The cohesin ATPase cycle is mediated by specific conformational dynamics and interface plasticity of SMC1A and SMC3 ATPase domains.

Cell Rep

Université de Strasbourg, IGBMC UMR 7104 - UMR-S 1258, 67400 Illkirch, France; CNRS, UMR 7104, 67400 Illkirch, France; INSERM, UMR-S 1258, 67400 Illkirch, France; Institut de Génétique et de Biologie Moléculaire et Cellulaire, Department of Integrated Structural Biology, 67400 Illkirch, France. Electronic address:

Published: September 2024

AI Article Synopsis

  • Cohesin is essential for organizing the eukaryotic genome and operates using ATP throughout the cell cycle, although its ATPase activity mechanisms are not well understood.
  • This study explores the human cohesin ATPase cycle, revealing specific structural changes in the SMC1A and SMC3 ATPase domains during the process.
  • The SMC3 domain exhibits flexibility that is influenced by ATP binding, while its interaction with NIPBL and DNA stabilizes the structure, ultimately impacting the formation of the DNA-binding chamber.

Article Abstract

Cohesin is key to eukaryotic genome organization and acts throughout the cell cycle in an ATP-dependent manner. The mechanisms underlying cohesin ATPase activity are poorly understood. Here, we characterize distinct steps of the human cohesin ATPase cycle and show that the SMC1A and SMC3 ATPase domains undergo specific but concerted structural rearrangements along this cycle. Specifically, whereas the proximal coiled coil of the SMC1A ATPase domain remains conformationally stable, that of the SMC3 displays an intrinsic flexibility. The ATP-dependent formation of the heterodimeric SMC1A/SMC3 ATPase module (engaged state) favors this flexibility, which is counteracted by NIPBL and DNA binding (clamped state). Opening of the SMC3/RAD21 interface (open-engaged state) stiffens the SMC3 proximal coiled coil, thus constricting together with that of SMC1A the ATPase module DNA-binding chamber. The plasticity of the ATP-dependent interface between the SMC1A and SMC3 ATPase domains enables these structural rearrangements while keeping the ATP gate shut. VIDEO ABSTRACT.

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Source
http://dx.doi.org/10.1016/j.celrep.2024.114656DOI Listing

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