Use of computational biology to compare the theoretical tertiary structures of the most common forms of RhCE and RhD.
Rocio Trueba-GómezFany Rosenfeld-MannHector A Baptista-GonzálezMaría L Domínguez-LópezHiginio Estrada-JuárezPublished in: Vox sanguinis (2023)
The physicochemical properties of Rh proteins made them different, although their genes are homologous. Using computational biology, we model structures with sufficient precision, similar to those obtained experimentally. An amino acid variation alters the folding of the tertiary structure and the interactions with other proteins, modifying the electrostatic environment, the spatial conformations and therefore the antigenic recognition.