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      •   صفحهٔ اصلی
      • نشریات انگلیسی
      • Iranian Journal of Pharmaceutical Sciences
      • Volume 12, Issue 2
      • مشاهده مورد
      •   صفحهٔ اصلی
      • نشریات انگلیسی
      • Iranian Journal of Pharmaceutical Sciences
      • Volume 12, Issue 2
      • مشاهده مورد
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      FORMULATION DEVELOPMENT AND EVALUATION OF CLOPIDOGREL FASTDISSOLVING TABLETS

      (ندگان)پدیدآور
      RAGHAVENDRA KUMAR, GUNDAKUMAR, J.N. SURESHSATYANARAYANA, V.SWARUPA RANI, G.SATYA PRASAD, B.
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      نوع مدرک
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      Research Paper
      زبان مدرک
      English
      نمایش کامل رکورد
      چکیده
      The main objective of present research work is to formulate the Clopidogrel Fast Dissolving tablets. Clopidogrel, an antiplatelet drug, belongs to BCS Class-II and used to control Heart attack, Hypertension by inhibiting Platelet activation and aggregation .The Fast Dissolving tablets of Clopidogrel were prepared employing different concentrations of Crospovidone and Croscarmellose sodium in different combinations as a Superdisintegrants by Direct Compression technique using 32 factorial design. The concentration of Crospovidone and Croscarmellose sodium was selected as independent variables, X1 and X2 respectively whereas, wetting time, Disintegration time, t50% ,t90%were selected as dependent variables. Totally nine formulations were designed and are evaluated for hardness, friability, thickness, Assay, Wetting time, Disintegration time, In-vitro drug release. From the Results concluded that all the formulation were found to be with in the Pharmacopoeial limits and the In-vitro dissolution profiles of all formulations were fitted in to different Kinetic models, the statistical parameters like intercept (a), slope (b) & regression coefficient (r) were calculated. Polynomial equations were developed for Wetting time, Disintegration time, t50%, t90%. Validity of developed polynomial equations were verified by designing 2 check point formulations (C1, C2). According to SUPAC guidelines the formulation (F5) containing combination of 15% Crospovidone and 15% Croscarmellose, is the most similar formulation (similarity factor f2=91.3936, dissimilarity factor f1= 1.203& No significant difference, t= -0.00062) to marketed product (PLAVIX-75). The selected formulation (F1) follows First order, Higuchi's kinetics, mechanism of drug release was found to be Fickian Diffusion (n= 0.226).
      کلید واژگان
      Clopidogrel
      32Factorial Design
      super disintegrants
      Crospovidone
      croscarmellose Sodium
      Wetting Time
      Disintegration Time
      Fickian Diffusion
      Pharmaceutics

      شماره نشریه
      2
      تاریخ نشر
      2016-04-01
      1395-01-13
      ناشر
      Iranian Association of Pharmaceutical Scientists
      سازمان پدید آورنده
      Assistant.Professor, DEPARTMENT OF PHARMACEUTICS, NARASARAOPETA INSTITUTE OF PHARMACEUTICAL SCIENCES, YELLAMANDA(Po), NARASARAOPET, GUNTUR (Dt), ANDHRAPRADESH
      Professor & Principal, Narasaraopeta Institute of Pharmaceutical Sciences, Narasaraopet, Guntur(D.t), A.P. India-522601.
      Assistant Professor, Department of Pharmacy Practice, Narasaraopeta Institute of Pharmaceutical Sciences, Narasaraopet, Guntur(D.t), A.P. India-522601.
      Assistant Professor, Department of Pharmacology, Narasaraopeta Institute of Pharmaceutical Sciences, Narasaraopet, Guntur(D.t), A.P. India-522601.
      Assistant Professor, Department of Pharmaceutical Analysis, Narasaraopeta Institute of Pharmaceutical Sciences, Narasaraopet, Guntur(D.t), A.P. India-522601.

      شاپا
      1735-2444
      URI
      https://dx.doi.org/10.22034/ijps.2016.22802
      http://www.ijps.ir/article_22802.html
      https://iranjournals.nlai.ir/handle/123456789/79244

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