Cysteine-Specific Multifaceted Bioconjugation of Peptides and Proteins Using 5-Substituted 1,2,3-Triazines

Quan Zuo,Yiping Li, Xuanliang Lai,Guangjun Bao, Lu Chen,Zeyuan He, Xinyi Song, Ruiyao E,Pengxin Wang, Yuntao Shi,Huixin Luo,Wangsheng Sun,Rui Wang

ADVANCED SCIENCE(2024)

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Abstract
Peptide and protein postmodification have gained significant attention due to their extensive impact on biomolecule engineering and drug discovery, of which cysteine-specific modification strategies are prominent due to their inherent nucleophilicity and low abundance. Herein, the study introduces a novel approach utilizing multifunctional 5-substituted 1,2,3-triazine derivatives to achieve multifaceted bioconjugation targeting cysteine-containing peptides and proteins. On the one hand, this represents an inaugural instance of employing 1,2,3-triazine in biomolecular-specific modification within a physiological solution. On the other hand, as a powerful combination of precision modification and biorthogonality, this strategy allows for the one-pot dual-orthogonal functionalization of biomolecules utilizing the aldehyde group generated simultaneously. 1,2,3-Triazine derivatives with diverse functional groups allow conjugation to peptides or proteins, while bi-triazines enable peptide cyclization and dimerization. The examination of the stability of bi-triazines revealed their potential for reversible peptide modification. This work establishes a comprehensive platform for identifying cysteine-selective modifications, providing new avenues for peptide-based drug development, protein bioconjugation, and chemical biology research. 1,2,3-Triazines are used to modify biological molecules containing a thiol group in an aqueous solution for the first time, and the resulting aldehyde group served as a handle for secondary labeling. The innovative strategy is applied to double biorthogonal functionalization, secondary labeling of peptides and proteins, and cyclization or dimerization of peptides, highlighting its advantages. image
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Key words
1,2,3-triazines,cysteine,late-stage functionalization,macrocycles,peptides,proteins
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