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Design and Assessment of a Polyurethane Carrier Used for the Transmembrane Transfer of Acyclovir. | LitMetric

AI Article Synopsis

  • Herpes simplex viruses (HSV-1 and HSV-2) can cause a range of infections, including serious conditions affecting the nervous system and organs, and a commonly used treatment is acyclovir, though it requires caution in certain patients.
  • This study focused on creating new polyurethane nanoparticles to improve the delivery of acyclovir, utilizing a specific synthesis process that produced particles of uniform size and good thermal stability.
  • The nanoparticles showed high encapsulation efficiency and minimal skin irritation during testing, indicating their potential as effective transmembrane carriers for delivering acyclovir.

Article Abstract

THE Herpes simplex viruses (HSV-1, HSV-2) are responsible for a wide variety of conditions, from cutaneous-mucosal to central nervous system (CNS) infections and occasional infections of the visceral organs, some of them with a lethal end. Acyclovir is often used intravenously, orally, or locally to treat herpetic infections but it must be administered with caution to patients with kidney disease and to children of early age. The main objectives of this study were to synthesize and evaluate new polyurethane nanoparticles that might be used as proper transmembrane carriers for acyclovir. Polyurethane particles were obtained by a polyaddition process: a mixture of two aliphatic diisocyanates used as organic phase was added to a mixture of butanediol and polyethylene glycol used as aqueous phase. Two different samples (with and without acyclovir, respectively) were synthesized and characterized by UV-Vis spectra in order to assess the encapsulation efficacy and the release profile, FT-IR, DSC, SEM, and SANS for structural characterization, as well as skin irritation tests. Nearly homogeneous samples with particle sizes between 78 and 91 nm have been prepared and characterized revealing a medium tendency to form clusters and a high resistance to heat up to 300 °C. The release profile of these nanoparticles is characteristic to a drug delivery system with a late discharge of the loaded active agents. Very slight increases in the level of transepidermal water loss and erythema were found in a 15-day evaluation on human skin. The results suggest the synthesis of a non-irritative carrier with a high encapsulation efficacy that can be successfully used for the transmembrane transfer of acyclovir.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7823466PMC
http://dx.doi.org/10.3390/nano11010051DOI Listing

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