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不同化学结构对甲基苯丙胺疫苗研发的影响。

Impact of distinct chemical structures for the development of a methamphetamine vaccine.

机构信息

Department of Chemistry, Skaggs Institute for Chemical Biology, 10550 N. Torrey Pines Road, La Jolla, California 92037, USA.

出版信息

J Am Chem Soc. 2011 May 4;133(17):6587-95. doi: 10.1021/ja108807j. Epub 2011 Apr 7.

Abstract

(+)-Methamphetamine (METH) use and addiction has grown at alarming rates over the past two decades, while no approved pharmacotherapy exists for its treatment. Immunopharmacotherapy has the potential to offer relief through producing highly specific antibodies that prevent drug penetration across the blood-brain barrier thus decreasing reinforcement of the behavior. Current immunotherapy efforts against methamphetamine have focused on a single hapten structure, namely linker attachment at the aromatic ring of the METH molecule. Hapten design is largely responsible for immune recognition, as it affects presentation of the target antigen and thus the quality of the response. In the current paper we report the systematic generation of a series of haptens designed to target the most stable conformations of methamphetamine as determined by molecular modeling. On the basis of our previous studies with nicotine, we show that introduction of strategic molecular constraint is able to maximize immune recognition of the target structure as evidenced by higher antibody affinity. Vaccination of GIX(+) mice with six unique METH immunoconjugates resulted in high antibody titers for three particularly promising formulations (45-108 μg/mL, after the second immunization) and high affinity (82, 130, and 169 nM for MH2, MH6, and MH7 hapten-based vaccines, respectively). These findings represent a unique approach to the design of new vaccines against methamphetamine abuse.

摘要

(+)-甲基苯丙胺(METH)的使用和成瘾在过去二十年中以惊人的速度增长,而目前尚无批准的药物疗法可用于治疗。免疫药理学有可能通过产生高度特异性的抗体来提供缓解,这些抗体可以阻止药物穿透血脑屏障,从而减少行为的强化。目前针对甲基苯丙胺的免疫疗法主要集中在单一半抗原结构上,即 METH 分子的芳环上的连接物附着。半抗原设计在免疫识别中起主要作用,因为它会影响靶抗原的呈现,从而影响反应的质量。在当前的论文中,我们报告了一系列半抗原的系统生成,这些半抗原旨在针对通过分子建模确定的最稳定的甲基苯丙胺构象。基于我们以前对尼古丁的研究,我们表明,引入战略性分子约束能够最大程度地提高对目标结构的免疫识别,这表现在抗体亲和力更高。用六种独特的 METH 免疫缀合物对 GIX(+)小鼠进行免疫接种,导致三种特别有前途的制剂产生高抗体滴度(第二次免疫后为 45-108 μg/mL)和高亲和力(MH2、MH6 和 MH7 半抗原疫苗的亲和力分别为 82、130 和 169 nM)。这些发现代表了针对甲基苯丙胺滥用设计新型疫苗的独特方法。

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