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首页> 外文期刊>Physiologia plantarum >Sterol partitioning by HMGR and DXR for routing intermediates toward withanolide biosynthesis
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Sterol partitioning by HMGR and DXR for routing intermediates toward withanolide biosynthesis

机译:HMGR和DXR进行的甾醇分配可将中间体路由至醇化物生物合成

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Withanolides biosynthesis in the plant Withania somnifera (L.) Dunal is hypothesized to be diverged from sterol pathway at the level of 24-methylene cholesterol. The conversion and translocation of intermediates for sterols and withanolides are yet to be characterized in this plant. To understand the influence of mevalonate (MVA) and 2-C-methyl-d-erythritol-4-phosphate (MEP) pathways on sterols and withanolides biosynthesis in planta, we overexpressed the WsHMGR2 and WsDXR2 in tobacco, analyzed the effect of transient suppression through RNAi, inhibited MVA and MEP pathways and fed the leaf tissue with different sterols. Overexpression of WsHMGR2 increased cycloartenol, sitosterol, stigmasterol and campesterol compared to WsDXR2 transgene lines. Increase in cholesterol was, however, marginally higher in WsDXR2 transgenic lines. This was further validated through transient suppression analysis, and pathway inhibition where cholesterol reduction was found higher due to WsDXR2 suppression and all other sterols were affected predominantly by WsHMGR2 suppression in leaf. The transcript abundance and enzyme analysis data also correlate with sterol accumulation. Cholesterol feeding did not increase the withanolide content compared to cycloartenol, sitosterol, stigmasterol and campesterol. Hence, a preferential translocation of carbon from MVA and MEP pathways was found differentiating the sterols types. Overall results suggested that MVA pathway was predominant in contributing intermediates for withanolides synthesis mainly through the campesterol/stigmasterol route in planta.
机译:植物中的Withanolides生物合成Withmnania somnifera(L.)Dunal被认为在24-亚甲基胆固醇水平上与固醇途径不同。固醇和withanolides的中间体的转化和易位尚未在该植物中进行表征。为了了解甲羟戊酸(MVA)和2-C-甲基-d-赤藓糖醇-4-磷酸(MEP)途径对植物中甾醇和withanolides生物合成的影响,我们在烟草中过表达了WsHMGR2和WsDXR2,分析了瞬态抑制的作用通过RNAi抑制MVA和MEP途径,并给叶组织喂食不同的固醇。与WsDXR2转基因品系相比,WsHMGR2的过表达增加了环烯醇,谷固醇,豆甾醇和菜油甾醇。但是,在WsDXR2转基因品系中,胆固醇的增加略高。这通过瞬态抑制分析和通路抑制得到了进一步验证,其中WsDXR2抑制导致胆固醇降低更高,而其他所有固醇主要受WsHMGR2抑制影响。转录本丰度和酶分析数据也与固醇积累相关。与环戊烯醇,谷固醇,豆甾醇和菜油甾醇相比,胆固醇喂养并未增加with醇含量。因此,发现了从MVA和MEP途径优先转移的碳可区分固醇类型。总体结果表明,MVA途径主要是通过植物中的菜油甾醇/豆甾醇途径为甲醇化物合成提供中间体。

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