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Utility of Ki-67, p53, Bcl-2, and Cox-2 biomarkers for low-grade endometrial cancer and disordered proliferative/benign hyperplastic endometrium by imprint cytology

机译:Ki-67,p53,Bcl-2和Cox-2生物标志物通过印迹细胞学在低度子宫内膜癌和增生/良性增生性子宫内膜失调中的应用

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In this report, the authors examined the characteristic features of morphology and molecular biology of Ki-67, p53, Bcl-2, and cyclooxygenase-2 (Cox-2) immunocytochemistry in low-grade endometrioid endometrial carcinoma (LG-ENEC) and disordered proliferative (DP)/benign hyperplastic (BH) endometrium. We carried out a prospective study by collecting endometrial imprints from freshly resected uteri over a 20-month period and finally 104 patients were evaluated with endometrial cytology. We focused on LG-ENECs, as well as on BH endometrium and its precursor lesion, DP endometrium, firstly because of the overlapping cytomorphology of these pathologic entities and secondly because of the lack of agreement in the differential diagnosis of atypical hyperplasia from complex hyperplasia and well-differentiated endometrial carcinoma, even in curettage specimens. Ki-67 expression of LG-ENEC showed predominance in comparison with DP/BH endometrium. Furthermore, high levels of Bcl-2 (>50%) were expressed only in DP/BH endometrium. DP/BH endometrium was negative for p53 marker, except from two cases of BH endometrium. Cox-2 expression ≥50% was found only in LG-ENECs. Using Ki-67, Bcl-2, p53, and Cox-2 markers, we managed to distinguish fully DP/BH endometrium from LG-ENEC. Higher Ki-67%/Bcl-2% rate and also higher Cox-2 expression were found in LG-ENEC cases with FIGO stage ≥ IC, than in cases with FIGO stage < IC. The immunocytochemical findings from a combination of Ki-67, p53, Bcl-2, and Cox-2, may differentiate LG-ENEC from DP/BH endometrium with overlapping cytomorphology. Immunocytochemistry appeared to be useful also for the correlation between LG-ENEC and FIGO stage.
机译:在本报告中,作者研究了低度子宫内膜样子宫内膜癌(LG-ENEC)和疾病紊乱的Ki-67,p53,Bcl-2和环氧合酶2(Cox-2)免疫细胞化学的形态学和分子生物学特征。增生(DP)/良性增生(BH)子宫内膜。我们通过收集20个月内刚切除的子宫的子宫内膜印记进行了一项前瞻性研究,最后对104例患者进行了子宫内膜细胞学评估。我们关注LG-ENECs以及BH子宫内膜及其前体病变DP子宫内膜,首先是因为这些病理实体的细胞形态重叠,其次是因为在复杂性增生和非典型增生的鉴别诊断中缺乏共识高分化子宫内膜癌,即使在刮宫标本中也是如此。与DP / BH子宫内膜相比,LG-ENEC的Ki-67表达占优势。此外,仅在DP / BH子宫内膜中表达高水平的Bcl-2(> 50%)。除2例BH子宫内膜病例外,DP / BH子宫内膜p53标记阴性。仅在LG-ENEC中发现Cox-2表达≥50%。使用Ki-67,Bcl-2,p53和Cox-2标记,我们设法将DP / BH子宫内膜与LG-ENEC完全区分开。在FIGO期≥IC的LG-ENEC病例中,与FIGO期

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