E2 design and development of immediate and sustained release tablets of vildagliptin
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This study focused on the design and development of immediate release and sustained release tablets of vildagliptin, an oral antidiabetic drug. The formulation utilized pharmabrust as a super disintegrant for immediate release and methocel k4m cr as a rate-retarding polymer for sustained release, with successful in-vitro release profiles achieved. The physical evaluations indicated that all tablets complied with the desired specifications, demonstrating satisfactory drug content and physical properties.
![ISSN: 0975-8585
July - August 2014 RJPBCS 5(4) Page No. 812
INTRODUCTION
Type 2 diabetes mellitus is a growing problem in most parts of the world. There is now good evidence that controlling hyperglycaemia can help prevent many of the serious complications associated with the disease [1]. Current drugs used for managing TYPE II Diabetes and its precursor syndromes, such as insulin resistance, fall into different classes of compound such as the biguanides, thiazolidinediones, the sulfonylureas peptide analogus, dipeptidyl Peptidase-IV inhibitors and alpha glucosidase inhibitors [2]. Among the most promising new classes of drugs for type 2 diabetes are those that leverage the incretin hormone glucagon-like peptide-1 (GLP-1) [1]. Vildagliptin is an oral anti diabetic drug from the peptide analogues (DPP- 4 inhibitor class).Vildagliptin can be given in monotherapy as well as in combination with other antidiabetic drugs. It rapidly and completely inhibits the activity of DPP- 4 enzymes this results in increase of the two incretin hormones available in our body, they are glucose-like peptide- 1(GLP-1) and glucose dependent insulinotropic peptide (GIP). The activation of these two hormones results in decrease of the blood glucose level by decreasing the glucagon secretion and increase of insulin sensitivity. GLP-1 activation enhances the β-cell sensitivity and reduces the α-cell sensitivity which results in increase in amount of insulin and decreases the amount of glucagon and reduces the glucose level in blood [6].
Sustained-release oral delivery systems are designed to achieve therapeutically effective concentrations of drug in the systemic circulation over an extended period of time, thus achieving better patient compliance and allowing a reduction of both the total dose of drug administered and the incidence of adverse side effects [3]. In long-term therapy, for the treatment of chronic disease conditions, conventional formulations are required to be administered in multiple doses and therefore have several disadvantages [4]. Matrix devices, due to their chemical inertness, drug embedding ability and drug release character, have gained steady popularity for sustaining the release of a drug [5].
The literature survey shows that there is no any published paper on discriminating dissolution study of Vildagliptin tablets and there is no any information about dissolution medium and λmax value of Vildagliptin in BP and USP for in-vitro. So we conducted the discriminating dissolution study for the selection of appropriate dissolution medium and suitable λmax. The purpose of this work is to design the immediate and sustained release tablets of Vildagliptin. To formulate immediate release tablets polymer pharmabrust was used in increasing amount from FI-1 to FI-7 formulations and polymer methocel k4M CR at increasing order were used to formulate sustained release tablets FS-1 to Fs-7 formulations. Pharmabrust is a co-processed excipient system with specific excipients, which allows rapid disintegration and low adhesion to punches. Pharmabrust is smooth and creamy and helps to mask taste and grittiness of the actives. Main advantages Pharmabrust is highly compatible, rapid disintegration and cost effective [7]. Methocel K4M premium are semi synthetic derivative of cellulose. They are swellable and hydrophilic polymer. They are suitable to use as a retardant material in SR matrix tablets, as they are non toxic and easy to handle [8]. Matrix tablets prepared using Methocel polymer on contact with aqueous fluids gets hydrated to form a](https://image.slidesharecdn.com/e2designanddevelopmentofimmediateandsustainedreleasetabletsofvildagliptin-140912011647-phpapp02/85/E2-design-and-development-of-immediate-and-sustained-release-tablets-of-vildagliptin-2-320.jpg)
![ISSN: 0975-8585
July - August 2014 RJPBCS 5(4) Page No. 813
viscous gel layer through which drug will be released by diffusion and/or by erosion of the matrix [9].
MATERIALS AND METHODS
Materials
The Vildagliptin were provided by Popular Pharmaceutical Ltd., Dhaka, Bangladesh. Acetonitrile of HPLC grade was purchased from E. Merck, Darmstadt, Germany. Anhydrous Potassium Dihydrogen Phosphate, Potassium Hydroxide, Phosphoric acid and other reagents were of analytical-reagent grade and purchased from E. Merck, Darmstadt, Germany. Water was deionised and double distilled. Six commercial brands of tablets containing 50 mg Vildagliptin were purchased from local drug shops in Dhaka city after checking their manufacturing license numbers, batch numbers, production and expiry dates.
Preparation of immediate release (IR) sustained release (SR) tablets of Vildagliptin
Immediate release (IR) tablet of Vildagliptin were formulated using superdisintegrating polymer i.e. pharmabrust in increasing amount 10, 20, 30, 40, 60, 70 and 80 mg. In the same way, sustained release (SR) tablet of Vildagliptin were formulated using methocel K4M CR polymer in increasing amount in the same range respectively. The compositions of immediate release tablet FI and sustained release tablet FS are summarized in Table 1 and Table 2.
Table 1: Immediate release formulation of Vildagliptin
Ingredients for Immediate Formulations
FI-1
FI-2
FI-3
FI-4
FI-5
FI-6
FI-7
Vildagliptin
50
50
50
50
50
50
50
Pharmabrust
10
20
30
40
60
70
80
Mannitol
60
60
60
60
60
60
60
Microcrystalline Cellulose (Avicel PH 101)
150
150
150
150
150
150
150
Mg-Stearate
1
1
1
1
1
1
1
Table 2: Sustained release formulation of Vildagliptin
Ingredients for Sustained Formulations
FS-1
FS-2
FS-3
FS-4
FS-5
FS-6
FS-7
Vildagliptin
50
50
50
50
50
50
50
Methocel K4M CR
10
20
30
40
60
70
80
Mannitol
60
60
60
60
60
60
60
Microcrystalline Cellulose (Avicel PH 101)
150
150
150
150
150
150
150
Mg-Stearate
1
1
1
1
1
1
1](https://image.slidesharecdn.com/e2designanddevelopmentofimmediateandsustainedreleasetabletsofvildagliptin-140912011647-phpapp02/85/E2-design-and-development-of-immediate-and-sustained-release-tablets-of-vildagliptin-3-320.jpg)
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July - August 2014 RJPBCS 5(4) Page No. 814
Evaluation of granules
Granules from all the formulation were evaluated for bulk density, compressibily index, angle of Repose.
LBD (Loose Bulk Density) and TBD (Tabbed Bulk Density) were determined by Tab density tester. Initial volume and tapped volume of 2 gm of granules were observed and LBD, TBD, compressibility index and hausner ratio was calculated from the following equations:
LBD = Weight of the powder / volume of the packing.
TBD = Weight of the powder / Tapping volume of the packing.
Carr’s index (%) = {(TBD – LBD) X 100}/TBD
Hausner ratio= Tabbed density/ Bulk density
The angle of repose of granules was determined by following granules through the funnel freely to surface. The radius ® and height (h) of the powder cone was measured and angle of repose was calculated using the following equation:
Angle of Repose θ = tan-1 h/r
Where, h = Height of the powder cone.
r = Radius of the powder cone
Evaluation of Tablets
All the prepared tablets were evaluated for its uniformity of weight, hardness, friability and thickness according to official methods. The average weights and percentage deviation were calculated by weighing 20 tablets from each brand by an analytical weighing balance. The crushing strength was determined with an Automatic Tablet Hardness Tester (8M, Dr Schleuniger, Switzerland).
HPLC Analysis of Vildagliptin
The HPLC method has been developed by using a mixture of acetonitrile and buffer (30:70 v/v) as a mobile phase which was pumped at a flow rate of 0.5 ml/min through the column (C18; 5μ, 4.6 X 150 mm, Waters, USA) at ambient temperature. The injection volume was 10 μl. The objective is to develop and validate a rapid, selective and sensitive HPLC method for determination of Vildagliptin from its pharmaceutical dosage form that have short and simple extraction procedures, consume small amount of solvent for extraction in a short turnaround time. The method is developed using the protocols set out in the International Conference on Harmonization (ICH) guidelines [10].
20 tablets were accurately weighed and the average weight was calculated. Then one tablet weight 50 mg was taken into 50 ml amber volumetric flask and 3 ml of water is added in it to disperse the tablet, then 30 ml of diluting solution was added and the solution was shake](https://image.slidesharecdn.com/e2designanddevelopmentofimmediateandsustainedreleasetabletsofvildagliptin-140912011647-phpapp02/85/E2-design-and-development-of-immediate-and-sustained-release-tablets-of-vildagliptin-4-320.jpg)
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July - August 2014 RJPBCS 5(4) Page No. 820
Figure 6: Percent release curve of IR tablets in water at different λmax values
The above result shows that the drug release profile from immediate release tablets was around 100% within an hour for all the formulation. The use of super disintegrating agent in formulation gives the faster release rate [11]. The percent release data of seven formulations of sustained release tablets (FS-1 to FS-7) are shown in the following figure 7. The drug release from the tablet was sustained for 8 hr. Drug release decreased with increase of polymer loading as methocelK4M CR polymers form viscous gelatinous layer (gel layer) upon exposure to aqueous medium by undergoing rapid hydration and chain relaxation and this gel layer acts as the barrier to release of drug and as a result drug release is prolonged.
Figure 7: Percent release from SR formulation at λmax 212nm](https://image.slidesharecdn.com/e2designanddevelopmentofimmediateandsustainedreleasetabletsofvildagliptin-140912011647-phpapp02/85/E2-design-and-development-of-immediate-and-sustained-release-tablets-of-vildagliptin-10-320.jpg)
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July - August 2014 RJPBCS 5(4) Page No. 825
methocelK4M CR polymer form viscous gelatinous layer which acts as the barrier to release of drug and as a result drug release is prolonged.
ACKNOWLEDGEMENT
The authors are thankful to the management and lab technicians of University of Asia Pacific, Department of Pharmacy, Dhaka, Bangladesh for providing the necessary facilities to carry out this work.
REFERENCES
[1] Pratley RE, Afshin S, Glenn M. Br J Diabetes Vasc Dis 2006; 6:150-6.
[2] https://www.aace.com/files/dm-guidelines-ccp.pdf
[3] Vergnaud JM. Controlled drug release from oral dosage forms, Ellis Horwood Limited, London, 1993.
[4] Chien YW. Novel drug delivery systems; ed. by Chien Y W, Marcel Dekker, Inc; New York, 1992; 139-196.
[5] Basak SC, Kumar KS and Ramalingam M. Brazilian J Pharm Sci 2008;44(3):477-482.
[6] Amori RE, Lau J, Pittas AG. J American Med Assoc 2007; 298:194-206.
[7] Chaudhary SA, Chaudharya AB, Mehtab TA. Int J Res Pharm Sci 2010; 2: 103-107.
[8] Perez-Marcos B, Ford JL, Amstrong DJ, Elliott PNC, Rostron C and Hogan JW. Int J Pharm 1994; 111: 251-259.
[9] Wagner JG. J Pharm Sci 1969; 58: 1253-1257.
[10] EMEA. European Medicines Agency. Validation of Analytical Procedures: Text and Methodology. London: Canary Wharf; 1995:1-15.
[11] Velmurugan S, Vinushitha S. Int J Chem Pharm Sci 2010; 1(2).](https://image.slidesharecdn.com/e2designanddevelopmentofimmediateandsustainedreleasetabletsofvildagliptin-140912011647-phpapp02/85/E2-design-and-development-of-immediate-and-sustained-release-tablets-of-vildagliptin-15-320.jpg)
E2 design and development of immediate and sustained release tablets of vildagliptin
- 1. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 811 Research Journal of Pharmaceutical, Biological and Chemical Sciences Design and Development of Immediate and Sustained Release Tablets of Vildagliptin. Priyanka Shrestha1*, Shiva Kumar Bhandari1, SM Ashraful Islam1, Md Selim Reza2, and Santosh Adhikari3. 1Department of Pharmacy, University of Asia Pacific, Dhanmondi, Dhaka-1209, Bangladesh 2Department of Pharmaceutical Technology, University of Dhaka, Dhaka-1000, Bangladesh 3Department of Pharmacy, Rajiv Gandhi University of Health Sciences, Banglore-560 041, Karnataka, India. ABSTRACT In this study immediate release and sustained release tablets of Vildagliptin was developed. Pharmabrust was used as super disintegrating agent in increasing order in immediate release formulations and methocel k4M CR as rate retarding polymer in sustained release formulations. Tablets were formulated by direct compression method. The in-vitro release profile were determined using USP I apparatus. The release profile of immediate release tablet of all the formulations was 95-100% within 45 minutes. The release profile of sustained release FS-1, FS-2, FS-3, FS-4, FS-5, FS-6 and FS-7 was 94%, 99%, 72%, 76%, 65% and 74% within 8 hours. Formulated tablets were evaluated for physical parameters such as average weight, thickness, disintegration time, potency, LBD, TBD, compressibility Index and angle of repose. All the physical properties of prepared tablets were within limit. Zero order, First order, Higuchi and Korsmeyer et al. models were used to estimate the kinetics of drug release. It was found that the release followed First order release kinetics, as the correlation coefficient R2 value was higher for first order i.e. 0.995. Formulation 6 of immediate release tablet (FI-6) seems to be best similar to the innovator brand for higher f2 i.e. 51.6 and lower f1 value i.e. 3. Formulations were characterized by Fourier transform infrared (FTIR). No any chemical interaction was observed between excipients and drug from IR spectrum. Keywords: Vildagliptin, immediate release, sustained release, pharmabrust, methocel k4M CR, in-vitro study. *Corresponding author
- 2. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 812 INTRODUCTION Type 2 diabetes mellitus is a growing problem in most parts of the world. There is now good evidence that controlling hyperglycaemia can help prevent many of the serious complications associated with the disease [1]. Current drugs used for managing TYPE II Diabetes and its precursor syndromes, such as insulin resistance, fall into different classes of compound such as the biguanides, thiazolidinediones, the sulfonylureas peptide analogus, dipeptidyl Peptidase-IV inhibitors and alpha glucosidase inhibitors [2]. Among the most promising new classes of drugs for type 2 diabetes are those that leverage the incretin hormone glucagon-like peptide-1 (GLP-1) [1]. Vildagliptin is an oral anti diabetic drug from the peptide analogues (DPP- 4 inhibitor class).Vildagliptin can be given in monotherapy as well as in combination with other antidiabetic drugs. It rapidly and completely inhibits the activity of DPP- 4 enzymes this results in increase of the two incretin hormones available in our body, they are glucose-like peptide- 1(GLP-1) and glucose dependent insulinotropic peptide (GIP). The activation of these two hormones results in decrease of the blood glucose level by decreasing the glucagon secretion and increase of insulin sensitivity. GLP-1 activation enhances the β-cell sensitivity and reduces the α-cell sensitivity which results in increase in amount of insulin and decreases the amount of glucagon and reduces the glucose level in blood [6]. Sustained-release oral delivery systems are designed to achieve therapeutically effective concentrations of drug in the systemic circulation over an extended period of time, thus achieving better patient compliance and allowing a reduction of both the total dose of drug administered and the incidence of adverse side effects [3]. In long-term therapy, for the treatment of chronic disease conditions, conventional formulations are required to be administered in multiple doses and therefore have several disadvantages [4]. Matrix devices, due to their chemical inertness, drug embedding ability and drug release character, have gained steady popularity for sustaining the release of a drug [5]. The literature survey shows that there is no any published paper on discriminating dissolution study of Vildagliptin tablets and there is no any information about dissolution medium and λmax value of Vildagliptin in BP and USP for in-vitro. So we conducted the discriminating dissolution study for the selection of appropriate dissolution medium and suitable λmax. The purpose of this work is to design the immediate and sustained release tablets of Vildagliptin. To formulate immediate release tablets polymer pharmabrust was used in increasing amount from FI-1 to FI-7 formulations and polymer methocel k4M CR at increasing order were used to formulate sustained release tablets FS-1 to Fs-7 formulations. Pharmabrust is a co-processed excipient system with specific excipients, which allows rapid disintegration and low adhesion to punches. Pharmabrust is smooth and creamy and helps to mask taste and grittiness of the actives. Main advantages Pharmabrust is highly compatible, rapid disintegration and cost effective [7]. Methocel K4M premium are semi synthetic derivative of cellulose. They are swellable and hydrophilic polymer. They are suitable to use as a retardant material in SR matrix tablets, as they are non toxic and easy to handle [8]. Matrix tablets prepared using Methocel polymer on contact with aqueous fluids gets hydrated to form a
- 3. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 813 viscous gel layer through which drug will be released by diffusion and/or by erosion of the matrix [9]. MATERIALS AND METHODS Materials The Vildagliptin were provided by Popular Pharmaceutical Ltd., Dhaka, Bangladesh. Acetonitrile of HPLC grade was purchased from E. Merck, Darmstadt, Germany. Anhydrous Potassium Dihydrogen Phosphate, Potassium Hydroxide, Phosphoric acid and other reagents were of analytical-reagent grade and purchased from E. Merck, Darmstadt, Germany. Water was deionised and double distilled. Six commercial brands of tablets containing 50 mg Vildagliptin were purchased from local drug shops in Dhaka city after checking their manufacturing license numbers, batch numbers, production and expiry dates. Preparation of immediate release (IR) sustained release (SR) tablets of Vildagliptin Immediate release (IR) tablet of Vildagliptin were formulated using superdisintegrating polymer i.e. pharmabrust in increasing amount 10, 20, 30, 40, 60, 70 and 80 mg. In the same way, sustained release (SR) tablet of Vildagliptin were formulated using methocel K4M CR polymer in increasing amount in the same range respectively. The compositions of immediate release tablet FI and sustained release tablet FS are summarized in Table 1 and Table 2. Table 1: Immediate release formulation of Vildagliptin Ingredients for Immediate Formulations FI-1 FI-2 FI-3 FI-4 FI-5 FI-6 FI-7 Vildagliptin 50 50 50 50 50 50 50 Pharmabrust 10 20 30 40 60 70 80 Mannitol 60 60 60 60 60 60 60 Microcrystalline Cellulose (Avicel PH 101) 150 150 150 150 150 150 150 Mg-Stearate 1 1 1 1 1 1 1 Table 2: Sustained release formulation of Vildagliptin Ingredients for Sustained Formulations FS-1 FS-2 FS-3 FS-4 FS-5 FS-6 FS-7 Vildagliptin 50 50 50 50 50 50 50 Methocel K4M CR 10 20 30 40 60 70 80 Mannitol 60 60 60 60 60 60 60 Microcrystalline Cellulose (Avicel PH 101) 150 150 150 150 150 150 150 Mg-Stearate 1 1 1 1 1 1 1
- 4. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 814 Evaluation of granules Granules from all the formulation were evaluated for bulk density, compressibily index, angle of Repose. LBD (Loose Bulk Density) and TBD (Tabbed Bulk Density) were determined by Tab density tester. Initial volume and tapped volume of 2 gm of granules were observed and LBD, TBD, compressibility index and hausner ratio was calculated from the following equations: LBD = Weight of the powder / volume of the packing. TBD = Weight of the powder / Tapping volume of the packing. Carr’s index (%) = {(TBD – LBD) X 100}/TBD Hausner ratio= Tabbed density/ Bulk density The angle of repose of granules was determined by following granules through the funnel freely to surface. The radius ® and height (h) of the powder cone was measured and angle of repose was calculated using the following equation: Angle of Repose θ = tan-1 h/r Where, h = Height of the powder cone. r = Radius of the powder cone Evaluation of Tablets All the prepared tablets were evaluated for its uniformity of weight, hardness, friability and thickness according to official methods. The average weights and percentage deviation were calculated by weighing 20 tablets from each brand by an analytical weighing balance. The crushing strength was determined with an Automatic Tablet Hardness Tester (8M, Dr Schleuniger, Switzerland). HPLC Analysis of Vildagliptin The HPLC method has been developed by using a mixture of acetonitrile and buffer (30:70 v/v) as a mobile phase which was pumped at a flow rate of 0.5 ml/min through the column (C18; 5μ, 4.6 X 150 mm, Waters, USA) at ambient temperature. The injection volume was 10 μl. The objective is to develop and validate a rapid, selective and sensitive HPLC method for determination of Vildagliptin from its pharmaceutical dosage form that have short and simple extraction procedures, consume small amount of solvent for extraction in a short turnaround time. The method is developed using the protocols set out in the International Conference on Harmonization (ICH) guidelines [10]. 20 tablets were accurately weighed and the average weight was calculated. Then one tablet weight 50 mg was taken into 50 ml amber volumetric flask and 3 ml of water is added in it to disperse the tablet, then 30 ml of diluting solution was added and the solution was shake
- 5. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 815 thoroughly at 250 rpm for 10 minutes by using vortex mixer. Then the volume was adjusted up to the mark with diluting solution. The prepared solution was sonicated for 10 minutes then cooled to room temperature and filtered through whatman filter paper. 1 ml of this solution was taken in 25 ml amber volumetric flask and diluted with diluting solution and volume adjusted up to the mark. Then the resultant solution was filtered through 0.45 μ- disc filter. Potency determination of Vildagliptin tablets 20 mg equivalent Vildagliptin was taken from each immediate release and sustained release formulation and dissolved in 100 ml water and sonicated. Then again 10 ml was taken from there and volume was adjusted upto100ml. From that solution absorbance was measured. Then the concentarion mcg/ml was calculated. Then the potency was calculated from the obtained result. Dissolution method development for Vildagliptin tablet Selection of suitable rpm The dissolution study of Brand A of Vildagliptin was carried on different paddle rpm (75 and 50) for the selection of suitable rpm. Selection of dissolution medium The dissolution study of marketed product of Vildagliptin was carried in different media (Buffer pH 1.2, pH 4.5, pH 6.8, pH 7.8 and water) to select the suitable media for the dissolution study. In- vitro Release Studies of prepared tablets of Vildagliptin The in-vitro dissolution tests were performed by using the selected rpm, wavelength and dissolution medium. In-vitro dissolution study was performed in 900 ml distilled water. The temperature of the medium was maintained at 37oC ± 0.5oC throughout the experiment. The USP dissolution test apparatus type II (Paddle type) was used and the rpm (rotation per minute) was set to 75. At 5, 15, 30, 45 and 60 minutes for immediate release formulations and 0.25, 0.5, 1, 2, 3, 4, 5, 6, 7 and 8 hours for sustained release formulations (10ml) of aliquots were collected for analysis which was then replaced with equal volume of fresh dissolution medium. From the samples collected, absorbance was measured at both λmax values 210 and 212nm using Shimadzu UV – 1700 UV/Visible Double Beam Spectrophotometer (Shimadzu, Japan). Percentage of the drug release was calculated.
- 6. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 816 RESULTS AND DISCUSSION Formulation development of immediate release and sustained release tablets of Vildagliptin The results of physical parameters (weight, hardness, thickness, LBD, TBD, angle of repose, Compressibility index and disintegration time) and potency of the prepared immediate release tablets are shown in Table 3, 4 and 5. The thickness of the tablets were found between 5.43 ± 0.05 mm to 6.67 ± 0.09 mm, hardness of the tablets ranged from 8.69 ± 0.52 kg/cm2 to 9.29 ± 0.14 kg/cm2. And of sustain release tablets are shown in Table 6, 7, 8. The thickness of the SR tablets was found between 4.36 ± 0.04 mm to 4.87 ± 0.12 mm. The weight variations of prepared IR and SR tablets complied with the pharmacopoeial specifications. The drug content of every formulation was found about to 100% of labeled content. So it can be said that physical properties and drug content of the compressed immediate release tablets were satisfactory. Table 3: Physical properties of the prepared powder of different immediate formulations Parameters FI-1 FI-2 FI-3 FI-4 FI-5 FI-6 FI-7 LBD (g/cm3) 0.3 0.305 0.332 0.332 0.356 0.377 0.385 TBD (g/cm3) 0.469 0.48 0.498 0.521 0.516 0.58 0.565 Compressibility Index (%) 36.03 36.45 33.33 36.27 31.1 35 31.85 Angle of Repose 50 49 48 52 45 47 49 Table 4: Evaluation of physical properties of IR tablet formulation Formulation Average Weight (mg) Thickness (mm) Hardness (N) Disintegration Time (min) FI-1 261.425 5.43 ± 0.05 8.90 ± 0.60 1.2 FI-2 271.725 5.55 ± 0.1 9.13 ± 0.37 1.3 FI-3 275.225 6.3 ± 0.14 8.82 ± 0.08 1.2 FI-4 278.25 6.48 ± 0.01 8.73 ± 0.24 1 FI-5 292.65 6.55 ± 0.05 9.29 ± 0.14 1.4 FI-6 301.5 6.1 ± 0.08 9.01 ± 0.33 1.2 FI-7 291.5 6.67 ± 0.09 8.69 ± 0.52 1.3 Table 5: Potency determination of immediate release tablet Formulation Code Potency % FI-1 100.60 ± 0.19 FI-2 99.12 ± 0.37 FI-3 99.26 ± 0.42 FI-4 99.67 ± 0.71 FI-5 100.27 ± 0.36 FI-6 99.44 ± 0.21 FI-7 100 ± 0.62
- 7. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 817 Table 6: Physical properties of the prepared powder of different sustained formulations Parameters FS-1 FS-2 FS-3 FS-4 FS-5 FS-6 FS-7 LBD (g/cm3) 0.313 0.324 0.353 0.375 0.392 0.412 0.416 TBD (g/cm3) 0.5 0.506 0.529 0.554 0.562 0.58 0.585 Compressibility Index (%) 37.4 35.96 33.27 32.31 30.24 28.96 28.88 Angle of Repose 48 46 43 42 40 40 38 Table 7: Evaluation of physical properties of SR tablet formulation Formulation Average Weight (mg) Thickness (mm) Disintegration Time (min) FS-1 221.65 4.36 ± 0.04 25 FS-2 204.65 4.33 ± 0.01 64 FS-3 238.35 4.39 ± 0.01 120 FS-4 316.85 4.72 ± 0.07 Not disintegrated till 120 min FS-5 308.55 4.565 ± 0.04 Not disintegrated till 120 min FI-6 313.75 4.685 ± 0.02 Not disintegrated till 120 min FI-7 320.8 4.865 ± 0.12 Not disintegrated till 120 min Table 8: Potency determination of sustained release tablet Formulation Code Potency % FS-1 100.60 ± 0.56 FS-2 99.53 ± 0.37 FS-3 97.80 ± 0.42 FS-4 100.67 ± 0.71 FS-5 98.27 ± 0.47 FS-6 99.00 ±0.89 FS-7 99.39 ±0.19 Dissolution method development Selection of suitable rpm The dissolution study of Brand A of Vildagliptin was carried on different paddle rpm for the selection of suitable rpm. The result shows that the percent release of brand A Vildagliptin was greater in the case of 75 rpm as compared to the 50 rpm so we select the 75 rpm for further in vitro dissolution study.
- 8. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 818 Figure 2: Percent release curve in 75 rpm and 50 rpm Selection of suitable medium for dissolution study At first Brand A market product of Vildagliptin was used for dissolution study. In the study different dissolution medium was used, the percent release data of brand A in different dissolution medium is shown in following Figure3 and 4. From the above result we can conclude that the percent release from Brand A product was best in water as a dissolution medium and wavelength at 212nm. Figure 3: Percent release from Brand A Vildagliptin at 210 nm (left) and 212nm (right)
- 9. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 819 HPLC Figure 4: Chromatogram of Vildagliptin Determination of potency of marketed product of immediate release Vildagliptin tablets by HPLC The proposed method was used to determine the potency of commercially available tablets (Six brands) containing 50 mg of Vildagliptin. Three replicate determinations i.e. n=3 were carried out and the results are summarized in Figure 5. Figure 5: Graph showing potency of marketed product of immediate release tablets of Vildagliptin by HPLC In the above bar graph, we can see that the market product F has the maximum potency i.e.95.43%. The other products A, B, C, D, E have 92.11%, 93.83%, 94.77%, 91.98% and 90.05% respectively. In- vitro Release Studies of prepared tablets of Vildagliptin As from the above market product in vitro dissolution study we are able to select the water as a dissolution medium and value of λmax 212nm. So the in-vitro dissolution study of formulated tablet was carried on water medium. The percent release data of seven formulations of immediate release tablet (FI-1 to FI-7) are shown in the following figure 6.
- 10. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 820 Figure 6: Percent release curve of IR tablets in water at different λmax values The above result shows that the drug release profile from immediate release tablets was around 100% within an hour for all the formulation. The use of super disintegrating agent in formulation gives the faster release rate [11]. The percent release data of seven formulations of sustained release tablets (FS-1 to FS-7) are shown in the following figure 7. The drug release from the tablet was sustained for 8 hr. Drug release decreased with increase of polymer loading as methocelK4M CR polymers form viscous gelatinous layer (gel layer) upon exposure to aqueous medium by undergoing rapid hydration and chain relaxation and this gel layer acts as the barrier to release of drug and as a result drug release is prolonged. Figure 7: Percent release from SR formulation at λmax 212nm
- 11. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 821 Drug release kinetics of sustained release formulations The correlation coefficients values of the trend lines of the graphs showed that all 7 formulations best fit in First order release pattern, as the highest correlation coefficient i.e. R2=0.995 was obtained from this drug release kinetics which shows that our sustained release formulations release pattern depends on the initial concentration of drug. As the amount of drug decreases, the release rate gradually decreases. Figure 9: First order release curve Figure 8: Zero order release curve Figure 10: Higuchi curve Figure 11: Korsmeyer curve
- 12. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 822 Table 10: Correlation coefficient (R²) values of different formulation in different plot Zero order 1st order Higuchi Korsmeyer R² R² R² R² FS-1 y = 9.504x + 27.66 y = -0.055x + 1.625 y = 31.56x + 8.879 y = 0.751x + 0.059 R² = 0.733 R² = 0.983 R² = 0.927 R² = 0.974 FS-2 y = 8.941x + 31.68 y = -0.093x + 1.706 y = 30.70x + 12.07 y = 0.751x + 0.067 R² = 0.657 R² = 0.808 R² = 0.888 R² = 0.967 Fs-3 y = 8.719x + 25.95 y = -0.068x + 1.748 y = 29.20x + 8.241 y = 0.737x + 0.056 R² = 0.733 R² = 0.995 R² = 0.943 R² = 0.976 FS-4 y = 7.116x + 26.39 y = -0.03x + 1.681 y = 24.78x + 10.12 y = 0.718x + 0.062 R² = 0.639 R² = 0.973 R² = 0.888 R² = 0.970 Fs-5 y = 7.018x +33.57 y = -0.016x + 1.506 y = 25.74x + 15.04 y = 0.731x + 0.076 R² = 0.516 R² = 0.972 R² = 0.797 R² = 0.957 FS-6 y = 6.319x + 26.58 y = -0.017x + 1.664 y = 22.58x + 11.03 y = 0.728x + 0.153 R² = 0.579 R² = 0.880 R² = 0.848 R² = 0.667 FS-7 y = 8.018x + 21.83 y = -0.046x + 1.759 y = 26.72x + 5.803 y = 0.721x + 0.043 R² = 0.736 R² = 0.805 R² = 0.937 R² = 0.983 Table 11: Comparison of dissolution (f1 and f2) data with innovator brand Immediate release formulations (IR) f2 f1 FI-1 50.89 14 FI-2 50.98 10 FI-3 50.98 10 FI-4 51.02 13 FI-5 51.38 5 FI-6 51.6 3 FI-7 50.98 13
- 13. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 823 Table 11 shows the f1 and f2 values of different brands in respect of innovator brand. Similarity factor f2 has been adopted by FDA (1997) and the European Agency for the Evaluation of Medicinal Products by the Committee for Proprietary Medicinal Products (CPMP) to compare dissolution profile. Two dissolution profiles are considered similar and bioequivalent, if f1 is between 0 and 15 and f2 is between 50 and 100. F-6 seems to be best similar to the innovator brand for higher f2 (51.6) and lower f1 value (3). Drug-Excipients compatibility studies Physical compatibility studies were assured by FT-IR studies. The IR spectrums of the mixed powders were taken by preparing potassium bromide pellets under dry condition by using pellet press. Spectra are superimposed. The transmission minima (absorption maxima) in the spectra obtained with the sample corresponded in position and relative size to those in the spectrum obtained with the working/reference standards. The polymer and the drug compatibility were evaluated by spectral as show in Figure 12, 13 and 14. Figure 12: FT-IR Spectra of pure drug Vildagliptin
- 14. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 824 Figure 13: FTIR Spectra of immediate release formulation of Vildagliptin Figure 14: FTIR Spectra of sustained release formulation of Vildagliptin CONCLUSION The present work was to design the immediate and sustained release tablets of Vildagliptin and their in-vitro study. The immediate release tablets were prepared by using pharmabrust as superdisintegrating agent. The use of super disintegrating agent in formulation gave the faster release rate. The sustained release tablets were prepared by using methocel K4M CR as retardant polymer. Drug release decreased with increase of polymer loading as
- 15. ISSN: 0975-8585 July - August 2014 RJPBCS 5(4) Page No. 825 methocelK4M CR polymer form viscous gelatinous layer which acts as the barrier to release of drug and as a result drug release is prolonged. ACKNOWLEDGEMENT The authors are thankful to the management and lab technicians of University of Asia Pacific, Department of Pharmacy, Dhaka, Bangladesh for providing the necessary facilities to carry out this work. REFERENCES [1] Pratley RE, Afshin S, Glenn M. Br J Diabetes Vasc Dis 2006; 6:150-6. [2] https://www.aace.com/files/dm-guidelines-ccp.pdf [3] Vergnaud JM. Controlled drug release from oral dosage forms, Ellis Horwood Limited, London, 1993. [4] Chien YW. Novel drug delivery systems; ed. by Chien Y W, Marcel Dekker, Inc; New York, 1992; 139-196. [5] Basak SC, Kumar KS and Ramalingam M. Brazilian J Pharm Sci 2008;44(3):477-482. [6] Amori RE, Lau J, Pittas AG. J American Med Assoc 2007; 298:194-206. [7] Chaudhary SA, Chaudharya AB, Mehtab TA. Int J Res Pharm Sci 2010; 2: 103-107. [8] Perez-Marcos B, Ford JL, Amstrong DJ, Elliott PNC, Rostron C and Hogan JW. Int J Pharm 1994; 111: 251-259. [9] Wagner JG. J Pharm Sci 1969; 58: 1253-1257. [10] EMEA. European Medicines Agency. Validation of Analytical Procedures: Text and Methodology. London: Canary Wharf; 1995:1-15. [11] Velmurugan S, Vinushitha S. Int J Chem Pharm Sci 2010; 1(2).