8 research outputs found
Gyrospun antimicrobial nanoparticle loaded fibrous polymeric filters
A one step approach to prepare hybrid nanoparticle embedded polymer fibres using pressurised gyration is presented. Two types of novel antimicrobial nanoparticles and poly(methylmethacrylate) polymer were used in this work. X-ray diffraction analysis of the nanoparticles revealed Ag, Cu and W are the main elements present in them. The concentration of the polymer solution and the nanoparticle concentration had a significant influence on the fibre diameter, pore size and morphology. Fibres with a diameter in the range of 6-20. μm were spun using 20. wt% polymer solutions containing 0.1, 0.25 and 0.5 wt% nanoparticles under 0.3. MPa working pressure and a rotational speed of 36,000. rpm. Continuous, bead-free fibre morphologies were obtained for each case. The pore size in the fibres varied between 36 and 300. nm. Successful incorporation of the nanoparticles in polymer fibres was confirmed by energy dispersive x-ray analysis. The fibres were also gyrospun on to metallic discs to prepare filters which were tested for their antibacterial activity on a suspension of Pseudomonas aeruginosa. Nanoparticle loaded fibres showed higher antibacterial efficacy than pure poly(methylmethacrylate) fibres
Harnessing Polyhydroxyalkanoates and Pressurized Gyration for Hard and Soft Tissue Engineering
Organ dysfunction is a major cause of morbidity and mortality. Transplantation is typically the only definitive cure, challenged by the lack of sufficient donor organs. Tissue engineering encompasses the development of biomaterial scaffolds to support cell attachment, proliferation, and differentiation, leading to tissue regeneration. For efficient clinical translation, the forming technology utilized must be suitable for mass production. Herein, uniaxial polyhydroxyalkanoate scaffolds manufactured by pressurized gyration, a hybrid scalable spinning technique, are successfully used in bone, nerve, and cardiovascular applications. Chorioallantoic membrane and in vivo studies provided evidence of vascularization, collagen deposition, and cellular invasion for bone tissue engineering. Highly efficient axonal outgrowth was observed in dorsal root ganglion-based 3D ex vivo models. Human induced pluripotent stem cell derived cardiomyocytes exhibited a mature cardiomyocyte phenotype with optimal calcium handling. This study confirms that engineered polyhydroxyalkanoate-based gyrospun fibers provide an exciting and unique toolbox for the development of scalable scaffolds for both hard and soft tissue regeneration
Gyrospun antimicrobial nanoparticle loaded fibrous polymeric filters
© 2016 The Authors. Published by Elsevier B.V. © 2016 The Authors. Published by Elsevier B.V. This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).A one step approach to prepare hybrid nanoparticle embedded polymer fibres using pressurised gyration is presented. Two types of novel antimicrobial nanoparticles and poly (methylmethacrylate) polymer were used in this work. X-ray diffraction analysis of the nanoparticles revealed Ag, Cu and W are the main elements present in them. The concentration of the polymer solution and the nanoparticle concentration had a significant influence on the fibre diameter, pore size and morphology. Fibres with a diameter in the range of 6-20 ìm were spun using 20 wt% polymer solutions containing 0.1, 0.25 and 0.5 w% nanoparticles under 0.3 MPa working pressure and a rotational speed of 36000 rpm. Continuous, bead-free fibre morphologies were obtained for each case. The pore size in the fibres varied between 36-300 nm. Successful incorporation of the nanoparticles in polymer fibres was confirmed by energy dispersive x-ray analysis. The fibres were also gyrospun on to metallic disks to prepare filters which were tested for their antibacterial activity on a suspension of Pseudomonas aeruginosa. Nanoparticle loaded fibres showed higher antibacterial efficacy than pure poly(methylmethacrylate) fibres.8pÍuPeer reviewedFinal Published versio
Amorphous formulations of indomethacin and griseofulvin prepared by electrospinning
Following an array of optimization
experiments, two series of electrospun
polyvinylpyrrolidone (PVP) fibers were prepared. One set of fibers
contained various loadings of indomethacin, known to form stable glasses,
and the other griseofulvin (a poor glass former). Drug loadings of
up to 33% w/w were achieved. Electron microscopy data showed the fibers
largely to comprise smooth and uniform cylinders, with evidence for
solvent droplets in some samples. In all cases, the drug was found
to exist in the amorphous physical state in the fibers on the basis
of X-ray diffraction and differential scanning calorimetry (DSC) measurements.
Modulated temperature DSC showed that the relationship between a formulation’s
glass transition temperature (<i>T</i><sub>g</sub>) and
the drug loading follows the Gordon–Taylor equation, but not
the Fox equation. The results of Gordon–Taylor analysis indicated
that the drug/polymer interactions were stronger with indomethacin.
The interactions between drug and polymer were explored in more detail
using molecular modeling simulations and again found to be stronger
with indomethacin; the presence of significant intermolecular forces
was further confirmed using IR spectroscopy. The amorphous form of
both drugs was found to be stable after storage of the fibers for
8 months in a desiccator (relative humidity <25%). Finally, the
functional performance of the fibers was studied; in all cases, the
drug-loaded fibers released their drug cargo very rapidly, offering
accelerated dissolution over the pure drug
Harnessing Polyhydroxyalkanoates and Pressurized Gyration for Hard and Soft Tissue Engineering
Organ dysfunction is a major cause of morbidity and mortality. Transplantation is typically the only definitive cure, challenged by the lack of sufficient donor organs. Tissue engineering encompasses the development of biomaterial scaffolds to support cell attachment, proliferation, and differentiation, leading to tissue regeneration. For efficient clinical translation, the forming technology utilized must be suitable for mass production. Herein, uniaxial polyhydroxyalkanoate scaffolds manufactured by pressurized gyration, a hybrid scalable spinning technique, are successfully used in bone, nerve, and cardiovascular applications. Chorioallantoic membrane and in vivo studies provided evidence of vascularization, collagen deposition, and cellular invasion for bone tissue engineering. Highly efficient axonal outgrowth was observed in dorsal root ganglion-based 3D ex vivo models. Human induced pluripotent stem cell derived cardiomyocytes exhibited a mature cardiomyocyte phenotype with optimal calcium handling. This study confirms that engineered polyhydroxyalkanoate-based gyrospun fibers provide an exciting and unique toolbox for the development of scalable scaffolds for both hard and soft tissue regeneration