Sarcolipin Promotes Uncoupling of the SERCA Ca2+ Pump by Inducing a Structural Rearrangement in the Energy-Transduction Domain
Sarcolipin Promotes Uncoupling of the SERCA Ca2+ Pump by Inducing a Structural Rearrangement in the Energy-Transduction Domain
We have performed microsecond (μs) molecular dynamics simulation (MDS) to identify structural mechanisms for sarcolipin (SLN) uncoupling of Ca2+ transport from ATP hydrolysis for the sarcoplasmic reticulum Ca2+-ATPase (SERCA). SLN regulates muscle metabolism and energy expenditure to provide resistance against diet-induced obesity and extreme cold. MDS demonstrated that the cytosolic domain of SLN induces a salt bridge-mediated structural rearrangement in the energy-transduction domain of SERCA. We propose that this structural change uncouples SERCA by perturbing Ca2+ occlusion at residue E309 in transport site II, thus facilitating Ca2+ backflux to the cytosol. Our results have important implications for designing muscle-based therapies for human obesity.
- University of Minnesota United States
- University of Minnesota Morris United States
- University of Minnesota System United States
Protein Conformation, Proteolipids, Muscle Proteins, Energy Metabolism, Sarcoplasmic Reticulum Calcium-Transporting ATPases, Signal Transduction
Protein Conformation, Proteolipids, Muscle Proteins, Energy Metabolism, Sarcoplasmic Reticulum Calcium-Transporting ATPases, Signal Transduction
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