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Effect of size, surface charge, and hydrophobicity on the translocation of polystyrene microspheres through gastrointestinal mucin
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1997
Year
Tissue EngineeringNanotherapeuticsEngineeringBiofabricationPolystyrene MicrospheresBiomedical EngineeringNanomedicineDrug Delivery SystemMicrofluidicsCell-based Drug DeliveryMucin PacketImmunoengineeringMicro-encapsulationBiopolymersSurface ChargeGastrointestinal MucinPharmacologyDelivery SystemPolymer ScienceMicroemulsionDrug Delivery SystemsNano-drug DeliveryAmphiphilic SystemMucin LayerMedicineMs TranslocationBiomedical Applications
Microspheres (MS) have been proposed for use as oral vaccine delivery vehicles (VDV); however, due to poor and variable absorption their clinical utility is limited. The effects of size, ζ-potential, and surface hydrophobicity on the translocation (PT) permeabilities of polystyrene (PS) MS with varying surface functional groups (amidine, carboxyl, carboxylate-modified [CML], and sulfate) were determined through gastrointestinal (GI) mucin. PT were determined, under steady-state conditions, using a modified Ussing-type diffusion chamber and a mucin packet developed for use with the Transwell-Snapwell system. PT followed the Stokes-Einstein relationship, demonstrating the limited ability of larger MS (>0.5 μm) to diffuse through the mucin layer. PT also varied according to the surface characteristics. Even though the ζ-potential did not correlate with the transport of MS through mucin, surface ionization appears to be important in MS translocation. The PS-amidine MS were significantly less hydrophobic and had a higher PT than that of the other MS, suggesting that hydrophobicity is also a significant factor in MS transport through mucin. While these results suggest that mucin may be a significant barrier to the oral absorption of vaccines and VDVs in vivo, the rate-limiting barrier for the absorption of MS will be the intestinal mucosa. © 1997 John Wiley & Sons, Inc. J Appl Polym Sci 63: 1481–1492, 1997