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鉴定迷幻鼠尾草中细胞色素 P450(CYP728D26)修饰的 clerodane 二萜 - 通向精神活性 salvinorin A 的生物合成。

Identification of clerodane diterpene modifying cytochrome P450 (CYP728D26) in Salvia divinorum - en route to psychotropic salvinorin A biosynthesis.

机构信息

Department of Biological Sciences, University of Calgary, 2500 University Dr. NW, Calgary, Alberta, Canada.

The Metabolomics Innovation Centre and Department of Chemistry, University of Alberta, Edmonton, Alberta, Canada.

出版信息

Physiol Plant. 2024 Sep-Oct;176(5):e14569. doi: 10.1111/ppl.14569.

DOI:10.1111/ppl.14569
PMID:39377159
Abstract

Salvia divinorum is a hallucinogenic plant native to the Oaxaca in Mexico. The active ingredient for psychotropic effects in this plant is salvinorin A, a potent and highly selective κ-opioid receptor agonist. Salvinorin A is distinct from other well-known opioids, such as morphine and codeine, in that it is a non-nitrogenous diterpenoid with no affinity for μ-opioid receptor, the prime receptor of alkaloidal opioids. A terpene opioid that selectively targets a new opioid receptor (κ-opioid receptor) can be instrumental in developing alternative analgesics. Elucidation of the salvinorin A biosynthetic pathway can help bio-manufacture diverse semi-synthetic derivatives of salvinorin A but, to date, only two enzymes in the Salvinorin A pathway have been identified. Here, we identify CYP728D26 that catalyzes a C18 oxygenation on crotonolide G, which bears a clerodane backbone. Biochemical identity of CYP728D26 was validated by in vivo reconstitution in yeast, H- and C-NMR analyses of the purified product, and kinetic analysis of CYP728D26 with a K value of 13.9 μM. Beyond the single oxygenation on C18, collision-induced dissociation analysis suggested two additional oxygenations are catalyzed by CYP728D26 to form crotonoldie G acid, although this carboxylic acid form is a minor product. Its close homologue CYP728D25 exhibited a C1-hydroxylation on the clerodane backbone in a reconstituted yeast system. However, CYP728D25 showed no activity in in vitro assays. This result implies that catalytic activities observed from overexpression systems should be interpreted cautiously. This work identified a new CYP catalyst and advanced our knowledge of salvinorin A biosynthesis.

摘要

迷幻鼠尾草是一种原产于墨西哥瓦哈卡的致幻植物。该植物中产生致幻作用的活性成分是 Salvinorin A,它是一种强效且高度选择性的 κ-阿片受体激动剂。Salvinorin A 与其他著名的阿片类药物(如吗啡和可待因)不同,它是一种不含氮的二萜,对阿片类生物碱的主要受体 μ-阿片受体没有亲和力。一种对新型阿片受体(κ-阿片受体)具有选择性的萜类阿片类药物,可以为开发替代镇痛剂提供帮助。阐明 Salvinorin A 的生物合成途径有助于生物制造 Salvinorin A 的各种半合成衍生物,但迄今为止,Salvinorin A 途径中仅鉴定出两种酶。在这里,我们鉴定出 CYP728D26,它催化克罗酮内酯 G 上的 C18 氧化,该内酯 G 具有 clerodane 骨架。CYP728D26 的生化特性通过在酵母体内的体内重建、对纯化产物的 H-NMR 和 C-NMR 分析以及对 CYP728D26 的动力学分析得到验证,其 K 值为 13.9 μM。除了 C18 上的单一氧化外,碰撞诱导解离分析表明 CYP728D26 还催化了另外两次氧化,形成克罗酮酸 G,尽管这种羧酸形式是次要产物。其密切同源物 CYP728D25 在重组酵母系统中对 clerodane 骨架进行 C1-羟化。然而,CYP728D25 在体外测定中没有活性。这一结果表明,从过表达系统观察到的催化活性应谨慎解释。这项工作鉴定了一种新的 CYP 催化剂,并提高了我们对 Salvinorin A 生物合成的认识。

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