Lessons from a single amino acid substitution: anticancer and antibacterial properties of two phospholipase A2-derived peptides.

Franchi, Gilberto C.; Almeida, José R.; Mendes, Bruno; Lancellotti, Marcelo; Passos, Óscar; Ramos, Maria J.; Fernandes, Pedro A.; Alves, Cláudia; Vale, Nuno; Gomes, Paula; Da Silva, Saulo Luis

Please use this identifier to cite or link to this item: http://dspace.ucuenca.edu.ec/handle/123456789/40275

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DC Field	Value	Language
dc.contributor.author	Franchi, Gilberto C.
dc.contributor.author	Almeida, José R.
dc.contributor.author	Mendes, Bruno
dc.contributor.author	Lancellotti, Marcelo
dc.contributor.author	Passos, Óscar
dc.contributor.author	Ramos, Maria J.
dc.contributor.author	Fernandes, Pedro A.
dc.contributor.author	Alves, Cláudia
dc.contributor.author	Vale, Nuno
dc.contributor.author	Gomes, Paula
dc.contributor.author	Da Silva, Saulo Luis
dc.date.accessioned	2022-11-18T16:52:21Z	-
dc.date.available	2022-11-18T16:52:21Z	-
dc.date.issued	2022
dc.identifier.issn	1467-3037
dc.identifier.uri	http://dspace.ucuenca.edu.ec/handle/123456789/40275	-
dc.identifier.uri	https://www.scopus.com/record/display.uri?eid=2-s2.0-85123110418&origin=inward&txGid=0dfbd951e81c72d058171833923bf5be&featureToggles=FEATURE_NEW_DOC_DETAILS_EXPORT:1
dc.description.abstract	The membrane-active nature of phospholipase A2-derived peptides makes them potential candidates for antineoplastic and antibacterial therapies. Two short 13-mer C-terminal fragments taken from snake venom Lys49-PLA2 toxins (p-AppK and p-Acl), differing by a leucine/phenylalanine substitution, were synthesized and their bioactivity was evaluated. Their capacity to interfere with the survival of Gram-positive and Gram-negative bacteria as well as with solid and liquid tumors was assessed in vitro. Toxicity to red blood cells was investigated via in silico and in vitro techniques. The mode of action was mainly studied by molecular dynamics simulations and membrane permeabilization assays. Briefly, both peptides have dual activity, i.e., they act against both bacteria, including multidrug-resistant strains and tumor cells. All tested bacteria were susceptible to both peptides, Pseudomonas aeruginosa being the most affected. RAMOS, K562, NB4, and CEM cells were the main leukemic targets of the peptides. In general, p-Acl showed more significant activity, suggesting that phenylalanine confers advantages to the antibacterial and antitumor mechanism, particularly for osteosarcoma lines (HOS and MG63). Peptide-based treatment increased the uptake of a DNA-intercalating dye by bacteria, suggesting membrane damage. Indeed, p-AppK and p-Acl did not disrupt erythrocyte membranes, in agreement with in silico predictions. The latter revealed that the peptides deform the membrane and increase its permeability by facilitating solvent penetration. This phenomenon is expected to catalyze the permeation of solutes that otherwise could not cross the hydrophobic membrane core. In conclusion, the present study highlights the role of a single amino acid substitution present in natural sequences towards the development of dual-action agents. In other words, dissecting and fine-tuning biomembrane remodeling proteins, such as snake venom phospholipase A2 isoforms, is again demonstrated as a valuable source of therapeutic peptides.
dc.language.iso	es_ES
dc.source	Current Issues in Molecular Biology
dc.subject	Membrane
dc.subject	Venom peptides
dc.subject	Leucine
dc.subject	Agkistrodon
dc.subject	Phenylalanine
dc.title	Lessons from a single amino acid substitution: anticancer and antibacterial properties of two phospholipase A2-derived peptides.
dc.type	ARTÍCULO
dc.ucuenca.idautor	0000-0002-3756-6425
dc.ucuenca.idautor	0000-0002-8138-7088
dc.ucuenca.idautor	Sgrp-5423-003
dc.ucuenca.idautor	Sgrp-5423-005
dc.ucuenca.idautor	0000-0001-7743-7364
dc.ucuenca.idautor	0000-0003-2748-4722
dc.ucuenca.idautor	0000-0002-5996-2621
dc.ucuenca.idautor	0000-0002-1283-1042
dc.ucuenca.idautor	0000-0002-6018-4724
dc.ucuenca.idautor	1757872526
dc.ucuenca.idautor	0000-0002-4637-4468
dc.identifier.doi	10.3390/cimb44010004
dc.ucuenca.version	Versión publicada
dc.ucuenca.areaconocimientounescoamplio	09 - Salud y Bienestar
dc.ucuenca.afiliacion	Fernandes, P., Universidade do Porto, Porto, Portugal
dc.ucuenca.afiliacion	Ramos, M., Universidade do Porto, Porto, Portugal
dc.ucuenca.afiliacion	Passos, Ó., Universidade do Porto, Porto, Portugal
dc.ucuenca.afiliacion	Lancellotti, M., Universidade Estadual de Campinas, Campinas, Brasil
dc.ucuenca.afiliacion	Almeida, J., Universidad Regional Amazónica IKIAM, Tena, Ecuador
dc.ucuenca.afiliacion	Mendes, B., Universidad Regional Amazónica IKIAM, Tena, Ecuador
dc.ucuenca.afiliacion	Da, S., Universidad de Cuenca, Facultad de Ciencias Químicas, Cuenca, Ecuador
dc.ucuenca.afiliacion	Gomes, P., Universidade do Porto, Porto, Portugal
dc.ucuenca.afiliacion	Franchi, G., Universidade Estadual de Campinas, Campinas, Brasil
dc.ucuenca.afiliacion	Vale, N., Center for Health Technology and Services Research (CINTESIS), Rua Doutor Plácido da Costa, Portugal
dc.ucuenca.afiliacion	Alves, C., Universidade do Porto, Porto, Portugal
dc.ucuenca.correspondencia	Vale, Nuno, vale@med.up.pt
dc.ucuenca.volumen	Volumen 44, número 1
dc.ucuenca.indicebibliografico	SCOPUS
dc.ucuenca.factorimpacto	0.703
dc.ucuenca.cuartil	Q2
dc.ucuenca.numerocitaciones	0
dc.ucuenca.areaconocimientofrascatiamplio	3. Ciencias Médicas y de la Salud
dc.ucuenca.areaconocimientofrascatiespecifico	3.1 Medicina Básica
dc.ucuenca.areaconocimientofrascatidetallado	3.1.5 Farmacología y Farmacia
dc.ucuenca.areaconocimientounescoespecifico	091 - Salud
dc.ucuenca.areaconocimientounescodetallado	0916 - Farmacia
dc.ucuenca.urifuente	https://www.mdpi.com/1467-3045/44
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