AI Article Synopsis

  • Rev-Erbβ is a nuclear receptor that links circadian rhythm, metabolism, and inflammation, with heme binding playing a crucial role in its function.
  • The study reveals that Rev-Erbβ maintains an Fe form in the cell, allowing it to remain heme-filled even at low heme levels, which is important for its gas-sensing role.
  • The findings suggest that the interaction of diatomic gases like CO/NO with Rev-Erbβ triggers redox changes that could influence circadian regulation, highlighting the importance of ligand-mediated reactions in protein function and interactions.

Article Abstract

Rev-Erbβ is a nuclear receptor that couples circadian rhythm, metabolism, and inflammation. Heme binding to the protein modulates its function as a repressor, its stability, its ability to bind other proteins, and its activity in gas sensing. Rev-Erbβ binds Fe-heme more tightly than Fe-heme, suggesting its activities may be regulated by the heme redox state. Yet, this critical role of heme redox chemistry in defining the protein's resting state and function is unknown. We demonstrate by electrochemical and whole-cell electron paramagnetic resonance experiments that Rev-Erbβ exists in the Fe form within the cell allowing the protein to be heme replete even at low concentrations of labile heme in the nucleus. However, being in the Fe redox state contradicts Rev-Erb's known function as a gas sensor, which dogma asserts must be Fe This paper explains why the resting Fe state is congruent both with heme binding and cellular gas sensing. We show that the binding of CO/NO elicits a striking increase in the redox potential of the Fe/Fe couple, characteristic of an EC mechanism in which the unfavorable lectrochemical reduction of heme is coupled to the highly favorable hemical reaction of gas binding, making the reduction spontaneous. Thus, Fe-Rev-Erbβ remains heme-loaded, crucial for its repressor activity, and undergoes reduction when diatomic gases are present. This work has broad implications for proteins in which ligand-triggered redox changes cause conformational changes influencing its function or interprotein interactions (e.g., between NCoR1 and Rev-Erbβ). This study opens up the possibility of CO/NO-mediated regulation of the circadian rhythm through redox changes in Rev-Erbβ.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7826342PMC
http://dx.doi.org/10.1073/pnas.2016717118DOI Listing

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