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Calcium depletion-mediated protease inhibition and apical-junctional- complex disassembly via an EGTA-conjugated carrier for oral insulin delivery
E.-Y. Chuang, K.-J. Lin, F.-Y. Su, H.-L. Chen, , Y.-C. Ho, T.-C. Yen, N. Panda, H.-W. Sung
Published in Elsevier B.V.
2013
Volume: 169
   
Issue: 3
Pages: 296 - 305
Abstract
Calcium (Ca2+) has a crucial role in maintaining the intestinal protease activity and in forming the apical junctional complex (AJC) that preserves epithelial barrier function. Ethylene glycol tetraacetic acid (EGTA) is a Ca2+-specific chelating agent. To maintain the concentration of this chelator in areas where enzyme inhibition and paracellular permeation enhancement are needed, this study synthesized a poly(γ-glutamic acid)-EGTA conjugate (γPGA-EGTA) to form nanoparticles (NPs) with chitosan (CS) for oral insulin delivery. The results of our molecular dynamic (MD) simulations indicate that Ca2+ ions could be specifically chelated to the nitrogen atoms, ether oxygen atoms, and carboxylate oxygen atoms in [Ca(EGTA)]2- anions. By che-lating Ca2+, γPGA-EGTA conferred a significant insulin protection effect against proteases in intestinal tracts isolated from rats. Additionally, calcium depletion by γPGA-EGTA could stimulate the endocytosis of AJC components in Caco-2 cell monolayers, which led to a reversible opening of AJCs and thus increased their paracellular permeability. Single-photon emission computed tomography images performed in the biodistribution study clearly show the 123I-insulin orally delivered by CS/γPGA-EGTA NPs in the heart, aorta, renal cortex, renal pelvis and liver, which ultimately produced a significant and prolonged hypoglyce-mic effect in diabetic rats. The above results confirm that this γPGA-EGTA conjugate is a promising candidate for oral insulin delivery. © 2012 Elsevier B.V. All rights reserved.
About the journal
JournalData powered by TypesetJournal of Controlled Release
PublisherData powered by TypesetElsevier B.V.
ISSN01683659