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Immunohistochemical analysis of c-myc, c-jun and estrogen receptor in normal, hyperplastic and neoplastic endometrium

机译:正常,增生和赘生性子宫内膜中c-myc,c-jun和雌激素受体的免疫组织化学分析

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To evaluate the role of c-jun and c-myc proto-oncogenes in normal, hyperplastic and neoplastic endometrium in relation to estrogen receptor (ER) status and to investigate whether these genes can be related to other histopathological features of endometrial carcinoma, 32 endometrial carcinomas, 38 endometrial hyperplasias and 22 cyclic endometria (10 proliferative and 12 secretory) were evaluated histologically. Endometrial hyperplasia cases were classified as simple and complex hyperplasia without atypia, and atypical hyperplasia. Endometrial carcinoma cases were subtyped according to the International Society of Gynecological Pathologists. Modified FIGO system was used for both grading and staging. Immunohistochemical examination was performed using antibodies to ER-alpha, c-myc and c-jun with streptavidin-biotin-peroxidase technique. The mean percentage of ER-alpha positive cells changed cyclically during the menstrual cycle, and it was the highest (96%) and the lowest (31.6%) in proliferative and carcinomatous endometrium, respectively. There was a statistically significant difference between proliferative and secretory phases and proliferative and carcinomatous endometrium in relation to ER-alpha staining (p0.05). There was also a statistically significant difference with respect to ER-alpha reactivity between secretory phase and each hyperplastic group, as well as between the carcinoma group and each hyperplastic group (p0.05). Although not significant, the mean percentage of c-myc expressing cells in the carcinoma group was higher (15.3%) than that of proliferative phase and hyperplastic groups. The mean percentage of c-jun positive cells in proliferative endometrium was slightly higher than in secretory endometrium, and it was the highest in atypical hyperplastic endometrium (28.3%), but there was no statistically significant difference between the groups. In carcinoma cases, a positive correlation was observed between c-jun positivity and tumor grade (p=0.027, r=0.3908), but such a correlation with c-myc was not found. A positive correlation was detected between ER-alpha and c-myc expression (p=0.038, r=0.3686). A progressive loss of ER seems to be correlated with increasing malignant transformation. C-myc expression might play a role in the development of endometrial carcinoma via ER. The association between c-jun and ER appears to be lost in endometrial carcinoma. The relationship between c-myc, c-jun and ER appears to be altered in endometrial carcinoma compared to that of menstrual endometrium.
机译:评估c-jun和c-myc原癌基因在正常,增生和赘生性子宫内膜中与雌激素受体(ER)状态相关的作用,并研究这些基因是否可能与子宫内膜癌,32子宫内膜癌的其他组织病理学特征相关组织学评估了癌,38例子宫内膜增生和22例环状子宫内膜增生和12个分泌性增生。子宫内膜增生病例分为无异型的单纯性和复杂性增生以及非典型性增生。根据国际妇科病理学家学会将子宫内膜癌病例亚型化。修改后的FIGO系统用于分级和分段。使用链霉亲和素-生物素-过氧化物酶技术,使用抗ER-α,c-myc和c-jun的抗体进行免疫组织化学检查。 ER-α阳性细胞的平均百分比在月经周期中呈周期性变化,在增生和癌内膜中分别最高(96%)和最低(31.6%)。与ER-α染色有关,增殖期和分泌期与增殖期和癌性子宫内膜之间存在统计学上的显着差异(p <0.05)。在分泌期与每个增生组之间以及癌组与每个增生组之间,ER-α反应性也有统计学上的显着差异(p <0.05)。尽管不显着,但癌组中c-myc表达细胞的平均百分比高于增生期和增生组的平均百分比(15.3%)。增生性子宫内膜中c-jun阳性细胞的平均百分比略高于分泌性子宫内膜,在非典型增生性子宫内膜中平均最高(28.3%),但两组之间无统计学差异。在癌病例中,观察到c-jun阳性与肿瘤分级呈正相关(p = 0.027,r = 0.3908),但未发现与c-myc呈正相关。在ER-alpha和c-myc表达之间检测到正相关(p = 0.038,r = 0.3686)。 ER的逐渐丧失似乎与恶性转化的增加有关。 C-myc表达可能通过ER在子宫内膜癌的发生中起作用。在子宫内膜癌中,c-jun和ER之间的联系似乎消失了。与月经子宫内膜相比,子宫内膜癌中c-myc,c-jun和ER之间的关系似乎有所改变。

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