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ERalpha 在 Stat5a 缺失对乳腺前期病变和 DMBA 诱导的肿瘤发生易感性的差异反应中的作用。

Role of ERalpha in the differential response of Stat5a loss in susceptibility to mammary preneoplasia and DMBA-induced carcinogenesis.

机构信息

Department of Oncology, Georgetown University, Washington, DC 20007, USA.

出版信息

Carcinogenesis. 2010 Jun;31(6):1124-31. doi: 10.1093/carcin/bgq048. Epub 2010 Feb 24.

DOI:10.1093/carcin/bgq048
PMID:20181624
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2878361/
Abstract

Deregulated estrogen signaling is evidently linked to breast cancer pathophysiology, although the role of signal transducer and activator of transcription (Stat)5a, integral to normal mammary gland development, is less clear. A mouse model of mammary epithelial cell-targeted deregulated estrogen receptor alpha (ERalpha) expression [conditional ERalpha in mammary epithelium (CERM)] was crossed with mice carrying a germ line deletion of Stat5a [Stat5a-/-] to investigate interactions between ERalpha and Stat5a in mammary tissue. CERM, CERM/Stat5a+/-, CERM/Stat5a-/-, Stat5a+/-, Stat5a-/- and wild-type (WT) mice were generated to test the roles of ERalpha and Stat5a on pubertal differentiation and cancer progression with and without exposure to the chemical carcinogen 7,12-dimethylbenz[a]anthracene (DMBA). Only CERM/Stat5a-/- mice demonstrated delayed pubertal terminal end bud differentiation. Without DMBA exposure, Stat5a loss abrogated ERalpha-initiated hyperplastic alveolar nodule (HAN) development and, similarly, Stat5a-/- mice did not develop HANs. However, although Stat5a loss still reduced ERalpha-initiated HAN prevalence following DMBA exposure, Stat5a loss without deregulated ERalpha was associated with an increased HAN prevalence compared with WT. Progression to ERalpha(+) and ERalpha(-) adenocarcinoma was found in all CERM-containing genotypes (CERM, CERM/Stat5a+/-, CERM/Stat5a-/-) and ERalpha(+) adenocarcinoma in the Stat5a-/- genotype. The mammary epithelial cell proliferative index was increased only in CERM mice independent of Stat5a loss. No differences in apoptotic indices were found. In summary, Stat5a cooperated with deregulated ERalpha in retarding pubertal mammary differentiation and contributed to ERalpha-initiated preneoplasia, but its loss did not prevent development of invasive cancer. Moreover, in the absence of deregulated ERalpha, Stat5a loss was associated with development of both HANs and invasive cancer following DMBA exposure.

摘要

雌激素信号失调显然与乳腺癌的病理生理学有关,尽管信号转导子和转录激活子(Stat)5a 是正常乳腺发育所必需的,但它的作用尚不明确。我们构建了一种乳腺上皮细胞靶向表达失控的雌激素受体 alpha(ERalpha)的小鼠模型[乳腺上皮细胞条件性 ERalpha 表达(CERM)],并将其与携带 Stat5a 种系缺失的小鼠[Stat5a-/-]进行杂交,以研究 ERalpha 和 Stat5a 在乳腺组织中的相互作用。我们生成了 CERM、CERM/Stat5a+/-、CERM/Stat5a-/-、Stat5a+/-、Stat5a-/-和野生型(WT)小鼠,以检测 ERalpha 和 Stat5a 在有无化学致癌剂 7,12-二甲基苯并[a]蒽(DMBA)暴露的情况下对青春期分化和癌症进展的作用。只有 CERM/Stat5a-/-小鼠表现出青春期终末芽分化延迟。在没有 DMBA 暴露的情况下,Stat5a 的缺失消除了 ERalpha 引发的增生性肺泡结节(HAN)的发生,同样地,Stat5a-/-小鼠也不会发生 HAN。然而,尽管 Stat5a 的缺失仍然降低了 DMBA 暴露后 ERalpha 引发的 HAN 的发生率,但与 WT 相比,在没有失控的 ERalpha 的情况下,Stat5a 的缺失与 HAN 的发生率增加相关。在所有含有 CERM 的基因型(CERM、CERM/Stat5a+/-、CERM/Stat5a-/-)中均发现 CERM 诱导的 ERalpha(+)和 ERalpha(-)腺癌,并且在 Stat5a-/-基因型中也发现 ERalpha(+)腺癌。仅在 CERM 小鼠中观察到乳腺上皮细胞增殖指数增加,而与 Stat5a 的缺失无关。未发现凋亡指数的差异。总之,Stat5a 与失控的 ERalpha 合作,延缓青春期乳腺分化,并促进 ERalpha 引发的癌前病变,但它的缺失并不能阻止侵袭性癌症的发生。此外,在没有失控的 ERalpha 的情况下,Stat5a 的缺失与 DMBA 暴露后 HAN 和侵袭性癌症的发生有关。

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