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乳腺癌中的DNA倍体、增殖及神经癌基因蛋白过表达

DNA ploidy, proliferation, and neu-oncogene protein overexpression in breast carcinoma.

作者信息

Lee A K, Wiley B, Loda M, Bosari S, Dugan J M, Hamilton W, Heatley G J, Cook L, Silverman M L

机构信息

Department of Anatomic Pathology, Lahey Clinic Medical Center, Burlington, Massachusetts.

出版信息

Mod Pathol. 1992 Jan;5(1):61-7.

PMID:1347424
Abstract

DNA content, proliferative activity (Ki-67 immuno-staining and S-phase fraction by flow cytometry), and neu-oncogene overexpression were studied in 135 patients with invasive breast carcinoma. Image analysis and flow cytometry of fresh tumors showed good correlation between the two methods and yielded 39% diploid tumors and 61% aneuploid tumors. Aneuploidy, including tetraploidy, was significantly related to the loss of estrogen (p = 0.0002) and progesterone (p = 0.03) receptors, high histologic (p = 0.014) and nuclear (p less than 0.0001) grades, and mitotic rate (p = 0.0001). Immunohistochemical evaluation of proliferation by staining with Ki-67 monoclonal antibody and of neu-oncogene protein overexpression was performed in fresh frozen tissue from 83 tumors. The Ki-67 score, quantitated by the CAS-200 image analyzer, correlated only moderately with S-phase fraction obtained by flow cytometry by linear regression analysis (r = 0.39, p less than 0.001). However, both of these proliferation markers correlated strongly with the mitotic rate (p less than 0.0001). Aneuploid and tetraploid tumors demonstrated higher Ki-67 scores and S-phase fractions than diploid tumors. Neu-oncogene protein overexpression was seen in 24 tumors (29%) overall and was much higher in aneuploid tumors (38%) and tetraploid tumors (50%) than in diploid tumors (7%). However, the concentration of neu-oncogene protein positive tumors in the tetraploid region reported by others was not observed. Neu-oncogene protein overexpression was also associated with higher Ki-67 scores (p = 0.016) and S-phase fractions (p = 0.037).(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

对135例浸润性乳腺癌患者的DNA含量、增殖活性(Ki-67免疫染色及流式细胞术检测S期细胞比例)和neu癌基因过表达情况进行了研究。对新鲜肿瘤组织进行图像分析和流式细胞术检测,结果显示两种方法具有良好的相关性,其中二倍体肿瘤占39%,非整倍体肿瘤占61%。非整倍体(包括四倍体)与雌激素(p = 0.0002)和孕激素(p = 0.03)受体缺失、高组织学分级(p = 0.014)、高核分级(p < 0.0001)及有丝分裂率(p = 0.0001)显著相关。采用Ki-67单克隆抗体染色对83例肿瘤的新鲜冰冻组织进行增殖的免疫组化评估,并检测neu癌基因蛋白过表达情况。通过CAS-200图像分析仪对Ki-67评分进行定量,经线性回归分析,其与流式细胞术检测的S期细胞比例仅呈中度相关(r = 0.39,p < 0.001)。然而,这两种增殖标志物均与有丝分裂率密切相关(p < 0.0001)。非整倍体和四倍体肿瘤的Ki-67评分及S期细胞比例均高于二倍体肿瘤。总体上,24例肿瘤(29%)出现neu癌基因蛋白过表达,非整倍体肿瘤(38%)和四倍体肿瘤(50%)中的过表达率远高于二倍体肿瘤(7%)。然而,未观察到其他人报道的四倍体区域neu癌基因蛋白阳性肿瘤的浓度情况。neu癌基因蛋白过表达还与较高的Ki-67评分(p = 0.016)和S期细胞比例(p = 0.037)相关。(摘要截稿于250词)

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