Improved Pharmacokinetics of Aceclofenac Immediate Release Tablets Incorporating ist Inclusion Complex with Hydroxypropyl-β-Cyclodextrin

Dahiya, Sunita; Kaushik, Atul; Pathak, Kamla

doi:10.3797/scipharm.1409-07

Cited by 12 publications

(10 citation statements)

References 3 publications

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“…Pharmacokinetic studies revealed that the optimized formulation (F2) of aceclofenac fast dissolving tablets reached peak plasma concentration in less time (1 sec) and with increased absorption and relative bioavailability (182.77) when compared to pure drug. These results were in agreement with the results obtained by Dahiya et al [21]. Summary of pharmacokinetic parameters was shown in table 8.…”

Section: Pharmacokinetics Studiessupporting

confidence: 93%

Optimization of Statistically Designed Aceclofenac Fast Dissolving Tablets Employing Starch Glutamate as a Novel Superdisintegrant

Kumar

Mudili

2019

Int J App Pharm

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Objective: To optimize aceclofenac fast dissolving tablets employing starch glutamate as novel superdisintegrant by 2 3 Methods: Starch glutamate was prepared by the esterification process. Starch glutamate physical and micromeritics properties had been evaluated and the prepared starch glutamate was used as a superdisintegrant for the formulation of the fast dissolving tablets of aceclofenac by direct compression method and optimized by employing 2 factorial design to improve bioavailability and enhance patient compliance.3 Results: The prepared starch glutamate was amorphous, insoluble in aqueous and organic solvents were tested. Fast dissolving tablets of aceclofenac were formulated by employing starch glutamate as a superdisintegrant showed good tablet properties and showed an increased dissolution efficiency of the drug. Among all the formulations (F1 to F8), the formulation F8 containing 5% concentration of starch glutamate, croscarmellose sodium and, crospovidone as a superdisintegrants showed 99.7±0.15% of drug release within 5 min. Whereas the formulation F2 containing 5% concentration of starch glutamate, drug release characters were comparable to the formulation F8. Optimized formulation F2 attained peak plasma concentration within a short period and showed increased relative bioavailability of the drug. factorial design. The prepared aceclofenac fast dissolving tablets were evaluated for post compression parameters as well as in vitro and in vivo release characteristics. Optimized formulation stability studies were performed at accelerated conditions for 6 mo as per ICH and WHO guidelines. Conclusion:From the physical properties, disintegration time, in vitro dissolution studies and pharmacokinetic studies, it was concluded that fast dissolving tablets of aceclofenac tablets formulated by employing starch glutamate as a superdisintegrant enhanced the dissolution efficiency and improved the bioavailability of the drug as compared to the pure drug and stable. I In nt te er rn na at ti io on na al l J Jo ou ur rn na al l o of f A Ap pp pl li ie ed d P Ph ha ar rm ma ac ce eu ut ti ic cs s

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Section: Pharmacokinetics Studiessupporting

confidence: 93%

Optimization of Statistically Designed Aceclofenac Fast Dissolving Tablets Employing Starch Glutamate as a Novel Superdisintegrant

Kumar

Mudili

2019

Int J App Pharm

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“…Approximately 40% of existing small molecules and 70% of new candidates under development pipelines suffer from the low solubility problem, which is a major reason for their suboptimal drug delivery as well as failures in their development process. Approaches such as cyclodextrin complexation and solid dispersions have been employed to address this challenge and recommend the better formulation over their existing dosage forms [193][194][195][196][197][198]. Likewise, peptides, being biomacromolecules, also exhibit various challenges such as limited water solubility, stability aspects, as well as structural and synthesis complexities, limiting their full exploitation in drug development [199,200].…”

Section: Issues Associated With Marine Peptides In Drug Developmentmentioning

confidence: 99%

Natural Bioactive Thiazole-Based Peptides from Marine Resources: Structural and Pharmacological Aspects

Dahiya

Fuloria

et al. 2020

Marine Drugs

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Peptides are distinctive biomacromolecules that demonstrate potential cytotoxicity and diversified bioactivities against a variety of microorganisms including bacteria, mycobacteria, and fungi via their unique mechanisms of action. Among broad-ranging pharmacologically active peptides, natural marine-originated thiazole-based oligopeptides possess peculiar structural features along with a wide spectrum of exceptional and potent bioproperties. Because of their complex nature and size divergence, thiazole-based peptides (TBPs) bestow a pivotal chemical platform in drug discovery processes to generate competent scaffolds for regulating allosteric binding sites and peptide–peptide interactions. The present study dissertates on the natural reservoirs and exclusive structural components of marine-originated TBPs, with a special focus on their most pertinent pharmacological profiles, which may impart vital resources for the development of novel peptide-based therapeutic agents.

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“…Henceforth, commonly recommended by the physicians of Asian and European countries [12]. Aceclofenac is a BCS (Biopharmaceutics Class System) class II drug with the log partition coefficient value of 2.170 [13]. The daily recommended dose of aceclofenac in an adult is 100 mg twice daily, necessitating adjustment of doses in hepatic impairments [10].…”

Section: Introductionmentioning

confidence: 99%

Pharmacokinetics and bioequivalence assessment of optimized directly compressible Aceclofenac (100 mg) tablet formulation in healthy human subjects

et al. 2020

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The aim of the study was to determine the various pharmacokinetic parameters of the newly developed cost-effective aceclofenac 100 mg tablet formulation (F-15) and to establish the bioequivalence against the marketed brand (ACEMED). Both products (test and reference) were given to 12 healthy non-smokers male subjects with overnight fasting of >10hr. The study was a randomized, single-dose, open-label, two sequence, and two treatment crossover design, with a washout period of 2 weeks. Blood samples (5 mL) from the human subjects were collected before (0 hr) and after drug administration at 13different time points (0.5,

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Improved Pharmacokinetics of Aceclofenac Immediate Release Tablets Incorporating ist Inclusion Complex with Hydroxypropyl-β-Cyclodextrin

Cited by 12 publications

References 3 publications

Optimization of Statistically Designed Aceclofenac Fast Dissolving Tablets Employing Starch Glutamate as a Novel Superdisintegrant

Optimization of Statistically Designed Aceclofenac Fast Dissolving Tablets Employing Starch Glutamate as a Novel Superdisintegrant

Natural Bioactive Thiazole-Based Peptides from Marine Resources: Structural and Pharmacological Aspects

Pharmacokinetics and bioequivalence assessment of optimized directly compressible Aceclofenac (100 mg) tablet formulation in healthy human subjects

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