AI Article Synopsis

  • The study improved the bioavailability of irbesartan (IRB) by creating a nanocrystalline tablet (IRB-NP tablet) from its suspensions, addressing previous stability issues.
  • The IRB-NP tablet was developed using various additives and showed a smaller particle size (approximately 118 nm) upon redispersion, leading to enhanced solubility and absorption compared to the traditional microcrystalline tablet (IRB-MP tablet).
  • Additionally, the IRB-NP tablet demonstrated a greater ability to reduce blood pressure in stroke-prone hypertensive rats than the IRB-MP tablet, highlighting its potential therapeutic advantages.

Article Abstract

We previously reported that the bioavailability (BA) of irbesartan (IRB), a BSC class II drug, was improved by preparing nanocrystalline suspensions. However, nanocrystalline suspensions have chemical and physical instabilities and must be converted into tablets through drying approaches in order to overcome such instabilities. In this study, we attempted to design a molded tablet based on nanocrystalline IRB suspensions (IRB-NP tablet) and investigated the effects of this IRB-NP tablet on blood pressure (BP) in a stroke-prone spontaneously hypertensive (SHR-SP) rat. The IRB-NP tablet (with a hardness of 42.6 N) was developed by combining various additives (methylcellulose, 2-hydroxypropyl-β-cyclodextrin HPβCD, D-mannitol, polyvinylpyrrolidone, and gum arabic) followed by bead-milling and freeze-drying treatments. The mean particle size in the redispersions of the IRB-NP tablet was approximately 118 nm. The solubility and intestinal absorption of IRB in the IRB-NP tablet were significantly enhanced in comparison with the microcrystalline IRB tablet (IRB-MP tablet), and both solubility and clathrin-dependent endocytosis helped improve the low BA of the IRB. In addition, the BP-reducing effect of the IRB-NP tablet was significantly higher than that of the IRB-MP tablet. These results provide useful information for the preservation of nanocrystalline suspensions of BCS class II drugs, such as IRB.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8875686PMC
http://dx.doi.org/10.3390/pharmaceutics14020387DOI Listing

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