AI Article Synopsis
- A synthesized 40-residue precursor peptide (propeptide 5) was created by combining four anticancer peptide analogs linked with enzyme-cleavable lysyl-lysine linkers.
- Upon treatment with the enzyme trypsin, propeptide 5 was specifically cleaved to release individual peptides, identified using LC-MS.
- Propeptide 5 demonstrated stronger anticancer effects in vitro and in vivo compared to the separate peptides, indicating that this approach can effectively deliver multiple active peptides through basic amino acid linkers like Lys-Lys.
Article Abstract
A large 40-residue precursor peptide (propeptide 5) was synthesized by linking together four designed anticancer peptide analogs to the neuropeptides: vasoactive intestinal peptide, somatostatin, bombesin and substance P, using enzyme cleavable lysyl-lysine linkers. On incubation with the enzyme trypsin, propeptide 5 was cleaved in a sequence-specific manner at the lysyl-lysine residues in the linker to release the individual peptide fragments which were identified by LC-MS. Another precursor peptide (propeptide 5a), consisting of two of the peptide analogs linked through lysyl-lysine linker, was also preferentially cleaved at the Lys-Lys site on incubation with the enzyme trypsin. Propeptide 5 showed potent anticancer activity, both in vitro and in vivo, which was greater than that of the individual component peptides. The enhanced activity suggests that the propeptide is possibly cleaved in the biological system at the lysyl-lysine site to yield the individual peptide analogs, which together show a synergistic effect. On the basis of these experimental findings, it can be concluded that pairs of basic amino acids such as Lys-Lys can be used as facile linkers for delivering multiple biologically active peptides.
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| http://dx.doi.org/10.1002/psc.867 | DOI Listing |
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