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利用基因型辅助临床监测:中国家族性腺瘤性息肉病患者的回顾性研究

Using genotype to assist clinical surveillance: a retrospective study of Chinese familial adenomatous polyposis patients.

作者信息

Ge Sai, Cheng Duo, Zhang Xuhui, Xu Ting, Wang Zhenghang, Dong Fengxiao, Su Lan, Song Jinlei, Wang Jia, Li Jian, Shen Lin, Wang Xicheng

机构信息

Department of Gastrointestinal Oncology, Key Laboratory of Carcinogenesis and Translational Research (Ministry of Education/Beijing), Peking University Cancer Hospital and Institute Beijing, China.

Department of Oncology and Rehabilitation, Zhengzhou Central Hospital Affiliated to Zhengzhou University Zhengzhou, China.

出版信息

Am J Cancer Res. 2022 Sep 15;12(9):4254-4266. eCollection 2022.

Abstract

Without treatment, familial adenomatous polyposis (FAP) patients will inevitably develop colorectal cancer (CRC) during lifetime. Yet, surgical trauma is a high risk of desmoid tumor (DT), one of the main causes of death in FAP patients. So far, the timing for colectomy is primarily based on the clinician's experience and the patient's preference; most patients undergo surgery at mid-20's. In this study, we analyzed the germline mutation distribution in 35 FAP patients from different families, 16 of them diagnosed with DTs. We also investigated the association between the molecular alterations and the clinicopathological features. Capture-based targeted sequencing using a panel of 520 genes was performed on tumor tissue and paired normal mucosa or white blood cells from 18 FAP probands who were initially diagnosed with CRC. Of all 35 FAP patients, 30 (85.7%) of them harbored germline mutations scattered from codon 161 to 1578. The mutations in the 16 DT patients scattered from codon 457 to 1578. All three patients with the mutation at the 3' of 1444 codon were diagnosed with DT. The percentage of high-risk DT (stage III or IV) harboring mutations at the 5' of 1062 or 1062-1578 was 14.3% and 77.8%, respectively, and all three patients with 3' of 1399 codon mutation had high risk. In addition, by using public database, we compared 140 FAP patients with DT to all 1880 FAP patients on the Leiden Open Variation Database and found that the odd ratio of DT in codon 159 to 495 was 0.34, while in codon 1310 to 2011 was 2.36. Compared to sporadic CRCs, the somatic spectrum of FAP CRCs was similar to the early onset CRCs, with higher (94.1%) and lower somatic mutations (65.7%), but the mutation rate was the highest (58.5%). One of the 18 FAP CRCs was identified as microsatellite instability-high (MSI-H), with tumor mutation burden (TMB) of 115.65 mut/Mb. Given that no mutations were detected in the low- and high-grade adenomas, ctDNA sequencing might be used for the close monitoring before FAP colectomy. In conclusion, except mutations at the 5' end of (5' to 495), all FAP patients need to consider the risk of DT after colectomy. The chance of life-threating DTs was higher in patients with 3' 1062 codon mutation and peaked in patients with 3' 1399 codon mutation. Scheduled monitoring of ctDNA is proposed to be a novel tool for optimizing the operation time.

摘要

未经治疗的家族性腺瘤性息肉病(FAP)患者在一生中将不可避免地发展为结直肠癌(CRC)。然而,手术创伤是硬纤维瘤(DT)的高风险因素,DT是FAP患者的主要死亡原因之一。到目前为止,结肠切除术的时机主要基于临床医生的经验和患者的偏好;大多数患者在25岁左右接受手术。在本研究中,我们分析了来自不同家族的35例FAP患者的种系突变分布,其中16例被诊断为DT。我们还研究了分子改变与临床病理特征之间的关联。对18例最初诊断为CRC的FAP先证者的肿瘤组织以及配对的正常黏膜或白细胞进行了基于捕获的靶向测序,该测序使用了一组520个基因。在所有35例FAP患者中,30例(85.7%)携带从密码子161到1578的种系突变。16例DT患者的突变分布在密码子457到1578之间。所有3例在密码子1444 3'端发生突变的患者均被诊断为DT。携带密码子1062 5'端或1062 - 1578突变的高危DT(III期或IV期)患者的比例分别为14.3%和77.8%,并且所有3例在密码子1399 3'端发生突变的患者均为高危患者。此外,通过使用公共数据库,我们将140例患有DT的FAP患者与莱顿开放变异数据库中的所有1880例FAP患者进行了比较,发现密码子159至495处发生DT的比值比为0.34,而在密码子1310至2011处为2.36。与散发性CRC相比,FAP CRC的体细胞谱与早发性CRC相似,具有较高的(94.1%)和较低的体细胞突变(65.7%),但突变率最高(58.5%)。18例FAP CRC中有1例被鉴定为微卫星高度不稳定(MSI - H),肿瘤突变负荷(TMB)为115.65 mut/Mb。鉴于在低级别和高级别腺瘤中未检测到突变,ctDNA测序可用于FAP结肠切除术之前的密切监测。总之,除了(5'至495)5'端的突变外,所有FAP患者在结肠切除术后都需要考虑DT的风险。密码子1062 3'端突变的患者发生危及生命的DT的几率更高,在密码子1399 3'端突变的患者中达到峰值。建议对ctDNA进行定期监测是优化手术时间的一种新工具。

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本文引用的文献

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A Case of Microsatellite Instability-High Colon Cancer in a Young Woman With Familial Adenomatous Polyposis.
J Natl Compr Canc Netw. 2021 Dec;19(12):1377-1381. doi: 10.6004/jnccn.2021.7073.
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