Temporizin and Temporizin-1 Peptides as Novel Candidates for Eliminating Trypanosoma cruzi.

Temporizin and Temporizin-1 Peptides as Novel Candidates for Eliminating Trypanosoma cruzi.

Tropical diseases caused by parasitic infections continue to cause socioeconomic distress worldwide. Among these, Chagas disease has become a great concern because of globalization. Caused by Trypanosoma cruzi, there is an increasing need to discover new, more effective methods to manage infections...

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Main Authors: André L A Souza, Robson X Faria, Kátia S Calabrese, Daiane J Hardoim, Noemi Taniwaki, Luiz A Alves, Salvatore G De Simone
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2016-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4934777?pdf=render
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spelling doaj-b593f780cac047239f7290d1f183f7db2020-11-25T02:05:17ZengPublic Library of Science (PLoS)PLoS ONE1932-62032016-01-01117e015767310.1371/journal.pone.0157673Temporizin and Temporizin-1 Peptides as Novel Candidates for Eliminating Trypanosoma cruzi.André L A SouzaRobson X FariaKátia S CalabreseDaiane J HardoimNoemi TaniwakiLuiz A AlvesSalvatore G De SimoneTropical diseases caused by parasitic infections continue to cause socioeconomic distress worldwide. Among these, Chagas disease has become a great concern because of globalization. Caused by Trypanosoma cruzi, there is an increasing need to discover new, more effective methods to manage infections that minimize disease onset. Antimicrobial peptides represent a possible solution to this challenge. As effector molecules of the innate immune response against pathogens, they are the first line of defense found in all multi-cellular organisms. In amphibians, temporins are a large family of antimicrobial peptides found in skin secretions. Their functional roles and modes of action present unique properties that indicate possible candidates for therapeutic applications. Here, we investigated the trypanocide activity of temporizin and temporizin-1. Temporizin is an artificial, hybrid peptide containing the N-terminal region of temporin A, the pore-forming region of gramicidin and a C-terminus consisting of alternating leucine and lysine. Temporizin-1 is a modification of temporizin with a reduction in the region responsible for insertion into membranes. Their activities were evaluated in a cell permeabilization assay by flow cytometry, an LDH release assay, electron microscopy, an MTT assay and patch clamp experiments. Both temporizin and temporizin-1 demonstrated toxicity against T. cruzi with temporizin displaying slightly more potency. At concentrations up to 100 μg/ ml, both peptides exhibited low toxicity in J774 cells, a macrophage lineage cell line, and no toxicity was observed in mouse primary peritoneal macrophages. In contrast, the peptides showed some toxicity in rat adenoma GH3 cells and Jurkat human lymphoma cells with temporizin-1 displaying lower toxicity. In summary, a shortened form of the hybrid temporizin peptide, temporizin-1, was efficient at killing T. cruzi and it has low toxicity in wild-type mammalian cells. These data suggest that temporizin-1 might be a candidate for Chagas disease therapy.http://europepmc.org/articles/PMC4934777?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author André L A Souza
Robson X Faria
Kátia S Calabrese
Daiane J Hardoim
Noemi Taniwaki
Luiz A Alves
Salvatore G De Simone
spellingShingle André L A Souza
Robson X Faria
Kátia S Calabrese
Daiane J Hardoim
Noemi Taniwaki
Luiz A Alves
Salvatore G De Simone
Temporizin and Temporizin-1 Peptides as Novel Candidates for Eliminating Trypanosoma cruzi.
PLoS ONE
author_facet André L A Souza
Robson X Faria
Kátia S Calabrese
Daiane J Hardoim
Noemi Taniwaki
Luiz A Alves
Salvatore G De Simone
author_sort André L A Souza
title Temporizin and Temporizin-1 Peptides as Novel Candidates for Eliminating Trypanosoma cruzi.
title_short Temporizin and Temporizin-1 Peptides as Novel Candidates for Eliminating Trypanosoma cruzi.
title_full Temporizin and Temporizin-1 Peptides as Novel Candidates for Eliminating Trypanosoma cruzi.
title_fullStr Temporizin and Temporizin-1 Peptides as Novel Candidates for Eliminating Trypanosoma cruzi.
title_full_unstemmed Temporizin and Temporizin-1 Peptides as Novel Candidates for Eliminating Trypanosoma cruzi.
title_sort temporizin and temporizin-1 peptides as novel candidates for eliminating trypanosoma cruzi.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2016-01-01
description Tropical diseases caused by parasitic infections continue to cause socioeconomic distress worldwide. Among these, Chagas disease has become a great concern because of globalization. Caused by Trypanosoma cruzi, there is an increasing need to discover new, more effective methods to manage infections that minimize disease onset. Antimicrobial peptides represent a possible solution to this challenge. As effector molecules of the innate immune response against pathogens, they are the first line of defense found in all multi-cellular organisms. In amphibians, temporins are a large family of antimicrobial peptides found in skin secretions. Their functional roles and modes of action present unique properties that indicate possible candidates for therapeutic applications. Here, we investigated the trypanocide activity of temporizin and temporizin-1. Temporizin is an artificial, hybrid peptide containing the N-terminal region of temporin A, the pore-forming region of gramicidin and a C-terminus consisting of alternating leucine and lysine. Temporizin-1 is a modification of temporizin with a reduction in the region responsible for insertion into membranes. Their activities were evaluated in a cell permeabilization assay by flow cytometry, an LDH release assay, electron microscopy, an MTT assay and patch clamp experiments. Both temporizin and temporizin-1 demonstrated toxicity against T. cruzi with temporizin displaying slightly more potency. At concentrations up to 100 μg/ ml, both peptides exhibited low toxicity in J774 cells, a macrophage lineage cell line, and no toxicity was observed in mouse primary peritoneal macrophages. In contrast, the peptides showed some toxicity in rat adenoma GH3 cells and Jurkat human lymphoma cells with temporizin-1 displaying lower toxicity. In summary, a shortened form of the hybrid temporizin peptide, temporizin-1, was efficient at killing T. cruzi and it has low toxicity in wild-type mammalian cells. These data suggest that temporizin-1 might be a candidate for Chagas disease therapy.
url http://europepmc.org/articles/PMC4934777?pdf=render
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