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      Formulation development and evaluation of zolmitriptan oral soluble films using 2 2 factorial designs

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          Abstract

          Objective:

          The present investigation involves the development of zolmitriptan oral soluble film (OSF) formulations and optimization with quality by design (QBD) using natural polymers and evaluation.

          Materials and Methods:

          Initially, various natural polymers such as sodium alginate, pectin, and gelatin were screened by casting films using solvent casting technique and the prepared films were evaluated. Based on the physical and mechanical properties, sodium alginate was selected as best film former and zolmitriptan-loaded films were casted. The formulation was optimized with the help of 2 2 factorial experimental designs (QBD) in which sodium alginate concentration and plasticizer concentrations were used as factors and at two levels. The drug-loaded films were evaluated for various mechanical, physicochemical properties, and in vitro drug release properties. Factor effects were interpreted by calculating the main factor effects and by plotting the interaction plots.

          Results:

          Thickness of the films, disintegration time, and percent drug loading efficiency were in the range of 0.698 ± 0.13–1.318 ± 0.22 mm, 175 ± 3.1–280 ± 1.7 s, and 68.34 ± 0.5–94.70 ± 0.7% w/v, respectively. Cumulative percent drug released was 61.8 ± 2.6–94.7 ± 4.1% after 30 min. Polymer concentration at two levels of plasticizer had statistically significant effect on drug loading efficiency and in vitro drug release rate. X 2 formulation was found to be excellent in drug loading efficiency and in vitro drug release profiles; hence, drug excipient compatibility studies using Fourier transform infrared spectroscopy and stability studies for 60 days were carried out for X 2 formulation and found to be stable.

          Conclusion:

          Sodium alginate OSFs containing zolmitriptan was successfully prepared, optimized, and evaluated.

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          Most cited references19

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          Migraine symptoms: results of a survey of self-reported migraineurs.

          Migraine is an episodic headache disorder associated with various combinations of neurologic, gastrointestinal, and autonomic symptoms. Gastrointestinal disturbances including nausea, vomiting, abdominal cramps, or diarrhea are almost universal. Sensory hyperexcitability manifested by photophobia, phonophobia, and osmophobia are frequently experienced. Other symptoms include blurry vision, nasal stuffiness, tenesmus, polyuria, pallor, and sweating. Our telephone interview survey of 500 self-reported migraine sufferers was performed in 1994. The most common reported symptoms associated with migraine were pain, nausea, problems with vision, and vomiting. Nausea occurred in more than 90% of all migraineurs; nearly one third of these experienced nausea during every attack. Vomiting occurred in almost 70% of all migraineurs; nearly one third of these vomited in the majority of attacks. In those who experienced nausea, 30.5% indicated that it interfered with their ability to take their oral migraine medication; in those with vomiting, 42.2% indicated that it interfered with their ability to take their oral migraine medication. The most important features of a migraine medication were rapid and effective relief of headache pain, decreasing the likelihood of headache recurrence, and not causing nausea. Many migraine patients suffer needlessly because their nausea and vomiting are both unreported to, and unrecognized by physicians. The presence of these symptoms is crucial to diagnose migraine not accompanied by aura.
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            Biostatistics

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              Formulation and evaluation of fast dissolving films for delivery of triclosan to the oral cavity.

              The present investigation was undertaken with the objective of formulating TC containing fast dissolving films for local delivery to oral cavity. Various film forming agents, film modifiers and polyhydric alcohols were evaluated for optimizing the composition of fast dissolving films. The potential of poloxamer 407 and hydroxypropyl-beta- cyclodextrin (HPBCD) to improve solubility of TC was investigated. Fast dissolving films containing hydroxypropyl methylcellulose (HPMC), xanthan gum, and xylitol were formulated. Use of poloxamer 407 and HPBCD resulted in significant improvement in the solubility of TC. Fast dissolving films containing TC-HPBCD complex and TC-Poloxamer 407 were formulated and were evaluated for the in vitro dissolution profile and in vitro microbiological assay. Films containing TC-Poloxamer 407 exhibited better in vitro dissolution profile and in vitro antimicrobial activity as compared to the films containing TC-HPBCD complex. Effect of incorporation of eugenol on the in vivo performance of TC-Poloxamer 407 containing films was evaluated in human volunteers. Eugenol containing films improved the acceptability of TC-Poloxamer 407 films with respect to taste masking and mouth freshening without compromising the in vivo dissolution time.
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                Author and article information

                Journal
                Int J Pharm Investig
                Int J Pharm Investig
                IJPI
                International Journal of Pharmaceutical Investigation
                Medknow Publications & Media Pvt Ltd (India )
                2230-973X
                2230-9713
                Oct-Dec 2016
                : 6
                : 4
                : 201-206
                Affiliations
                [1] Department of Pharmaceutics, Hindu College of Pharmacy, Guntur, Andhra Pradesh, India
                [1 ] Department of Pharmaceutics, Vignan Pharmacy College, Guntur, Andhra Pradesh, India
                Author notes
                Address for correspondence: Dr. Poluri Koteswari, Hindu College of Pharmacy, Guntur, Andhra Pradesh, India. E-mail: polurikoteswari@ 123456gmail.com
                Article
                IJPI-6-201
                10.4103/2230-973X.195927
                5204251
                b10746b0-038c-4cca-bd38-a6c881ba40cd
                Copyright: © International Journal of Pharmaceutical Investigation

                This is an open access article distributed under the terms of the Creative Commons Attribution-NonCommercial-ShareAlike 3.0 License, which allows others to remix, tweak, and build upon the work non-commercially, as long as the author is credited and the new creations are licensed under the identical terms.

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                Categories
                Original Research Article

                Pharmacology & Pharmaceutical medicine
                interaction plots,oral soluble film,quality by design,sodium alginate,zolmitriptan

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