Designing Site Specificity in the Mechanochemical Cargo Release of Small Molecules.

Abstract

Mechanical force can trigger the predictable and precise release of small molecules from macromolecular carriers. In this article, based on mechanochemical simulations, we show that norborn-2-en-7-one (NEO), I, and its derivatives can selectively release CO, N2, and SO2 and produce two distinctly different products, A ((3E,5Z,7E)-dimethyl-5,6-diphenyldeca-3,5,7-triene-1,10-diyl bis(2-bromo-2-methylpropanoate)) and B (4',5'-dimethyl-4',5'-dihydro-[1,1':2',1''-terphenyl]-3',6'-diyl)bis(ethane-2,1-diyl) bis(2-bromo-2-methylpropanoate). Site-specific design in the pulling points (PP) ensures that by changing the regioselectivity, either A or B can be exclusively generated. Controlling the rigidity of the NEO scaffold by replacing a 6-membered ring with an 8-membered ring and concomitantly tuning the pulling groups makes it mechanolabile toward the selective formation of B. The diradical intermediate formed during I → A is predicted to be persistent for ∼150 fs. The structural design holds the key to the trade-off between mechanochemical rigidity and lability.