Identification and molecular cloning of a novel amphibian Bowman Birk-type trypsin inhibitor from the skin of the Hejiang Odorous Frog; Odorrana hejiangensis

  • Min Wang
  • , Lei Wang
  • , Tianbao Chen
  • , Brian Walker
  • , Mei Zhou
  • , Dayuan Sui
  • , J. Michael Conlon
  • , Chris Shaw

Research output: Contribution to journalArticlepeer-review

Abstract

In this study, an amphibian (Odorrana hejiangensis) skin extract was fractionated by reverse phase HPLC and fractions were screened for trypsin inhibitory activity. Using this initial approach, a novel trypsin inhibitory peptide was detected with an apparent protonated molecular mass of 1804.83 Da, as determined by MALDI-TOF mass spectrometry. It was named Hejiang trypsin inhibitor (HJTI) in accordance. The primary structure of the biosynthetic precursor of HJTI was deduced from a cDNA sequence cloned from a skin-derived cDNA library. The primary structure of the encoded predicted mature active peptide was established as: GAPKGCWTKSYPPQPCS (non-protonated monoisotopic molecular mass - 1802.81 Da). On the basis of this unequivocal amino acid sequence, a synthetic replicate was synthesized by solid phase Fmoc chemistry. This replicate displayed a moderately potent trypsin inhibition with a K i of 388 nM. Bioinformatic analysis of the primary structure of this peptide indicated that it was a member of the Bowman-Birk family of protease inhibitors. The substitutions of Gln-14 and Ser-17 by Lys, resulted in an increase in cationicity and a small increase in potency to a K i value of 218 nM. Neither HJTI nor its synthetic analog, possessed any significant antimicrobial activity.

Original languageEnglish
Pages (from-to)245-250
Number of pages6
JournalPeptides
Volume33
Issue number2
DOIs
Publication statusPublished (in print/issue) - Feb 2012

Keywords

  • Amphibian
  • Cloning
  • Inhibitor
  • Peptide
  • Protease
  • Skin

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