在肥胖和乳腺癌的临床前模型中,雄激素受体支持卵巢功能丧失后的肿瘤进展。

IF 3 4区 医学 Q3 Biochemistry, Genetics and Molecular Biology
Elizabeth A Wellberg, L Allyson Checkley, Erin D Giles, Stevi J Johnson, Robera Oljira, Reema Wahdan-Alaswad, Rebecca M Foright, Greg Dooley, Susan M Edgerton, Sonali Jindal, Ginger C Johnson, Jennifer K Richer, Peter Kabos, Ann D Thor, Pepper Schedin, Paul S MacLean, Steven M Anderson
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引用次数: 15

摘要

雄激素受体(AR)在乳腺癌的生长和进展中具有环境依赖性作用。总体而言,高肿瘤AR水平预示着有利的患者预后,但一些研究已经确立了AR对肿瘤的促进作用,特别是在内分泌治疗后支持雌激素受体阳性(er阳性)乳腺癌的生长。我们之前的研究表明,在绝经后乳腺癌大鼠模型中,肥胖促进卵巢切除术(OVX)后乳腺肿瘤进展。在这里,我们研究了AR在卵巢雌激素缺失后肥胖相关的ovx后乳腺肿瘤进展中的潜在作用。在这个模型中,我们发现肥胖而不是瘦弱的大鼠在OVX后3周进展的肿瘤中有核局限性AR,与那些退化的大鼠相比。AR核定位与AR依赖性转录的激活是一致的。长期研究(ovx后8周)显示,进展的肿瘤中AR核定位和表达得以维持,但在退行性肿瘤中AR表达几乎消失。抗雄激素enzalutamide通过促进肿瘤坏死有效阻断肥胖大鼠肿瘤进展,并阻止OVX后新肿瘤的形成。与瘦鼠相比,肥胖大鼠的循环和乳腺脂肪组织中AR配体睾酮水平均未升高;然而,我们之前报道的肥胖大鼠血浆中IL-6比瘦大鼠血浆中IL-6更高,使乳腺癌细胞对低水平的睾酮敏感。我们的研究表明,在肥胖的背景下,AR在低雌激素可用性环境下驱动er阳性乳腺肿瘤进展中发挥作用,并且肥胖宿主特有的循环因子,包括IL-6,可能影响癌细胞对类固醇激素的反应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

The Androgen Receptor Supports Tumor Progression After the Loss of Ovarian Function in a Preclinical Model of Obesity and Breast Cancer.

The Androgen Receptor Supports Tumor Progression After the Loss of Ovarian Function in a Preclinical Model of Obesity and Breast Cancer.

The Androgen Receptor Supports Tumor Progression After the Loss of Ovarian Function in a Preclinical Model of Obesity and Breast Cancer.

The Androgen Receptor Supports Tumor Progression After the Loss of Ovarian Function in a Preclinical Model of Obesity and Breast Cancer.

The androgen receptor (AR) has context-dependent roles in breast cancer growth and progression. Overall, high tumor AR levels predict a favorable patient outcome, but several studies have established a tumor promotional role for AR, particularly in supporting the growth of estrogen receptor positive (ER-positive) breast cancers after endocrine therapy. Our previous studies have demonstrated that obesity promotes mammary tumor progression after ovariectomy (OVX) in a rat model of postmenopausal breast cancer. Here, we investigated a potential role for AR in obesity-associated post-OVX mammary tumor progression following ovarian estrogen loss. In this model, we found that obese but not lean rats had nuclear localized AR in tumors that progressed 3 weeks after OVX, compared to those that regressed. AR nuclear localization is consistent with activation of AR-dependent transcription. Longer-term studies (8 weeks post-OVX) showed that AR nuclear localization and expression were maintained in tumors that had progressed, but AR expression was nearly lost in tumors that were regressing. The anti-androgen enzalutamide effectively blocked tumor progression in obese rats by promoting tumor necrosis and also prevented the formation of new tumors after OVX. Neither circulating nor mammary adipose tissue levels of the AR ligand testosterone were elevated in obese compared to lean rats; however, IL-6, which we previously reported to be higher in plasma from obese versus lean rats, sensitized breast cancer cells to low levels of testosterone. Our study demonstrates that, in the context of obesity, AR plays a role in driving ER-positive mammary tumor progression in an environment of low estrogen availability, and that circulating factors unique to the obese host, including IL-6, may influence how cancer cells respond to steroid hormones.

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来源期刊
Hormones & Cancer
Hormones & Cancer ONCOLOGY-ENDOCRINOLOGY & METABOLISM
CiteScore
4.60
自引率
0.00%
发文量
0
期刊介绍: Hormones and Cancer is a unique multidisciplinary translational journal featuring basic science, pre-clinical, epidemiological, and clinical research papers. It covers all aspects of the interface of Endocrinology and Oncology. Thus, the journal covers two main areas of research: Endocrine tumors (benign & malignant tumors of hormone secreting endocrine organs) and the effects of hormones on any type of tumor. We welcome all types of studies related to these fields, but our particular attention is on translational aspects of research. In addition to basic, pre-clinical, and epidemiological studies, we encourage submission of clinical studies including those that comprise small series of tumors in rare endocrine neoplasias and/or negative or confirmatory results provided that they significantly enhance our understanding of endocrine aspects of oncology. The journal does not publish case studies.
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