ELECTROPHORETIC PRECISION DELIVERY DECOUPLES DOSE FROM VOLUME FOR IN SITU PHARMACOLOGY
Linköping University
Presentation
Date TBA
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Poster Board
PS02-07PM-610
Poster
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We develop implantable electrophoretic drug delivery devices that use polyelectrolyte hydrogels for selective transport of charged biomolecules or drug compounds. In contrast to pressure driven approaches, electrophoretic transport enables programmable local release without bulk solvent flow, thereby decoupling delivered dose from infused volume. Dose control is quantitative in principle because delivery can be related to passed charge and calibrated by transport efficiency. After release, molecules spread from the outlet primarily by diffusion and clearance, making the approach naturally compatible with diffusion-based modeling to design dosing protocols that shape or maintain local concentration gradients over time. Together, this establishes electrophoretic implants as a general, flow-free strategy for in situ pharmacology in tissue environments that are difficult to access with systemic dosing.
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