Signaling activations through G-protein-coupled-receptor aggregations

Masaki Watabe, Hideaki Yoshimura, Satya N. V. Arjunan, Kazunari Kaizu, and Koichi Takahashi
Phys. Rev. E 102, 032413 – Published 22 September 2020
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Abstract

Eukaryotic cells transmit extracellular signal information to cellular interiors through the formation of a ternary complex made up of a ligand (or agonist), G-protein, and G-protein-coupled receptor (GPCR). Previously formalized theories of ternary complex formation have mainly assumed that observable states of receptors can only take the form of monomers. Here, we propose a multiary complex model of GPCR signaling activations via the vector representation of various unobserved aggregated receptor states. Our results from model simulations imply that receptor aggregation processes can govern cooperative effects in a regime inaccessible by previous theories. In particular, we show how the affinity of ligand-receptor binding can be largely varied by various oligomer formations in the low concentration range of G-protein stimulus.

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  • Received 16 April 2020
  • Revised 3 August 2020
  • Accepted 31 August 2020

DOI:https://doi.org/10.1103/PhysRevE.102.032413

©2020 American Physical Society

Physics Subject Headings (PhySH)

Physics of Living Systems

Authors & Affiliations

Masaki Watabe1,*, Hideaki Yoshimura2, Satya N. V. Arjunan1,3, Kazunari Kaizu1, and Koichi Takahashi1,4,†

  • 1Laboratory for Biologically Inspired Computing, RIKEN Center for Biosystems Dynamics Research, Suita, Osaka 565-0874, Japan
  • 2School of Science, The University of Tokyo, 7-3-1 Hongo, Bunkyo-ku, Tokyo 113-0033, Japan
  • 3Lowy Cancer Research Centre, The University of New South Wales, Sydney 2052, Australia
  • 4Institute for Advanced Biosciences, Keio University, Fujisawa, Kanagawa 252-8520, Japan

  • *Corresponding author: masaki@riken.jp
  • Corresponding author: ktakahashi@riken.jp

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Issue

Vol. 102, Iss. 3 — September 2020

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