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膜结合型雌激素受体 ERα 的表达对于乳腺上皮细胞间的通讯是必需的。

Membrane expression of the estrogen receptor ERα is required for intercellular communications in the mammary epithelium.

机构信息

INSERM U1048, I2MC, Université de Toulouse, Toulouse 31432, France.

Swiss Institute for Experimental Cancer Research, School of Life Sciences, Ecole Polytechnique Fédérale de Lausanne, CH-1015 Lausanne, Switzerland.

出版信息

Development. 2020 Mar 11;147(5):dev182303. doi: 10.1242/dev.182303.

DOI:10.1242/dev.182303
PMID:32098763
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7075076/
Abstract

17β-Estradiol induces the postnatal development of mammary gland and influences breast carcinogenesis by binding to the estrogen receptor ERα. ERα acts as a transcription factor but also elicits rapid signaling through a fraction of ERα expressed at the membrane. Here, we have used the C451A-ERα mouse model mutated for the palmitoylation site to understand how ERα membrane signaling affects mammary gland development. Although the overall structure of physiological mammary gland development is slightly affected, both epithelial fragments and basal cells isolated from C451A-ERα mammary glands failed to grow when engrafted into cleared wild-type fat pads, even in pregnant hosts. Similarly, basal cells purified from hormone-stimulated ovariectomized C451A-ERα mice did not produce normal outgrowths. , C451A-ERα basal cells displayed reduced matrix degradation capacities, suggesting altered migration properties. More importantly, C451A-ERα basal cells recovered repopulating ability when co-transplanted with wild-type luminal cells and specifically with ERα-positive luminal cells. Transcriptional profiling identified crucial paracrine luminal-to-basal signals. Altogether, our findings uncover an important role for membrane ERα expression in promoting intercellular communications that are essential for mammary gland development.

摘要

17β-雌二醇通过与雌激素受体 ERα 结合诱导乳腺的产后发育,并影响乳腺癌的发生。ERα 作为转录因子发挥作用,但也通过在膜上表达的一部分 ERα 引发快速信号转导。在这里,我们使用 C451A-ERα 小鼠模型,该模型突变了棕榈酰化位点,以了解 ERα 膜信号转导如何影响乳腺发育。尽管生理乳腺发育的整体结构受到轻微影响,但从 C451A-ERα 乳腺中分离的上皮片段和基底细胞在植入清除的野生型脂肪垫时均无法生长,即使在怀孕的宿主中也是如此。同样,从激素刺激的卵巢切除 C451A-ERα 小鼠中纯化的基底细胞也不会产生正常的生长。C451A-ERα 基底细胞显示出降低的基质降解能力,表明迁移特性发生改变。更重要的是,当与野生型腔细胞共移植时,特别是与 ERα 阳性腔细胞共移植时,C451A-ERα 基底细胞恢复了再定植能力。转录谱分析确定了重要的旁分泌腔细胞-基底细胞信号。总之,我们的发现揭示了膜 ERα 表达在促进细胞间通讯中的重要作用,这对于乳腺发育至关重要。

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