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甲基茉莉酮酸诱导的甜罗勒转录反应和五环三萜生物合成。

Methyl jasmonate-elicited transcriptional responses and pentacyclic triterpene biosynthesis in sweet basil.

机构信息

Biotechnology Division , Central Institute of Medicinal and Aromatic Plants, Lucknow 226015, India.

出版信息

Plant Physiol. 2014 Feb;164(2):1028-44. doi: 10.1104/pp.113.232884. Epub 2013 Dec 23.

Abstract

Sweet basil (Ocimum basilicum) is well known for its diverse pharmacological properties and has been widely used in traditional medicine for the treatment of various ailments. Although a variety of secondary metabolites with potent biological activities are identified, our understanding of the biosynthetic pathways that produce them has remained largely incomplete. We studied transcriptional changes in sweet basil after methyl jasmonate (MeJA) treatment, which is considered an elicitor of secondary metabolites, and identified 388 candidate MeJA-responsive unique transcripts. Transcript analysis suggests that in addition to controlling its own biosynthesis and stress responses, MeJA up-regulates transcripts of the various secondary metabolic pathways, including terpenoids and phenylpropanoids/flavonoids. Furthermore, combined transcript and metabolite analysis revealed MeJA-induced biosynthesis of the medicinally important ursane-type and oleanane-type pentacyclic triterpenes. Two MeJA-responsive oxidosqualene cyclases (ObAS1 and ObAS2) that encode for 761- and 765-amino acid proteins, respectively, were identified and characterized. Functional expressions of ObAS1 and ObAS2 in Saccharomyces cerevisiae led to the production of β-amyrin and α-amyrin, the direct precursors of oleanane-type and ursane-type pentacyclic triterpenes, respectively. ObAS1 was identified as a β-amyrin synthase, whereas ObAS2 was a mixed amyrin synthase that produced both α-amyrin and β-amyrin but had a product preference for α-amyrin. Moreover, transcript and metabolite analysis shed light on the spatiotemporal regulation of pentacyclic triterpene biosynthesis in sweet basil. Taken together, these results will be helpful in elucidating the secondary metabolic pathways of sweet basil and developing metabolic engineering strategies for enhanced production of pentacyclic triterpenes.

摘要

甜罗勒(Ocimum basilicum)以其多样的药理特性而闻名,已被广泛用于传统医学治疗各种疾病。尽管已经鉴定出多种具有强大生物活性的次生代谢物,但我们对产生这些代谢物的生物合成途径的理解仍基本不完整。我们研究了甜罗勒在茉莉酸甲酯(MeJA)处理后的转录变化,MeJA 被认为是次生代谢物的诱导剂,并鉴定出 388 个候选 MeJA 响应的独特转录本。转录分析表明,除了控制自身的生物合成和应激反应外,MeJA 还上调了各种次生代谢途径的转录本,包括萜类化合物和苯丙素类/类黄酮。此外,结合转录物和代谢物分析揭示了 MeJA 诱导的具有重要药用价值的乌苏烷型和齐墩果烷型五环三萜的生物合成。鉴定并表征了两个 MeJA 响应的角鲨烯环化酶(ObAS1 和 ObAS2),它们分别编码 761-和 765 个氨基酸的蛋白质。ObAS1 和 ObAS2 在酿酒酵母中的功能表达导致了 β-香树脂醇和 α-香树脂醇的产生,分别是齐墩果烷型和乌苏烷型五环三萜的直接前体。ObAS1 被鉴定为 β-香树脂醇合酶,而 ObAS2 是一种混合的香树脂醇合酶,既能产生 α-香树脂醇又能产生 β-香树脂醇,但对 α-香树脂醇的产物有偏好。此外,转录物和代谢物分析揭示了甜罗勒中五环三萜生物合成的时空调控。总之,这些结果将有助于阐明甜罗勒的次生代谢途径,并开发用于增强五环三萜生产的代谢工程策略。

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