MSH6和PMS2基因突变与监测发现的结直肠癌风险之间的关联
Associations Between Mutations in MSH6 and PMS2 and Risk of Surveillance-detected Colorectal Cancer.
作者信息
Lamba Mehul, Wakeman Chris, Ebel Rosy, Hamilton Sarah, Frampton Chris, Kiesanowski Maxene, Griffiths Ben, Keating John, Parry Susan, Chalmers-Watson Teresa
机构信息
Department of Gastroenterology, Christchurch Hospital, Christchurch.
New Zealand Familial Gastrointestinal Cancer Service, Christchurch.
出版信息
Clin Gastroenterol Hepatol. 2020 Nov;18(12):2768-2774. doi: 10.1016/j.cgh.2020.03.048. Epub 2020 Mar 30.
BACKGROUND & AIMS: Lynch syndrome is the most common inherited cause of colorectal cancer (CRC). Contemporary and mutation-specific estimates of CRC-risk in patients undergoing colonoscopy would optimize surveillance strategies. We performed a prospective national cohort study, using data from New Zealand, to assess overall and mutation-specific risk of CRC in patients with Lynch syndrome undergoing surveillance.
METHODS
We performed a prospective study of 381 persons with Lynch syndrome in New Zealand (98 with Lynch-syndrome associated variants in MLH1, 159 in MSH2, 103 in MSH6, and 21 in PMS2). Participants were offered annual colonoscopy starting at age 25 y, and those who underwent 2 or more colonoscopies before December 31, 2017 were included in the final analysis. Patients with previous colonic resection, history of CRC or diagnosis of CRC at index colonoscopy were excluded.
RESULTS
Study participants underwent 2061 colonoscopies during 2296 person-y; the median observation-period was 4.43 y and mean-age at enrollment was 43 y. Eighteen patients developed CRC (8 with variants in MLH1, 8 in MSH2, and 2 in MSH6) after a median follow-up period of 6.5 y (range 1-16 y). Eighty-three percent of patients had a surveillance colonoscopy in preceding 24 months before diagnosis of CRC; 94% were diagnosed with stage 0-II CRC and there was no CRC-related mortality. The overall-risk of developing CRC in the 5 y after first surveillance colonoscopy was 2.49% (95% CI, 1.18-5.23); cumulative risks for CRC in patients with Lynch syndrome-associated variants in MLH1, MSH2, or MSH6 by age 70 y were 17.7%, 17.8%, and 8.5%, respectively. Age-adjusted CRC-risk in patients with variants in MSH6 was lower than in MLH1 (hazard ratio, 0.2; 95% CI, 0.04-0.94; P = .02). Of patients with CRC, 33% had an adenomatous polyp resected from same segment in which a colorectal tumor later developed.
CONCLUSIONS
The risk of CRC in patients with Lynch syndrome-associated mutations in MSH6 or PMS2 was significantly lower than in patients with mutations in MLH1. Incomplete adenomatous polyp resection might be responsible for one third of surveillance-detected CRCs.
背景与目的
林奇综合征是结直肠癌(CRC)最常见的遗传病因。对接受结肠镜检查的患者进行当代及特定突变的CRC风险评估,将优化监测策略。我们利用来自新西兰的数据进行了一项前瞻性全国队列研究,以评估接受监测的林奇综合征患者患CRC的总体风险和特定突变风险。
方法
我们对新西兰的381例林奇综合征患者进行了前瞻性研究(98例MLH1基因有林奇综合征相关变异,159例MSH2基因变异,103例MSH6基因变异,21例PMS2基因变异)。参与者从25岁开始每年接受一次结肠镜检查,在2017年12月31日前接受过2次或更多次结肠镜检查的患者纳入最终分析。排除既往有结肠切除术、CRC病史或在首次结肠镜检查时诊断为CRC的患者。
结果
研究参与者在2296人年期间接受了2061次结肠镜检查;中位观察期为4.43年,入组时的平均年龄为43岁。18例患者在中位随访期6.5年(范围1 - 16年)后发生CRC(8例MLH1基因变异,8例MSH2基因变异,2例MSH6基因变异)。83%的患者在CRC诊断前的24个月内接受了监测结肠镜检查;94%被诊断为0-II期CRC,且无CRC相关死亡。首次监测结肠镜检查后5年内发生CRC的总体风险为2.49%(95%CI,1.18 - 5.23);到70岁时,MLH1、MSH2或MSH6基因有林奇综合征相关变异的患者患CRC的累积风险分别为17.7%、17.8%和8.5%。MSH6基因变异患者的年龄调整后CRC风险低于MLH1基因变异患者(风险比,0.2;95%CI,0.04 - 0.94;P = 0.02)。在患有CRC的患者中,33%在后来发生结直肠肿瘤的同一节段切除了腺瘤性息肉。
结论
MSH6或PMS2基因有林奇综合征相关突变的患者患CRC的风险显著低于MLH1基因突变的患者。腺瘤性息肉切除不完全可能是监测发现的CRC的三分之一的原因。
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