NMR structures of a nonapeptide from DNA binding domain of human polymerase-alpha determined by iterative complete-relaxation-matrix approach

Nuclear magnetic resonance structures of a nonapeptide, ERFKCPCPT, selected from the DNA binding domain of human polymerase-alpha, were determined by complete relaxation matrix analysis of transverse NOE data. The structures exhibit a type III rum with residues KCPC, and the remaining residues exhib it non-ordered structures. The turn was confirmed by alpha, N (i, i+3) conn ectivity, a low temperature coefficient of NH chemical shift (-3.1 x 10(-3) ) of the fourth residue, (3)J(NHa) coupling constants, and characteristic C D peaks at 228 and 200 nm. Furthermore, phi and psi dihedral angles for the i + 1, and i + 2 residues of the rum are found to be -80 and -41 and -60 a nd -40 degrees. The first proline residue is trans- while the second exists in both cis- and trans- configurations, with trans- being more than 80% po pulated. The trans-configuration was established from C5 alpha-P6 alpha cor relation and phi and psi angles of the proline. The five-membered proline r ing is in DOWN puckered (C-beta-exo/C-gamma-endo) conformation. The structu re of the peptide reveals that the two cysteine thiols are similar to 5 Ang strom degrees apart and appropriately positioned to covalently bind cis-dia mminedichloroplatinum(II), a widely used anti-cancer drug.