Structure Report for: 5K3F

Pedram Mehrabi, Tae Hun Kim, Scott R. Prosser, Emil F. Pai

Title: The role of dimer asymmetry and protomer dynamics in enzyme catalysis
Kim TH, Mehrabi P, Ren Z, Sljoka A, Ing C, Bezginov A, Ye L, Pomes R, Prosser RS, Pai EF
Ref: Science, 355:, 2017 : PubMed
Abstract


ESTHER: Kim_2017_Science_355_
PubMedSearch: Kim 2017 Science 355
PubMedID: 28104837
Gene_locus related to this paper: rhopa-q6nam1

Abstract

Freeze-trapping x-ray crystallography, nuclear magnetic resonance, and computational techniques reveal the distribution of states and their interconversion rates along the reaction pathway of a bacterial homodimeric enzyme, fluoroacetate dehalogenase (FAcD). The crystal structure of apo-FAcD exhibits asymmetry around the dimer interface and cap domain, priming one protomer for substrate binding. This asymmetry is dynamically averaged through conformational exchange on a millisecond time scale. During catalysis, the protomer conformational exchange rate becomes enhanced, the empty protomer exhibits increased local disorder, and water egresses. Computational studies identify allosteric pathways between protomers. Water release and enhanced dynamics associated with catalysis compensate for entropic losses from substrate binding while facilitating sampling of the transition state. The studies provide insights into how substrate-coupled allosteric modulation of structure and dynamics facilitates catalysis in a homodimeric enzyme.