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所有上尿路尿路上皮癌均应进行普遍林奇综合征筛查。

Universal Lynch Syndrome Screening Should be Performed in All Upper Tract Urothelial Carcinomas.

机构信息

Departments of Pathology.

Urology.

出版信息

Am J Surg Pathol. 2018 Nov;42(11):1549-1555. doi: 10.1097/PAS.0000000000001141.

Abstract

Lynch syndrome (LS) is defined by germline mutations in DNA mismatch repair (MMR) genes, and affected patients are at high risk for multiple cancers. Reflexive testing for MMR protein loss by immunohistochemistry (IHC) is currently only recommended for colorectal and endometrial cancers, although upper tract urothelial carcinoma (UTUC) is the third-most common malignancy in patients with LS. To study the suitability of universal MMR IHC screening for UTUC, we investigated MMR expression and microsatellite status in UTUC in comparison to bladder UC (BUC), and evaluated the clinicopathologic features of UTUC. We found that 9% of UTUC showed MMR IHC loss (8 MSH6 alone; 1 MSH2 and MSH6; 1 MLH1 and PMS2; n=117) compared with 1% of BUC (1 MSH6 alone; n=160) (P=0.001). Of these, 4/10 (40%) of UTUC (3% overall; 3 MSH6 alone; 1 MLH1 and PMS2) and none (0%) of BUC had high microsatellite instability on molecular testing (P=0.03). The only predictive clinicopathologic feature for MMR loss was a personal history of colorectal cancer (P=0.0003). However, UTUC presents at a similar age to colon carcinoma in LS and thus UTUC may be the sentinel event in some patients. Combining our results with those of other studies suggests that 1% to 3% of all UTUC cases may represent LS-associated carcinoma. LS accounts for 2% to 6% of both colorectal and endometrial cancers. As LS likely accounts for a similar percentage of UTUC, we suggest that reflexive MMR IHC screening followed by microsatellite instability testing be included in diagnostic guidelines for all UTUC.

摘要

林奇综合征 (LS) 由 DNA 错配修复 (MMR) 基因的种系突变定义,受影响的患者患多种癌症的风险很高。目前仅推荐对结直肠癌和子宫内膜癌进行免疫组织化学 (IHC) 反射性检测 MMR 蛋白缺失,尽管上尿路上皮癌 (UTUC) 是 LS 患者的第三大常见恶性肿瘤。为了研究 UTUC 普遍进行 MMR IHC 筛查的适用性,我们研究了 UTUC 与膀胱癌 (BUC) 相比的 MMR 表达和微卫星状态,并评估了 UTUC 的临床病理特征。我们发现,9%的 UTUC 显示 MMR IHC 缺失 (8 个 MSH6 单独缺失;1 个 MSH2 和 MSH6 缺失;1 个 MLH1 和 PMS2 缺失;n=117),而 1%的 BUC 显示 MMR IHC 缺失 (1 个 MSH6 单独缺失;n=160) (P=0.001)。在这些患者中,4/10(40%)的 UTUC(3%总体;3 个 MSH6 单独缺失;1 个 MLH1 和 PMS2 缺失)和 0%的 BUC(0%)的分子检测显示高度微卫星不稳定性 (P=0.03)。唯一可预测 MMR 缺失的临床病理特征是结直肠癌的个人史 (P=0.0003)。然而,LS 中的 UTUC 与结肠癌的发病年龄相似,因此 UTUC 可能是某些患者的首发事件。将我们的结果与其他研究的结果相结合表明,所有 UTUC 病例中可能有 1%至 3%是 LS 相关的癌。LS 占结直肠癌和子宫内膜癌的 2%至 6%。由于 LS 可能占 UTUC 的相似比例,我们建议将 MMR IHC 反射性筛查与微卫星不稳定性检测纳入所有 UTUC 的诊断指南。

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