Controlled release of photoswitch drugs by degradable polymer microspheres

R Groynom, E Shoffstall, LS Wu, RH Kramer… - Journal of drug …, 2015 - Taylor & Francis
R Groynom, E Shoffstall, LS Wu, RH Kramer, EB Lavik
Journal of drug targeting, 2015Taylor & Francis
Background: QAQ (quaternary ammonium-azobenzene-quaternary ammonium) and
DENAQ (diethylamine-azobenzene-quaternary ammonium) are synthetic photoswitch
compounds that change conformation in response to light, altering current flow through
voltage-gated ion channels in neurons. These compounds are drug candidates for restoring
light sensitivity in degenerative blinding diseases, such as age-related macular
degeneration (AMD). Purpose: However, these photoswitch compounds are cleared from …
Abstract
Background: QAQ (quaternary ammonium-azobenzene-quaternary ammonium) and DENAQ (diethylamine-azobenzene-quaternary ammonium) are synthetic photoswitch compounds that change conformation in response to light, altering current flow through voltage-gated ion channels in neurons. These compounds are drug candidates for restoring light sensitivity in degenerative blinding diseases, such as age-related macular degeneration (AMD).
Purpose: However, these photoswitch compounds are cleared from the eye within several days, they must be administered through repeated intravitreal injections. Therefore, we are investigating local, sustained delivery formulations to constantly replenish these molecules and have the potential to restore sight.
Methods: Here, we encapsulate QAQ and DENAQ into several molecular weights of poly(lactic-co-glycolic) acid (PLGA) through an emulsion technique to assess the viability of delivering the compounds in their therapeutic window over many weeks. We characterize the loading efficiency, release profile and bioactivity of the compounds after encapsulation.
Results: A very small burst release was observed for all of the formulations with the majority being delivered over the following two months. The lowest molecular weight PLGA led to the highest loading and most linear delivery for both QAQ and DENAQ. Bioactivity was retained for both compounds across the polymers.
Conclusion: These results present encapsulation into polymers by emulsion as a viable option for controlled release of QAQ and DENAQ.
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