| Literature DB >> 30895623 |
Jiawei Zhou1,2, Tianyuan Hu2, Linhui Gao1, Ping Su3, Yifeng Zhang2, Yujun Zhao3, Shang Chen1, Lichan Tu2, Yadi Song1, Xing Wang1, Luqi Huang3, Wei Gao1,2,4.
Abstract
Celastrol is a promising bioactive compound isolated from Tripterygium wilfordii and has been shown to possess many encouraging preclinical applications. However, the celastrol biosynthetic pathway is poorly understood, especially the key oxidosqualene cyclase (OSC) enzyme responsible for cyclisation of the main scaffold. Here, we report on the isolation and characterisation of three OSCs from T. wilfordii: TwOSC1, TwOSC2 and TwOSC3. Both TwOSC1 and TwOSC3 were multiproduct friedelin synthases, while TwOSC2 was a β-amyrin synthase. We further found that TwOSC1 and TwOSC3 were involved in the biosynthesis of celastrol and that their common product, friedelin, was a precursor of celastrol. We then reconstituted the biosynthetic pathway of friedelin in engineered yeast constructed by the CRISPR/Cas9 system, with protein modification and medium optimisation, leading to heterologous production of friedelin at 37.07 mg l-1 in a shake flask culture. Our study was the first to identify the genes responsible for biosynthesis of the main scaffold of celastrol and other triterpenes in T. wilfordii. As friedelin has been found in many plants, the results and approaches described here have laid a solid foundation for further explaining the biosynthesis of celastrol and related triterpenoids. Moreover, our results provide insights for metabolic engineering of friedelane-type triterpenes.Entities:
Keywords: zzm321990Tripterygium wilfordiizzm321990; biosynthesis; celastrol; oxidosqualene cyclases (OSC); triterpenes
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Year: 2019 PMID: 30895623 DOI: 10.1111/nph.15809
Source DB: PubMed Journal: New Phytol ISSN: 0028-646X Impact factor: 10.151