We have recently advanced the field of hyperpolarized (HP) 129Xe magnetic resonance imaging (MRI) with the in vivo detection of cucurbit[6]uril (CB6), a highly sensitive MR contrast agent. CB6 is biochemically inactive, which makes its natural bio-distribution non-specific; thus, it cannot be precisely localized within a living mammalian body using HP 129Xe MRI. We have previously identified cyclodextrin-based pseudorotaxanes as conjugatable scaffolds for xenon biosensors; in this work, we introduce a second class of conjugatable scaffolds, with the hyperCEST detection of benzene-appended CB6, a potential precursor to a wide variety of targeted molecular imaging probes.
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