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首页> 外文期刊>Human Pathology >Optimal protocol for PTEN immunostaining; Role of analytical and preanalytical variables in PTEN staining in normal and neoplastic endometrial, breast, and prostatic tissues
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Optimal protocol for PTEN immunostaining; Role of analytical and preanalytical variables in PTEN staining in normal and neoplastic endometrial, breast, and prostatic tissues

机译:PTEN免疫染色的最佳方案;分析和分析前变量在正常和赘生性子宫内膜,乳腺和前列腺组织中PTEN染色中的作用

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摘要

In some tumors, phosphatase and tensin homolog (PTEN) inactivation may have prognostic importance and predictive value for targeted therapies. Immunohistochemistry (IHC) may be an effective method to demonstrate PTEN loss. It was claimed that PTEN IHC showed poor reproducibility, lack of standardization, and variable effects of preanalytical factors. In this study, we developed an optimal protocol for PTEN IHC, with clone 6H2.1, by checking the relevance of analytical variables in normal tissue and tumors of endometrium, breast, and prostate. Pattern and intensity of cellular staining and background nonspecific staining were quantified and subjected to statistical analysis by linear mixed models. The proposed protocol showed a statistically best performance (P <.05) and included a high target retrieval solution, 1:100 primary antibody dilution (2.925 mg/L), FLEX diluent, and EnVisionFLEX+ detection method, with a sensitivity and specificity of 72.33% and 78.57%, respectively. Staining specificity was confirmed in cell lines and animal models. Endometrial carcinomas with PTEN genetic abnormalities showed statistically lower staining than tumors without alterations (mean histoscores, 34.66 and 119.28, respectively; P =.01). Controlled preanalytical factors (delayed fixation and overfixation) did not show any statistically significant effect on staining with optimal protocol (P >.001). However, there was a trend of significance for decreased staining and fixation under high temperature. Moreover, staining was better in endometrial aspirates than in matched hysterectomy specimens, subjected to less controlled preanalytical variables (mean histoscores, 80 and 40, respectively; P =.002). A scoring system combining intensity of staining and percentage of positive cells was statistically associated with PTEN alterations (P =.01).
机译:在某些肿瘤中,磷酸酶和张力蛋白同源物(PTEN)的失活对于靶向治疗可能具有预后的重要性和预测价值。免疫组织化学(IHC)可能是证明PTEN丢失的有效方法。据称,PTEN IHC显示出差的可重复性,缺乏标准化和分析前因素的可变影响。在这项研究中,我们通过检查正常组织和子宫内膜,乳腺和前列腺肿瘤中分析变量的相关性,为克隆6H2.1开发了PTEN IHC的最佳方案。对细胞染色和背景非特异性染色的模式和强度进行定量,并通过线性混合模型进行统计分析。拟议的方案显示出统计学上的最佳性能(P <.05),包括高靶标检索溶液,1:100一级抗体稀释液(2.925 mg / L),FLEX稀释剂和EnVisionFLEX +检测方法,灵敏度和特异性为72.33。 %和78.57%。在细胞系和动物模型中证实了染色特异性。具有PTEN基因异常的子宫内膜癌的染色明显低于未发生改变的肿瘤(平均组织分数分别为34.66和119.28; P = 0.01)。分析前的受控因素(延迟固定和过度固定)对最佳方案的染色无统计学意义(P> .001)。但是,存在减少高温下的染色和固着的重要趋势。此外,子宫内膜抽吸物的染色效果要好于匹配的子宫切除术标本,且其分析前控制变量较少(平均组织分数分别为80和40; P = .002)。结合染色强度和阳性细胞百分比的评分系统与PTEN改变在统计学上相关(P = .01)。

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