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  4. Constitutionally selective amplification of multicomponent 84-membered macrocyclic hosts for (−)-cytidine•H+
 
research article

Constitutionally selective amplification of multicomponent 84-membered macrocyclic hosts for (−)-cytidine•H+

Chung, Mee-Kyung
•
Severin, Kay  
•
Lee, Stephen J.
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2011
Chemical Science

Mixtures of dipeptide monomers create stereochemically and constitutionally complex dynamic libraries of potential receptors. When (−)-cytidine was utilized as guest an 84-membered cyclic host was amplified (70–175 fold) from a nearly undetectable initial concentration. Only the specified diastereomeric combination of the two chiral building blocks yielded a dynamic library from which the macrocyclic receptor could be amplified.

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