| Literature DB >> 25044757 |
Maribel G Vallespí1, Gilmara Pimentel, Ania Cabrales-Rico, Julio Garza, Brizaida Oliva, Osmani Mendoza, Yolanda Gomez, Tais Basaco, Iraida Sánchez, Carlos Calderón, Juan C Rodriguez, Maria Rivera Markelova, Iduna Fichtner, Soledad Astrada, Mariela Bollati-Fogolín, Hilda E Garay, Osvaldo Reyes.
Abstract
Accumulation of the COMMD1 protein as a druggable pharmacology event to target cancer cells has not been evaluated so far in cancer animal models. We have previously demonstrated that a second-generation peptide, with cell-penetrating capacity, termed CIGB-552, was able to induce apoptosis mediated by stabilization of COMMD1. Here, we explore the antitumor effect by subcutaneous administration of CIGB-552 in a therapeutic schedule. Outstandingly, a significant delay of tumor growth was observed at 0.2 and 0.7 mg/kg (p < 0.01) or 1.4 mg/kg (p < 0.001) after CIGB-552 administration in both syngeneic murine tumors and patient-derived xenograft models. Furthermore, we evidenced that (131)I-CIGB-552 peptide was actually accumulated in the tumors after administration by subcutaneous route. A typical serine-proteases degradation pattern for CIGB-552 in BALB/c mice serum was identified. Further, biological characterization of the main metabolites of the peptide CIGB-552 suggests that the cell-penetrating capacity plays an important role in the cytotoxic activity. This report is the first in describing the antitumor effect induced by systemic administration of a peptide that targets COMMD1 for stabilization. Moreover, our data reinforce the perspectives of CIGB-552 for cancer targeted therapy.Entities:
Keywords: COMMD1; cancer animal models; cancer targeted therapy; cytotoxic peptide; pharmacokinetic
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Year: 2014 PMID: 25044757 DOI: 10.1002/psc.2676
Source DB: PubMed Journal: J Pept Sci ISSN: 1075-2617 Impact factor: 1.905