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Pre and post characterization of ODTs with emphasis on compression force and quality of super-disintegrants: In vivo analysis in healthy volunteers. | LitMetric

AI Article Synopsis

  • - Oral dispersible tablets (ODTs) are designed to dissolve quickly in the mouth, providing fast relief, but face challenges related to compression that can affect their hardness and drug release.
  • - In this study, various formulations (F1-F9) of ODTs were tested using different compression forces (44, 54, and 64 kN) with two excipients, CCS and SSG, to determine optimal conditions for hardness and drug release.
  • - Results showed that the formulations compressed at 44 kN had the best hardness and quickest drug release, making 44 kN the ideal compression force for producing effective ODTs, while all formulations met USP standards for friability.

Article Abstract

Oral dispersible tablets (ODTs) are patient compliant dosage forms which rapidly disintegrate in the mouth following active absorption with rapid onset of action. The current study was designed to resolve compression problems used for ODTs, as high compression force exhibited hardness and drug release problems. Formulations, F1-F9 were compressed at three different forces 44, 54 and 64 kN using cross-carmellose sodium (CCS) and sodium starch glycolate (SSG) and evaluated for pre and post compression. Formulations F1, F4 and F7 which were compressed at 44 kN showed hardness ranges between 5.09-6.15 with lowest DT (less than 15 s) and better LTZ release. While F2, F5 and F8 (compressed at 54 kN) demonstrated hardness in between 6.90-7.02. Similarly, F3, F6 and F9 compressed at 64 kN showed hardness values between 8.70-8.98 with increased DT and slow LTZ release. Friability results for all the formulations were within United States Pharmacopeial (USP) specifications (<1%). All formulations depicted t-test value <0.5, hence it found that all formulations showed significant statistical value within limits, however best compression force 44 kN showed low p value. It was concluded that optimized compression force for ODTs was 44 kN among all employed forces that exhibited desirable drug release.

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