Department of Oncology and Metabolism, The Mellanby Centre for Musculoskeletal Research, The University of Sheffield, Sheffield, United Kingdom.
Front Endocrinol (Lausanne). 2021 Oct 18;12:749428. doi: 10.3389/fendo.2021.749428. eCollection 2021.
Clinical trials have demonstrated that adding zoledronic acid (Zol) to (neo)adjuvant standard of care has differential antitumour effects in pre- and post-menopausal women: Both benefit from reduced recurrence in bone; however, while postmenopausal women also incur survival benefit, none is seen in premenopausal women treated with adjuvant bisphosphonates. In the current study, we have used mouse models to investigate the role of oestradiol in modulating potential antitumour effects of Zol. Pre-, peri-, and post-menopausal concentrations of oestradiol were modelled in BALB/c wild-type, BALB/c nude, and C57BL/6 mice by ovariectomy followed by supplementation with oestradiol. Mice also received 40 mg/kg/day goserelin to prevent ovariectomy-induced increases in follicle-stimulating hormone (FSH). Metastasis was modelled following injection of MDA-MB-231, 4T1, or E0771 cells after ovariectomy and saline or 100 μg/kg Zol administered weekly. Supplementing ovariectomised mice with 12.5 mg/ml, 1.38 mg/ml, and 0 ng/ml oestradiol, in the presence of goserelin, resulted in serum concentrations of 153.16 ± 18.10 pg/ml, 48.64 ± 18.44 pg/ml, and 1.00 ± 0.27 pg/ml oestradiol, which are equivalent to concentrations found in pre-, peri-, and post-menopausal humans. Osteoclast activity was increased 1.5-1.8-fold with peri- and post-menopausal compared with premenopausal oestradiol, resulting in a 1.34-1.69-fold reduction in trabecular bone. Zol increased trabecular bone in all groups but did not restore bone to volumes observed under premenopausal conditions. In tumour-bearing mice, Zol reduced bone metastases in BALB/c (wild-type and nude), with greatest effects seen under pre- and post-menopausal concentrations of oestradiol. Zol did not affect soft tissue metastases in immunocompetent BALB/c mice but increased metastases 3.95-fold in C57BL/6 mice under premenopausal concentrations of oestradiol. In contrast, Zol significantly reduced soft tissue metastases 2.07 and 4.69-fold in immunocompetent BALB/c and C57BL/6 mice under postmenopausal oestradiol, mirroring the results of the clinical trials of (neo)adjuvant bisphosphonates. No effects on soft tissue metastases were observed in immunocompromised mice, and differences in antitumour response did not correlate with , , or expression. In conclusion, oestradiol contributes to altered antitumour effects of Zol observed between pre- and post-menopausal women. However, other immunological/microenvironmental factors are also likely to contribute to this phenomenon.
临床试验表明,在绝经前和绝经后妇女中,添加唑来膦酸(zol)到(新)辅助标准治疗中具有不同的抗肿瘤作用:两者都能减少骨复发;然而,虽然绝经后妇女也能获得生存获益,但在接受辅助双膦酸盐治疗的绝经前妇女中未见获益。在本研究中,我们使用小鼠模型研究了雌激素在调节唑来膦酸潜在抗肿瘤作用中的作用。通过卵巢切除术并用雌激素补充,在 BALB/c 野生型、BALB/c 裸鼠和 C57BL/6 小鼠中模拟绝经前、围绝经期和绝经后浓度。小鼠还接受了 40mg/kg/天的戈舍瑞林,以防止卵巢切除引起的卵泡刺激素(FSH)增加。在卵巢切除后注射 MDA-MB-231、4T1 或 E0771 细胞,并每周给予 100μg/kg Zol,模拟转移。在存在戈舍瑞林的情况下,用 12.5mg/ml、1.38mg/ml 和 0ng/ml 雌激素补充卵巢切除小鼠,导致血清雌二醇浓度为 153.16±18.10pg/ml、48.64±18.44pg/ml 和 1.00±0.27pg/ml,相当于绝经前、围绝经期和绝经后人类的浓度。与绝经前雌二醇相比,围绝经期和绝经后雌二醇使破骨细胞活性增加 1.5-1.8 倍,导致小梁骨减少 1.34-1.69 倍。唑来膦酸增加了所有组的小梁骨,但不能使骨体积恢复到绝经前状态。在荷瘤小鼠中,唑来膦酸减少了 BALB/c(野生型和裸鼠)的骨转移,在绝经前和绝经后雌二醇浓度下观察到最大的效果。唑来膦酸对免疫功能正常的 BALB/c 小鼠的软组织转移没有影响,但在绝经前雌二醇浓度下,C57BL/6 小鼠的转移增加了 3.95 倍。相比之下,在免疫功能正常的 BALB/c 和 C57BL/6 小鼠中,唑来膦酸在绝经后雌二醇下显著减少了 2.07 和 4.69 倍的软组织转移,与(新)辅助双膦酸盐临床试验的结果一致。在免疫功能低下的小鼠中未观察到对软组织转移的影响,抗肿瘤反应的差异与、或表达无关。总之,雌激素导致绝经前和绝经后妇女中唑来膦酸观察到的抗肿瘤作用改变。然而,其他免疫/微环境因素也可能促成这种现象。
