Bismuth Lipophilic Nanoparticles (BisBAL NP) Inhibit the Growth of Tumor Cells in a Mouse Melanoma Model

Author:

Cabral-Romero Claudio1ORCID,García-Cuellar Claudia María2,Hernández-Delgadillo Rene1,Solis-Soto Juan Manuel1,Meester Irene3,Sánchez-Pérez Yesennia2,Nakagoshi-Cepeda Sergio Eduardo1,Pineda-Aguilar Nayely4,Sánchez-Nájera Rosa Isela1,Nakagoshi-Cepeda María Argelia Akemi1,Chellam Shankararaman5

Affiliation:

1. Laboratorio de Biología Molecular, Facultad de Odontología, Universidad Autónoma de Nuevo León, UANL, Monterrey, Nuevo León, México

2. Subdirección de Investigación Básica, Instituto Nacional de Cancerología, Ciudad de México, México

3. Departamento de Ciencias Básicas, Universidad de Monterrey, San Pedro Garza García, México

4. Centro de Investigación en Materiales Avanzados, S.C. (CIMAV), Unidad Monterrey, Nuevo León, México

5. Texas A&M University, TX 77843, USA

Abstract

Aim: The objective of this study was to analyze the antitumor effect of BisBAL NP in a mouse melanoma model. Material and Methods: The antitumor activity of BisBAL NP on murine B16-F10 melanoma cells was determined both in vitro (PrestoBlue cell viability assay and Live/Dead fluorescence) and in vivo, in a mouse model, with the following 15-day treatments: BisBAL NP, negative control (PBS), and cell-death control (docetaxel; DTX). Mouse survival and weight, as well as the tumor volume, were recorded daily during the in vivo study. Results: BisBAL NP were homogeneous in size (mean diameter, 14.7 nm) and bismuth content. In vitro, 0.1 mg/mL BisBAL NP inhibited B16-F10 cell growth stronger (88%) than 0.1 mg/mL DTX (82%) (*p<0.0001). In vivo, tumors in mice treated with BisBAL NP (50 mg/kg/day) or DTX (10 mg/kg/day) were 76% and 85% smaller than the tumors of negative control mice (*p<0.0001). The average weight of mice was 18.1 g and no statistically significant difference was detected among groups during the study. Alopecia was only observed in all DTX-treated mice. The survival rate was 100% for the control and BisBAL NP groups, but one DTX- treated mouse died at the end of the treatment period. The histopathological analysis revealed that exposure to BisBAL NP was cytotoxic for tumor tissue only, without affecting the liver or kidney. Conclusion: BisBAL NP decreased the tumor growing in a mouse melanoma model without secondary effects, constituting an innovative low-cost alternative to treat melanoma.

Funder

CONACyT

Publisher

Bentham Science Publishers Ltd.

Subject

Cancer Research,Pharmacology,Molecular Medicine

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