Abstract
Calmodulin is a calcium-binding protein ubiquitous in eukaryotic cells, involved in numerous calcium-regulated biological phenomena, such as synaptic plasticity, muscle contraction, cell cycle, and circadian rhythms. It exibits a characteristic dumbell shape, with two globular domains (N- and C-terminal lobe) joined by a linker region. Each lobe can take alternative conformations, affected by the binding of calcium and target proteins.Calmodulin displays considerable functional flexibility due to its capability to bind different targets, often in a tissue-specific fashion. In various specific physiological environments (e.g. skeletal muscle, neuron dendritic spines) several targets compete for the same calmodulin pool, regulating its availability and affinity for calcium. In this work, we sought to understand the general principles underlying calmodulin modulation by different target proteins, and to account for simultaneous effects of multiple competing targets, thus enabling a more realistic simulation of calmodulin-dependent pathways. We built a mechanistic allosteric model of calmodulin, based on an hemiconcerted framework: each calmodulin lobe can exist in two conformations in thermodynamic equilibrium, with different affinities for calcium and different affinities for each target. Each lobe was allowed to switch conformation on its own. The model was parameterised and validated against experimental data from the literature. In spite of its simplicity, a two-state allosteric model was able to satisfactorily represent several sets of experiments, in particular the binding of calcium on intact and truncated calmodulin and the effect of different skMLCK peptides on calmodulin’s saturation curve. The model can also be readily extended to include multiple targets. We show that some targets stabilise the low calcium affinity T state while others stabilise the high affinity R state. Most of the effects produced by calmodulin targets can be explained as modulation of a pre-existing dynamic equilibrium between different conformations of calmodulin’s lobes, in agreement with linkage theory and MWC-type models.
Highlights
Calmodulin is a ubiquitous calcium-binding protein involved in many cellular processes, from synaptic plasticity to muscular contraction, cell cycle regulation, and circadian rhythms
Taking advantage of existing experimental data sets, we modelled the behavior of the TR2C tryptic fragment in the presence of peptides WFF and WF10 and Nav1.2IQp
We parameterised a model of TR2C, parameterised a model of TR1C, and the two submodels were merged into a model of intact calmodulin
Summary
Calmodulin is a ubiquitous calcium-binding protein involved in many cellular processes, from synaptic plasticity to muscular contraction, cell cycle regulation, and circadian rhythms. It is organized in two highly homologous globular domains joined by a flexible linker [1]. Each domain contains two calcium-binding EF-hands that can undergo a transition between closed and open conformations, the latter favored by calcium binding [2, 3]. The binding domains that preferably interact with calcium-free calmodulin are called IQ motifs, a family of 14-residue sequences named after the two most frequent initial amino acids (usually isoleucine, followed by a highly conserved glutamate) [5]
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