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人体细胞中吗啡的内源性形成。

Endogenous formation of morphine in human cells.

作者信息

Poeaknapo Chotima, Schmidt Jürgen, Brandsch Matthias, Dräger Birgit, Zenk Meinhart H

机构信息

Biocenter, Martin Luther University Halle-Wittenberg, Weinbergweg 22, 06120 Halle, Germany.

出版信息

Proc Natl Acad Sci U S A. 2004 Sep 28;101(39):14091-6. doi: 10.1073/pnas.0405430101. Epub 2004 Sep 21.

Abstract

Morphine is a plant (opium poppy)-derived alkaloid and one of the strongest known analgesic compounds. Studies from several laboratories have suggested that animal and human tissue or fluids contain trace amounts of morphine. Its origin in mammals has been believed to be of dietary origin. Here, we address the question of whether morphine is of endogenous origin or derived from exogenous sources. Benzylisoquinoline alkaloids present in human neuroblastoma cells (SH-SY5Y) and human pancreas carcinoma cells (DAN-G) were identified by GC/tandem MS (MS/MS) as norlaudanosoline (DAN-G), reticuline (DAN-G and SH-SY5Y), and morphine (10 nM, SH-SY5Y). The stereochemistry of reticuline was determined to be 1-(S). Growth of the SH-SY5Y cell line in the presence of (18)O(2) led to the [(18)O]-labeled morphine that had the molecular weight 4 mass units higher than if grown in (16)O(2), indicating the presence of two atoms of (18)O per molecule of morphine. Growth of DAN-G cells in an (18)O(2) atmosphere yielded norlaudanosoline and (S)-reticuline, both labeled at only two of the four oxygen atoms. This result clearly demonstrates that all three alkaloids are of biosynthetic origin and suggests that norlaudanosoline and (S)-reticuline are endogenous precursors of morphine. Feeding of [ring-(13)C(6)]-tyramine, [1-(13)C, N-(13)CH(3)]-(S)-reticuline and [N-CD(3)]-thebaine to the neuroblastoma cells led each to the position-specific labeling of morphine, as established by GC/MS/MS. Without doubt, human cells can produce the alkaloid morphine. The studies presented here serve as a platform for the exploration of the function of "endogenous morphine" in the neurosciences and immunosciences.

摘要

吗啡是一种源自植物(罂粟)的生物碱,是已知最强的镇痛化合物之一。多个实验室的研究表明,动物和人体组织或体液中含有微量吗啡。人们一直认为其在哺乳动物体内的来源是饮食摄入。在此,我们探讨吗啡是内源性来源还是外源性来源的问题。通过气相色谱/串联质谱(MS/MS)在人神经母细胞瘤细胞(SH-SY5Y)和人胰腺癌细胞(DAN-G)中鉴定出的苄基异喹啉生物碱为去甲劳丹碱(DAN-G)、网叶番荔枝碱(DAN-G和SH-SY5Y)以及吗啡(10 nM,SH-SY5Y)。网叶番荔枝碱的立体化学结构确定为1-(S)型。在含有(18)O(2)的条件下培养SH-SY5Y细胞系,产生了分子量比在(16)O(2)中培养时高4个质量单位的[(18)O]标记吗啡,这表明每个吗啡分子含有两个(18)O原子。在(18)O(2)气氛中培养DAN-G细胞,产生了去甲劳丹碱和(S)-网叶番荔枝碱,二者仅在四个氧原子中的两个被标记。这一结果清楚地表明,所有这三种生物碱均为生物合成来源,并表明去甲劳丹碱和(S)-网叶番荔枝碱是吗啡的内源性前体。向神经母细胞瘤细胞喂食[环-(13)C(6)]-酪胺、[1-(13)C, N-(13)CH(3)]-(S)-网叶番荔枝碱和[N-CD(3)]-蒂巴因,经气相色谱/质谱/质谱测定,每种物质均导致吗啡发生位置特异性标记。毫无疑问,人体细胞能够产生生物碱吗啡。本文所呈现的研究为探索“内源性吗啡”在神经科学和免疫科学中的功能提供了一个平台。

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