Division of Environmental Genetics and Molecular Toxicology, Department of Environmental Health, University of Cincinnati College of Medicine, Cincinnati, OH.
Neoplasia. 2013 Nov;15(11):1262-71. doi: 10.1593/neo.131184.
Alternative splicing of estrogen receptor β (ERβ) yields five isoforms, but their functions remain elusive. ERβ isoform 5 (ERβ5) has been positively correlated with better prognosis and longer survival of patients with breast cancer (BCa) in various clinical studies. In this study, we investigated the inhibitory role of ERβ5 in BCa cells. Although ERβ5 does not reduce proliferation of BCa cell lines MCF-7 and MDA-MB-231, its ectopic expression significantly decreases their survival by sensitizing them to doxorubicin- or cisplatin-induced apoptosis through the intrinsic apoptotic pathway. Moreover, we discovered Bcl2L12, which belongs to the Bcl-2 family regulating apoptosis, to be a specific interacting partner of ERβ5, but not ERβ1 or ERα, in an estradiol-independent manner. Knockdown of Bcl2L12 enhanced doxorubicin- or cisplatin-induced apoptosis, and this process was further promoted by ectopic expression of ERβ5. Whereas Bcl2L12 was previously shown to inhibit apoptosis through binding to caspase 7, such interaction is reduced in the presence of ERβ5, suggesting a mechanism by which ERβ5 sensitizes cells to apoptosis. In conclusion, ERβ5 interacts with Bcl2L12 and functions in a novel estrogen-independent molecular pathway that promotes chemotherapeutic Agent-Induced in vitro apoptosis of BCa cell lines.
雌激素受体 β(ERβ)的选择性剪接产生了五种异构体,但它们的功能仍不清楚。在各种临床研究中,ERβ 异构体 5(ERβ5)与乳腺癌(BCa)患者更好的预后和更长的生存时间呈正相关。在这项研究中,我们研究了 ERβ5 在 BCa 细胞中的抑制作用。尽管 ERβ5 不会减少 BCa 细胞系 MCF-7 和 MDA-MB-231 的增殖,但通过内在凋亡途径使它们对阿霉素或顺铂诱导的凋亡敏感,其异位表达显著降低了它们的存活。此外,我们发现 Bcl2L12 是一种调节凋亡的 Bcl-2 家族成员,以雌激素非依赖性方式成为 ERβ5 的特定相互作用伙伴,而不是 ERβ1 或 ERα。Bcl2L12 的敲低增强了阿霉素或顺铂诱导的凋亡,而 ERβ5 的异位表达进一步促进了这一过程。虽然 Bcl2L12 先前被证明通过与 caspase 7 结合来抑制凋亡,但在存在 ERβ5 的情况下,这种相互作用减少,这表明了 ERβ5 使细胞对凋亡敏感的一种机制。总之,ERβ5 与 Bcl2L12 相互作用,并在一种新的雌激素非依赖性分子途径中发挥作用,该途径促进 BCa 细胞系中化疗药物诱导的体外凋亡。
