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Design and Synthesis of Benzene Congeners of Resolvin E2, a Proresolving Lipid Mediator, as Its Stable Equivalents

机译:替代脂质介质溶质凝胶蛋白E2,脂质介质的苯同质的设计与合成,作为其稳定的等同物

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Resolvins (Rvs) are highly potent anti-inflammatory lipid mediators that are chemically and biologically unstable because of their polyunsaturated structures. To address this issue, we designed benzene congeners of RvE2, i.e., o-, m-, and p-BZ-RvE2s, as stable equivalents of RvE2 by replacing the unstable skipped diene moiety with a benzene ring on the basis of computational conformation studies and synthesized these congeners via a short common route through two Stille couplings. o-BZ-RvE2 exhibited more potent anti-inflammatory activity and much higher metabolic stability than RvE2. Thus, o-BZ-RvE2 was identified as a stable equivalent of RvE2, which is useful as a lead for anti-inflammatory drugs with a new mechanism of action as well as a biotool for investigating RvE2-mediated inflammation resolving pathways.
机译:Reqorvins(RVS)是高效的抗炎脂质介质,其由于其多不饱和结构而在化学和生物学上不稳定。 为了解决这个问题,我们通过在计算构象研究的基础上,设计了RVE2,即O-,M-和P-BZ-RVE2S的苯同一步,即O-,M-和P-BZ-RVE2S,作为RVE2的稳定等同物 并通过两个STILLE联轴器通过短常见的途径合成这些同觉。 O-BZ-RVE2表现出更多有效的抗炎活性和比RVE2更高的代谢稳定性。 因此,O-BZ-RVE2被鉴定为RVE2的稳定等同物,其用作具有新的作用机制以及用于研究RVE2介导的炎症途径的生物可能的抗炎药的铅。

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