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首页> 外文期刊>Current opinion in pharmacology >The molecular mechanisms underlying the pharmacological actions of ER modulators: implications for new drug discovery in breast cancer.
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The molecular mechanisms underlying the pharmacological actions of ER modulators: implications for new drug discovery in breast cancer.

机译:ER调节剂的药理作用的分子机制:对乳腺癌新药发现的影响。

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Our understanding of the molecular mechanisms underlying the pharmacological actions of estrogen receptor (ER) ligands has evolved considerably in recent years. Much of this knowledge has come from a detailed dissection of the mechanism(s) of action of the Selective Estrogen Receptor Modulators (SERMs) tamoxifen and raloxifene, so called for their ability to function as ER agonists or antagonists depending on the tissue in which they operate. These mechanistic insights have had a significant impact on the discovery of second generation SERMs, some of which are in late stage clinical development for the treatment/prevention of breast cancer as well as other estrogenopathies. In addition to the SERMs, however, have emerged the Selective Estrogen Degraders (SERDs), which as their name suggests, interact with and facilitate ER turnover in cells. One drug of this class, fulvestrant, has been approved as a third line treatment for ER-positive metastatic breast cancer. Whereas the first generation SERMs/SERDs were discovered in a serendipitous manner, this review will highlight how our understanding of the molecular pharmacology of ER ligands has been utilized in the development of the next generation of SERMs/SERDs, some of which are likely to have a major impact on the pharmacotherapy of breast cancer.
机译:近年来,我们对雌激素受体(ER)配体的药理作用基础的分子机制的理解已有很大的发展。这些知识的大部分来自对选择性雌激素受体调节剂(SERMs)他莫昔芬和雷洛昔芬的作用机理的详细剖析,因此称它们具有根据它们所处的组织充当ER激动剂或拮抗剂的能力。操作。这些机制的见解对第二代SERMs的发现产生了重大影响,其中第二代SERMs处于晚期临床开发中,用于治疗/预防乳腺癌以及其他雌激素病。然而,除了SERM之外,还出现了选择性雌激素降解剂(SERD),正如其名称所暗示的那样,它可以与细胞中的ER相互作用并相互作用。这类药物中的一种是氟韦司汀,已被批准作为ER阳性转移性乳腺癌的三线治疗药物。第一代SERM / SERD是偶然发现的,而本综述将着重介绍我们如何将ER配体的分子药理学理解用于下一代SERM / SERD的开发中。对乳腺癌的药物治疗有重大影响。

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