AI Article Synopsis

  • In-depth studies have shown that half-of-the-sites activity is influenced by structural asymmetry from cooperative motion, but recent research suggests subunit-intrinsic properties also play a role.
  • By using all-atom molecular dynamics simulations on specific enzymes, the research shows that structural fluctuation can induce structural asymmetry, indicating this could be a common aspect of half-of-the-sites activity across enzymes.

Article Abstract

Enzymatic activity is regulated by various mechanisms to ensure biologically proper functions. Notable instances of such regulation in homodimeric enzymes include "all-of-the-sites activity" and "half-of-the-sites activity". The difference in these activities lies in whether one or both of the subunits are simultaneously active. Owing to its uniqueness, the mechanism of half-of-the-sites activity has been widely investigated. Consequently, structural asymmetry derived from cooperative motion is considered to induce half-of-the-sites activity. In contrast, recent investigations have suggested that subunit-intrinsic properties or structural fluctuation also induces structural asymmetry. Hence, the mechanism underlying half-of-the-sites activity has not been completely elucidated. Additionally, most previous studies have focused only on half-of-the-sites activity. Therefore, by comparing the structural and dynamical properties of two representative homodimers exhibiting all-of-the-sites and half-of-the-sites activities, respectively, we attempted to elucidate the mechanism of half-of-the-sites activity. Specifically, all-atom molecular dynamics simulations were applied to lysyl-tRNA synthetase and tyrosyl-tRNA synthetase. Our analysis revealed that structural fluctuation is sufficient to induce structural asymmetry in addition to the well-established factor of cooperative motion. Considering that structural fluctuation is a common characteristic of any enzyme, it could be a general factor in half-of-the-sites activity.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11551958PMC
http://dx.doi.org/10.1021/acs.jpcb.4c05191DOI Listing

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