Novel pH- and Temperature-Responsive Blend Hydrogel Microspheres of Sodium Alginate and PNIPAAm-g-GG for Controlled Release of Isoniazid

Kajjari, Praveen B.; Manjeshwar, Lata S.; Aminabhavi, Tejraj M.

doi:10.1208/s12249-012-9838-8

Cited by 54 publications

(18 citation statements)

References 30 publications

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“…A similar observation was noted by Krishna Rao et al, [33] from the cefedroxil drug release studies through interpenetrating network microgels of chitosan/acrylamide grafted PVA. …”

Section: X-ray Diffractometric Analysissupporting

confidence: 85%

Sodium Alginate–locust Bean Gum Ipn Hydrogel Beads for the Controlled Delivery of Nimesulide-Anti-Inflammatory Drug

Madhavi¹,

Babu²,

Maruthi³

et al. 2017

Int J Pharm Pharm Sci

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Objective: The objective of this study was to formulate and evaluate the drug release studies using locust bean gum (LBG) and sodium alginate (NaAlg) and cross-linked with glutaraldehyde for the controlled release (CR) of Nimesulide, an anti-inflammatory drug.Methods: Locust bean gum (LBG) and sodium alginate (NaAlg) blend hydrogel beads were prepared by an extrusion method using glutaraldehyde as a crosslinker. Nimesulide an anti-inflammatory drug was encapsulation within LBG/NaAlg blend hydrogel beads. Morphology, size, encapsulation efficiency and drug release from these hydrogel beads were evaluated by different characterization techniques such as fourier transform infrared spectroscopy (FTIR), differential scanning calorimetry (DSC), scanning electron microscopy (SEM), x-ray diffraction (X-RD) studies.Results: Drug-loaded hydrogel beads were analyzed by FTIR, which indicates the interaction between drug and polymers. DSC thermograms on drug-loaded microbeads confirmed the polymorphism of Nimesulide and indicated a molecular level dispersion of the drug in the hydrogel beads. SEM confirmed the spherical nature and rough surface of the hydrogel beads produced. X-RD study was performed to understand the crystalline nature of drug after encapsulated into the hydrogel beads and confirmed the complete dispersion of the drug in the polymer matrix. In vitro release studies conducted in pH-7.4 which indicated a dependence of release rate on the amount of drug loading and the amount of LBG/NaAlg, but slow release rates were extended up to 48 h. The cumulative release data were fitted to an empirical equation to compute diffusion exponent (n) which indicated the non-fickian trend for drug release. Conclusion:These results clearly demonstrated that the ability of these newly developed hydrogel beads containing Nimesulide for its sustained release could possibly be advantageous to patient compliance with reduced dosing interval.

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“…A similar observation was noted by Krishna Rao et al, [33] from the cefedroxil drug release studies through interpenetrating network microgels of chitosan/acrylamide grafted PVA. …”

Section: X-ray Diffractometric Analysissupporting

confidence: 85%

Sodium Alginate–locust Bean Gum Ipn Hydrogel Beads for the Controlled Delivery of Nimesulide-Anti-Inflammatory Drug

Madhavi¹,

Babu²,

Maruthi³

et al. 2017

Int J Pharm Pharm Sci

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“…It has been found previously that a higher temperature alters the viscosity and hydrophilicity of polymers such as ALG and CS, which can be used to improve control of the release of an active agent [26,50]. This was not observed here for the carrier systems containing GA 3 .…”

Section: Release Kinetics At Different Ph and Temperaturementioning

confidence: 44%

Chitosan nanoparticles as carrier systems for the plant growth hormone gibberellic acid

Pereira

Silva

Oliveira

et al. 2017

Colloids and Surfaces B: Biointerfaces

169

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This work concerns the development of nanocarriers composed of alginate/chitosan (ALG/CS) and chitosan/tripolyphosphate (CS/TPP) for the plant growth regulator gibberellic acid (GA). ALG/CS nanoparticles with and without GA presented mean size of 450±10nm, polydispersity index (PDI) of 0.3, zeta potential of -29±0.5mV, concentrations of 1.52×10 and 1.92×10 nanoparticles mL, respectively, and 100% encapsulation efficiency. CS/TPP nanoparticles with and without GA presented mean size of 195±1nm, PDI of 0.3, zeta potential of +27±3mV, concentrations of 1.92×10 and 3.54×10 nanoparticles mL, respectively, and 90% encapsulation efficiency. The nanoparticles were stable during 60days and the two systems differed in terms of the release mechanism, with the release depending on factors such as pH and temperature. Bioactivity assays using Phaseolus vulgaris showed that the ALG/CS-GA nanoparticles were most effective in increasing leaf area and the levels of chlorophylls and carotenoids. The systems developed showed good potential, providing greater stability and efficiency of this plant hormone in agricultural applications.

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“…In this section, we will review the two types of cross-linking preparations according to the development of cross-linkers. Many bifunctional small molecules such as glutaraldehyde, urea formaldehyde and pyromellitic dianhydride have been successfully applied to cross-link to chitosan-based polymers for intestinal drug delivery, as shown in Table 1 [41][42][43][44][45]. These molecules could take advantage of the available -NH 2 and -OH chemical handles on the chitosan backbone to form linkage chemistries, including Schiff base and amide formation.…”

Section: Chemical Cross-linking Preparationsmentioning

confidence: 99%

The design of pH-sensitive chitosan-based formulations for gastrointestinal delivery

Liu

Yang

et al. 2015

Drug Discovery Today

146

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Novel pH- and Temperature-Responsive Blend Hydrogel Microspheres of Sodium Alginate and PNIPAAm-g-GG for Controlled Release of Isoniazid

Cited by 54 publications

References 30 publications

Sodium Alginate–locust Bean Gum Ipn Hydrogel Beads for the Controlled Delivery of Nimesulide-Anti-Inflammatory Drug

Sodium Alginate–locust Bean Gum Ipn Hydrogel Beads for the Controlled Delivery of Nimesulide-Anti-Inflammatory Drug

Chitosan nanoparticles as carrier systems for the plant growth hormone gibberellic acid

The design of pH-sensitive chitosan-based formulations for gastrointestinal delivery

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