Literature DB >> 21855304

Protein delivery based on uncoated and chitosan-coated mesoporous silicon microparticles.

Ester Pastor1, Eugenia Matveeva, Angela Valle-Gallego, Francisco M Goycoolea, Marcos Garcia-Fuentes.   

Abstract

Mesoporous silicon is a biocompatible, biodegradable material that is receiving increased attention for pharmaceutical applications due to its extensive specific surface. This feature enables to load a variety of drugs in mesoporous silicon devices by simple adsorption-based procedures. In this work, we have addressed the fabrication and characterization of two new mesoporous silicon devices prepared by electrochemistry and intended for protein delivery, namely: (i) mesoporous silicon microparticles and (ii) chitosan-coated mesoporous silicon microparticles. Both carriers were investigated for their capacity to load a therapeutic protein (insulin) and a model antigen (bovine serum albumin) by adsorption. Our results show that mesoporous silicon microparticles prepared by electrochemical methods present moderate affinity for insulin and high affinity for albumin. However, mesoporous silicon presents an extensive capacity to load both proteins, leading to systems were protein could represent the major mass fraction of the formulation. The possibility to form a chitosan coating on the microparticles surface was confirmed both qualitatively by atomic force microscopy and quantitatively by a colorimetric method. Mesoporous silicon microparticles with mean pore size of 35 nm released the loaded insulin quickly, but not instantaneously. This profile could be slowed to a certain extent by the chitosan coating modification. With their high protein loading, their capacity to provide a controlled release of insulin over a period of 60-90 min, and the potential mucoadhesive effect of the chitosan coating, these composite devices comprise several features that render them interesting candidates as transmucosal protein delivery systems.
Copyright © 2011 Elsevier B.V. All rights reserved.

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Year:  2011        PMID: 21855304     DOI: 10.1016/j.colsurfb.2011.07.049

Source DB:  PubMed          Journal:  Colloids Surf B Biointerfaces        ISSN: 0927-7765            Impact factor:   5.268


  7 in total

Review 1.  Application of polysaccharides for surface modification of nanomedicines.

Authors:  Kyung-Oh Doh; Yoon Yeo
Journal:  Ther Deliv       Date:  2012-12

2.  Development of an oral push-pull osmotic pump of fenofibrate-loaded mesoporous silica nanoparticles.

Authors:  Zongzhe Zhao; Chao Wu; Ying Zhao; Yanna Hao; Ying Liu; Wenming Zhao
Journal:  Int J Nanomedicine       Date:  2015-03-03

3.  Novel technique of insulin loading into porous carriers for oral delivery.

Authors:  Sarah Y Eilleia; Mahmoud E Soliman; Samar Mansour; Ahmed S Geneidi
Journal:  Asian J Pharm Sci       Date:  2018-04-17       Impact factor: 6.598

4.  Bone Morphogenic Protein 2-Loaded Porous Silicon Carriers for Osteoinductive Implants.

Authors:  Michal Rosenberg; Dekel Shilo; Leonid Galperin; Tal Capucha; Karim Tarabieh; Adi Rachmiel; Ester Segal
Journal:  Pharmaceutics       Date:  2019-11-12       Impact factor: 6.321

5.  Pore size is a critical parameter for obtaining sustained protein release from electrochemically synthesized mesoporous silicon microparticles.

Authors:  Ester L Pastor; Elaine Reguera-Nuñez; Eugenia Matveeva; Marcos Garcia-Fuentes
Journal:  PeerJ       Date:  2015-10-06       Impact factor: 2.984

6.  Mesoporous silicon microparticles enhance MHC class I cross-antigen presentation by human dendritic cells.

Authors:  A Jiménez-Periáñez; B Abos Gracia; J López Relaño; C M Diez-Rivero; P A Reche; E Martínez-Naves; E Matveyeva; M Gómez del Moral
Journal:  Clin Dev Immunol       Date:  2013-11-10

7.  Monitoring of degradation of porous silicon photonic crystals using digital photography.

Authors:  Maria Ariza-Avidad; Alejandra Nieto; Alfonso Salinas-Castillo; Luis F Capitan-Vallvey; Gordon M Miskelly; Michael J Sailor
Journal:  Nanoscale Res Lett       Date:  2014-08-21       Impact factor: 4.703

  7 in total

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