Literature DB >> 15147809

Mucosal insulin delivery systems based on complexation polymer hydrogels: effect of particle size on insulin enteral absorption.

Mariko Morishita1, Takahiro Goto, Nicholas A Peppas, Jeffery I Joseph, Marc C Torjman, Carey Munsick, Koji Nakamura, Tetsuo Yamagata, Kozo Takayama, Anthony M Lowman.   

Abstract

Insulin-loaded polymer (ILP) microparticles composed of poly(methacrylic acid) and poly(ethylene glycol), which have pH-dependent complexation and mucoadhesive properties have been thought to be potential carriers for insulin via an oral route. Nevertheless, further optimization of the polymer delivery system is required to improve clinical application. Therefore, the effect of particle size of the ILP (L-ILP: 180-230 microm, S-ILP: 43-89 microm, SS-ILP: <43 microm) on insulin absorption was studied in the in situ loop system, hypothesizing smaller particle sizes of ILP could induce bigger hypoglycemic effects due to increase mucoadhesive capacity. To verify the hypothesis, the adhesive capacities of differently sized ILPs to the mucosal tissues were evaluated. Additionally, the intestinal site-specificity of ILP for insulin absorption was investigated. Intra- and inter-cellular integrity and/or damage were also examined by lactate dehydrogenase leakage and membrane electrical resistance change to ensure the safety of ILP as a carrier for oral route. As hypothesized, the smaller sized microparticles (SS-ILP) showed a rapid burst-type insulin release and higher insulin absorption compared with the microparticles having larger sizes, resulting in greater hypoglycemic effects without detectable mucosal damage. In fact, SS-ILP demonstrated higher mucoadhesive capacity to the jejunum and the ileum than those of L-ILP. Moreover, SS-ILP's enhancement effect of insulin mucosal absorption showed a site-specificity, demonstrating maximum effect at the ileal segment. These results imply that the particle size and delivery site are very important factors for ILP with respect to increasing the bioavailability of insulin following oral administration. Coyright 2004 Elsevier B.V.

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Year:  2004        PMID: 15147809     DOI: 10.1016/j.jconrel.2004.03.008

Source DB:  PubMed          Journal:  J Control Release        ISSN: 0168-3659            Impact factor:   9.776


  22 in total

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2.  A chemomechanical polymer that functions in blood plasma with high glucose selectivity.

Authors:  George K Samoei; Weihua Wang; Jorge O Escobedo; Xiangyang Xu; Hans-Jörg Schneider; Robert L Cook; Robert M Strongin
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3.  Novel oral insulin delivery systems based on complexation polymer hydrogels: single and multiple administration studies in type 1 and 2 diabetic rats.

Authors:  Mariko Morishita; Takahiro Goto; Koji Nakamura; Anthony M Lowman; Kozo Takayama; Nicholas A Peppas
Journal:  J Control Release       Date:  2005-12-02       Impact factor: 9.776

4.  Efficacy and mechanism of action of chitosan nanocapsules for oral peptide delivery.

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Journal:  Pharm Res       Date:  2006-03-16       Impact factor: 4.200

5.  Confocal microscopic analysis of transport mechanisms of insulin across the cell monolayer.

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Review 6.  Novel platforms for oral drug delivery.

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7.  Quantifying Tight Junction Disruption Caused by Biomimetic pH-Sensitive Hydrogel Drug Carriers.

Authors:  Omar Z Fisher; Nicholas A Peppas
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Review 8.  Therapeutic applications of hydrogels in oral drug delivery.

Authors:  Lindsey A Sharpe; Adam M Daily; Sarena D Horava; Nicholas A Peppas
Journal:  Expert Opin Drug Deliv       Date:  2014-06       Impact factor: 6.648

9.  In vitro evaluation of polyethylene glycol based microparticles containing azithromycin.

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Journal:  Drug Deliv Transl Res       Date:  2014-04       Impact factor: 4.617

10.  Complexation hydrogels for intestinal delivery of interferon beta and calcitonin.

Authors:  Noriyasu Kamei; Mariko Morishita; Hitomi Chiba; Nikhil J Kavimandan; Nicholas A Peppas; Kozo Takayama
Journal:  J Control Release       Date:  2008-11-27       Impact factor: 9.776

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