Fabrication and characterization of nifedipine loaded β-cyclodextrin nanosponges: An in vitro and in vivo evaluation
Cyclodextrin based nanosponges are gaining much consideration due to their aptitude to augment oral solubility of poorly water-soluble medications such as nifedipine. Here in the contemporary research, diphenyl carbonate was employed for crosslinking the cyclodextrin successfully. DLS studies confir...
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Published in | Journal of drug delivery science and technology Vol. 41; pp. 344 - 350 |
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01.10.2017
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Abstract | Cyclodextrin based nanosponges are gaining much consideration due to their aptitude to augment oral solubility of poorly water-soluble medications such as nifedipine. Here in the contemporary research, diphenyl carbonate was employed for crosslinking the cyclodextrin successfully. DLS studies confirmed particle size in the range of 400–500 nm with monodisperse size distribution. TEM measurement established spherical shape and size range of the nanosuspension. SEM photomicrograph confirmed porous structure of placebo nanosponges while drug loaded nanosponge formulation NS3 revealed solid surface. FTIR studies established no drug-polymer interaction. DSC thermograms showed molecular level dispersion of drug in nanosponges. In vitro drug release exhibited a burst release for first fourth hour and delivered drug in sustained manner for subsequent 24 h. When encapsulated within nanosponges, oral bioavailability of nifedipine was enhanced in comparison to control formulation (Cmax for test formulation was 0.2; 0.055 for control). The fabricated nanosponges displayed admirable stability under normal and stress conditions. %Drug entrapment encountered a slight decline (77.33 ± 1.62% to 74.13 ± 1.47%) during storage while %drug release from initial batch was almost identical when compared with stored nanosponges.
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AbstractList | Cyclodextrin based nanosponges are gaining much consideration due to their aptitude to augment oral solubility of poorly water-soluble medications such as nifedipine. Here in the contemporary research, diphenyl carbonate was employed for crosslinking the cyclodextrin successfully. DLS studies confirmed particle size in the range of 400–500 nm with monodisperse size distribution. TEM measurement established spherical shape and size range of the nanosuspension. SEM photomicrograph confirmed porous structure of placebo nanosponges while drug loaded nanosponge formulation NS3 revealed solid surface. FTIR studies established no drug-polymer interaction. DSC thermograms showed molecular level dispersion of drug in nanosponges. In vitro drug release exhibited a burst release for first fourth hour and delivered drug in sustained manner for subsequent 24 h. When encapsulated within nanosponges, oral bioavailability of nifedipine was enhanced in comparison to control formulation (Cmax for test formulation was 0.2; 0.055 for control). The fabricated nanosponges displayed admirable stability under normal and stress conditions. %Drug entrapment encountered a slight decline (77.33 ± 1.62% to 74.13 ± 1.47%) during storage while %drug release from initial batch was almost identical when compared with stored nanosponges.
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Author | Shringirishi, Madhuri Mahor, Alok Kesharwani, Prashant Gupta, Rishikesh Prajapati, Sunil Kumar Bansal, Kuldeep |
Author_xml | – sequence: 1 givenname: Madhuri surname: Shringirishi fullname: Shringirishi, Madhuri email: mshringirishi5@gmail.com organization: Institute of Pharmacy, Bundelkhand University, Jhansi, Uttar Pradesh, India – sequence: 2 givenname: Alok surname: Mahor fullname: Mahor, Alok organization: Institute of Pharmacy, Bundelkhand University, Jhansi, Uttar Pradesh, India – sequence: 3 givenname: Rishikesh surname: Gupta fullname: Gupta, Rishikesh organization: Institute of Pharmacy, Bundelkhand University, Jhansi, Uttar Pradesh, India – sequence: 4 givenname: Sunil Kumar surname: Prajapati fullname: Prajapati, Sunil Kumar organization: Institute of Pharmacy, Bundelkhand University, Jhansi, Uttar Pradesh, India – sequence: 5 givenname: Kuldeep surname: Bansal fullname: Bansal, Kuldeep organization: Institute of Pharmaceutical Research, GLA University, Mathura, Uttar Pradesh, India – sequence: 6 givenname: Prashant surname: Kesharwani fullname: Kesharwani, Prashant email: prashantdops@gmail.com, Prashant_pharmacy04@rediffmail.com organization: Department of Pharmaceutical Technology, International Medical University, Bukit Jalil, Kuala Lumpur, 57000, Malaysia |
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Keywords | β-Cyclodextrin Nanosponges Anti-hypertensive Diphenyl carbonate Nifedipine |
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SubjectTerms | Anti-hypertensive Diphenyl carbonate Nanosponges Nifedipine β-Cyclodextrin |
Title | Fabrication and characterization of nifedipine loaded β-cyclodextrin nanosponges: An in vitro and in vivo evaluation |
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