Controlled drug release from policaprolactone-piperine electrospun scaffold for bone tissue engineering

Samara Raquel Pereira Oliveira,Gabriely Goncalves Lima, Marleane Maria Felix de Azevedo, Andre Sales Aguiar Furtado, Suziete Batista soares Gusmao, Emerson da Silva Nascimento, Ricardo Rodrigues de Franca Bento, Francisco Eroni Paz Santos, Lucielma Salmito Soares Pinto,Thiago Domingues Stocco, Antonio Martins Maia Filho,Bartolomeu Cruz Viana,Anderson Oliveira Lobo,Gustavo Oliveira de Meira Gusmao

JOURNAL OF DRUG DELIVERY SCIENCE AND TECHNOLOGY(2024)

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摘要
Polymeric drug scaffolds have been intensively studied in orthopedic surgery due to their capacity for the regimented and site-specific liberation of the therapeutic agent at the intended locus. In this context, electrospinning is a promising technique for producing scaffolds using biodegradable and biocompatible polymers. In the present study, scaffolds of Polycaprolactone (PCL) with Piperine (PIP) incorporated at different concentrations (1, 3, and 5 %) were obtained by electrospinning. The electrospun PCL, PCL/PIP 1 %, PCL/PIP 3 %, and PCL/PIP 5 % groups were analyzed by FTIR spectroscopy to identify the incorporated drug and through UV-VIS spectroscopy to evaluate its controlled release. In addition, the bone repair was verified by Raman spectroscopy using ?1PO43- vibration data obtained by in vivo analysis. The morphology and diameter of the nanofibers were obtained by scanning electron microscopy (SEM). The PCL, PCL/PIP 1 %, PCL/PIP 3 %, PCL/PIP 5 % scaffolds had diameters of 0.0015 +/- 0.002 mu m, 1.08 +/- 0.007 mu m, 1.09 +/- 0.02 mu m, 0.59 +/- 0.016 mu m, respectively. Piperine release was pronounced after 15 days. Therefore, at 30 days, the PCL/PIP 1 % scaffold released 64 % +/- 0.00062, while the PCL/PIP 3 % and PCL/PIP 5 % scaffolds released only 16.06 +/- 0.00012 and 9.08 % +/- 0.00031, respectively. This study provided evidence that PCL/Piperine can be used to significantly increase bone regeneration. Results from Raman spectroscopy and histological analysis demonstrated that the PCL/PIP 1 %, 3 %, and 5 % groups had better bone regeneration than the negative control group after 15 days and 30 days of treatment. The prolonged release of piperine promoted by PCL, a hydrophobic drug carrier, caused the neoformation of the bones to be restricted to the inner part of the bone defect, creating an immature bone with evident cellular differentiation.
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关键词
Electrospinning,Polycaprolactone,Piperine,Controlled release,Bone repair
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