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正常及新生期经雌激素处理的小鼠子宫和阴道中表皮生长因子(EGF)及其受体以及C-fos原癌基因表达和雌激素依赖性的免疫组织化学研究

Immunohistochemical studies on the expression and estrogen dependency of EGF and its receptor and C-fos proto-oncogene in the uterus and vagina of normal and neonatally estrogen-treated mice.

作者信息

Falck L, Forsberg J G

机构信息

Department of Anatomy, University of Lund, Sweden.

出版信息

Anat Rec. 1996 Jul;245(3):459-71. doi: 10.1002/(SICI)1097-0185(199607)245:3<459::AID-AR2>3.0.CO;2-N.

Abstract

BACKGROUND

The final target cell response to estrogen is dependent not only on the estrogen receptor, but also on autocrine/paracrine interactions with growth factors (e.g., EGF) and proto-oncogenes (e.g., c-fos). Because neonatal estrogen treatment results in permanent changes in the female mouse genital tract (permanent vaginal cornification, cervical adenosis and tumors, changed growth control mechanisms in uterus), it was of interest to study possible acute and permanent effects of such treatment on distribution and levels of EGF, its receptor (EGF-r), and c-fos and to relate such changes to morphological development and appearance of epithelial abnormalities.

METHODS

Immunohistochemical techniques using frozen sections from the uterus and vagina of neonatal and adult (ovariectomized, estradiol-treated) females, treated with olive oil or diethylstilbestrol in neonatal life.

RESULTS

A difference in stromal-epithelial distribution of EGF was demonstrated with respect to region studied (uterus, vagina) and age (neonatal, adult). EGF was localized mainly in the uterine stroma but in both vaginal epithelium and stroma (with a different pattern compared to uterus). In neonatal females, EGF occurred in both tissue components in both regions, and the distribution pattern was quite different from that in adult females. The EGF level was increased by estrogen in adult but not in neonatal females. EGF-r and c-fos occurred in both uterine epithelium and stroma and in the vaginal epithelium; levels and distribution pattern were affected by estrogen. Neonatal estrogen treatment increased the levels of uterine EGF and c-fos in adult life.

CONCLUSIONS

There are distinct developmental changes in the distribution and estrogen sensitivity of EGF. Only further studies can prove or disprove the association between the earlier reported disturbed growth control mechanisms in the uterus of adult but neonatally estrogen-treated females and the increased levels of uterine EGF and c-fos. The present results do not seem to explain mechanisms involved in the origin of neonatally estrogen-induced cervicovaginal epithelial abnormalities, nor do they explain the earlier described difference in estrogen-induced proliferative response between the uterine cervix and uterus proper.

摘要

背景

雌激素最终的靶细胞反应不仅取决于雌激素受体,还取决于与生长因子(如表皮生长因子,EGF)和原癌基因(如c-fos)的自分泌/旁分泌相互作用。由于新生期雌激素处理会导致雌性小鼠生殖道发生永久性变化(永久性阴道角化、宫颈腺病和肿瘤、子宫生长控制机制改变),因此研究这种处理对EGF及其受体(EGF-r)以及c-fos的分布和水平可能产生的急性和永久性影响,并将这些变化与形态发育和上皮异常的出现相关联,具有重要意义。

方法

采用免疫组织化学技术,使用新生期和成年期(去卵巢、经雌二醇处理)雌性小鼠子宫和阴道的冰冻切片,新生期用橄榄油或己烯雌酚处理。

结果

在研究的区域(子宫、阴道)和年龄(新生期、成年期)方面,EGF的基质-上皮分布存在差异。EGF主要定位于子宫基质,但在阴道上皮和基质中均有分布(与子宫的分布模式不同)。在新生雌性小鼠中,两个区域的两种组织成分中均有EGF,其分布模式与成年雌性小鼠有很大不同。成年雌性小鼠中雌激素可使EGF水平升高,但新生雌性小鼠中则不然。EGF-r和c-fos在子宫上皮和基质以及阴道上皮中均有表达;其水平和分布模式受雌激素影响。新生期雌激素处理可使成年期子宫EGF和c-fos水平升高。

结论

EGF的分布和雌激素敏感性存在明显的发育变化。只有进一步的研究才能证实或否定成年期但新生期经雌激素处理的雌性小鼠子宫中早期报道的生长控制机制紊乱与子宫EGF和c-fos水平升高之间的关联。目前的结果似乎无法解释新生期雌激素诱导的宫颈阴道上皮异常的发生机制,也无法解释早期描述的宫颈和子宫体在雌激素诱导的增殖反应方面的差异。

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