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卵巢类固醇与人类乳腺:干细胞的调控及细胞增殖

Ovarian steroids and the human breast: regulation of stem cells and cell proliferation.

作者信息

Clarke Robert B

机构信息

Breast Biology Group, CR-UK Department of Medical Oncology, University of Manchester, Christie Hospital, Manchester, M20 4BX, UK.

出版信息

Maturitas. 2006 Jul 20;54(4):327-34. doi: 10.1016/j.maturitas.2006.06.002. Epub 2006 Jun 30.

Abstract

Ovarian steroidal control of mammary gland proliferation and differentiation is not well defined in the human. We therefore developed the athymic nude mouse model in which intact normal human breast tissue is xenografted subcutaneously and treated with human physiological serum levels of oestrogen (E) and/or progesterone (P). We showed that: (i) E, and not P, is the major steroid hormone inducing proliferation of epithelial cells in the adult non-pregnant, non-lactating breast; (ii) E induces progesterone receptor (PR) expression; and (iii) PR expression is maximally induced at low E concentrations while a higher amount of E was required to induce proliferation. Using double label immuno-fluorescence, we demonstrated that cells expressing the oestrogen receptor-alpha (ER alpha) invariably contained the PR but that steroid receptor expression and cell proliferation (Ki67 antigen) were dissociated. Recently, we have demonstrated that some ER alpha/PR-positive epithelial cells are quiescent breast stem cells suggesting that they act as "steroid hormone sensors" that secrete paracrine factors to regulate the proliferative activity of adjacent ER alpha/PR-negative epithelial cells. The dissociation between steroid receptor expression and cell proliferation in normal epithelium was lost at an early stage in ER alpha/PR-positive breast tumour formation perhaps indicating that they arise from deregulation of the normally quiescent breast stem cells.

摘要

在人类中,卵巢甾体激素对乳腺增殖和分化的调控作用尚未完全明确。因此,我们构建了无胸腺裸鼠模型,将完整的正常人类乳腺组织皮下异种移植,并用人生理血清水平的雌激素(E)和/或孕激素(P)进行处理。我们发现:(i)在成年非孕、非泌乳乳腺中,E而非P是诱导上皮细胞增殖的主要甾体激素;(ii)E诱导孕激素受体(PR)表达;(iii)低浓度E时PR表达诱导达到最大值,而诱导增殖则需要更高剂量的E。通过双标免疫荧光法,我们证明表达雌激素受体α(ERα)的细胞总是含有PR,但甾体激素受体表达与细胞增殖(Ki67抗原)是分离的。最近,我们证明一些ERα/PR阳性上皮细胞是静止的乳腺干细胞,这表明它们作为“甾体激素传感器”,分泌旁分泌因子来调节相邻ERα/PR阴性上皮细胞的增殖活性。在ERα/PR阳性乳腺肿瘤形成的早期阶段,正常上皮中甾体激素受体表达与细胞增殖之间的分离消失,这可能表明它们源于正常静止乳腺干细胞的失调。

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