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第 8 版 TNM 分期及其对皮肤癌的影响:英国皮肤科医师协会和英国皇家病理学院的综述

The new 8th edition of TNM staging and its implications for skin cancer: a review by the British Association of Dermatologists and the Royal College of Pathologists, U.K.

机构信息

Portsmouth Hospitals NHS Trust, Portsmouth, U.K.

University of Dundee, Dundee, U.K.

出版信息

Br J Dermatol. 2018 Oct;179(4):824-828. doi: 10.1111/bjd.16892. Epub 2018 Sep 5.

DOI:10.1111/bjd.16892
PMID:29923189
Abstract

The 8th edition of TNM (tumour, node and metastasis) has numerous and important changes compared with the 7th edition. Public Health England and the Royal College of Pathologists, U.K., have adopted the 8th edition of TNM (TNM8) published by the Union for International Cancer Control for skin cancer staging. These changes will have an impact on the management and commissioning of melanoma and nonmelanoma skin cancer (NMSC). The T1-T3 categories for NMSC staging require the clinician to measure the maximum dimension (usually diameter) of every potential invasive cancer. For squamous, basal and adnexal carcinomas, but not Merkel cell carcinoma (MCC), the T1-T3 categories are defined by new 20-mm and 40-mm divisions based on the maximum dimension of the lesion. In addition, new risk factors upstage T1 or T2 to T3. For melanoma, mitotic index no longer influences separation of pathological stage (pT1). There is a new, additional stratification level at 0·8-mm Breslow thickness. Subdivision pT1b, with a negative sentinel lymph node biopsy (SLNB) of pN0, is now stage IA compared with the previous IB. For MCC, SLNB is now included specifically in the pN staging system. The pT1 subdivision requires clinical information as to whether histologically involved nodes were clinically occult or detectable. For both melanoma and MCC the clinician must state whether the lymph nodes are occult or clinically detectable. Eyelid carcinoma continues to have a staging system different from that in general skin and the system is substantially revised in TNM8.

摘要

第八版 TNM(肿瘤、淋巴结和转移)与第七版相比有许多重要的变化。英国公共卫生署和皇家病理学家学院采用了国际癌症控制联盟发布的第八版 TNM(TNM8)用于皮肤癌分期。这些变化将对黑色素瘤和非黑色素瘤皮肤癌(NMSC)的管理和委托产生影响。NMSC 分期的 T1-T3 类别要求临床医生测量每一个潜在侵袭性癌症的最大尺寸(通常是直径)。对于鳞状细胞癌、基底细胞癌和附属器癌,但不包括 Merkel 细胞癌(MCC),T1-T3 类别是根据病变的最大尺寸用新的 20mm 和 40mm 划分来定义的。此外,新的危险因素将 T1 或 T2 升级为 T3。对于黑色素瘤,有丝分裂指数不再影响病理分期(pT1)的分离。在 0.8mm Breslow 厚度处增加了一个新的、额外的分层级别。pT1b 亚组,伴阴性前哨淋巴结活检(SLNB)的 pN0,现在是 IA 期,而不是以前的 IB 期。对于 MCC,SLNB 现在专门包含在 pN 分期系统中。pT1 亚组需要临床信息,以确定组织学上受累的淋巴结是临床隐匿性的还是可检测的。对于黑色素瘤和 MCC,临床医生必须说明淋巴结是隐匿性的还是临床上可检测的。眼睑癌的分期系统仍然与一般皮肤的分期系统不同,在 TNM8 中进行了实质性修订。

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