Molecular insights into the catalytic promiscuity of a bacterial diterpene synthase

Author:

Li Zhong,Zhang Lilan,Xu KangweiORCID,Jiang Yuanyuan,Du Jieke,Zhang XingwangORCID,Meng Ling-Hong,Wu Qile,Du Lei,Li Xiaoju,Hu Yuechan,Xie Zhenzhen,Jiang Xukai,Tang Ya-Jie,Wu RuiboORCID,Guo Rey-TingORCID,Li ShengyingORCID

Abstract

AbstractDiterpene synthase VenA is responsible for assembling venezuelaene A with a unique 5-5-6-7 tetracyclic skeleton from geranylgeranyl pyrophosphate. VenA also demonstrates substrate promiscuity by accepting geranyl pyrophosphate and farnesyl pyrophosphate as alternative substrates. Herein, we report the crystal structures of VenA in bothapoform andholoform in complex with a trinuclear magnesium cluster and pyrophosphate group. Functional and structural investigations on the atypical115DSFVSD120motif of VenA,versusthe canonical Asp-rich motif of DDXX(X)D/E, reveal that the absent second Asp of canonical motif is functionally replaced by Ser116 and Gln83, together with bioinformatics analysis identifying a hidden subclass of type I microbial terpene synthases. Further structural analysis, multiscale computational simulations, and structure-directed mutagenesis provide significant mechanistic insights into the substrate selectivity and catalytic promiscuity of VenA. Finally, VenA is semi-rationally engineered into a sesterterpene synthase to recognize the larger substrate geranylfarnesyl pyrophosphate.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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