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Evolution of Cinnamate/p-Coumarate Carboxyl Methyltransferases and Their Role in the Biosynthesis of Methylcinnamate[W]

机译:肉桂酸/对香豆酸酯羧甲基转移酶的进化及其在肉桂酸甲酯生物合成中的作用[W]

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摘要

Methylcinnamate, which is widely distributed throughout the plant kingdom, is a significant component of many floral scents and an important signaling molecule between plants and insects. Comparison of an EST database obtained from the glandular trichomes of a basil (Ocimum basilicum) variety that produces high levels of methylcinnamate (line MC) with other varieties producing little or no methylcinnamate identified several very closely related genes belonging to the SABATH family of carboxyl methyltransferases that are highly and almost exclusively expressed in line MC. Biochemical characterization of the corresponding recombinant proteins showed that cinnamate and p-coumarate are their best substrates for methylation, thus designating these enzymes as cinnamate/p-coumarate carboxyl methyltransferases (CCMTs). Gene expression, enzyme activity, protein profiling, and metabolite content analyses demonstrated that CCMTs are responsible for the formation of methylcinnamate in sweet basil. A phylogenetic analysis of the entire SABATH family placed these CCMTs into a clade that includes indole-3-acetic acid carboxyl methyltransferases and a large number of uncharacterized carboxyl methyltransferase–like proteins from monocots and lower plants. Structural modeling and ligand docking suggested active site residues that appear to contribute to the substrate preference of CCMTs relative to other members of the SABATH family. Site-directed mutagenesis of specific residues confirmed these findings.
机译:肉桂酸甲酯广泛分布于整个植物界,是许多花香的重要成分,也是植物和昆虫之间的重要信号分子。从罗勒(Ocimum basilicum)品种的腺毛中获得的EST数据库进行比较,该品种的罗勒产生了高水平的肉桂酸甲酯(MC系),与其他品种产生的肉桂酸几乎没有或几乎没有,而鉴定出了几个与SABATH羧基甲基转移酶家族密切相关的基因在MC行中高度且几乎全部表示出来。相应重组蛋白的生化特性表明,肉桂酸酯和对香豆酸酯是它们甲基化的最佳底物,因此将这些酶指定为肉桂酸酯/对香豆酸酯羧甲基转移酶(CCMT)。基因表达,酶活性,蛋白质谱分析和代谢物含量分析表明,CCMT负责甜罗勒中肉桂酸甲酯的形成。对整个SABATH家族进行的系统发育分析将这些CCMT放入了进化枝,其中包括吲哚-3-乙酸羧甲基转移酶和大量来自单子叶植物和低等植物的未表征的羧甲基转移酶样蛋白。结构建模和配体对接表明,相对于SABATH家族的其他成员,活性位点残基似乎有助于CCMT的底物偏爱。特定残基的定点诱变证实了这些发现。

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