Novel microsatellite instability test of sebaceous tumours to facilitate low-cost universal screening for Lynch syndrome.

IF 3.7 4区 医学 Q1 DERMATOLOGY
Richard Gallon, Georgie Holt, Waleed Alfailakawi, Akhtar Husain, Claire Jones, Peter Sowter, Mauro Santibanez-Koref, Michael S Jackson, John Burn, Sam Cook, Neil Rajan
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Abstract

Background: One in five patients with sebaceous tumours (STs) may have Lynch syndrome (LS), an inherited disorder that increases the risk of developing cancer. Patients with LS benefit from cancer surveillance and prevention programmes and immunotherapy. While universal tumour mismatch repair (MMR) deficiency testing is recommended in colorectal and endometrial cancers to screen for LS, there is no consensus screening strategy for STs, leading to low testing rates and inequity of care.

Objectives: To assess a low-cost and scalable sequencing-based microsatellite instability (MSI) assay, previously shown to enhance LS screening of colorectal cancers, for MMR deficiency detection in STs against the current clinical standard of immunohistochemistry (IHC).

Methods: Consecutive ST cases (n = 107) were identified from the records of a single pathology department. MMR protein IHC staining was interpreted by a consultant histopathologist. MSI analysis used amplicon sequencing of 14 microsatellites and a naive Bayesian classifier to calculate the sample MSI score.

Results: Loss of MMR protein expression was observed in 49/104 STs with interpretable IHC [47.1%, 95% confidence interval (CI) 37.3-57.2]. MMR deficiency was less frequent in carcinoma than in adenoma and sebaceoma (P = 4.74 × 10-3). The majority of MMR-deficient STs had concurrent loss of MSH2 and MSH6 expression. The MSI score achieved a receiver operator characteristic area under curve of 0.944 relative to IHC. Lower MSI scores were associated with MSH6 deficiency.

Conclusions: These data support MSI testing as an adjunct or alternative to MMR IHC in STs. Integration of STs into established LS screening pathways using this high-throughput methodology could increase testing and reduce costs.

一种新型的皮脂腺肿瘤微卫星不稳定性试验,以促进低成本的Lynch综合征的普遍筛查。
背景:五分之一的皮脂腺肿瘤(ST)患者可能患有Lynch综合征(LS),这是一种遗传性癌症易感性。LS患者受益于癌症监测和预防规划以及免疫治疗。虽然普遍的肿瘤错配修复(MMR)缺陷检测被推荐用于结肠直肠癌和子宫内膜癌的LS筛查,但对于ST的筛查策略尚无共识,导致检测率低和护理不公平。目的:评估一种低成本、可扩展、基于测序的微卫星不稳定性(MSI)检测方法,该方法先前被证明可以增强LS对结直肠癌的筛查,用于检测ST中MMR缺陷,而不是当前的免疫组织化学(IHC)临床标准。方法:在同一病理科连续发现107例ST病例。MMR蛋白免疫组化染色由组织病理学顾问解释。MSI分析使用14颗微卫星的扩增子测序和naïve贝叶斯分类器计算样本MSI评分。结果:49/104 ST中MMR蛋白表达缺失,IHC可解释(47.1%;95% ci: 37.3-57.2%)。MMR缺乏在癌中的发生率低于腺瘤和皮脂腺瘤(P = 4.74x10-3)。大多数MMR缺陷ST同时缺失MSH2和MSH6的表达。相对于IHC, MSI得分达到了0.944的接受者操作者特征曲线下面积。MSI评分较低与MSH6缺乏有关。结论:这些数据支持MSI检测作为ST中MMR IHC的辅助或替代方法,使用这种高通量方法将ST整合到已建立的LS筛选途径中可以增加检测并降低成本。
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来源期刊
CiteScore
3.20
自引率
2.40%
发文量
389
审稿时长
3-8 weeks
期刊介绍: Clinical and Experimental Dermatology (CED) is a unique provider of relevant and educational material for practising clinicians and dermatological researchers. We support continuing professional development (CPD) of dermatology specialists to advance the understanding, management and treatment of skin disease in order to improve patient outcomes.
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