Kinetics and Mechanism of Aspartic Acid Adsorption and Its Explosive Decomposition on Cu(100).

The mechanism and kinetics of aspartic acid (Asp, HO2CCH(NH2)CH2CO2H) decomposition on Cu(100) have been studied using X-ray photoemission spectroscopy and temperature-programmed reaction spectroscopy. We investigate the Asp decomposition mechanism in detail using unlabeled d-Asp and isotopically labeled l-Asp-4-13C (HO2CCH(NH2)CH213CO2H), l-Asp- d7 (DO2CCD(ND2)CD2CO2D), l-Asp-2,3,3- d3 (HO2CCD(NH2)CD2CO2H), and l-Asp-15N-2,3,3- d3 (HO2CCD(15NH2)CD2CO2H). The monolayer of Asp adsorbed on the Cu(100) surface is in a doubly deprotonated bi-aspartate form (-O2CCH(NH2)CH2CO2-). During heating, Asp decomposes on Cu(100) with kinetics consistent with a vacancy-mediated explosion mechanism. The mechanistic steps yield CO2 by sequential cleavage of the C3-C4 and C1-C2 bonds, and N≡CCH3 and H2 via decomposition of the remaining CH(NH2)CH2 intermediate. Deuterium labeling has been used to demonstrate that scrambling of H(D) occurs during the decomposition to acetonitrile of the CD(NH2)CD2 intermediate formed by decarboxylation of l-Asp-2,3,3- d3 and l-Asp-15N-2,3,3- d3.

A Most Enantioselective Chiral Surface: Tartaric Acid on All Surfaces Vicinal to Cu(110).

Enantioselective chemistry on intrinsically chiral surfaces is the quintessential form of structure-sensitive surface chemistry, arising purely from the dissymmetry of the surface structure. Identification or design of chiral surface structures that maximize enantioselectivity for a given processes is extremely challenging because of the limited magnitude of the enantiospecific interaction energetics of chiral molecules with chiral surfaces. Using spherical Cu single crystals exposing surfaces with a continuous two-dimensional distribution of crystallographic orientations, we mapped the enantiospecific surface reaction kinetics of tartaric acid decomposition across the surface orientation space. These measurements reveal both the mechanistic origin of enantioselectivity and identify the structural features of the most enantiospecific surface orientation.