AI Article Synopsis
- Recifin A is a newly discovered peptide characterized by a distinctive "tyrosine-lock" structure that includes a four-stranded β-sheet stabilized by disulfide bonds.
- Researchers successfully synthesized recifin A using native chemical ligation of two fragments, finding that even in its linear form, it can adopt the complex fold easily.
- Five analogues of recifin A were created to study the importance of the central tyrosine residue and its role in inhibiting the cancer-related enzyme tyrosyl-DNA phosphodiesterase I.
Article Abstract
The peptide recifin A is the inaugural member of the structurally intriguing new fold referred to as a tyrosine-lock. Its central four stranded β-sheet is stabilized by a unique arrangement in which three disulfide bonds and their interconnecting backbone form a ring that wraps around one of the strands, resulting in a Tyr side chain being buried in the molecular core. Here we aimed to establish a synthetic route to this complex class of natural products. Full length recifin A was successfully generated through native chemical ligation chemistry joining two 21 amino acid residue fragments. Surprisingly, reduced linear recifin A readily adopts the correct, topologically-complex fold random oxidation of the cysteines, suggesting it is highly energetically favored. Utilizing our synthetic strategy, we generated five recifin A analogues to investigate the structural role of the central Tyr residue and provide the first insights into the structure activity relationship of recifin A towards its cancer target tyrosyl-DNA phosphodiesterase I.
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Source |
|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11339948 | PMC |
| http://dx.doi.org/10.1039/d4sc01976h | DOI Listing |
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