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Trans-ancestral genetic study of diabetes mellitus risk in survivors of childhood cancer: a report from the St. Jude Lifetime Cohort and the Childhood Cancer Survivor Study.儿童癌症幸存者糖尿病风险的跨祖先基因研究:来自圣裘德终身队列和儿童癌症幸存者研究的报告
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儿童癌症幸存者糖尿病风险的跨祖先基因研究:来自圣裘德终身队列和儿童癌症幸存者研究的报告

Trans-ancestral genetic study of diabetes mellitus risk in survivors of childhood cancer: a report from the St. Jude Lifetime Cohort and the Childhood Cancer Survivor Study.

作者信息

Im Cindy, Neupane Achal, Baedke Jessica L, Delaney Angela, Dixon Stephanie B, Chow Eric J, Mostoufi-Moab Sogol, Richard Melissa A, Gramatges M Monica, Lupo Philip J, Sharafeldin Noha, Bhatia Smita, Armstrong Gregory T, Hudson Melissa M, Ness Kirsten K, Robison Leslie L, Yasui Yutaka, Wilson Carmen L, Sapkota Yadav

出版信息

medRxiv. 2023 Jun 5:2023.06.02.23290868. doi: 10.1101/2023.06.02.23290868.

DOI:10.1101/2023.06.02.23290868
PMID:37333357
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10274964/
Abstract

Type 2 diabetes mellitus (T2D) is an established late effect of treatment for childhood cancer. Leveraging detailed cancer treatment and whole-genome sequencing data among survivors of childhood cancer of European (EUR) and African (AFR) genetic ancestry in the St. Jude Lifetime Cohort (N=3,676; 304 cases), five novel diabetes mellitus (DM) risk loci were identified with independent trans-/within-ancestry replication, including in 5,965 survivors of the Childhood Cancer Survivor Study. Among these, common risk variants at 5p15.2 ( ), 2p25.3 ( ), and 19p12 ( ) modified alkylating agent-related risks across ancestry groups, but AFR survivors with risk alleles experienced disproportionately greater risk of DM (AFR, variant ORs: 3.95-17.81; EUR, variant ORs: 2.37-3.32). Novel risk locus was identified in the first genome-wide DM rare variant burden association analysis in survivors (OR=8.65, 95% CI: 3.02-24.74, P=8.1×10 ). Lastly, a general-population 338-variant multi-ancestry T2D polygenic risk score was informative for DM risk in AFR survivors, and showed elevated DM odds after alkylating agent exposures (quintiles: combined OR =8.43, P=1.1×10 ; OR =13.85, P=0.033). This study supports future precision diabetes surveillance/survivorship care for all childhood cancer survivors, including those with AFR ancestry.

摘要

2型糖尿病(T2D)是儿童癌症治疗后已明确的晚期效应。利用圣裘德终身队列中欧洲(EUR)和非洲(AFR)遗传血统的儿童癌症幸存者的详细癌症治疗和全基因组测序数据(N = 3676;304例病例),通过独立的跨血统/血统内复制鉴定出五个新的糖尿病(DM)风险位点,包括在儿童癌症幸存者研究的5965名幸存者中。其中,5p15.2( )、2p25.3( )和19p12( )的常见风险变异改变了各血统组中与烷化剂相关的风险,但携带风险等位基因的AFR幸存者患DM的风险不成比例地更高(AFR,变异比值比:3.95 - 17.81;EUR,变异比值比:2.37 - 3.32)。在幸存者的首次全基因组DM罕见变异负担关联分析中鉴定出了新的风险位点(比值比 = 8.65,95%置信区间:3.02 - 24.74,P = 8.1×10 )。最后,一个通用人群的338变异多血统T2D多基因风险评分对AFR幸存者的DM风险具有参考价值,并且在接触烷化剂后显示出患DM的几率升高(五分位数:合并比值比 = 8.43,P = 1.1×10 ;比值比 = 13.85,P = 0.033)。这项研究支持未来对所有儿童癌症幸存者,包括那些具有AFR血统的幸存者进行精准糖尿病监测/生存护理。