Chitosan-PEG Gels Loaded with Jatropha mollissima (Pohl) Baill. Ethanolic Extract: An Efficient and Effective Biomaterial in Hemorrhage Control

Author:

Rodrigues José F. B.1,Queiroz João V. S. de A.1ORCID,Medeiros Rebeca P.1,Santos Rafaela O.1,Fialho Djair A.1,Neto João E. S.1,Santos Rogério L. dos2ORCID,Barbosa Rossemberg C.1,Sousa Wladymyr J. B.1ORCID,Torres Maria da C. de M.13,Medeiros Luanna A. D. M.1,Silva Suédina M. de L.1,Montazerian Maziar1ORCID,Fook Marcus V. L.1,Amoah Solomon K. S.4ORCID

Affiliation:

1. Materials Science and Engineering Department, Northeast Laboratory for Evaluation and Development of Biomaterials, Academic Unit of Materials Science and Engineering, Federal University of Campina Grande, Campina Grande 58429-000, PB, Brazil

2. Department of Dentistry, Life Science Institute, Federal University of Juiz de Fora, Governador Valadares 36036-900, MG, Brazil

3. Chemistry Department, Science and Technology Center, State University of Paraiba, Campina Grande 58429-500, PB, Brazil

4. Brazilian Association of Support Cannabis Esperança, João Pessoa 58013-130, PB, Brazil

Abstract

A lack of control over blood loss can have catastrophic implications, including death. Although several hemostatic medications have been employed to reduce bleeding, a vast majority of them are ineffective, expensive, or pose health risks to the patient. To overcome these constraints, chitosan-polyethylene glycol (CS-PEG) hemostatic gels loaded with ethanolic extract of Jatropha mollissima sap (EES) were prepared and their hemostatic, physicochemical, and cytotoxic properties were evaluated. The gels were produced by mixing CS with PEG (an external plasticizer) and EES. The phytochemical analysis revealed a significant concentration of total polyphenols and tannins content in the extract and catechin was identified as one of the key compounds of EES. Infrared spectroscopy analysis revealed the presence of EES in the gels, as well as the chemical interaction between CS and PEG. The gels were thermally stable between 25 and 37 °C (ambient and human body temperature range), had pseudoplastic deformation behavior (rheological properties preserved after shearing), were simple to inject (compression force 30 N), and were biocompatible. In vivo experiments showed that both CS-PEG-EES gels exhibited greater hemostatic action in preventing tail hemorrhage in Wistar rats, with decreased bleeding time and blood weight compared with unloaded CS-PEG gels (control groups) and Hemostank, a commercial product. However, the gel prepared with acetic acid was more efficient in controlling bleeding. These findings reveal that CS-PEG-EES gels can reduce hemorrhages and are a potent, simple, and safe hemostatic agent.

Funder

Paraiba State Research Support Foundation

Publisher

MDPI AG

Subject

Drug Discovery,Pharmaceutical Science,Molecular Medicine

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