在综合医疗保健系统中,通过通用肿瘤筛查计划识别林奇综合征患者。
Identifying patients with Lynch syndrome using a universal tumor screening program in an integrated healthcare system.
作者信息
Crain Philip R, Zepp Jamilyn M, Gille Sara, Jenkins Lindsay, Kauffman Tia L, Shuster Elizabeth, Goddard Katrina A B, Wilfond Benjamin S, Hunter Jessica Ezzell
机构信息
Department of Biostatistics, School of Public Health, University of Washington, Seattle, WA, USA.
Department of Translational and Applied Genomics, Center for Health Research, Kaiser Permanente Northwest, Portland, OR, USA.
出版信息
Hered Cancer Clin Pract. 2022 Apr 18;20(1):17. doi: 10.1186/s13053-022-00217-1.
INTRODUCTION
Lynch syndrome (LS) is associated with an increased risk of colorectal (CRC) and endometrial (EC) cancers. Universal tumor screening (UTS) of all individuals diagnosed with CRC and EC is recommended to increase identification of LS. Kaiser Permanente Northwest (KPNW) implemented a UTS program for LS among individuals newly diagnosed with CRC in January 2016 and EC in November 2016. UTS at KPNW begins with immunohistochemistry (IHC) of tumor tissue to determine loss of mismatch repair proteins associated with LS (MLH1, MSH2, MSH6, and PMS2)., IHC showing loss of MLH1 is followed by reflex testing (automatic testing) to detect the presence of the BRAF V600E variant (in cases of CRC) and MLH1 promoter hypermethylation to rule out likely sporadic cases.
MATERIALS AND METHODS
Individuals newly diagnosed with CRC and EC were identified between the initiation of the respective UTS programs and July 2018. Electronic medical records were reviewed to extract patient data related to UTS, including IHC and reflex testing results, date of referrals to the genetics department, and results of germline genetic testing for LS.
RESULTS
313 out of 362 individuals diagnosed with CRC and 61 out of 64 individuals diagnosed with EC who were eligible were screened by IHC for LS. Most (47/52 or 90%, including 46/49 CRC and 1/3 EC) individuals that were not screened by IHC only had a biopsy sample available. Fourteen individuals (3.7% overall, including 13/313 CRC and 1/61 EC) received an abnormal result after reflex testing and were referred for genetic counseling. Of these, 10 individuals (71% overall, including 9/13 CRC and 1/1 EC) underwent germline genetic testing for LS. Five individuals diagnosed with CRC were found to have pathogenic variants. in PMS2 (n = 3), MLH1 (n = 1), and MSH6 (n = 1). No pathogenic variants were identified in individuals diagnosed with EC.
CONCLUSIONS
UTS identified individuals at risk for LS. Most individuals who screened positive for LS had follow-up germline genetic testing for LS. The consistent use of biopsy samples is an opportunity to improve UTS.
引言
林奇综合征(LS)与结直肠癌(CRC)和子宫内膜癌(EC)风险增加相关。建议对所有诊断为CRC和EC的个体进行普遍肿瘤筛查(UTS),以提高LS的识别率。凯撒永久医疗集团西北分部(KPNW)于2016年1月针对新诊断为CRC的个体以及2016年11月针对新诊断为EC的个体实施了LS的UTS计划。KPNW的UTS首先对肿瘤组织进行免疫组化(IHC)检测,以确定与LS相关的错配修复蛋白(MLH1、MSH2、MSH6和PMS2)的缺失情况。免疫组化显示MLH1缺失后,进行反射试验(自动检测)以检测BRAF V600E变体的存在(在CRC病例中)以及MLH1启动子高甲基化,以排除可能的散发病例。
材料与方法
在各自UTS计划启动至2018年7月期间,确定新诊断为CRC和EC的个体。查阅电子病历以提取与UTS相关的患者数据,包括免疫组化和反射试验结果、转诊至遗传科的日期以及LS的种系基因检测结果。
结果
362例诊断为CRC的个体中有313例以及64例诊断为EC的个体中有61例符合条件,接受了免疫组化LS筛查。大多数(47/52或90%,包括46/49 CRC和1/3 EC)未接受免疫组化筛查的个体仅获得了活检样本。14例个体(总体占3.7%,包括13/313 CRC和1/61 EC)在反射试验后获得异常结果,并被转诊进行遗传咨询。其中,10例个体(总体占71%,包括9/13 CRC和1/1 EC)接受了LS的种系基因检测。5例诊断为CRC的个体被发现存在致病变体,分别为PMS2(n = 3)、MLH1(n = 1)和MSH6(n = 1)。诊断为EC的个体中未发现致病变体。
结论
UTS识别出了有LS风险的个体。大多数LS筛查呈阳性的个体接受了LS的后续种系基因检测。活检样本的持续使用是改善UTS的一个契机。
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