Binding constant of cell adhesion receptors and substrate-immobilized ligands depends on the distribution of ligands

Phys Rev E. 2018 Jan;97(1-1):012405. doi: 10.1103/PhysRevE.97.012405.

Abstract

Cell-cell adhesion and the adhesion of cells to tissues and extracellular matrix, which are pivotal for immune response, tissue development, and cell locomotion, depend sensitively on the binding constant of receptor and ligand molecules anchored on the apposing surfaces. An important question remains of whether the immobilization of ligands affects the affinity of binding with cell adhesion receptors. We have investigated the adhesion of multicomponent membranes to a flat substrate coated with immobile ligands using Monte Carlo simulations of a statistical mesoscopic model with biologically relevant parameters. We find that the binding of the adhesion receptors to ligands immobilized on the substrate is strongly affected by the ligand distribution. In the case of ligand clusters, the receptor-ligand binding constant can be significantly enhanced due to the less translational entropy loss of lipid-raft domains in the model cell membranes upon the formation of additional complexes. For ligands randomly or uniformly immobilized on the substrate, the binding constant is rather decreased since the receptors localized in lipid-raft domains have to pay an energetic penalty in order to bind ligands. Our findings help to understand why cell-substrate adhesion experiments for measuring the impact of lipid rafts on the receptor-ligand interactions led to contradictory results.

MeSH terms

  • Cell Adhesion / physiology*
  • Computer Simulation
  • Elasticity
  • Entropy
  • Ligands*
  • Membrane Microdomains / metabolism*
  • Models, Biological*
  • Monte Carlo Method
  • Receptors, Cell Surface / metabolism*

Substances

  • Ligands
  • Receptors, Cell Surface