Litcius/Paper detail

N–H⋯X interactions stabilize intra-residue C5 hydrogen bonded conformations in heterocyclic α-amino acid derivatives

Venkateswara Rao Mundlapati, Zeynab Imani, Viola C. D’mello, Valérie Brenner, Eric Gloaguen, Jean‐Pierre Baltaze, Sylvie Robin, Michel Mons, David J. Aitken

2021Chemical Science22 citationsDOIOpen Access PDF

Abstract

Nature makes extensive and elaborate use of hydrogen bonding to assemble and stabilize biomolecular structures. The shapes of peptides and proteins rely significantly on N-H⋯O[double bond, length as m-dash]C interactions, which are the linchpins of turns, sheets and helices. The C5 H-bond, in which a single residue provides both donor and acceptor, is generally considered too weak to force the backbone to adopt extended structures. Exploiting the synergy between gas phase (experimental and quantum chemistry) and solution spectroscopies to decipher IR spectroscopic data, this work demonstrates that the extended C5-based conformation in 4-membered ring heterocyclic α-amino acid derivatives is significantly stabilized by the formation of an N-H⋯X H-bond. In this synergic system the strength of the C5 interaction remains constant while the N-H⋯X H-bond strength, and thereby the support provided by it, varies with the heteroatom.

Topics & Concepts

Hydrogen bondChemistryResidue (chemistry)Ring (chemistry)Gas phaseAmino acid residuePolarAmino acidStereochemistryMoleculeOrganic chemistryPeptide sequenceBiochemistryAstronomyPhysicsGeneCrystallography and molecular interactionsMolecular Spectroscopy and StructureChemical Synthesis and Analysis