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(Reference retrieved automatically from SciELO through information on FAPESP grant and its corresponding number as mentioned in the publication by the authors.)

A Kunitz-type peptide from Dendroaspis polylepis venom as a simultaneous inhibitor of serine and cysteine proteases

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Author(s):
Roberto Tadashi Kodama [1] ; Alexandre Kazuo Kuniyoshi [2] ; Cristiane Castilho Fernandes da Silva [3] ; Daniela Cajado-Carvalho [4] ; Bruno Duzzi [5] ; Douglas Ceolin Mariano [6] ; Daniel C. Pimenta [7] ; Rafael Borges [8] ; Wilmar Dias da Silva [9] ; Fernanda Calheta Vieira Portaro [10]
Total Authors: 10
Affiliation:
[1] Butantan Institute. Laboratory of Immunochemistry - Brasil
[2] Butantan Institute. Laboratory of Immunochemistry - Brasil
[3] Butantan Institute. Laboratory of Immunochemistry - Brasil
[4] Butantan Institute. Laboratory of Immunochemistry - Brasil
[5] Butantan Institute. Laboratory of Immunochemistry - Brasil
[6] Butantan Institute. Laboratory of Biochemistry and Biophysics - Brasil
[7] Butantan Institute. Laboratory of Biochemistry and Biophysics - Brasil
[8] São Paulo State University. Botucatu Biosciences Institute. Department of Physics and Biophysics - Brasil
[9] Butantan Institute. Laboratory of Immunochemistry - Brasil
[10] Butantan Institute. Laboratory of Immunochemistry - Brasil
Total Affiliations: 10
Document type: Journal article
Source: Journal of Venomous Animals and Toxins including Tropical Diseases; v. 26, 2020-10-07.
Abstract

Abstract Background: Proteases play an important role for the proper physiological functions of the most diverse organisms. When unregulated, they are associated with several pathologies. Therefore, proteases have become potential therapeutic targets regarding the search for inhibitors. Snake venoms are complex mixtures of molecules that can feature a variety of functions, including peptidase inhibition. Considering this, the present study reports the purification and characterization of a Kunitz-type peptide present in the Dendroaspis polylepis venom as a simultaneous inhibitor of elastase-1 and cathepsin L. Methods: The low molecular weight pool from D. polylepis venom was fractionated in reverse phase HPLC and all peaks were tested in fluorimetric assays. The selected fraction that presented inhibitory activity over both proteases was submitted to mass spectrometry analysis, and the obtained sequence was determined as a Kunitz-type serine protease inhibitor homolog dendrotoxin I. The molecular docking of the Kunitz peptide on the elastase was carried out in the program Z-DOCK, and the program RosettaDock was used to add hydrogens to the models, which were re-ranked using ZRANK program. Results: The fraction containing the Kunitz molecule presented similar inhibition of both elastase-1 and cathepsin L. This Kunitz-type peptide was characterized as an uncompetitive inhibitor for elastase-1, presenting an inhibition constant (Ki) of 8 μM. The docking analysis led us to synthesize two peptides: PEP1, which was substrate for both elastase-1 and cathepsin L, and PEP2, a 30-mer cyclic peptide, which showed to be a cathepsin L competitive inhibitor, with a Ki of 1.96 µM, and an elastase-1 substrate. Conclusion: This work describes a Kunitz-type peptide toxin presenting inhibitory potential over serine and cysteine proteases, and this could contribute to further understand the envenomation process by D. polylepis. In addition, the PEP2 inhibits the cathepsin L activity with a low inhibition constant. (AU)

FAPESP's process: 15/13124-5 - Purification and characterization of peptides present in the venom of African snakes: searching for peptidase inhibitor of medical importance
Grantee:Roberto Tadashi Kodama
Support Opportunities: Scholarships in Brazil - Doctorate
FAPESP's process: 13/07467-1 - CeTICS - Center of Toxins, Immune-Response and Cell Signaling
Grantee:Hugo Aguirre Armelin
Support Opportunities: Research Grants - Research, Innovation and Dissemination Centers - RIDC
FAPESP's process: 13/15344-7 - Efficacy of the bothropic antivenom from Butantan Institute: obtention, characterization and neutralization of serinepeptidases from the venom of Bothrops jararaca
Grantee:Alexandre Kazuo Kuniyoshi
Support Opportunities: Scholarships in Brazil - Doctorate
FAPESP's process: 11/02061-1 - Analysis of proteolytic and peptidic components of the scorpion Tityus serrulatus venom: purification and characterization of a metallopeptidase and search for new inhibitors for human proteases
Grantee:Daniela Cajado de Oliveira Souza Carvalho
Support Opportunities: Scholarships in Brazil - Master
FAPESP's process: 15/15364-3 - Toxic potential analysis of proteases and peptides present in scorpion Tityus serrulatus venom and the blockage capacity of commercial antivenoms: Enhancing the knowledge of venom and its mechanism of action.
Grantee:Fernanda Calheta Vieira Portaro
Support Opportunities: Regular Research Grants