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Design and preliminary structure-activity relationship of redox-silent semisynthetic tocotrienol analogues as inhibitors for breast cancer proliferation and invasion.

机译:氧化还原沉默半合成蛋白与乳腺癌增殖和侵袭抑制剂的设计与初步结构关系。

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摘要

Vitamin E (VE) is a generic term that represents a family of compounds composed of various tocopherol and tocotrienol isoforms. Tocotrienols display potent anti-angiogenic and antiproliferative activities. Redox-silent tocotrienol analogues also display potent anticancer activity. The ultimate objective of this study was to develop semisynthetically C-6-modified redox-silent tocotrienol analogues with enhanced antiproliferative and anti-invasive activities as compared to their parent compound. Examples of these are carbamate and ether analogues of alpha-, gamma-, and delta-tocotrienols (1-3). Various aliphatic, olefinic, and aromatic substituents were used. Steric limitation, electrostatic, hydrogen bond donor (HBD) and hydrogen bond acceptor (HBA) properties were varied at this position and the biological activities of these derivatives were tested. Three-dimensional quantitative structure-activity relationship (3D QSAR) studies were performed using Comparative Molecular Field (CoMFA) and Comparative Molecular Similarity Indices Analyses (CoMSIA) to better understand the structural basis for biological activity and guide the future design of more potent VE analogues.
机译:维生素E(VE)是一种通用术语,其代表由各种生育酚和Tocotrienol同种型组成的化合物系列。 Tocotrienols显示有效的抗血管生成和抗增殖活动。氧化还原沉默的Tocotrienol类似物也显示有效的抗癌活动。本研究的最终目标是开发半交替的C-6-修饰的氧化还原沉默的Tocotrienol类似物,与其母体化合物相比,具有增强的抗增殖和抗侵入活性。这些实例是氨基甲酸酯和α-,γ-和δ-tocotrienols(1-3)的醚类似物。使用各种脂族,烯烃和芳族取代基。在该位置的情况下变化了空间限制,静电,氢键供体(HBD)和氢键受体(HBA)性质,并测试了这些衍生物的生物活性。使用比较分子领域(COMFA)和比较分子相似性指数分析(COMSIA)来进行三维定量结构 - 活性关系(3D QSAR)研究,以更好地了解生物活动的结构基础,并指导更有效的VE类似物的未来设计。

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