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整合素 αVβ3 的小分子激素或类激素配体:对癌细胞行为的影响。

Small molecule hormone or hormone-like ligands of integrin αVβ3: implications for cancer cell behavior.

机构信息

Albany College of Pharmacy and Health Sciences, Pharmaceutical Research Institute, One Discovery Drive, Rensselaer, NY, 12144, USA,

出版信息

Horm Cancer. 2013 Dec;4(6):335-42. doi: 10.1007/s12672-013-0156-8. Epub 2013 Aug 14.

Abstract

Integrins are heterodimeric structural components of the plasma membrane whose ligands include a large number of extracellular matrix (ECM) proteins. The ligands contain Arg-Gly-Asp (RGD) sequences that enable recognition of ECM proteins by as many as eight integrins, but other distinguishing features of the proteins permit the integrins to generate intracellular signals specific to the ECM molecules. Recently, integrin αvβ3 has been shown to have a panel of previously unappreciated small molecule receptor sites for thyroid hormone and hormone analogues, for dihydrotestosterone, and for resveratrol, a polyphenol that has certain estrogen-like features. These binding sites are close to the RGD recognition site of αvβ3. The thyroid hormone receptor site on the extracellular domain of αvβ3 contains two domains with discrete functions in terms of intracellular protein trafficking and gene expression. Occupancy of the receptor by a deaminated thyroid hormone analogue, tetraiodothyroacetic acid (tetrac), prevents cell responses to agonist thyroid hormones (L-thyroxine; 3, 5, 3'-triiodo-L-thyronine) and modulates expression of a number of cancer cell survival pathway genes in an up- or downregulation pattern coherent to induction of cell death. The small molecule thyroid hormone receptor on the integrin also regulates activity of five vascular growth factor receptors and/or their ligands, providing control of angiogenesis via specific pharmacologic regulation of this thyroid hormone receptor. The resveratrol receptor induces programmed cancer cell death via p53, even when the latter has undergone specific mutations. There is also evidence for the presence of several receptors on integrin αvβ3 for authentic steroids, including a dihydrotestosterone site that supports proliferation of breast cancer cells that lack nuclear androgen and estrogen receptors. The existence of these small molecule hormone receptors on an integrin with a remarkably complex functional profile defines novel pharmacologic options via individual small molecule receptor manipulation for control of cancer cell behavior. This refinement of up-down control at the level of discrete receptors is not a function of the use of αvβ3 antibody or RGD peptides that occlude regions of the integrin.

摘要

整合素是质膜的异二聚体结构成分,其配体包括大量细胞外基质 (ECM) 蛋白。配体含有精氨酸-甘氨酸-天冬氨酸 (RGD) 序列,使多达 8 种整合素能够识别 ECM 蛋白,但蛋白质的其他区别特征允许整合素生成针对 ECM 分子的特定细胞内信号。最近,已经表明整合素 αvβ3 具有一组先前未被重视的甲状腺激素和激素类似物、二氢睾酮和白藜芦醇(具有某些雌激素样特征的多酚)的小分子受体位点。这些结合位点靠近 αvβ3 的 RGD 识别位点。αvβ3 细胞外结构域上的甲状腺激素受体包含两个具有离散功能的结构域,涉及细胞内蛋白质运输和基因表达。脱氨酶甲状腺激素类似物四碘甲状腺乙酸 (tetrac) 占据受体,可防止细胞对激动剂甲状腺激素 (L-甲状腺素;3,5,3'-三碘-L-甲状腺素) 的反应,并调节许多癌细胞存活途径基因的表达,呈上调或下调模式,与诱导细胞死亡一致。整合素上的小分子甲状腺激素受体还调节 5 种血管生长因子受体及其配体的活性,通过对这种甲状腺激素受体的特定药理学调节来控制血管生成。白藜芦醇受体通过 p53 诱导程序性癌细胞死亡,即使后者发生了特定的突变。也有证据表明整合素 αvβ3 上存在几种真正的类固醇受体,包括二氢睾酮位点,该位点支持缺乏核雄激素和雌激素受体的乳腺癌细胞增殖。这种具有复杂功能谱的整合素上存在这些小分子激素受体,为通过单独的小分子受体操作控制癌细胞行为提供了新的药理选择。这种在离散受体水平上的上下控制的细化不是使用整合素 αvβ3 抗体或封闭整合素区域的 RGD 肽的功能。

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