The importance of stereochemistry in the disorder-order continuum of protein-protein interactions

Author:

Newcombe Estella A.ORCID,Due Amanda D.ORCID,Sottini AndreaORCID,Fernandes Catarina B.ORCID,Staby LasseORCID,Delaforge EliseORCID,Bartling Christian R. O.ORCID,Brakti InnaORCID,Bugge KatrineORCID,Schuler BenjaminORCID,Skriver KarenORCID,Olsen Johan G.ORCID,Kragelund Birthe B.ORCID

Abstract

ABSTRACTIntrinsically disordered proteins can bindviathe formation of highly disordered protein complexes without the formation of 3D-structure. Most naturally occurring proteins are “left-handed” or levorotatory (L), made up only of L-amino acids, imprinting molecular structure and communication with stereochemistry. In contrast, their mirror image “right-handed” or dextrorotatory (D) amino acids are rare in Nature. Whether disordered protein complexes are truly independent of 3D-topology and thus of chiral constraints is not clear. To test the chiral constraints of disordered protein-protein interactions, a set of interacting protein pairs covering the disorder-order continuum was chosen as representative examples. By observing both the natural ligands and their stereochemical mirror images in free and bound states, we discovered that chirality was inconsequential in a fully disordered complex. However, if the interaction relied on the ligand undergoing coupled folding and binding, correct stereochemistry was essential. Between these extremes, binding could be observed for the D-ligand with a strength that correlated with the amount of disorder in the final complex. These findings have important implications for our understanding of protein-protein interactions, the molecular processes leading to complex formation, the use of D-peptides in drug discovery, and the chemistry of protein evolution of the first living entities on Earth.

Publisher

Cold Spring Harbor Laboratory

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