Recurrent oligomers in proteins: An optimal scheme reconciling accurate and concise backbone representations in automated folding and design studies

A novel scheme is introduced to capture the spatial correlations of consecutive amino acids in naturally occurring proteins. This knowledge‐based strategy is able to carry out optimally automated subdivisions of protein fragments into classes of similarity. The goal is to provide the minimal set of protein oligomers (termed “oligons” for brevity) that is able to represent any other fragment. At variance with previous studies in which recurrent local motifs were classified, our concern is to provide simplified protein representations that have been optimised for use in automated folding and/or design attempts. In such contexts, it is paramount to limit the number of degrees of freedom per amino acid without incurring loss of accuracy of structural representations. The suggested method finds, by construction, the optimal compromise between these needs. Several possible oligon lengths are considered. It is shown that meaningful classifications cannot be done for lengths greater than six or smaller than four. Different contexts are considered for which oligons of length five or six are recommendable. With only a few dozen oligons of such length, virtually any protein can be reproduced within typical experimental uncertainties. Structural data for the oligons are made publicly available. Proteins 2000;40:662–674. © 2000 Wiley‐Liss, Inc.