Characterization and Engineering of Two Highly Paralogous Sesquiterpene Synthases Reveal a Regioselective Reprotonation Switch

Author:

Ye Dan1ORCID,Shao Yi‐Zhen1ORCID,Li Wen‐Rui1ORCID,Cui Zhen‐Jia1ORCID,Gong Ting1ORCID,Yang Jin‐Ling1ORCID,Wang Hai‐Qiang1ORCID,Dai Jun‐Gui1ORCID,Feng Ke‐Ping1ORCID,Ma Ming2ORCID,Ma Shuang‐Gang1ORCID,Liu Yun‐Bao1ORCID,Zhu Ping13ORCID,Yu Shi‐Shan1ORCID

Affiliation:

1. State Key Laboratory of Bioactive Substance and Function of Natural Medicines Institute of Materia Medica Chinese Academy of Medical Sciences & Peking Union Medical College Beijing 100050 People's Republic of China

2. Department State Key Laboratory of Natural and Biomimetic Drugs Institution School of Pharmaceutical Sciences Peking University Beijing 100191 People's Republic of China

3. NHC Key Laboratory of Biosynthesis of Natural Products Institute of Materia Medica Chinese Academy of Medical Sciences & Peking Union Medical College Beijing 100050 People's Republic of China

Abstract

AbstractSesquiterpene synthases (STPSs) catalyze carbocation‐driven cyclization reactions that can generate structurally diverse hydrocarbons. The deprotonation‐reprotonation process is widely used in STPSs to promote structural diversity, largely attributable to the distinct regio/stereoselective reprotonations. However, the molecular basis for reprotonation regioselectivity remains largely understudied. Herein, we analyzed two highly paralogous STPSs, Artabotrys hexapetalus (−)‐cyperene synthase (AhCS) and ishwarane synthase (AhIS), which catalyze reactions that are distinct from the regioselective protonation of germacrene A (GA), resulting in distinct skeletons of 5/5/6 tricyclic (−)‐cyperene and 6/6/5/3 tetracyclic ishwarane, respectively. Isotopic labeling experiments demonstrated that these protonations occur at C3 and C6 of GA in AhCS and AhIS, respectively. The cryo‐electron microscopy‐derived AhCS complex structure provided the structural basis for identifying different key active site residues that may govern their functional disparity. The structure‐guided mutagenesis of these residues resulted in successful functional interconversion between AhCS and AhIS, thus targeting the three active site residues [L311‐S419‐C458]/[M311‐V419‐A458] that may act as a C3/C6 reprotonation switch for GA. These findings facilitate the rational design or directed evolution of STPSs with structurally diverse skeletons.

Publisher

Wiley

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