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Plant tropane alkaloid biosynthesis evolved independently in the Solanaceae and Erythroxylaceae

机译:植物茄碱生物碱的生物合成在茄科和赤藓科中独立发生

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摘要

The pharmacologically important tropane alkaloids have a scattered distribution among angiosperm families, like many other groups of secondary metabolites. To determine whether tropane alkaloids have evolved repeatedly in different lineages or arise from an ancestral pathway that has been lost in most lines, we investigated the tropinone-reduction step of their biosynthesis. In species of the Solanaceae, which produce compounds such as atropine and scopolamine, this reaction is known to be catalyzed by enzymes of the short-chain dehydrogenase/reductase family. However, in Erythroxylum coca (Erythroxylaceae), which accumulates cocaine and other tropane alkaloids, no proteins of the short-chain dehydrogenase/reductase family were found that could catalyze this reaction. Instead, purification of E. coca tropinone-reduction activity and cloning of the corresponding gene revealed that a protein of the aldo-keto reductase family carries out this reaction in E. coca. This protein, designated methylecgonone reductase, converts methylecgonone to methylecgonine, the penultimate step in cocaine biosynthesis. The protein has highest sequence similarity to other aldo-keto reductases, such as chalcone reductase, an enzyme of flavonoid biosynthesis, and codeinone reductase, an enzyme of morphine alkaloid biosynthesis. Methylecgonone reductase reduces methylecgonone (2-carbomethoxy-3-tropinone) stereospecifically to 2-carbomethoxy-3β-tropine (methylecgonine), and has its highest activity, protein level, and gene transcript level in young, expanding leaves of E. coca. This enzyme is not found at all in root tissues, which are the site of tropane alkaloid biosynthesis in the Solanaceae. This evidence supports the theory that the ability to produce tropane alkaloids has arisen more than once during the evolution of the angiosperms.
机译:像许多其他次生代谢物组一样,具有重要药理作用的托烷生物碱在被子植物科中分布较分散。为了确定托帕烷生物碱是在不同谱系中重复进化还是从大多数谱系中丢失的祖传途径中衍生而来,我们研究了其生物合成中的肌钙蛋白还原步骤。在茄科物种中,产生诸如阿托品和东compounds碱的化合物,该反应已知是由短链脱氢酶/还原酶家族的酶催化的。但是,在积累可卡因和其他烷烃生物碱的古柯古柯(Erythroxylumeae)中,未发现可催化该反应的短链脱氢酶/还原酶家族的蛋白质。取而代之的是,纯化古柯大肠杆菌的肌钙蛋白还原活性并克隆相应的基因表明,醛酮还原酶家族的蛋白质在古柯大肠杆菌中进行了该反应。这种蛋白质称为甲基乙酮还原酶,可卡因生物合成中的倒数第二个步骤是将甲基乙酮转化为甲基乙酮。该蛋白质与其他醛酮还原酶(如查尔酮还原酶(一种类黄酮生物合成酶)和可待因酮还原酶(一种吗啡生物碱生物合成酶))具有最高的序列相似性。甲基乙酮还原酶将甲基乙酮(2-羰基甲氧基-3-肌醇酮)立体定向还原为2-羰基甲氧基-3β-tropine(甲基己烯碱),并且在新的,扩展的古柯叶中具有最高的活性,蛋白质水平和基因转录水平。这种酶在茄科中的烷烃生物碱合成的根组织中根本没有发现。该证据支持以下理论:在被子植物的进化过程中,产生托烷生物碱的能力已经出现了不止一次。

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