Literature DB >> 33688188

Investigating Halloysite Nanotubes as a Potential Platform for Oral Modified Delivery of Different BCS Class Drugs: Characterization, Optimization, and Evaluation of Drug Release Kinetics.

Tazeen Husain1, Muhammad Harris Shoaib1, Farrukh Rafiq Ahmed1, Rabia Ismail Yousuf1, Sadaf Farooqi1, Fahad Siddiqui1, Muhammad Suleman Imtiaz1, Madiha Maboos1, Sabahat Jabeen1.   

Abstract

PURPOSE: This study systematically investigated the potential of four model drugs (verapamil HCl, flurbiprofen, atenolol, and furosemide), each belonging to a different class of Biopharmaceutics Classification Systems (BCS) to be developed into oral modified release dosage forms after loading with halloysite nanotubes (HNTs).
METHODS: The drugs were studied for their loading (mass gain %) by varying solvent system, method, pH, and ratios of loading into the nanotubes using D-optimal split-plot design with the help of Design Expert software. Drug-loaded halloysites were characterized by XRD, DTA, FTIR, SEM, and HPLC-UV-based assay procedures. Dissolution studies were also performed in dissolution media with pH 1.2, 4.5, and 6.8. Moreover, the optimized samples were evaluated under stress stability conditions for determining prospects for the development of oral dosage forms.
RESULTS: As confirmed with the results of XRD and DTA, the drugs were found to be converted into amorphous form after loading with halloysite (HNTs). The drugs were loaded in the range of ~7-9% for the four drugs, with agitation providing satisfactory and equivalent loading as compared to vacuum plus agitation based reported methods. FTIR results revealed either only weak electrostatic (verapamil HCl and flurbiprofen) or no interaction with the surface structure of the HNTs. The dissolution profiling depicted significantly retarded release of drugs with Fickian diffusion from a polydisperse system as a model that suits well for the development of oral dosage forms. HPLC-UV-based assay indicated that except furosemide (BCS class IV), the other three drugs are quite suitable for development for oral dosage forms.
CONCLUSION: The four drugs investigated undergo phase transformation with HNTs. While agitation is an optimum method for loading drugs with various physicochemical attributes into HNTs; solvent system, loading ratios and pH play an important role in the loading efficiency respective to the drug properties. The study supports the capability of developing HNT-based modified release oral dosage forms for drugs with high solubility.
© 2021 Husain et al.

Entities:  

Keywords:  DTA; FTIR; HNT; SEM; XRD; atenolol; biopharmaceutics classification system; drug release kinetics; flurbiprofen; furosemide; halloysite nanotubes; verapamil HCl

Mesh:

Substances:

Year:  2021        PMID: 33688188      PMCID: PMC7935346          DOI: 10.2147/IJN.S299261

Source DB:  PubMed          Journal:  Int J Nanomedicine        ISSN: 1176-9114


  41 in total

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Authors:  Raghuvara Yendluri; Yuri Lvov; Melgardt M de Villiers; Vladimir Vinokurov; Ekaterina Naumenko; Evgenya Tarasova; Rawil Fakhrullin
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9.  Diclofenac sodium entrapment and release from halloysite nanotubules.

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10.  Developing micro-/nanoparticulate drug delivery systems using "design of experiments".

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3.  A Novel Efficient Piscine Oral Nano-Vaccine Delivery System: Modified Halloysite Nanotubes (HNTs) Preventing Streptococcosis Disease in Tilapia (Oreochromis sp.).

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  3 in total

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