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巯基-(+)-甲基苯丙胺半抗原的合成及其在提高 (+)-甲基苯丙胺缀合物疫苗表位密度中的应用。

Synthesis of mercapto-(+)-methamphetamine haptens and their use for obtaining improved epitope density on (+)-methamphetamine conjugate vaccines.

机构信息

Center for Organic and Medicinal Chemistry, Research Triangle Institute, P.O. Box 12194, Research Triangle Park, North Carolina 27709, USA.

出版信息

J Med Chem. 2011 Jul 28;54(14):5221-8. doi: 10.1021/jm2004943. Epub 2011 Jun 29.

Abstract

This study reports the synthesis of the mercapto-hapten (S)-N-(2-(mercaptoethyl)-6-(3-(2-(methylamino)propyl)phenoxy)hexanamide [3, (+)-METH HSMO9] and its use to prepare METH-conjugated vaccines (MCV) from maleimide-activated proteins. MALDI-TOF mass spectrometry analysis of the MCV synthesized using 3 showed there was a high and controllable epitope density on two different carrier proteins. In addition, the MCV produced a substantially greater immunological response in mice than previous METH haptens, and a monoclonal antibody generated from this MCV in mice showed a very high affinity for (+)-METH (K(D) = 6.8 nM). The efficient covalent coupling of (+)-METH HSMO9 to the activated carrier proteins suggests that this approach could be cost-effective for large-scale production of MCV. In addition, the general methods described for the synthesis of (+)-METH HSMO9 (3) and its use to synthesize MCV will be applicable for conjugated vaccines of small molecules and other substances of abuse such as morphine, nicotine, and cocaine.

摘要

本研究报告了巯基半抗原 (S)-N-(2-(巯基乙基)-6-(3-(2-(甲基氨基)丙基)苯氧基)己酰胺[3, (+)-METH HSMO9]的合成及其用于从马来酰亚胺活化的蛋白质制备 METH 结合疫苗 (MCV)。使用 3 合成的 MCV 的 MALDI-TOF 质谱分析表明,两种不同载体蛋白上的表位密度高且可控。此外,与以前的 METH 半抗原相比,该 MCV 在小鼠中产生了更大的免疫反应,并且从小鼠中产生的针对该 MCV 的单克隆抗体对 (+)-METH 表现出非常高的亲和力 (K(D) = 6.8 nM)。(+)-METH HSMO9 与活化载体蛋白的有效共价偶联表明,这种方法可能对 MCV 的大规模生产具有成本效益。此外,用于合成 (+)-METH HSMO9 (3)及其用于合成 MCV 的一般方法将适用于吗啡、尼古丁和可卡因等小分子和其他滥用物质的共轭疫苗。

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