Insights into taxadiene synthase catalysis and promiscuity facilitated by mutability landscape and molecular dynamics

Siqi He; Ingy I Abdallah; Ronald van Merkerk; Wim J Quax

doi:10.1007/s00425-024-04363-9

Insights into taxadiene synthase catalysis and promiscuity facilitated by mutability landscape and molecular dynamics

Planta. 2024 Mar 9;259(4):87. doi: 10.1007/s00425-024-04363-9.

Authors

Siqi He^#¹, Ingy I Abdallah^#^{1

2}, Ronald van Merkerk¹, Wim J Quax³

Affiliations

¹ Department of Chemical and Pharmaceutical Biology, Groningen Research Institute of Pharmacy, University of Groningen, Antonius Deusinglaan 1, 9713 AV, Groningen, The Netherlands.
² Department of Pharmacognosy, Faculty of Pharmacy, Alexandria University, Alexandria, Egypt.
³ Department of Chemical and Pharmaceutical Biology, Groningen Research Institute of Pharmacy, University of Groningen, Antonius Deusinglaan 1, 9713 AV, Groningen, The Netherlands. w.j.quax@rug.nl.

^# Contributed equally.

Abstract

Protein modeling, carbocation docking, and molecular dynamics along with structure-based mutability landscapes provided insight into taxadiene synthase catalysis (first step of the anticancer Taxol biosynthesis), protein structure-function correlations, and promiscuity. Plant terpenes belong to one of the largest and most diverse classes of natural products. This diversity is driven by the terpene synthase enzyme family which comprises numerous different synthases, several of which are promiscuous. Taxadiene synthase (TXS) is a class I diterpene synthase that catalyzes the first step in the biosynthesis pathway of the diterpene Taxol, an anticancer natural product produced by the Taxus plant. Exploring the molecular basis of TXS catalysis and its promiscuous potential garnered interest as a necessary means for understanding enzyme evolution and engineering possibilities to improve Taxol biosynthesis. A catalytically active closed conformation TXS model was designed using the artificial intelligence system, AlphaFold, accompanied by docking and molecular dynamics simulations. In addition, a mutability landscape of TXS including 14 residues was created to probe for structure-function relations. The mutability landscape revealed no mutants with improved catalytic activity compared to wild-type TXS. However, mutations of residues V584, Q609, V610, and Y688 showed high degree of promiscuity producing cembranoid-type and/or verticillene-type major products instead of taxanes. Mechanistic insights into V610F, V584M, Q609A, and Y688C mutants compared to the wild type revealed the trigger(s) for product profile change. Several mutants spanning residues V584, Q609, Y688, Y762, Q770, and F834 increased production of taxa-4(20),11(12)-diene which is a more favorable substrate for Taxol production compared to taxa-4(5),11(12)-diene. Finally, molecular dynamics simulations of the TXS reaction cascade revealed residues involved in ionization, carbocation stabilization, and cyclization ushering deeper understanding of the enzyme catalysis mechanism.

Keywords: AlphaFold model; Catalytic activity; Mutagenesis; Product profile; Terpenoid.

MeSH terms

Artificial Intelligence
Catalysis
Diterpenes* / metabolism
Isomerases*
Molecular Dynamics Simulation*
Paclitaxel

Substances

taxa-4(5),11(12)-diene synthase
Paclitaxel
Diterpenes
Isomerases