TNM：第九版胸部肿瘤学诞生了！

Q4 Medicine

Revue des Maladies Respiratoires Actualites Pub Date : 2024-10-01 DOI:10.1016/S1877-1203(24)00075-2

A. Agrafiotis , B. Grigoriu , P. Van Schil

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引用次数: 0

摘要

第九版肺癌 TNM 是基于一个包含 124,581 个病例的数据库，其中 18.9% 的病例是前瞻性输入的。由于第 8 版的描述指标在新数据库中表现良好，因此没有对 T 部分进行修改。关于 N 部分，N2 被细分为 N2a 和 N2b，分别代表单站和多站 N2 受累。每个站的单个淋巴结不计算在内。关于 M 部分，当单一器官系统或多个器官系统出现多个胸腔外转移灶时，M1c 又可细分为 M1c1 和 M1c2。骨骼和肌肉算作一个器官系统。特别是新的 N 描述符对整个分期分组产生了影响，例如 T1N1 属于 IIA 期，T1N2a 属于 IIB 期。M1c1 和 M1c2 都属于 IVB 期。关于胸腺上皮肿瘤（包括胸腺瘤和胸腺癌）的分期，第 9 版是基于对 9 147 个病例的分析。仅对 T 部分进行了修改：T1a 表示 5 厘米以下的肿瘤，T1b 表示最大尺寸超过 5 厘米的肿瘤。T2 表示部分或全厚心包侵犯，也可直接侵犯肺实质或膈神经。纵隔胸膜受侵现在作为额外的组织学描述指标单独考虑。关于胸膜间皮瘤，在对 3,481 个病例的数据库进行分析后，建议对临床 T 描述因子进行重要修改，而对 N 和 M 描述因子不做修改。现在，胸膜最大厚度在轴向 CT 切片的 3 个层面进行测量：胸部上部、中部和下部，并将 3 个测量值相加（Psum）。在矢状面图像上，裂隙中的最大胸膜厚度测量值为 Fmax。Psum 的临界值为 12 和 30 毫米，Fmax 的临界值为 5 毫米。这将最终确定具体的 T 类。对于病理学家来说，不可能对切除的标本进行完全相同的测量，因此，只对临床分期分组进行了重新定义，而病理分期分组没有任何变化。1877-1203/© 2024 splf.由 Elsevier Masson SAS 出版。保留所有权利。

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Le TNM : la 9e édition pour l’oncologie thoracique est née !

The 9^th TNM edition for lung cancer is based on a database of 124,581 cases, of which 18.9% were entered prospectively. Regarding the T component no changes are implemented as the 8^th edition descriptors performed well in the new database. Concerning the N component, N2 is subdivided into N2a and N2b representing single station and multiple stations N2 involvement, respectively. Individual lymph nodes in each station are not counted. With regard to the M component, M1c is subdivided into M1c1 and M1c2 when multiple extrathoracic metastases are present in a single organ system or multiple organ systems, respectively. Bone and muscle are counted as a single organ system. Especially the new N descriptors have an impact on the overall stage groupings, whereby e.g. T1N1 belongs to stage IIA and T1N2a to stage IIB. M1c1 and M1c2 both belong to stage IVB. For staging of thymic epithelial tumours comprising thymoma and thymic carcinoma, the 9^th edition is based on analysis of 9,147 cases. Changes are only proposed in the T component: T1a characterizes tumors until 5 cm and T1b tumors larger than 5 cm in greatest dimension. T2 denotes partial or full-thickness pericardial invasion but also direct invasion into lung parenchyma or phrenic nerve. Invasion of mediastinal pleura is now separately considered as additional histologic descriptor. There are no changes in the stage groupings with both T1a and T1b belonging to stage I.

Regarding pleural mesothelioma, after analysis of a database of 3,481 cases, important changes are proposed for the clinical T descriptors and no changes are implemented for the N and M descriptors. Maximal pleural thickness is now measured at 3 levels on axial CT slices: at upper, middle and lower chest and a sum of the 3 measurements is made (Psum). On a sagittal image maximal pleural thickness in the fissure is measured as Fmax. Cut-off values for Psum are 12 and 30 mm, and for Fmax 5 mm. These will finally determine the specific T-category. For a pathologist it is not possible to perform exactly the same measurements on a resected specimen and for this reason, only the clinical stage groupings were redefined without any changes in the pathological stage groupings. 1877-1203/© 2024 SPLF. Published by Elsevier Masson SAS. All rights reserved.

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来源期刊

Revue des Maladies Respiratoires Actualites Medicine-Pulmonary and Respiratory Medicine

CiteScore

0.10

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0.00%

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671