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An iodine-free and directed-disulfide-bond-forming route to insulin analogues

Organic Letters (2014) 16(11) 3126-3129
DOI: 10.1021/ol501252b
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Abstract

An iodine-free synthetic route to insulin analogues has been established via a directed disulfide bond formation strategy. This method is completely compatible with oxidation-sensitive residues. The key step is constructing the third disulfide bond via a novel procedure involving phenylacetylaminomethyl group (Phacm), immobilized Penicillin G Acylase, and Ellman's reagent. We expect that this method could be broadly utilized for synthesizing insulin-like and other cysteine-rich peptides, in particular, where oxidation-sensitive residues are present in the sequence. © 2014 American Chemical Society.

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Liu, F., Liu, Q., & Mezo, A. R. (2014). An iodine-free and directed-disulfide-bond-forming route to insulin analogues. Organic Letters, 16(11), 3126–3129. https://doi.org/10.1021/ol501252b

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