David Sigwalt scite author profile

We report the measurement of the binding constants (K) for cucurbit[n]uril (n = 7, 8) toward four series of guests based on 2,6-disubstituted adamantanes, 4,9-disubstituted diamantanes, 1,6-disubstituted diamantanes, and 1-substituted adamantane ammonium ions by direct and competitive H NMR spectroscopy. Compared to the affinity of CB[7]·Diam(NMe), the adamantane diammonium ion complexes (e.g., CB[7]·2,6-Ad(NH) and CB[7]·2,6-Ad(NMe)) are less effective at realizing the potential 1000-fold enhancement in affinity due to ion-dipole interactions at the second ureidyl C═O portal. Comparative crystallographic investigation of CB[7]·Diam(NMe), CB[7]·DiamNMe, and CB[7]·1-AdNMe revealed that the preferred geometry positions the NMe groups ≈0.32 Å above the C═O portal; the observed 0.80 Å spacing observed for CB[7]·Diam(NMe) reflects the simultaneous geometrical constraints of CH···O═C close contacts at both portals. Remarkably, the CB[8]·IsoDiam(NHMe) complex displays femtomolar binding affinity, placing it firmly alongside the CB[7]·Diam(NMe) complex. Primary or quaternary ammonium ion looping strategies lead to larger increases in binding affinity for CB[8] than for CB[7], which we attribute to the larger size of the carbonyl portals of CB[8]; this suggests routes to develop CB[8] as the tightest binding host in the CB[n] family. We report that alkyl group fluorination (e.g., CB[7]·1-AdNHEt versus CB[7]·1-AdNHCHCF) does not result in the expected increase in K value. Finally, we discuss the role of solvation in nonempirical quantum mechanical computational methodology, which is used to estimate the relative changes in Gibbs binding free energies.

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Gene delivery with polycationic fullerene hexakis-adducts

Sigwalt

Holler

Iehl

et al. 2011

Chem. Commun.

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David Sigwalt

Synthesis of giant globular multivalent glycofullerenes as potent inhibitors in a model of Ebola virus infection

Unraveling the Structure–Affinity Relationship between Cucurbit[n]urils (n = 7, 8) and Cationic Diamondoids

Gene delivery with polycationic fullerene hexakis-adducts

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