Physicochemical Stimuli-Mediated Precipitation Approach for the Modulation of Rifampicin's Dissolution and Oral Bioavailability.
Vineet Kumar RaiDeepak PradhanJitu HalderTushar Kanti RajwarRitu MahantyIvy SahaPriyanka DashChandan DashSaroj Kumar RoutJameel Al-TamimiHossan EbaidSalim ManoharadasBiswakanth KarGoutam GhoshGoutam RathPublished in: AAPS PharmSciTech (2024)
The intricate process of protein binding orchestrates crucial drug interactions within the bloodstream, facilitating the formation of soluble complexes. This research endeavours to improve the dissolution and oral bioavailability of Rifampicin (RMP) by strategically manipulating drug-protein binding dynamics and the hydrophobic characteristics of human serum albumin (HSA). Various precipitation techniques leveraging methanol, ammonium sulfate, and heat treatment were meticulously employed to tailor the properties of colloidal albumin (HSA NPs). The resultant complexes underwent comprehensive characterization encompassing evaluations of hydrophobicity, size distribution, surface charge, and structural analyses through FTIR, TG-DSC, XRD, and morphological examinations. The findings revealed a significant binding affinity of 78.07 ± 6.6% with native albumin, aligning with prior research. Notably, the complex RMP-HSA NPs-M13, synthesized via the methanolic precipitation method, exhibited the most substantial complexation, achieving a remarkable 3.5-fold increase, followed by the ammonium sulfate (twofold) and heat treatment (1.07-fold) methods in comparison to native albumin binding. The gastric simulated media exhibited accelerated drug release kinetics, with maximal dissolution achieved within two hours, contrasting with the prolonged release observed under intestinal pH conditions. These findings translated into significant improvements in drug permeation, as evidenced by pharmacokinetic profiles demonstrating elevated Cmax, AUC, t1/2, and MRT values for RMP-HSA NPs-M13 compared to free RMP. In summary, this innovative approach underscores the potential of precipitation methods in engineering stable colloidal carrier systems tailored to enhance the oral bioavailability of poorly soluble drugs, offering a pragmatic and scalable alternative to conventional surfactants, polymers, or high-energy methods for complex formation and production.
Keyphrases
- drug release
- binding protein
- mycobacterium tuberculosis
- human serum albumin
- ionic liquid
- drug delivery
- dna binding
- heat stress
- randomized controlled trial
- pulmonary tuberculosis
- protein protein
- emergency department
- risk assessment
- drug induced
- oxide nanoparticles
- heart rate
- clinical trial
- replacement therapy
- single cell
- study protocol
- adverse drug
- high intensity
- small molecule
- climate change
- multidrug resistant
- carbon dioxide