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方便地从 R-(-)-和 S-(+)-N-甲基-α-甲基去甲肾上腺素前体合成光学活性的 MDMA(“摇头丸”)潜在神经毒性代谢物。

A convenient biomimetic synthesis of optically active putative neurotoxic metabolites of MDMA ("ecstasy") from R-(-)- and S-(+)-N-methyl-α-methyldopamine precursors.

机构信息

UMR 8638 CNRS-Université Paris Descartes, Synthèse et Structure de Molécules d'Intérêt Pharmacologique, Faculté des Sciences Pharmaceutiques et Biologiques, Paris, France.

出版信息

Org Biomol Chem. 2012 May 14;10(18):3739-48. doi: 10.1039/c2ob25245g. Epub 2012 Mar 28.

DOI:10.1039/c2ob25245g
PMID:22456797
Abstract

(±)-3,4-Methylenedioxymethamphetamine (MDMA, also known as "ecstasy") is a psychoactive drug with selective neurotoxic potential toward brain serotonin (5-HT) neurons. One hypothesis holds that MDMA neurotoxicity may at least partially be a consequence of its metabolism. In most species (including primates), O-demethylenated MDMA metabolites such as N-methyl-α-methyldopamine (HHMA) have been postulated to serve as precursors for toxic thioether conjugates. As yet, chirality of MDMA was not considered in previously reported in vivo studies because HHMA was used as the racemate. Since the stereochemistry of this chiral drug needs to be considered, the total synthesis of enantiomerically pure precursors, R-(-)-HHMA and S-(+)-HHMA, was envisioned with the ultimate goal to prepare substantial amounts of optically active thioether conjugates. Recently, we reported the first total synthesis of the R-enantiomer. In this paper, a novel synthesis of the S-enantiomer is described, in 45% overall yield (six steps) and 99% ee, using commercially available l-Boc-alanine (99% ee) as the chiral source. Having at our disposal suitable amounts of R-(-)-HHMA and S-(+)-HHMA precursors, a straightforward one-pot electrochemical procedure has been further developed for the synthesis of several catechol-thioether conjugates in acceptable yields (40-53%) and high degree of purity (99%), with complete diastereoselectivity. The availability of these newly synthesized optically active catechol-thioether conjugates is crucial for ongoing future in vivo studies about their role in MDMA neurotoxicity.

摘要

(±)-3,4-亚甲二氧基甲基苯丙胺(MDMA,也称为“摇头丸”)是一种具有选择性神经毒性的精神活性药物,对大脑 5-羟色胺(5-HT)神经元具有潜在毒性。一种假设认为,MDMA 的神经毒性至少部分是由于其代谢产物。在大多数物种(包括灵长类动物)中,人们推测 O-去甲甲基 MDMA 代谢物,如 N-甲基-α-甲基多巴胺(HHMA),可作为有毒硫醚结合物的前体。然而,由于 HHMA 被用作外消旋体,以前的体内研究中并未考虑 MDMA 的手性。由于需要考虑这种手性药物的立体化学,因此设想了对映体纯前体 R-(-)-HHMA 和 S-(+)-HHMA 的全合成,最终目标是制备大量的手性硫醚结合物。最近,我们报道了 R-对映体的首次全合成。在本文中,描述了 S-对映体的一种新合成方法,总收率为 45%(六步),ee 值为 99%,使用商业可得的 l-Boc-丙氨酸(99%ee)作为手性源。由于我们拥有足够数量的 R-(-)-HHMA 和 S-(+)-HHMA 前体,因此进一步开发了一种简单的一锅电化学方法,以可接受的产率(40-53%)和高纯度(99%)合成了几种儿茶酚硫醚结合物,具有完全的非对映选择性。这些新合成的手性儿茶酚硫醚结合物的可用性对于正在进行的关于其在 MDMA 神经毒性中的作用的体内研究至关重要。

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