首页> 外文期刊>Diagnostic cytopathology >Expression of Ki-67 and p27(Kip1) in fine-needle aspirates from breast carcinoma and benign breast diseases.
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Expression of Ki-67 and p27(Kip1) in fine-needle aspirates from breast carcinoma and benign breast diseases.

机译:Ki-67和p27(Kip1)在乳腺癌和良性乳腺疾病的细针抽吸物中的表达。

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摘要

Cell atypia in breast fine needle aspiration (FNA) can introduce some diagnostic difficulties. Molecules reflecting proliferative cell potential, such as Ki-67 and p27(Kip1) , can help in recognizing the true biological nature of a cell. Thus, the objective of the study was to analyze the difference in Ki-67 and p27(Kip1) cell immunoexpression in breast FNA specimens between fibroadenomas, fibrocystic changes (FCC) with atypia, and breast carcinoma. Microscopic analyses of cell cytomorphology and Ki-67 and p27(Kip1) breast cell immunoexpression were done after standard Pappenheim and immunocytochemical staining (labeled streptavidin-biotin, LSAB) method in autostainer DakoCytomation TechMate. The study included 50 patients with breast carcinoma, 20 patients with fibroadenoma, and 20 patients with FCC with atypia. High Ki-67 and low or absent p27(Kip1) were found in most patients with breast carcinoma, while majority of FCC with atypia were characterized by low Ki-67 and moderate to high p27(Kip1) cell immunoexpression. Majority of fibroadenomas were associated with low Ki-67 and low to moderate p27(Kip1) cell immunoexpression indicating progressive decrease in cell cycle inhibition, but still not so high proliferative activity as in carcinoma. However, although statistically significant difference for Ki-67 and p27(Kip1) was found between breast lesions in our study, the large ranges observed for each marker make them essentially useless for better cytological diagnosis in a single case. Regarding their opposite role in cell cycle, inverse correlation of Ki-67 and p27(Kip1) was noticed. Poorly differentiated carcinoma cells had mostly high Ki-67 and low p27(Kip1) cell immunoexpression.
机译:乳腺细针穿刺术(FNA)中的细胞异型性会带来一些诊断困难。反映增殖细胞潜力的分子,例如Ki-67和p27(Kip1),可以帮助识别细胞的真正生物学性质。因此,本研究的目的是分析乳腺FNA标本中Ki-67和p27(Kip1)细胞免疫表达在纤维腺瘤,非典型性纤维囊变(FCC)和乳腺癌之间的差异。在自动染色机DakoCytomation TechMate中使用标准的Pappenheim和免疫细胞化学染色(标记为抗生蛋白链菌素-生物素,LSAB)方法后,进行了细胞形态学和Ki-67和p27(Kip1)乳腺癌细胞免疫表达的显微镜分析。该研究包括50例乳腺癌患者,20例纤维腺瘤患者和20例非典型性FCC患者。在大多数乳腺癌患者中发现高Ki-67和低或不存在p27(Kip1),而大多数非典型性FCC的特征是低Ki-67和中至高p27(Kip1)细胞免疫表达。大多数纤维腺瘤与低Ki-67和低至中度的p27(Kip1)细胞免疫表达有关,表明细胞周期抑制作用逐渐降低,但仍不像癌组织那样高。但是,尽管在我们的研究中发现乳腺病变之间Ki-67和p27(Kip1)在统计学上有显着差异,但是观察到的每种标记物的较大范围实际上使它们在单个病例中无法用于更好的细胞学诊断。关于它们在细胞周期中的相反作用,注意到Ki-67和p27(Kip1)呈负相关。分化较差的癌细胞大多具有较高的Ki-67和较低的p27(Kip1)细胞免疫表达。

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