基质在雌激素诱导的上皮细胞增殖中的作用。

Epithelial cell biology Pub Date : 1992-01-01
G R Cunha, P Young
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引用次数: 0

摘要

为了研究基质-上皮相互作用在上皮细胞对雌激素反应中的作用,我们将阴道(V)和膀胱(BL)的上皮(E)和基质(S),即雌激素靶组织(VS和VE)和非靶组织(BLS和BLE)进行组织重组。在完整的雌性宿主生长3周后,进行卵巢切除术,1周后进行各种激素治疗。虽然阴道组织重组(VS+VE)表现出上皮角化和黏液化(循环),但在膀胱重组(BLS+BLE)或阴道和膀胱组织之间的异型组织重组(VS+BLE和BLS+VE)中没有观察到这种活性。在BLS+VE重组中,上皮仍然萎缩,对外源性雌激素单独或联合黄体酮没有反应。当BLS+VE重组体的上皮恢复并与新鲜阴道间质(VS)重新结合时,阴道上皮的激素反应性缺失被完全重建。对上皮细胞增殖活性([3H]胸腺嘧啶标记指数)的检测显示,雌激素诱导的VS+VE重组细胞上皮细胞增殖明显增加。BLS+BLE重组体对雌激素无反应,BLS+VE重组体亦无反应。然而,当膀胱上皮与阴道间质(VS+BLE)结合生长时,上皮的标记指数比经油处理的标本增加了8倍。当这些重组体的阴道上皮恢复并与新鲜阴道基质重新相关时,BLS+VE重组体缺乏雌激素诱导的阴道上皮增殖反应被逆转。这些结果表明,雌激素和孕激素对上皮分化和增殖的影响严重依赖于适当的基质环境。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Role of stroma in oestrogen-induced epithelial proliferation.

To examine the role of stromal-epithelial interactions in the response of epithelial cells to oestrogens, tissue recombinations were prepared with epithelium (E) and stroma (S) from the vagina (V) and urinary bladder (BL), that is between oestrogen target tissues (VS and VE) and non-target tissues (BLS and BLE). Following 3 weeks of growth in intact female hosts, ovariectomy was performed and 1 week later the hosts subjected to various hormonal treatments. Whereas homotypic vaginal tissue recombinations (VS+VE) exhibited epithelial cornification and mucification (cycling), this activity was not observed in homotypic bladder recombinants (BLS+BLE) or in heterotypic tissue recombinants between vaginal and bladder tissues (VS+BLE and BLS+VE). In BLS+VE recombinants the epithelium remained atrophic and failed to respond to exogenous oestrogen alone or in combination with progesterone. This lack of hormonal responsiveness of vaginal epithelium was completely reconstituted when the epithelium of BLS+VE recombinants was recovered and reassociated with fresh vaginal stroma (VS). Examination of epithelial proliferative activity ([3H]thymidine labelling index) demonstrated a marked oestrogen-induced increase in epithelial proliferation in VS+VE recombinants. BLS+BLE recombinants were unresponsive to oestrogen as were recombinants composed of BLS+VE. However, when bladder epithelium was grown in association with vaginal stroma (VS+BLE) the epithelium exhibited an 8-fold oestrogen-induced increase in labelling index over oil-treated specimens. The lack of an oestrogen-induced proliferative response of vaginal epithelium in BLS+VE recombinants was reversed when the vaginal epithelium of these recombinants was recovered and reassociated with fresh vaginal stroma. These results indicate that the effects of oestrogen and progesterone on both epithelial differentiation and proliferation are critically dependent upon the appropriate stromal environment.

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