identified in Europeans, along with a known association of BRCA2 in ovarian serous cystadenocarcinoma (OR = 8.5 [95% CI, 1.5-47.4]; FDR = 0.045). In the East Asian ancestry, we discovered one previously known association of BRIP1 in stomach adenocarcinoma (OR = 12.8 [95% CI, 1.8-90.8]; FDR = 0.038). Rare variant burden analysis further identified 7 suggestive associations in African ancestry individuals previously described in European ancestry, including SDHB in pheochromocytoma and paraganglioma, ATM in prostate adenocarcinoma, VHL in kidney renal clear cell carcinoma, FH in kidney renal papillary cell carcinoma, and PTEN in uterine corpus endometrial carcinoma. Most predisposing variants were found exclusively in one ancestry in the TCGA and gnomAD datasets. Loss of heterozygosity was identified for 7 out of the 15 African ancestry carriers of predisposing variants. Further, tumors from the SDHB or BRCA2 carriers showed simultaneous allelic-specific expression and low gene expression of their respective affected genes, and FH splice-site variant carriers showed mis-splicing of FH.
While several CPGs are shared across patients, many pathogenic variants are found to be ancestry-specific and trigger somatic effects. Studies using larger cohorts of diverse ancestries are required to pinpoint ancestry-specific genetic predisposition and inform genetic screening strategies.
遗传易感性的不同流行率可能部分解释了不同种族间癌症风险的差异。需要对种系基因组进行特定种族的分析,以了解不同人群的癌症遗传风险和预后。
我们使用癌症基因组图谱(The Cancer Genome Atlas)生成的种系和体细胞测序数据进行了分析。将致病性和可能致病性变异合并为癌症易感基因(Cancer Predisposition Genes,CPG),我们分析了在祖先群体内 CPG 与癌症类型之间的关联。我们还鉴定了肿瘤中与易感性相关的双打击事件和基因表达效应。
遗传祖先分析将 9899 例癌症病例的队列分为主要为欧洲血统(N=8184,82.7%)、非洲血统(N=966,9.8%)、东亚血统(N=649,6.6%)、南亚血统(N=48,0.5%)、北美原住民/拉丁裔血统(N=41,0.4%)和混合血统(N=11,0.1%)。在非洲血统中,我们发现了 BRCA2 在肺鳞癌(OR=41.4[95%CI,6.1-275.6];FDR=0.002)中的一个潜在新关联,这在欧洲人中已被发现,同时在卵巢浆液性囊腺癌(OR=8.5[95%CI,1.5-47.4];FDR=0.045)中也发现了 BRCA2 的已知关联。在东亚血统中,我们发现了 BRIP1 在胃腺癌(OR=12.8[95%CI,1.8-90.8];FDR=0.038)中的一个先前已知的关联。罕见变异负担分析进一步鉴定了 7 个在非洲血统个体中具有先前在欧洲血统中描述的提示关联,包括 SDHB 在嗜铬细胞瘤和副神经节瘤、ATM 在前列腺腺癌、VHL 在肾透明细胞癌、FH 在肾乳头状细胞癌和 PTEN 在子宫体子宫内膜癌。在 TCGA 和 gnomAD 数据集中,大多数易感变异仅在一个祖系中发现。在 15 个携带易感变异的非洲血统个体中,有 7 个个体发生了杂合性缺失。此外,SDHB 或 BRCA2 携带者的肿瘤表现出等位基因特异性表达和各自受影响基因的低基因表达,而 FH 剪接位点变异携带者表现出 FH 的剪接错误。
虽然有几个 CPG 是在患者中共享的,但许多致病性变异被发现是特定于祖系的,并引发了体细胞效应。需要使用更多具有不同祖系的大型队列研究来确定特定于祖系的遗传易感性,并为遗传筛查策略提供信息。
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