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Research Article

Formulation and quality control of semi-solid containing harmless bacteria by-products: chronic wounds pro-healing activity

, , , , , & show all
Pages 911-918 | Received 26 May 2014, Accepted 23 Jun 2014, Published online: 08 Jul 2014
 

Abstract

Chronic wounds are those that remain in a chronic inflammatory state and fail to follow normal healing process. Infection is one of the most important causes of chronicity. A frequent pathogen isolated from chronic infections is Pseudomonas aeruginosa; refractory to therapy and host immune attack in its biofilm phenotype. Lactobacillus plantarum cultures supernatants (LAPS) interfere with its pathogenic capacity. In addition, LAPS showed bacteriostatic and bactericide properties and is neither cytotoxic nor an inductor of necrosis-apoptosis. LAPSs chemical composition was determined; allowing us to propose a correlation between its constituents and their biological activity. This article shows a pharmaceutical dosage form designed by using LAPS as an API with pro-healing activity and its quality control. Pharmacotechnical and anti-microbial assays were adapted to demonstrate that the vehicle used does not modify LAPS activities. Selected formulation (F100) showed fair mechanical and technological properties. From the in vitro release assays was found an adequate release from the carrier matrix and maintains its anti-pathogenic activity for 6 months. We propose F100 for chronic wounds treatment. The use of harmless bacteria by-products, such as LAPS, to antagonize infectious pathogens that have ability to form biofilm is an efficient and economic approach to treat infected chronic wounds.

Acknowledgements

The authors thank the Centro de Microscopia Eletrônica (CME/UFRGS) for technical assistance in electron microscopy.

Declaration of interest

This work was supported by grant Consejo de Investigación de la Universidad Nacional de Tucumán Programa CIUNT N° 26/D453, FAPERGS (grant number 1008844), MCTI/CNPq (grant number 576774/2008-1) and NANOBIOTEC-Brazil from CAPES (grant number 703/2009). The authors would like to acknowledge the Consejo Nacional de Investigaciones Científicas y Técnicas, CONICET, for providing funds for the Pos Doctoral grants of PhD M.E. Sesto Cabral and PhD A.N. Ramos and NANOBIOTEC-Brazil from CAPES for Trentin DS and Treter J fellowships. The authors declare no competing financial interest.

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