Berlin 2014 – wissenschaftliches Programm

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MO: Fachverband Molekülphysik

MO 2: Clusters

MO 2.4: Vortrag

Montag, 17. März 2014, 11:15–11:30, BEBEL SR144

Microsolvation of the Formanilide Cation (FA⁺) in a Nonpolar Solvent: Infrared Spectra of FA⁺-L_n clusters (L=Ar, N₂) — •Johanna Klyne¹, Aude Bouchet¹, Matthias Schmies¹, Mitsuhiko Miyazaki², Masaaki Fujii², and Otto Dopfer¹ — ¹Institut für Optik und Atomare Physik, Technische Universität Berlin — ²Chemical Resources Laboratory, Tokyo Institute of Technology, Japan

The peptide linkage is an essential component in biochemical regognition processes since its geometry, depending on its local environment, defines the conformation of proteins. Elucidating the sequential microsolvation of peptides is therefore crucial for a full description of their behaviour in biological media. The stepwise microsolvation of cationic formanilide (FA⁺-L_n) is characterized by IR spectroscopy of size-selected clusters generated in a molecular beam, combined with density functional calculations. Formanilide is the simplest aromatic molecule containing a peptide linkage (-NH-CO-). The observation of size- and isomer-specific NH stretch frequencies reveals the microsolvation of FA⁺ in a nonpolar (L=Ar) and a quadrupolar (L=N₂) solvent. Such aromatic amides exhibit at least two competing binding sites for nucleophilic ligands, namely H-bonding to the acidic N-H group of the amide and π-stacking to the the phenyl ring. The H-bound FA⁺-L dimer with L binding to the NH proton of the amide is the most stable isomer. Subsequent ligands are weaklier bound to the aromatic ring (π-stacking). These results demonstrate an ionization-induced change of the preferred binding motif from π-stacking to H-bonding.