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TERT 启动子突变分析作为辅助诊断工具在具有诊断挑战性的黑素细胞肿瘤中的应用。

TERT Promoter Mutational Analysis as an Ancillary Diagnostic Tool for Diagnostically Challenging Melanocytic Neoplasms.

机构信息

Department of Dermatology, Feinberg School of Medicine, Northwestern University, Chicago, IL; and.

Department of Molecular Pathology, Feinberg School of Medicine, Northwestern University, Chicago, IL.

出版信息

Am J Dermatopathol. 2023 May 1;45(5):289-299. doi: 10.1097/DAD.0000000000002366. Epub 2023 Feb 17.

Abstract

Telomerase reverse transcriptase promoter mutations (TPMs) have been shown to be common in melanoma and uncommon in benign nevi. To assess the use of TPMs as an ancillary diagnostic tool, we report the concordance of the TPM status with the final diagnosis in clinical cases with distinct differential diagnostic scenarios: dysplastic nevus versus melanoma, atypical Spitz nevus versus melanoma, atypical deep penetrating nevus (DPN) versus melanoma, and atypical blue nevus versus malignant blue nevus. In a control cohort, we found a positive TPM in 51/70 (73%) of the total melanomas with the highest frequency in vertical growth phase melanoma cases. Conversely, only 2/35 (6%) dysplastic nevi in our control cases were TPM-positive and b were severely atypical dysplastic nevi. Our clinical cohort of 257 cases had a positive TPM in 24% of cases diagnosed as melanoma and in 1% of cases with a benign diagnosis. The overall concordance of the TPM status with the final diagnosis was 86%. The TPM status had the greatest concordance (95%) with the final diagnosis in the atypical DPN versus melanoma group, with the rest of the groups ranging between 50% and 88%. Overall, our results suggest that TPMs are most useful in the differential diagnosis of atypical DPN versus melanoma. It also has some value in the differential diagnosis of atypical Spitz tumor versus melanoma and dysplastic nevus versus melanoma, whereas in our cohort, it did not contribute meaningfully to differentiating malignant blue nevus and atypical blue nevus.

摘要

端粒酶逆转录酶启动子突变(TPMs)在黑色素瘤中很常见,在良性痣中则很少见。为了评估 TPMs 作为辅助诊断工具的用途,我们报告了在具有明确鉴别诊断情况的临床病例中 TPM 状态与最终诊断的一致性:发育不良痣与黑色素瘤、非典型 Spitz 痣与黑色素瘤、非典型深部穿透痣(DPN)与黑色素瘤和非典型蓝痣与恶性蓝痣。在对照队列中,我们在总共 70 例黑色素瘤中有 51 例(73%)发现 TPM 阳性,其中垂直生长阶段黑色素瘤病例的阳性率最高。相反,在我们的对照病例中,只有 2/35(6%)发育不良痣为 TPM 阳性,且为严重非典型发育不良痣。在我们的 257 例临床病例中,24%的黑色素瘤诊断和 1%的良性诊断病例 TPM 阳性。TPM 状态与最终诊断的总体一致性为 86%。TPM 状态与非典型 DPN 与黑色素瘤组的最终诊断具有最高的一致性(95%),其余组的一致性在 50%至 88%之间。总体而言,我们的结果表明,TPMs 在非典型 DPN 与黑色素瘤的鉴别诊断中最有用。它在非典型 Spitz 肿瘤与黑色素瘤和发育不良痣与黑色素瘤的鉴别诊断中也具有一定价值,而在我们的队列中,它对区分恶性蓝痣和非典型蓝痣没有明显意义。

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