Rational design of an antitumor peptide based on the 32-51 region of the Limulus anti-LPS factor protein obtained from a chemical library

Guerra-Vallespi, Maribel; Fernández-Massó, Julio R; Reyes-Acosta, Osvaldo; Garay-Pérez, Hilda; Torrens-Madrazo, Isis; Granadillo-Rodríguez, Milaid; Oliva-Argüelles, Brizaida; García, Isbel; Guillén-Pérez, Isabel; Palenzuela-Gardón, Daniel; Vázquez-Blomquist, Dania; Falcón-Cama, Viviana; Mendoza-Fuentes, Osmany; Borras-Hidalgo, Orlando; Novoa-Pérez, Lidia I; Vázquez-Castillo, Mariela

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Biotecnología Aplicada

versão On-line ISSN 1027-2852

Resumo

GUERRA-VALLESPI, Maribel et al. Rational design of an antitumor peptide based on the 32-51 region of the Limulus anti-LPS factor protein obtained from a chemical library. Biotecnol Apl [online]. 2014, vol.31, n.4, pp. 328-331. ISSN 1027-2852.

In previous work, we identified the peptide comprising amino acids 32-51 on the antimicrobial protein limulus anti-LPS factor (LALF) from Limulus poliphemus, based on its capacity to bind to the bacterial lipopolysaccharide (LPS). In this study, we designed a chemical peptide library by alanine scanning from the sequence of the LALF32-51 peptide. Four new peptides, named L-2, L-8, L-12 and L-20 by the Ala residue substituted in the given position of the LALF32-51 peptide, were identified as retaining their penetrating activity but also showing antitumor effects when subcutaneously administered in female C57Bl/6 mice after the implantation of malignant TC-1 lung epithelial cells. They significantly increased animal survival (p < 0.05) as compared to LALF32-51. The substitution of Tyr residue to Ala at position 2 in the peptide sequence enhanced the cytotoxic effect, while residues Phe8, Lys12 and Trp20 were essential for the antitumor activity. Moreover, the administration of the L-2 peptide significantly reduced tumor growth in comparison to PBS- or L-20 peptide-treated lung TC-1 cells in C57Bl/6 mice. L-2 was found to deregulate the tumor cell cycle and induces apoptosis, through mechanisms affecting glycolytic and protein biosynthesis pathways. It also significantly increased survival in human colon cancer LS-174T xenotransplanted nude mice for up to 32 days, two of the animals being tumor free. The L-2 peptide could serve as peptide-based prototype drug with potential to reduce tumor load or could be coadministered with conventional chemotherapy. This research granted the 2013 Award of the Cuban National Academy of Sciences.

Palavras-chave : antitumor peptide; chemical peptide library; Limulus; LALF32-51; alanine scanning.

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