Geisinger Clinic, Geisinger Health System, Danville, Pennsylvania.
Clinical Genetics Branch, Division of Cancer Epidemiology and Genetics, National Cancer Institute, Rockville, Maryland.
JAMA Netw Open. 2021 Feb 1;4(2):e210112. doi: 10.1001/jamanetworkopen.2021.0112.
Genetic disorders are historically defined through phenotype-first approaches. However, risk estimates derived from phenotype-linked ascertainment may overestimate severity and penetrance. Pathogenic variants in DICER1 are associated with increased risks of rare and common neoplasms and thyroid disease in adults and children. This study explored how effectively a genome-first approach could characterize the clinical traits associated with germline DICER1 putative loss-of-function (pLOF) variants in an unselected clinical cohort.
To examine the prevalence, penetrance, and phenotypic characteristics of carriers of germline DICER1 pLOF variants via genome-first ascertainment.
DESIGN, SETTING, AND PARTICIPANTS: This cohort study classifies DICER1 variants in germline exome sequence data from 92 296 participants of the Geisinger MyCode Community Health Initiative. Data for each MyCode participant were used from the start of the Geisinger electronic health record to February 1, 2018.
Prevalence of germline DICER1 variation; penetrance of malignant tumors and thyroid disease in carriers of germline DICER1 variation; structured, manual review of electronic health records; and DICER1 sequencing of available tumors from an associated cancer registry.
A total of 92 296 adults (mean [SD] age, 59 [18] years; 98% white; 60% female) participated in the study. Germline DICER1 pLOF variants were observed in 1 in 3700 to 1 in 4600 participants, more than double the expected prevalence. Malignant tumors (primarily thyroid carcinoma) were observed in 4 of 25 participants (16%) with DICER1 pLOF variants, which is comparable (by 50 years of age) to the frequency of neoplasms in the largest registry- and clinic-based (phenotype-first) DICER1 studies published to date. DICER1 pLOF variants were significantly associated with risks of thyroidectomy (odds ratio [OR], 6.0; 95% CI, 2.2-16.3; P = .007) and thyroid cancer (OR, 9.2; 95% CI, 2.1-34.7; P = .02) compared with controls, but there was not a significant increase in the risk of goiter (OR, 1.8; 95% CI, 0.7-4.9). A female patient in her 80s who was a carrier of a germline DICER1 hotspot variant was apparently healthy on electronic health record review. The term DICER1 did not appear in any of the medical records of the 25 participants with a pLOF DICER1 variant, even in those affected with a known DICER1-associated tumor or thyroid phenotype.
This cohort study was able to ascertain individuals with germline DICER1 variants based on a genome-first approach rather than through a previously established DICER1-related phenotype. Use of the genome-first approach may complement more traditional approaches to syndrome delineation and may be an efficient approach for risk estimation.
遗传疾病在历史上是通过表型优先的方法来定义的。然而,源自与表型相关联的确定方法的风险估计可能会高估严重程度和外显率。DICER1 中的致病性变体与成人和儿童中罕见和常见肿瘤以及甲状腺疾病的风险增加有关。本研究探讨了在未经选择的临床队列中,通过全基因组优先方法是否能有效地描述与种系 DICER1 潜在功能丧失(pLOF)变体相关的临床特征。
通过全基因组优先确定来检查种系 DICER1 pLOF 变体携带者的患病率、外显率和表型特征。
设计、地点和参与者:本队列研究对来自 Geisinger MyCode 社区健康倡议的 92296 名参与者的外显子组序列数据中的 DICER1 变体进行分类。从每个 MyCode 参与者的 Geisinger 电子健康记录开始到 2018 年 2 月 1 日的数据都被用于研究。
种系 DICER1 变异的患病率;种系 DICER1 变异携带者恶性肿瘤和甲状腺疾病的外显率;电子健康记录的结构化、手动审查;以及来自相关癌症登记处的可用肿瘤的 DICER1 测序。
共有 92296 名成年人(平均[标准差]年龄,59[18]岁;98%为白人;60%为女性)参加了这项研究。在 3700 至 4600 名参与者中观察到 1 名种系 DICER1 pLOF 变体,这一比例是预期的两倍多。在 25 名携带 DICER1 pLOF 变体的参与者中,有 4 名(16%)患有恶性肿瘤(主要为甲状腺癌),这与迄今为止发表的最大的基于登记和诊所的(表型优先)DICER1 研究中报道的肿瘤发生频率相当(截至 50 岁)。与对照组相比,DICER1 pLOF 变体与甲状腺切除术(比值比[OR],6.0;95%置信区间[CI],2.2-16.3;P =.007)和甲状腺癌(OR,9.2;95% CI,2.1-34.7;P =.02)的风险显著相关,但甲状腺肿(OR,1.8;95% CI,0.7-4.9)的风险没有显著增加。一名 80 多岁的女性患者是携带种系 DICER1 热点变体的携带者,在电子健康记录审查中显然是健康的。在 25 名携带 pLOF DICER1 变体的参与者的所有医疗记录中都没有出现 DICER1 这个词,即使在那些患有已知的 DICER1 相关肿瘤或甲状腺表型的参与者中也是如此。
本队列研究能够通过全基因组优先方法确定携带种系 DICER1 变体的个体,而不是通过先前建立的 DICER1 相关表型。使用全基因组优先方法可能补充更传统的综合征描述方法,并且可能是一种有效的风险估计方法。
