Open Access Open Access  Restricted Access Subscription Access
Open Access Open Access Open Access  Restricted Access Restricted Access Subscription Access

In-Vitro and In-Vivo Evaluation of Multi Unit Stavudine Gastroretentive Dosage Forms


Affiliations
1 Hindu College of Pharmacy, Guntur-522002, Andhra Pradesh,, India
2 College of Pharmacy, Al-Jabal Al-Gharbi University, Al- Zawia, Libya
3 Centre for Pharmacy, JNT University, Hyderabad, India
     

   Subscribe/Renew Journal


GRDDSs helps in maintenance of constant therapeutic levels for prolonged periods and produce therapeutic efficacy and there by reduces the total dose of administration.GRDDSs are formulated as floating microparticles, tablets, pellets, capsules, etc among which the multiparticulate systems are more effective than the single unit dosage forms[1]. Assessment of dissolution study results revealed that formulations F7 (Stavudine: Gelucire 43/01- 1:1), F10 (Stavudine: Compritol 888 ATO - 1:1.5) and F19 (Stavudine: Lubritab - 1:2) had retarded the drug release in controlled manner upto 12 hours. The relative contributions of drug diffusion and matrix erosion to drug release were further confirmed by subjecting the dissolution data to Higuchi model and Erosion model. No prominent enthalpy changes was observed in the DSC thermograms of Stavudine+ Gelucire 43/01 physical mixtures and optimized formulations upon comparison with the peaks of drug and polymer alone. From the in vivo X-ray studies, conducted in the healthy human volunteers, it was found that the gastric residence time of the developed Stavudine multi unit granule system floating is dependent on the conditions of the stomach.

Keywords

Gastroretention, Buoyancy, Multi Unit, Melt Granulation.
Subscription Login to verify subscription
User
Notifications
Font Size


Abstract Views: 386

PDF Views: 0




  • In-Vitro and In-Vivo Evaluation of Multi Unit Stavudine Gastroretentive Dosage Forms

Abstract Views: 386  |  PDF Views: 0

Authors

Varun Dasari
Hindu College of Pharmacy, Guntur-522002, Andhra Pradesh,, India
Bahlul Z. Awen
College of Pharmacy, Al-Jabal Al-Gharbi University, Al- Zawia, Libya
Babu Rao Chandu
College of Pharmacy, Al-Jabal Al-Gharbi University, Al- Zawia, Libya
Mukkanti Khagga
Centre for Pharmacy, JNT University, Hyderabad, India

Abstract


GRDDSs helps in maintenance of constant therapeutic levels for prolonged periods and produce therapeutic efficacy and there by reduces the total dose of administration.GRDDSs are formulated as floating microparticles, tablets, pellets, capsules, etc among which the multiparticulate systems are more effective than the single unit dosage forms[1]. Assessment of dissolution study results revealed that formulations F7 (Stavudine: Gelucire 43/01- 1:1), F10 (Stavudine: Compritol 888 ATO - 1:1.5) and F19 (Stavudine: Lubritab - 1:2) had retarded the drug release in controlled manner upto 12 hours. The relative contributions of drug diffusion and matrix erosion to drug release were further confirmed by subjecting the dissolution data to Higuchi model and Erosion model. No prominent enthalpy changes was observed in the DSC thermograms of Stavudine+ Gelucire 43/01 physical mixtures and optimized formulations upon comparison with the peaks of drug and polymer alone. From the in vivo X-ray studies, conducted in the healthy human volunteers, it was found that the gastric residence time of the developed Stavudine multi unit granule system floating is dependent on the conditions of the stomach.

Keywords


Gastroretention, Buoyancy, Multi Unit, Melt Granulation.