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手性毛细管电泳-质谱法分析四氢异喹啉衍生的神经毒素:复杂立体异构现象的观察。

Chiral capillary electrophoresis-mass spectrometry of tetrahydroisoquinoline-derived neurotoxins: observation of complex stereoisomerism.

机构信息

Department of Chemistry and Biochemistry, Jackson State University, Jackson, MS 39110, USA.

出版信息

J Chromatogr A. 2011 May 20;1218(20):3118-23. doi: 10.1016/j.chroma.2011.03.026. Epub 2011 Mar 21.

Abstract

Previous studies have shown that certain 1,2,3,4-tetrahydroisoquinoline derivatives (TIQs) are neurotoxins inducing Parkinsonism. Further, individual enantiomers of these toxins such as (R/S)-N-methylsalsolinol ((R/S)-NMSal) possess distinct neurotoxicological properties. In this work, a chiral capillary electrophoresis (CE) method with electrospray ionization-tandem mass spectrometric (ESI-MS/MS) detection was developed for the quantification of TIQ enantiomers. Enantioseparation was achieved with sulfated β-cyclodextrin (sulfated β-CD) as chiral selector. To avoid any potential contamination of MS ionization source by the non-volatile chiral selector, partial filling technique was deployed in the CE separation. TIQ derivatives, including (R/S)-6,7-dihydroxy-1-methy-TIQ (salsolinol, Sal), (R/S)-1-benzyl-TIQ (BTIQ), and (R/S)-NMSal, were base-line resolved with resolution values (R) ranging from 3 (for Sal) to 4.5 (for BTIQ), which were much better than those reported previously by HPLC methods. ESI-MS/MS detection of the resolved TIQ enantiomers was specific and sensitive (LOD=1.2 μM for Sal enantiomers). The proposed chiral CE-MS/MS method was used to study in vitro formation of (R/S)-NMSal. It was found that NMSal was formed from the incubation of epinine (a dopamine metabolite) with acetaldehyde (a metabolite of alcohol). More interestingly, four isomers of NMSal were separated and detected in the incubation solution. They were identified as (R)-e.e-NMSal, (R)-e.a-NMSal, (S)-e.e-NMSal, and (S)-e.a-NMSal. This was the first lab evidence that this Parkinsonian neurotoxin exists in multiple isomeric forms.

摘要

先前的研究表明,某些 1,2,3,4-四氢异喹啉衍生物(TIQs)是诱导帕金森病的神经毒素。此外,这些毒素的单个对映异构体,如(R/S)-N-甲基萨尔索利诺尔((R/S)-NMSal),具有不同的神经毒理学特性。在这项工作中,开发了一种手性毛细管电泳(CE)方法,结合电喷雾电离串联质谱(ESI-MS/MS)检测,用于 TIQ 对映异构体的定量。使用硫酸化β-环糊精(硫酸化β-CD)作为手性选择剂实现对映体分离。为了避免非挥发性手性选择剂对 MS 离子源的任何潜在污染,在 CE 分离中采用了部分填充技术。TIQ 衍生物,包括(R/S)-6,7-二羟基-1-甲基-TIQ(萨索利诺尔,Sal)、(R/S)-1-苄基-TIQ(BTIQ)和(R/S)-NMSal,均得到基线分离,分辨率值(R)范围从 3(Sal)到 4.5(BTIQ),优于先前 HPLC 方法报道的值。分离的 TIQ 对映异构体的 ESI-MS/MS 检测具有特异性和灵敏度(Sal 对映异构体的 LOD=1.2 μM)。所提出的手性 CE-MS/MS 方法用于研究体外(R/S)-NMSal 的形成。结果发现,NMSal 是由去甲肾上腺素(多巴胺代谢物)与乙醛(酒精代谢物)孵育形成的。更有趣的是,在孵育溶液中分离并检测到四种 NMSal 异构体。它们被鉴定为(R)-e.e-NMSal、(R)-e.a-NMSal、(S)-e.e-NMSal 和(S)-e.a-NMSal。这是第一个实验室证据,证明这种帕金森病神经毒素存在多种异构体形式。

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