Niewisch Marena R, Kim Jung, Giri Neelam, Lunger Judith C, McReynolds Lisa J, Savage Sharon A
Clinical Genetics Branch, Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Bethesda, Maryland.
Department of Pediatric Hematology and Oncology, Medical School Hannover, Hannover, Germany.
JAMA Netw Open. 2024 Dec 2;7(12):e2450111. doi: 10.1001/jamanetworkopen.2024.50111.
Telomere biology disorders (TBDs) are inherited cancer-prone bone marrow failure syndromes with differences in morbidity and mortality based on mode of inheritance.
To quantify cancer risks in TBDs by genetic subgroups.
DESIGN, SETTING, AND PARTICIPANTS: This longitudinal cohort study of TBDs assessed cancer occurrences from 2002 through 2022. Participants were individuals with a TBD-associated pathogenic germline variant recruited across institutions by self-referral. Data were collected and analyzed through June 30, 2022.
The exposure was TBD genotypes, with subgroups defined by inheritance pattern (autosomal-dominant [AD-non-TINF2] vs autosomal-recessive/X-linked [AR/XLR] vs AD-TINF2).
The main outcome was cancer; secondary outcomes included death, or organ transplant. Cumulative cancer incidence was determined considering death or transplant as competing events. Observed:expected (O:E) ratios of cancer before and after any organ transplant were calculated using the National Cancer Institute's Surveillance, Epidemiology, and End Results Program.
Among 230 individuals with TBD (135 [58.7%] male; median [range] age at last follow-up, 34.6 [1.4-82.2] years) included, the risk of cancer was 3-fold higher than the general population (O:E, 3.35 [95% CI, 2.32-4.68]). The highest risk was observed in individuals with AR/XLR (O:E, 19.16 [95% CI, 9.19-35.24]) with a significantly younger cancer onset than in individuals with AD-non-TINF2 (median [range] age, 36.7 [25.2-53.6] years vs 44.5 [32.2-67.5] years; P = .01). The risk of solid tumors was highest in individuals with AR/XLR (O:E = 23.97 [95% CI, 10.96-45.50]), predominantly head and neck squamous cell carcinomas (O:E, 276.00 [95% CI, 75.20-706.67]). Hematologic malignant neoplasm risk was highest in individuals with AD-non-TINF2 (O:E, 9.41 [95% CI, 4.30-17.86]). Solid tumor cumulative incidence increased to 12% for individuals with AR/XLR by age 45 years and to 13% for individuals with AD-non-TINF2 by age 70 years. The cumulative incidence of hematologic malignant neoplasms leveled off at 2% by age 30 years and 19% by age 70 years in individuals with AR/XLR and AD-non-TINF2, respectively. Individuals with AD-TINF2 showed the highest cumulative incidence for transplant or death (49% by age 15 years). Following transplant, individuals with AR/XLR (O:E, 136.11 [95% CI, 54.72-280.44) or AD-TINF2 (O:E, 81.07 [95% CI, 16.72-236.92]) had the highest cancer risk, predominantly young-onset head and neck squamous cell carcinomas (median [range] age, 32.2 [10.5-35.5] years).
This cohort study of individuals with TBDs found an increased cancer risk compared with the general population, with the earliest age at onset for individuals with AR/XLR inheritance. Cancer risks increased after organ transplant across all subgroups. These differences in TBD-associated cancer risks by mode of inheritance suggest cancer screening could be tailored by genotype, but additional research is warranted.
端粒生物学障碍(TBDs)是遗传性的易患癌症的骨髓衰竭综合征,其发病率和死亡率因遗传方式而异。
按基因亚组量化TBDs中的癌症风险。
设计、设置和参与者:这项TBDs的纵向队列研究评估了2002年至2022年期间的癌症发生情况。参与者是通过自我推荐在多个机构招募的携带与TBD相关的致病性种系变异的个体。数据收集至2022年6月30日并进行分析。
暴露因素为TBD基因型,亚组由遗传模式定义(常染色体显性遗传[AD-non-TINF2]与常染色体隐性/ X连锁遗传[AR/XLR]与AD-TINF2)。
主要结局是癌症;次要结局包括死亡或器官移植。考虑将死亡或移植作为竞争事件来确定累积癌症发病率。使用美国国立癌症研究所的监测、流行病学和最终结果计划计算任何器官移植前后癌症的观察值:预期值(O:E)比率。
在纳入的230例TBD个体中(135例[58.7%]为男性;最后随访时的年龄中位数[范围]为34.6[1.4 - 82.2]岁),癌症风险比一般人群高3倍(O:E,3.35[95%CI,2.32 - 4.68])。AR/XLR个体的风险最高(O:E,19.16[95%CI,9.19 - 35.24]),其癌症发病年龄明显低于AD-non-TINF2个体(年龄中位数[范围],36.7[25.2 - 53.6]岁对44.5[32.2 - 67.5]岁;P = 0.01)。实体瘤风险在AR/XLR个体中最高(O:E = 23.97[95%CI,10.96 - 45.50]),主要是头颈部鳞状细胞癌(O:E,276.00[95%CI,75.20 - 706.67])。血液系统恶性肿瘤风险在AD-non-TINF2个体中最高(O:E,9.41[95%CI,4.30 - 17.86])。到45岁时,AR/XLR个体的实体瘤累积发病率增加到12%,到70岁时,AD-non-TINF2个体的实体瘤累积发病率增加到13%。在AR/XLR和AD-non-TINF2个体中,血液系统恶性肿瘤的累积发病率在30岁时分别稳定在2%,在70岁时分别稳定在19%。AD-TINF2个体的移植或死亡累积发病率最高(15岁时为49%)。移植后,AR/XLR个体(O:E,136.11[95%CI,54.72 - 280.44])或AD-TINF2个体(O:E,81.07[95%CI,16.72 - 236.92])的癌症风险最高,主要是早发性头颈部鳞状细胞癌(年龄中位数[范围],32.2[10.5 - 35.5]岁)。
这项对TBD个体的队列研究发现,与一般人群相比,癌症风险增加,AR/XLR遗传个体的发病年龄最早。所有亚组在器官移植后癌症风险均增加。TBD相关癌症风险因遗传方式的这些差异表明,癌症筛查可根据基因型进行调整,但仍需进一步研究。
