cytochrome-c-t and phenylalanylglycine

Experimental and computational studies suggest that few general principles govern protein/protein interactions and aggregation. The knowledge of these rules may be exploited to design peptides that are able to interfere with the self-assembly and aggregation of proteins. This work is aimed to verify the validity of this hypothesis by investigating the interaction of cytochrome c with Phe and Gly amino acids, Ala-His (carnosine), and two water-soluble dipeptides Phe-Gly and Gly-Phe. The combined use of (1)H NMR, MD, and DSC has shown that: (i) at neutral pH, only Phe-Gly is able to prevent the thermally induced aggregation of cytochrome c; (ii) Phe-Gly interacts with Gly45 and Phe46 residues of the protein, either when the protein is in the folded or in the unfolded state; and (iii) the interaction of Phe-Gly with cytochrome c is sequence-dependent. These results support the hypothesis that the basic principles that describe protein aggregation can be used for the design of peptides with antiaggregating properties.

Topics: Animals; Binding Sites; Computer Simulation; Cytochromes c; Dipeptides; Enzyme Activation; Enzyme Inhibitors; Glycine; Horses; Models, Chemical; Models, Molecular; Motion; Multiprotein Complexes; Myocardium; Phenylalanine; Protein Binding; Protein Conformation; Protein Folding