Use este identificador para citar ou linkar para este item: http://repositorio.ufc.br/handle/riufc/59701
Tipo: Artigo de Periódico
Título: The antiproliferative peptide Ctn[15-34] is active against multidrug-resistant yeasts and Candida albicans and C. neoforms
Título em inglês: The antiproliferative peptide Ctn[15-34] is active against multidrug-resistant yeasts and Candida albicans and C. neoforms
Autor(es): Aguiar, Francisca Lidiane Linhares de
Cavalcante, Carolina Sidrim De Paula
Fontenelle, Raquel Oliveira dos Santos
Falcão, Cláudio Borges
Andreu, David
Rádis-Baptista, Gandhi
Palavras-chave: Antimicrobiano;Resistência;Fármacos
Data do documento: 2019
Instituição/Editor/Publicador: Journal Of Applied Microbiology
Citação: AGUIAR, Francisca Lidiane Linhares de; CAVALCANTE, Carolina Sidrim de Paula; FONTENELLE, Raquel Oliveira dos Santos; FALCÃO, Cláudio Borges; ANDREU, David; RÁDIS-BAPTISTA, Gandhi. The antiproliferative peptide Ctn[15-34] is active against multidrug-resistant yeasts and Candida albicans and C. Neoforms Journal Of Applied Microbiology, United States, v. 10, 2019.
Abstract: ims: Crotalicidin (Ctn), a cathelicidin-related antimicrobial peptide from theSouth American rattlesnake venom gland, and its C-terminal Ctn[15-34] fragment,have exhibited important activities against micro-organisms, trypanosomatidprotozoa and certain lines of tumour cells. Herein, the activity against clinicalstrains of fluconazole-resistant Candida albicans and of amphotericin B andfluconazole-resistant Cryptococcus neoformans was investigated.Methods and Results: Microdilution and luminescent cell viability tests wereused to evaluate and compare the susceptibility of pathogenic yeasts to thesepeptides. The time–kill curves of the most active Ctn[15-34] alone or incombination with fluconazole against drug-resistant yeasts were determined.Concomitantly, the fungicidal and/or fungistatic effects of Ctn[15-34] werevisualized by the spotting test. The peptides were active against all strains,including those resistant to antifungal agents. The association of fluconazolewith both Ctn and Ctn[15-34], although not synergic, was additive. Incontrast, such pattern was not observed for C. neoformans.Conclusions: Overall, Ctn and Ctn[15-34] are potential antifungal leadsdisplaying anti-yeast activities against clinical isolates endowed with drugresistance mechanisms.Significance and Impact of the Study: The effective peptide activity againstresistant strains of pathogenic yeasts demonstrates that crotalicidin-derivedpeptides are promising templates to develop new antifungal pharmaceuthicals
URI: http://www.repositorio.ufc.br/handle/riufc/59701
ISSN: 1364-5072
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