Sujit Chandra Mazumder’s research while affiliated with Noakhali Science and Technology University and other places

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Publications (1)


Figure 1. Effect of concentration of superdisintegrants on disintegration time.  
Figure 2. Zero order release model of allopurinol FDTs of group A formulations containing croscarmellose sodium (F-1, F-2 and F-3).  
Figure 3. First order release model of allopurinol FDTs of group A formulations containing croscarmellose sodium (F-1, F-2 and F-3).  
Figure 4.Higuchi release model of allopurinol FDTs of Group A formulations containing croscarmellose sodium (F-1, F-2 and F-3).  
Table 4 . Percent drug release of different batches of allopurinol FDTs.

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Fabrication and in vitro Evaluation of Allopurinol Fast Dissolving Tablets Using Croscarmellose Sodium, Sodium Starch Glycolate and Crospovidone as Superdisintegrants
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June 2016

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2 Citations

Dhaka University Journal of Pharmaceutical Sciences

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Sujit Chandra Mazumder

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p>The main objective of the study was to formulate fast dissolving tablets of allopurinol to achieve better dissolution rate and further improving the bioavailability to provide a quick onset of action. Nine formulations of fast dissolving tablets of allopurinol were prepared by direct compression technique using croscarmellose sodium (Group A), sodium starch glycolate (Group B) and crospovidone (Group C) as superdisintegrants in different concentrations. All formulations showed satisfactory mechanical strength, uniform weight & drug content, and lesser wetting time & dispersion time. In vitro disintegration time, dispersion time, wetting time of all nine formulations were obtained from 11.67±0.88 to 40.67±1.20 seconds, 32.67±0.88 to 65.33±1.45 seconds and 21.67±0.33 to 50.00±1.53 seconds respectively. Amongst all formulations, formulation F-9 prepared by 4.17% crospovidone showed least disintegrating time of 11.67±0.88 seconds along with rapid drug release (98.88% within 15 minutes). Dhaka Univ. J. Pharm. Sci. 15(1): 73-81, 2016 (June)</p

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Citations (1)


... Naringin significantly increases the bioavailability of paclitaxel at a dose of 3.3 mg/kg. Other types of drugs, such as diltiazem, verapamil, saquinavir, and cyclosporine, may also be increased (Oladimeji et al., 2018). Naringin inhibits CYP-450 enzymes, particularly CYP-3A4. ...

Reference:

The development and process optimization of atorvastatin calcium and Naringin bilayer tablet to improve the bioavailability of atorvastatin calcium by two-level factorial design using Design-Expert®
Fabrication and in vitro Evaluation of Allopurinol Fast Dissolving Tablets Using Croscarmellose Sodium, Sodium Starch Glycolate and Crospovidone as Superdisintegrants

Dhaka University Journal of Pharmaceutical Sciences