软组织肉瘤的预后因素。组织微阵列免疫染色,全肿瘤切片的重要性和时间依赖性。

Jacob Engellau
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引用次数: 0

摘要

在四肢和躯干壁的成人软组织肉瘤(STS)中,需要改善预后因素来识别转移高危患者。目前使用的许多预后系统包括各种因素,生物标志物的免疫组织化学(IHC)表达的预后价值尚不清楚。用于分析Ki-67生物标志物免疫组织化学表达的组织保存、高通量组织微阵列(TMA)技术已被验证,并发现其结果与传统染色方法相当。采用TMA法研究了218例恶性纤维组织细胞瘤(MFH)和140例混合型STS中多种标志物(Ki-67、p53、细胞周期蛋白A、bcl-2、β -连环蛋白、CD44和Pgp)的IHC表达。在MFH系列中,肿瘤大小和Ki-67作为唯一的IHC标志物,提供了独立的预后信息。在混合STS系列中,采用全肿瘤切片,并在肿瘤周围生长区进行TMA。全肿瘤切片有助于评估转移血管侵犯的强独立预后因素,风险比(HR) 3.5,肿瘤坏死(HR 2.8)和肿瘤生长模式(HR 3.2),后者也与局部复发(LR)相关。相比之下,组织学恶性分级、肿瘤大小和深度并没有独立的预后价值。当从肿瘤周围生长区进行TMA时,Ki-67 (HR 1.9)、β -连环蛋白(HR 2.7)、CD44 (HR 2.1)和Pgp (HR 2.4)的IHC表达是独立的预后因素。最后,发现预后因素具有时间依赖性,大多数在2年后失去了其预后价值,而无论何时发生转移,LR都是一个强有力的预后因素。
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Prognostic factors in soft tissue sarcoma. Tissue microarray for immunostaining, the importance of whole-tumor sections and time-dependence.

In adult soft tissue sarcoma (STS) of the extremities and trunk wall, improved prognostic factors are needed to identify patients at high-risk for metastasis. Various factors are included in the many prognostic systems currently in use and the prognostic value of immunohistochemical (IHC) expression of biological markers is unclear. The tissue-preserving, high throughput tissue microarray (TMA) technique for analysis of immunohistochemical expression of biological markers was validated for Ki-67, and was found to yield results comparable to conventional staining methods. TMA was used to study the IHC expression of multiple markers (Ki-67, p53, cyclin A, bcl-2, beta-catenin, CD44, and Pgp) in 218 malignant fibrous histiocytomas (MFH) and in 140 mixed STS. In the MFH series, tumor size and Ki-67, as the only IHC marker, provided independent prognostic information. In the mixed STS series whole-tumor sections were used and TMA was performed in the peripheral tumor growth zone. Whole-tumor sections facilitated assessment of the strong independent prognostic factors for metastasis vascular invasion, hazard ratio (HR) 3.5, tumor necrosis (HR 2.8), and tumor growth pattern (HR 3.2), and the latter also correlated with local recurrence (LR). In comparison, histological malignancy grade, tumor size, and depth were not of independent prognostic value. When TMA was performed from the peripheral tumor growth zone, the IHC expression of Ki-67 (HR 1.9), beta-catenin (HR 2.7), CD44 (HR 2.1) and Pgp (HR 2.4) were independent prognostic factors. Finally, prognostic factors were found to be time-dependent, and most had lost their prognostic value after 2 years, whereas LR was a strong prognostic factor for metastasis whenever it occurred.

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