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      Peptide ligations accelerated by N-terminal aspartate and glutamate residues.

      Organic Letters
      American Chemical Society (ACS)

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          Abstract

          A novel application of intramolecular base catalysis confers enhanced reaction rates for aminolysis ligations between peptide thioesters and peptides bearing N-terminal aspartate or glutamate residues. The broad scope of this process and its application in the total synthesis of the diabetes drug exenatide is demonstrated.

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          Journal
          21830797
          10.1021/ol2017356

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