AI Article Synopsis
- E-selectin is a cell adhesion molecule that helps white blood cells attach to inflamed blood vessels during inflammation, and it can exist in two different conformations affecting its binding ability.
- Molecular dynamics simulations showed that E-selectin can switch between these conformations naturally, and changing a specific amino acid (serine to tyrosine) promotes the higher binding affinity state.
- Experiments demonstrated that the modified E-selectin binds more effectively to its partner PSGL-1 than the normal version, enhancing our understanding of how E-selectin's structure impacts its function in inflammation.
Article Abstract
Introduction: E-selectin is a member of the selectin family of cell adhesion molecules expressed on the plasma membrane of inflamed endothelium and facilitates initial leukocyte tethering and subsequent cell rolling during the early stages of the inflammatory response binding to glycoproteins expressing sialyl Lewis and sialyl Lewis (sLe). Existing crystal structures of the extracellular lectin/EGF-like domain of E-selectin complexed with sLe have revealed that E-selectin can exist in two conformation states, a low affinity (bent) conformation, and a high affinity (extended) conformation. The differentiating characteristic of the two conformations is the interdomain angle between the lectin and the EGF-like domain.
Methods: Using molecular dynamics (MD) simulations we observed that in the absence of tensile force E-selectin undergoes spontaneous switching between the two conformational states at equilibrium. A single amino acid substitution at residue 2 (serine to tyrosine) on the lectin domain favors the extended conformation.
Results: Steered molecular dynamics (SMD) simulations of E-selectin and PSGL-1 in conjunction with experimental cell adhesion assays show a longer binding lifetime of E-selectin (S2Y) to PSGL-1 compared to wildtype protein.
Conclusions: The findings in this study advance our understanding into how the structural makeup of E-selectin allosterically influences its adhesive dynamics.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7878631 | PMC |
| http://dx.doi.org/10.1007/s12195-021-00666-z | DOI Listing |
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