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    Developing a Comparative Docking Protocol for the Prediction of Peptide Selectivity Proļ¬les: Investigation of Potassium Channel Toxins

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    During the development of selective peptides against highly homologous targets, a reliable tool is sought that can predict information on both mechanisms of binding and relative afļ¬nities. These tools must ļ¬rst be tested on known proļ¬les before application on novel therapeutic candidates. We therefore present a comparative docking protocol in HADDOCK using critical motifs, and use it to ā€œpredictā€ the various selectivity proļ¬les of several major Ī±KTX scorpion toxin families versus Kv1.1, Kv1.2 and Kv1.3. By correlating results across toxins of similar proļ¬les, a comprehensive set of functional residues can be identiļ¬ed. Reasonable models of channel-toxin interactions can be then drawn that are consistent with known afļ¬nity and mutagenesis. Without biological information on the interaction, HADDOCK reproduces mechanisms underlying the universal binding of Ī±KTX-2 toxins, and Kv1.3 selectivity of Ī±KTX-3 toxins. The addition of constraints encouraging the critical lysine insertion conļ¬rms these ļ¬ndings, and gives analogous explanations for other families, including models of partial pore-block in Ī±KTX-6. While qualitatively informative, the HADDOCK scoring function is not yet sufļ¬cient for accurate afļ¬nity-ranking. False minima in low-afļ¬nity complexes often resemble true binding in high-afļ¬nity complexes, despite steric/conformational penalties apparent from visual inspection. This contamination signiļ¬cantly complicates energetic analysis, although it is usually possible to obtain correct ranking via careful interpretation of binding-well characteristics and elimination of false positives. Aside from adaptations to the broader potassium channel family, we suggest that this strategy of comparative docking can be extended to other channels of interest with known structure, especially in cases where a critical motif exists to improve docking effectiveness
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