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索贝替罗的乙醇胺衍生前药的酯到酰胺重排,其血脑屏障穿透性增强。

Ester-to-amide rearrangement of ethanolamine-derived prodrugs of sobetirome with increased blood-brain barrier penetration.

作者信息

Ferrara Skylar J, Meinig J Matthew, Placzek Andrew T, Banerji Tapasree, McTigue Peter, Hartley Meredith D, Sanford-Crane Hannah S, Banerji Tania, Bourdette Dennis, Scanlan Thomas S

机构信息

Program in Chemical Biology, Department of Physiology & Pharmacology, Oregon Health & Science University, 3181 SW Sam Jackson Park Rd, Portland, OR 97239, United States.

Department of Neurology, Oregon Health & Science University, 3181 SW Sam Jackson Park Rd, Portland, OR 97239, United States.

出版信息

Bioorg Med Chem. 2017 May 15;25(10):2743-2753. doi: 10.1016/j.bmc.2017.03.047. Epub 2017 Mar 23.

Abstract

Current therapeutic options for treating demyelinating disorders such as multiple sclerosis (MS) do not stimulate myelin repair, thus creating a clinical need for therapeutic agents that address axonal remyelination. Thyroid hormone is known to play an important role in promoting developmental myelination and repair, and CNS permeable thyromimetic agents could offer an increased therapeutic index compared to endogenous thyroid hormone. Sobetirome is a clinical stage thyromimetic that has been shown to have promising activity in preclinical models related to MS and X-linked adrenoleukodystrophy (X-ALD), a genetic disease that involves demyelination. Here we report a new series of sobetirome prodrugs containing ethanolamine-based promoieties that were found to undergo an intramolecular O,N acyl migration to form the pharmacologically relevant amide species. Several of these systemically administered prodrugs deliver more sobetirome to the brain compared to unmodified sobetirome. Pharmacokinetic properties of the parent drug sobetirome and amidoalcohol prodrug 3 are described and prodrug 3 was found to be more potent than sobetirome in target engagement in the brain from systemic dosing.

摘要

目前用于治疗脱髓鞘疾病(如多发性硬化症,MS)的治疗方法并不能刺激髓鞘修复,因此临床上需要能够促进轴突髓鞘再生的治疗药物。已知甲状腺激素在促进发育性髓鞘形成和修复中起重要作用,与内源性甲状腺激素相比,可透过中枢神经系统的拟甲状腺药物可能具有更高的治疗指数。索贝罗米是一种处于临床阶段的拟甲状腺药物,已证明其在与MS和X连锁肾上腺脑白质营养不良(X-ALD,一种涉及脱髓鞘的遗传病)相关的临床前模型中具有良好的活性。在此,我们报告了一系列新的索贝罗米前药,其含有基于乙醇胺的前体部分,发现这些前药会发生分子内O,N酰基迁移,形成具有药理活性的酰胺类物质。与未修饰的索贝罗米相比,其中几种经全身给药的前药可将更多的索贝罗米输送至大脑。描述了母体药物索贝罗米和酰胺醇前药3的药代动力学性质,发现前药3在全身给药后对大脑靶点的作用比索贝罗米更强。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3c90/5505648/67e709eaec3f/nihms865532f1.jpg

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