Abstract
We have developed a convenient method for the direct synthesis of peptide thioesters, versatile intermediates for peptide ligation and cyclic peptide synthesis. The technology uses a modified Boc SPPS strategy that avoids the use of anhydrous HF. Boc in situ neutralization protocols are used in combination with Merrifield hydroxymethyl resin and TFA/TMSBr cleavage. Avoiding HF extends the scope of Boc SPPS to post‐translational modifications that are compatible with the milder cleavage conditions, demonstrated here with the synthesis of the phosphorylated protein CHK2. Peptide thioesters give easy, direct, access to cyclic peptides, illustrated by the synthesis of cyclorasin, a KRAS inhibitor.
Highlights
Peptide thioesters are key precursors for the synthesis of proteins[1] and cyclic peptides[2] (Scheme 1)
We have developed a convenient method for the direct synthesis of peptide thioesters, versatile intermediates for peptide ligation and cyclic peptide synthesis
The technology uses a modified by tertbutyloxycarbonyl (Boc) solid phase peptide synthesis (SPPS) strategy that avoids the use of anhydrous HF
Summary
Peptide thioesters are key precursors for the synthesis of proteins[1] and cyclic peptides[2] (Scheme 1). Boc in situ neutralization protocols are used in combination with Merrifield hydroxymethyl resin and TFA/ TMSBr cleavage. Avoiding HF extends the scope of Boc SPPS to post-translational modifications that are compatible with the milder cleavage conditions, demonstrated here with the synthesis of the phosphorylated protein CHK2.
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