Modeling reveals the strength of weak interactions in stacked-ring assembly

Leonila Lagunes; Koan Briggs; Paige Martin-Holder; Zaikun Xu; Dustin Maurer; Karim Ghabra; Eric J Deeds

doi:10.1016/j.bpj.2024.05.015

Modeling reveals the strength of weak interactions in stacked-ring assembly

Biophys J. 2024 May 18:S0006-3495(24)00329-1. doi: 10.1016/j.bpj.2024.05.015. Online ahead of print.

Authors

Leonila Lagunes¹, Koan Briggs², Paige Martin-Holder³, Zaikun Xu⁴, Dustin Maurer⁴, Karim Ghabra⁵, Eric J Deeds⁶

Affiliations

¹ Department of Integrative Biology and Physiology, UCLA, Los Angeles, California; Institute for Quantitative and Computational Biosciences, UCLA, Los Angeles, California.
² Department of Physics, University of Kansas, Lawrence, Kansas.
³ Department of Molecular Immunology, Microbiology and Genetics, UCLA, Los Angeles, California.
⁴ Center for Computational Biology, University of Kansas, Lawrence, Kansas.
⁵ Computational and Systems Biology IDP, UCLA, Los Angeles, California.
⁶ Department of Integrative Biology and Physiology, UCLA, Los Angeles, California; Institute for Quantitative and Computational Biosciences, UCLA, Los Angeles, California; Center for Computational Biology, University of Kansas, Lawrence, Kansas. Electronic address: deeds@ucla.edu.

PMID: 38762753
DOI: 10.1016/j.bpj.2024.05.015

Abstract

Cells employ many large macromolecular machines for the execution and regulation of processes that are vital for cell and organismal viability. Interestingly, cells cannot synthesize these machines as functioning units. Instead, cells synthesize the molecular parts that must then assemble into the functional complex. Many important machines, including chaperones such as GroEL and proteases such as the proteasome, comprise protein rings that are stacked on top of one another. While there is some experimental data regarding how stacked-ring complexes such as the proteasome self-assemble, a comprehensive understanding of the dynamics of stacked-ring assembly is currently lacking. Here, we developed a mathematical model of stacked-trimer assembly and performed an analysis of the assembly of the stacked homomeric trimer, which is the simplest stacked-ring architecture. We found that stacked rings are particularly susceptible to a form of kinetic trapping that we term "deadlock," in which the system gets stuck in a state where there are many large intermediates that are not the fully assembled structure but that cannot productively react. When interaction affinities are uniformly strong, deadlock severely limits assembly yield. We thus predicted that stacked rings would avoid situations where all interfaces in the structure have high affinity. Analysis of available crystal structures indicated that indeed the majority-if not all-of stacked trimers do not contain uniformly strong interactions. Finally, to better understand the origins of deadlock, we developed a formal pathway analysis and showed that, when all the binding affinities are strong, many of the possible pathways are utilized. In contrast, optimal assembly strategies utilize only a small number of pathways. Our work suggests that deadlock is a critical factor influencing the evolution of macromolecular machines and provides general principles for understanding the self-assembly efficiency of existing machines.