Matthew Barea scite author profile

Matthew Barea

2Publications

70Citation Statements Received

66Citation Statements Given

How they've been cited

133

How they cite others

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University of Birmingham

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Evaluation of liposomes coated with a pH responsive polymer

Barea

Jenkins

Gaber

et al. 2010

International Journal of Pharmaceutics

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Liposomes have been coated with the pH responsive polymer, Eudragit S100, and the formulation's potential for lower GI targeting following oral administration assessed.Cationic liposomes were coated with the anionic polymer through simple mixing. The evolution of a polymer coat was studied using zeta potential measurements and laser diffraction size analysis. Further evidence of an association between polymer and liposome was obtained using light and cryo electron microscopy. Drug release studies were carried out at pH 1.4, pH 6.3 and pH 7.8, representing the pH conditions of the stomach, small intestine and ileocaecal junction, respectively.The polymer significantly reduced liposomal drug release at pH 1.4 and pH 6.3 but drug release was equivalent to the uncoated control at pH 7.8, indicating that the formulation displayed appropriate pH responsive release characteristics. While the coating layer was not able to withstand the additional challenge of bile salts this reinforces the importance of evaluating these types of formulations in more complex media.

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Encapsulation of Liposomes within pH Responsive Microspheres for Oral Colonic Drug Delivery

Barea

Jenkins²,

Lee³

et al. 2012

International Journal of Biomaterials

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A novel liposome-in-microsphere (LIM) formulation has been created comprising drug-loaded liposomes within pH responsive Eudragit S100 microspheres. The liposomes contained the model drug 5-ASA and were coated with chitosan in order to protect them during encapsulation within the microspheres and to improve site-specific release characteristics. In vitro drug release studies showed that LIMs prevented drug release within simulated stomach and small intestine conditions with subsequent drug release occurring in large intestine conditions. The formulation therefore has potential for oral colonic drug delivery.

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Matthew Barea

Evaluation of liposomes coated with a pH responsive polymer

Encapsulation of Liposomes within pH Responsive Microspheres for Oral Colonic Drug Delivery

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