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一组区域选择性 O-甲基转移酶导致甜罗勒中甲氧基黄酮的复杂模式。

A set of regioselective O-methyltransferases gives rise to the complex pattern of methoxylated flavones in sweet basil.

机构信息

Institute of Biological Chemistry, Washington State University, Pullman, Washington 99164, USA.

出版信息

Plant Physiol. 2012 Oct;160(2):1052-69. doi: 10.1104/pp.112.204164. Epub 2012 Aug 24.

Abstract

Polymethoxylated flavonoids occur in a number of plant families, including the Lamiaceae. To date, the metabolic pathways giving rise to the diversity of these compounds have not been studied. Analysis of our expressed sequence tag database for four sweet basil (Ocimum basilicum) lines afforded identification of candidate flavonoid O-methyltransferase genes. Recombinant proteins displayed distinct substrate preferences and product specificities that can account for all detected 7-/6-/4'-methylated, 8-unsubstituted flavones. Their biochemical specialization revealed only certain metabolic routes to be highly favorable and therefore likely in vivo. Flavonoid O-methyltransferases catalyzing 4'- and 6-O-methylations shared high identity (approximately 90%), indicating that subtle sequence changes led to functional differentiation. Structure homology modeling suggested the involvement of several amino acid residues in defining the proteins' stringent regioselectivities. The roles of these individual residues were confirmed by site-directed mutagenesis, revealing two discrete mechanisms as a basis for the switch between 6- and 4'-O-methylation of two different substrates. These findings delineate major pathways in a large segment of the flavone metabolic network and provide a foundation for its further elucidation.

摘要

多甲氧基黄酮存在于许多植物科中,包括唇形科。迄今为止,尚未研究产生这些化合物多样性的代谢途径。对我们用于四种甜罗勒(Ocimum basilicum)品系的表达序列标签数据库进行分析,提供了鉴定候选类黄酮 O-甲基转移酶基因的方法。重组蛋白显示出明显的底物偏好和产物特异性,可解释所有检测到的 7-/6-/4'-甲基化,8-未取代黄酮。它们的生化特化仅揭示了某些代谢途径是高度有利的,因此可能在体内也是如此。催化 4'-和 6-O-甲基化的类黄酮 O-甲基转移酶具有很高的同一性(约 90%),表明细微的序列变化导致了功能分化。结构同源建模表明,涉及几个氨基酸残基来确定蛋白质严格的区域选择性。通过定点诱变证实了这些单个残基的作用,揭示了两种不同底物之间 6-O-和 4'-O-甲基化之间转换的两个离散机制。这些发现描绘了黄酮代谢网络的一个大部分的主要途径,并为进一步阐明其提供了基础。

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