2026-04-13T00:57:23Zhttps://recercat.cat/oai/request

oai:recercat.cat:10256/232352024-06-18T13:58:25Zcom_2072_452955com_2072_2054col_2072_453073

RECERCAT author Maria-Solano, Miguel A. author Iglesias-Fernández, Javier author Osuna Oliveras, Sílvia 2024-06-18T13:58:25Z 2024-06-18T13:58:25Z 2019-07-29 http://hdl.handle.net/10256/23235 Multimeric enzyme complexes are ubiquitous in nature and catalyze a broad range of useful biological transformations. They are often characterized by a tight allosteric coupling between subunits, making them highly inefficient when isolated. A good example is Tryptophan synthase (TrpS), an allosteric heterodimeric enzyme in the form of an αββα complex that catalyzes the biosynthesis of L-tryptophan. In this study, we decipher the allosteric regulation existing in TrpS from Pyrococcus furiosus (PfTrpS), and how the allosteric conformational ensemble is recovered in laboratory-evolved stand-alone β-subunit variants. We find that recovering the conformational ensemble of a subdomain of TrpS affecting the relative stabilities of open, partially closed, and closed conformations is a prerequisite for enhancing the catalytic efficiency of the β-subunit in the absence of its binding partner. The distal mutations resuscitate the allosterically driven conformational regulation and alter the populations and rates of exchange between these multiple conformational states, which are essential for the multistep reaction pathway of the enzyme. Interestingly, these distal mutations can be a priori predicted by careful analysis of the conformational ensemble of the TrpS enzyme through computational methods. Our study provides the enzyme design field with a rational approach for evolving allosteric enzymes toward improved stand-alone function for biosynthetic applicationsWe thank the Generalitat de Catalunya for the emerging group CompBioLab (2017 SGR-1707) and Spanish MINECO for project PGC2018-102192-B-I00. We are grateful for the computer resources, technical expertise, and assistance provided by the Barcelona Supercomputing Center - Cen-tro Nacional de Supercomputación. M. A. M. S. was sup-ported by the Spanish MINECO for a PhD fellowship (BES-2015-074964), J. I. F. was supported by the European Community for Marie Curie fellowship (H2020-MSCA-IF-2016-753045). S.O. is grateful to the funding from the Eu-ropean Research Council (ERC) under the European Un-ion’s Horizon 2020 research and innovation program (ERC-2015-StG-679001) Tots els drets reservats info:eu-repo/semantics/openAccess Enzims Enzymes Deciphering the Allosterically Driven Conformational Ensemble in Tryptophan Synthase Evolution info:eu-repo/semantics/article info:eu-repo/semantics/acceptedVersion peer-reviewed