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Current and Future Development of Estrogen Receptor Ligands: Applications in Estrogen-Related Cancers

机译:雌激素受体配体的当前和未来发展:在雌激素相关癌症中的应用

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17 beta-Estradiol (E2), via its cognate receptors (ERs), regulates several aspects of human physiology including development, reproduction and tissue homeostasis. Consequently, E2 could also be implicated in the development or progression of several pathologies, including cancer. Two different ER subtypes are present in mammals (ERa and ERP), which display specific roles in E2-related cancers, different tissue distribution, and multiple action mechanisms (i.e., ge-nomic and extranuclear mechanisms). Here, the complex pattern of the relative contribution of each ER subtype in the E2-dependent cancers has been summarized by taking into consideration the molecular events which occur both in the nucleus and in extranuclear compartments. In the second part of this paper, we reviewed the current literature available on the drug-targeting of the ERs, as well as the recent literature and patents describing new and upcoming molecules. These new molecules will probably greatly improve the repertoire of anti-hormonal therapeutic strategies. However, further new drug design programs, which should include all molecular mechanisms at the basis of ER biology, are needed to expand the anti-ER treatments in new and more efficient therapeutic directions. This review also outlines relevant patents.
机译:17 β-雌二醇 (E2) 通过其同源受体 (ER) 调节人体生理学的几个方面,包括发育、繁殖和组织稳态。因此,E2 也可能与包括癌症在内的多种病理的发展或进展有关。哺乳动物中存在两种不同的内质网亚型(ERa 和 ERP),它们在 E2 相关癌症、不同的组织分布和多种作用机制(即基因和核外机制)中显示出特定作用。在这里,通过考虑细胞核和核外区室中发生的分子事件,总结了每种 ER 亚型在 E2 依赖性癌症中相对贡献的复杂模式。在本文的第二部分,我们回顾了目前关于ER药物靶向的文献,以及描述新的和即将到来的分子的最新文献和专利。这些新分子可能会大大改善抗激素治疗策略的库。然而,需要进一步的新药物设计计划,其中应包括内质网生物学基础上的所有分子机制,以将抗内质网治疗扩展到新的和更有效的治疗方向。本综述还概述了相关专利。

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