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

Comparing activity, toxicity and model membrane interactions of Jelleine-I and Trp/Arg analogs: analysis of peptide aggregation

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Author(s):
Martins, Danubia Batista [1] ; Pacca, Carolina Colombelli [2] ; da Silva, Annielle Mendes Brito [3] ; de Souza, Bibiana Monson [4] ; de Almeida, Margarete Teresa Gottardo [5] ; Palma, Mario Sergio [4] ; Arcisio-Miranda, Manoel [3] ; dos Santos Cabrera, Marcia Perez [1, 6]
Total Authors: 8
Affiliation:
[1] Univ Estadual Paulista Unesp, Inst Biociencias Letras & Ciencias Exatas Ibilce, Dept Fis, R Cristovao Colombo 2265, Sao Jose Do Rio Preto 15054000, SP - Brazil
[2] Faceres Med Sch, Sao Jose Do Rio Preto 15090305, SP - Brazil
[3] Univ Fed Sao Paulo, Dept Biofis, Lab Neurobiol Estrutural & Func LaNEF, R Botucatu 862, Edificio ECB, 7 Andar, Sao Paulo 04023062, SP - Brazil
[4] Univ Estadual Paulista Unesp, Ctr Estudos Insetos Sociais, Campus Rio Claro, Av 24-A, 1515, Rio Claro 13506900, SP - Brazil
[5] Fac Med Sao Jose Do Rio Preto, Dept Doencas Dermatol Infecc & Parasitarias, Sao Jose Do Rio Preto 15090000, SP - Brazil
[6] Univ Estadual Paulista Unesp, Inst Biociencias Letras & Ciencias Exatas Ibilce, Dept Quim & Ciencias Ambientais, R Cristovao Colombo 2265, Sao Jose Do Rio Preto 15054000, SP - Brazil
Total Affiliations: 6
Document type: Journal article
Source: Amino Acids; v. 52, n. 5 MAY 2020.
Web of Science Citations: 0
Abstract

Increasing resistance in antibiotic and chemotherapeutic treatments has been pushing studies of design and evaluation of bioactive peptides. Designing relies on different approaches from minimalist sequences and endogenous peptides modifications to computational libraries. Evaluation relies on microbiological tests. Aiming a deeper understanding, we chose the octapeptide Jelleine-I (JI) for its selective and low toxicity profile, designed small modifications combining the substitutions of Phe by Trp and Lys/His by Arg and tested the antimicrobial and anticancer activity on melanoma cells. Biophysical methods identified environment-dependent modulation of aggregation, but critical aggregation concentrations of JI and analogs in buffer show that peptides start membrane interactions as monomers. The presence of model membranes increases or reduces the partial aggregation of peptides. Compared to JI, analog JIF2WR shows the lowest tendency to aggregation on bacterial model membranes. JI and analogs are lytic to model membranes. Their composition-dependent performance indicates preference for the higher charged anionic bilayers in line with their superior performance toward Staphylococcus aureus and Streptococcus pneumoniae. JIF2WR presented the higher partitioning, higher lytic activity and lower aggregated contents. Despite these increased membranolytic activities, JIF2WR exhibited comparable antimicrobial activity in relation to JI at the expenses of some loss in selectivity. We found that the substitution Phe/Trp (JIF2W) tends to decrease antimicrobial but to increase anticancer activity and aggregation on model membranes and the toxicity toward human cells. However, the concomitant substitution Lys/His by Arg (JIF2WR) modulates some of these tendencies, increasing both the antimicrobial and the anticancer activity while decreasing the aggregation tendency. (AU)

FAPESP's process: 16/16212-5 - Natural proteopeptides from the Brazilian fauna, flora and microbiota as potential models for the rational development of new drugs of therapeutic use: isolation, structure elucidation, chemical synthesis and functional activity assays
Grantee:Mario Sergio Palma
Support Opportunities: BIOTA-FAPESP Program - Thematic Grants
FAPESP's process: 16/13368-4 - Nanostructured systems: from membrane biomimetic models to carriers of bioactives
Grantee:Karin Do Amaral Riske
Support Opportunities: Research Projects - Thematic Grants
FAPESP's process: 16/17951-6 - OBSERVING THE INTRACELLULAR pH OF MICROGLIAL CELLS
Grantee:Manoel de Arcisio Miranda Filho
Support Opportunities: Regular Research Grants
FAPESP's process: 14/08372-7 - Peptide and chitosan conjugates with pharmacological potential: synthesis, prospecting of activity in membrane mimetic systems, and evaluation in cells
Grantee:Marcia Perez dos Santos Cabrera
Support Opportunities: Scholarships in Brazil - Young Researchers
FAPESP's process: 12/24259-0 - Peptide and chitosan conjugates with pharmacological potential: synthesis, prospecting of activity in membrane mimetic systems, and evaluation in cells
Grantee:Marcia Perez dos Santos Cabrera
Support Opportunities: Research Grants - Young Investigators Grants