Literature DB >> 14703987

Mapping of human plasma kallikrein active site by design of peptides based on modifications of a Kazal-type inhibitor reactive site.

V A Nunes1, A J Gozzo, M U Sampaio, M A Juliano, C A M Sampaio, M S Araujo.   

Abstract

Human plasma kallikrein (huPK) is a proteinase that participates in several biological processes. Although various inhibitors control its activity, members of the Kazal family have not been identified as huPK inhibitors. In order to map the enzyme active site, we synthesized peptides based on the reactive site (PRILSPV) of a natural Kazal-type inhibitor found in Cayman plasma, which is not an huPK inhibitor. As expected, the leader peptide (Abz-SAPRILSPVQ-EDDnp) was not cleaved by huPK. Modifications to the leader peptide at P'1, P'3 and P'4 positions were made according to the sequence of a phage display-generated recombinant Kazal inhibitor (PYTLKWV) that presented huPK-binding ability. Novel peptides were identified as substrates for huPK and related enzymes. Both porcine pancreatic and human plasma kallikreins cleaved peptides at Arg or Lys bonds, whereas human pancreatic kallikrein cleaved bonds involving Arg or a pair of hydrophobic amino acid residues. Peptide hydrolysis by pancreatic kallikrein was not significantly altered by amino acid replacements. The peptide Abz-SAPRILSWVQ-EDDnp was the best substrate and a competitive inhibitor for huPK, indicating that Trp residue at the P'4 position is important for enzyme action.

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Year:  2003        PMID: 14703987     DOI: 10.1023/b:jopc.0000005503.20628.4e

Source DB:  PubMed          Journal:  J Protein Chem        ISSN: 0277-8033


  2 in total

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Authors:  Brian L Henry; Jay N Thakkar; Aiye Liang; Umesh R Desai
Journal:  Biochem Biophys Res Commun       Date:  2011-12-01       Impact factor: 3.575

2.  Common variation in KLKB1 and essential hypertension risk: tagging-SNP haplotype analysis in a case-control study.

Authors:  Xiangfeng Lu; Weiyan Zhao; Jianfeng Huang; Hongfan Li; Wei Yang; Laiyuan Wang; Wentao Huang; Shufeng Chen; Dongfeng Gu
Journal:  Hum Genet       Date:  2007-02-23       Impact factor: 4.132

  2 in total

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