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Use of different fixation times and application of two immunohistochemical methods for detection of KIT and Ki67 proteins in canine cutaneous mast cell tumors

机译:使用不同的固定时间和应用两种免疫组化方法检测犬皮肤肿瘤细胞瘤中的试剂盒和KI67蛋白

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摘要

ABSTRACT: Due to the high prevalence of mast cell tumors (MCTs) in the diagnostic routine, several factors, especially prognostic, have been sought to determine the biological behavior of these neoplasms. Immunohistochemistry (IHC) is one of the main tools utilized to biologically differentiate more aggressive tumors from less aggressive ones. However, some immunostainings are influenced by formalin fixation, interfering with the results. This is both a retrospective and prospective study of MCTs diagnosed in laboratory routine. A total of 25 samples, without knowledge about fixation time, were analyzed in the retrospective study, whereas 12 samples, with known fixation times, were assessed in the prospective study. Two histologic grading systems (Patnaik and Kiupel), special staining of toluidine blue, and IHC for KIT and Ki67 proteins were applied in both studies. Additionally, two amplification systems (biotinylated and non-biotinylated) for Ki67 protein and counting of the argyrophilic nucleolar organizing regions (AgNOR method) were tested in the prospective study. In the retrospective study, greater agreement between the evaluating pathologists was observed when the Kiupel system was used. IHC staining for KIT protein was effective in both studies, regardless of fixation time. IHC staining for Ki67 protein was highly sensitive to formaldehyde, and staining failure was observed in 56% of the cases in the retrospective study. In the prospective study, samples fixed for longer than 24 hours showed a reduction in the number of stained cells (altering the determination of the cell growth fraction) or showed absence of IHC staining in both amplification systems. The use of the AgNOR method to evaluate the rate of cell proliferation may be an alternative when the fixation time of the neoplasm is unknown or longer than 24 hours.
机译:摘要:由于施用常规中肥大细胞肿瘤(MCT)的高患病率,已经寻求几个因素,特别是预后,确定这些肿瘤的生物学行为。免疫组织化学(IHC)是用于生物学上不同于侵略性的侵袭性肿瘤的主要工具之一。然而,一些免疫抑制受福尔马林固定的影响,干扰结果。这是诊断在实验室常规中的MCT的回顾性和前瞻性研究。在回顾性研究中分析了总共25个样品,没有关于固定时间的知识,而在前瞻性研究中评估了12个样品,具有已知的固定时间。两种组织学分级系统(PATNAIK和KIUPEL),甲苯胺蓝的特殊染色和胰蛋白质的IHC和KI67蛋白质应用。另外,在前瞻性研究中测试了用于KI67蛋白的两个扩增系统(生物素化和非生物素化),以及艾滋病毒核仁组织区(Agnor方法)的计数。在回顾性研究中,当使用Kiupel系统时,观察到评估病理学家之间的更大协议。无论固定时间如何,IHC染色在两项研究中都有效。对于Ki67蛋白的IHC染色对甲醛高度敏感,并且在回顾性研究的56%的病例中观察到染色衰竭。在前瞻性研究中,固定的样品超过24小时显示染色细胞数量的减少(改变细胞生长级分的测定)或显示在两个扩增系统中没有IHC染色。当肿瘤的固定时间未知或长于24小时时,使用Agnor方法可以是替代的替代方案。

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