Thiocarbazate building blocks enable the construction of azapeptides for rapid development of therapeutic candidates

Author:

Altiti Ahmad,He MingzhuORCID,VanPatten SonyaORCID,Cheng Kai Fan,Ahmed UmairORCID,Chiu Pui Yan,Mughrabi Ibrahim T.,Jabari Bayan Al,Burch Ronald M.,Manogue Kirk R.,Tracey Kevin J.ORCID,Diamond BettyORCID,Metz Christine N.,Yang Huan,Hudson LaQueta K.,Zanos StavrosORCID,Son MyoungsunORCID,Sherry BarbaraORCID,Coleman Thomas R.,Al-Abed YousefORCID

Abstract

AbstractPeptides, polymers of amino acids, comprise a vital and expanding therapeutic approach. Their rapid degradation by proteases, however, represents a major limitation to their therapeutic utility and chemical modifications to native peptides have been employed to mitigate this weakness. Herein, we describe functionalized thiocarbazate scaffolds as precursors of aza-amino acids, that, upon activation, can be integrated in a peptide sequence to generate azapeptides using conventional peptide synthetic methods. This methodology facilitates peptide editing—replacing targeted amino acid(s) with aza-amino acid(s) within a peptide—to form azapeptides with preferred therapeutic characteristics (extending half-life/bioavailability, while at the same time typically preserving structural features and biological activities). We demonstrate the convenience of this azapeptide synthesis platform in two well-studied peptides with short half-lives: FSSE/P5779, a tetrapeptide inhibitor of HMGB1/MD-2/TLR4 complex formation, and bradykinin, a nine-residue vasoactive peptide. This bench-stable thiocarbazate platform offers a robust and universal approach to optimize peptide-based therapeutics.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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