Literature DB >> 12852971

Improvement of biological activity and proteolytic stability of peptides by coupling with a cyclic peptide.

Kenji Shibata1, Toshiyuki Suzawa, Shiro Soga, Tamio Mizukami, Koji Yamada, Nobuo Hanai, Motoo Yamasaki.   

Abstract

The cyclic moiety of an endothelin antagonist peptide RES-701-1, composed of 10 amino acids with an amide bond between alpha-NH(2) of Gly1 and beta-COOH of Asp9, was coupled to some biologically active peptides aiming to improve their activities and stabilities against proteolytic degradation. Coupling of the cyclic peptide to the N-terminal of RGD-peptides, maximally 4-fold improvement of in vitro activity compared to the original peptide has been achieved. Coupling of it to protein farnesyltransferase inhibiting peptides resulted to improve in vitro activity maximally 3-fold. These peptides coupled with the cyclic peptide also showed enhanced stability against some typical proteases. These results indicate that this cyclic peptide can stabilize the conformations of the peptides coupled to its C-terminus. Coupling of our cyclic peptide is anticipated to be a novel conformational stabilizing method for biologically active peptides, results to improve their activity and stability.

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Year:  2003        PMID: 12852971     DOI: 10.1016/s0960-894x(03)00476-1

Source DB:  PubMed          Journal:  Bioorg Med Chem Lett        ISSN: 0960-894X            Impact factor:   2.823


  3 in total

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2.  β-Turn sequences promote stability of peptide substrates for kinases within the cytosolic environment.

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Authors:  Shitian Jiang; Lishuang Zhao; Jingwan Wu; Yujun Bao; Zhiqiang Wang; Yingxue Jin
Journal:  RSC Adv       Date:  2019-12-24       Impact factor: 4.036

  3 in total

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