Your search keyword '"Maqsood Ahmed"' showing total 16 results

1. Empagliflozin: HPLC based analytical method development and application to pharmaceutical raw material and dosage form

Author

Anas, M Hanif, Rabia, Bushra, Nahlah Elkudssiah, Ismail, Rahila, Bano, Saima, Abedin, Shazia, Alam, Maqsood, Ahmed Khan, and Hafiz, Muhammad Arif

Subjects

Dosage Forms, Glucosides, Chemistry, Pharmaceutical, Reproducibility of Results, Benzhydryl Compounds, Sodium-Glucose Transporter 2 Inhibitors, Chromatography, High Pressure Liquid

Abstract

The current investigation is based on efficient method development for the quantification of empagliflozin in raw and pharmaceutical dosage forms, as no pharmacopoeial method for the drug is available so far. The developed analytical method was validated as per ICH guidelines. C18 column with mobile phase (pH 4.8) consisted of 0.1% trifluoroacetic acid solution and acetonitrile (70:30 v/v) was used for drug analysis. The calibration plot showed good linear regression (r20.999) over the concentration of 0.025-30 μg mL

Published

2021

2. Influence of different gelling polymers on dexibuprofen gel formulation: In- vitro characterization and stability profile.

Author

Hanif, Anas M., Bushra, Rabia, Shafiq, Yousra, Aslam, Nousheen, Mughal, Muhammad Azhar, Huma, Ambreen, Ali, Sobia Iftikhar, and Khan, Maqsood Ahmed

Abstract

The present study was designed to formulate a 5% topical gel formulation containing dexibuprofen. Herein, we reported the utilization of different gelling polymers including hydroxyl propyl methyl cellulose (HPMC), carboxy methyl cellulose (CMC), carbopol 940 and leutrol F127 at three concentration levels. Overall, twelve trials (TD1 to TD12) were prepared in four batches (DEX-I to DEX-IV), each having three trial dexibuprofen gel formulations. All formulations were evaluated for organoleptic properties, clarity, pH, consistency, viscosity and spreadability. Trials of DEX-I and DEX- III batches (containing HPMC and carbopol 940polymers respectively), were a lack in smoothness, clarity and viscosity. Contra wise, TD5, TD6 dexibuprofen gel formulations of batch DEX-II and TD10, TD11 and TD12 of DEX-IV having CMC and lutrol® F127 correspondingly were found to be viscous and free from grittiness and precipitation. In vitro drug kinetics revealed the Weibull kinetic model as the best (r2>0.999, AIC 31.427-37.381, MSC 2.259-3.421). Stability testing was performed on the selected formulations (TD5, TD6, TD10, TD11 and TD12) having acceptable physicochemical attributes. Only TD11 and TD12 were found to be stable at room temperature after three months. Based on the findings, it is concluded that lutrol® F127 based dexibuprofen gel formulations delivered excellent spreadability, better drug release, and satisfactory stability profile. [ABSTRACT FROM AUTHOR]

Published

2023

3. Development and validation of reverse phase HPLC method for determination of angiotensin receptor blocking agent irbesartan in plasma

Author

Zebun, Nisa, Syed Imran, Ali, Mehwish, Rizvi, Maqsood Ahmed, Khan, Rafi Akhter, Sultan, Rasheeda, Fatima, Najma, Shaheen, Farya, Zafar, Sadia Suri, Kashif, and Najeeb, Khatian

Subjects

Chromatography, Reverse-Phase, Drug Stability, Limit of Detection, Calibration, Humans, Irbesartan, Angiotensin II Type 1 Receptor Blockers, Sensitivity and Specificity, Chromatography, High Pressure Liquid

Abstract

A sensitive, reproducible and modest analytical procedure was developed and validated for evaluation of irbesartan in human plasma. LLE (Liquid-Liquid extraction) of the drug was carried out with acetonitrile (1:1 v/v). Chromatographic separation of irbesartan was conducted by the help of 4.0mm × 25cm column having L1 packing from plasma and mobile phase utilizing HPLC. The mobile phase comprise of phosphate buffer and acetonitrile in a ratio of 67:33 v/v. The flow rate was set at 1ml/minute and the detector at a wavelength of 220 nm. The resolution of irbesartan was well performed from plasma components. This method was validated and demonstrated linearity with a concentration range of 0.1to 6μg/ml of irbesartan in plasma. Intra-day, inter-day accuracy was found 89.33% to 96.37% while intra-day, inter-day precision was found within the limit of 0.02 and 2.15 respectively. The mean recovery of irbesartan was 97.28%. The efficacy of extraction was proved by above-mentioned results. In plasma, the 0.05 and 0.1μg/ml dilutions were exhibited as the LOD and LOQ of irbesartan. Stability studies disclosed that irbesartan showed stability at -20°C storage.

Published

2019

4. Formulation design, characterization and optimization of cinitapride (1mg) immediate release tablets using direct compression technology

Author

Rabia, Bushra, Attaur, Rehman, Sana, Ghayas, Farya, Zafar, Huma, Ali, Yousra, Shafiq, Farah, Khalid, Maqsood Ahmed, Khan, Anas, Hanif, and Omer, Mustapha

Subjects

Compressive Strength, Chemistry, Pharmaceutical, Drug Compounding, Drug Design, Benzamides, Tablets

Abstract

Cinitapride hydrogen tartarate is relatively a new prokinetic agent that widely prescribed for GERD and epigastric pain. Present study was aimed to develop and optimize cinitapride (1 mg) immediate release (IR) tablet formulation(s) by direct compression using central composite rotatable technique. Overall nine formulations (FC1-FC9) were generated by varying the composition of binder avicel PH 102 (X1) and superdisintegrant crospovidone (X2). The effect of interaction of excipients on hardness (Y1), friability (Y2), disintegration (Y3) and dissolution at 15 min (Y4) were analyzed by RSM plotting. On the basis of physico-chemical evaluation FC3, FC4 and FC6 were found to be the optimized formulations however; FC3 was selected to be the best trial owing to excellent drug release (100.17%) with least friability (0.14%). These IR tablets showed the release pattern similar to the Weibull model with r2 value of 0.978-0.998. The dissimilarity (f1) and similarity indexes (f2) of FC3, FC4, FC6 with the marketed product were estimated to be 2.57 and 76.51, 4.51 and 64.46, 4.32 and 66.78 respectively. Trial optimized formulations were highly stable with the shelf lives of 58-64 months. So, keeping in view the results of present investigation, it is concluded that the technique of manufacturing and optimization is found to be excellent for developing immediate release cinitapride tablets.

Published

2018

5. Dexibuprofen: Statistical assessment of drug release kinetics and investigative quality perspective

Author

Anas M, Hanif, Ali Akbar, Sial, Huma, Ali, Farya, Zafar, Mirza Tasawar, Baig, Rabia, Bushra, Maqsood Ahmed, Khan, Amber, Nawab, Omer, Mustapha, and Shumaila, Shafique

Subjects

Drug Liberation, Therapeutic Equivalency, Anti-Inflammatory Agents, Non-Steroidal, Humans, Ibuprofen, Qualitative Research

Abstract

Healthcare professionals including physicians and pharmacists have been trying since long to come across and work out regarding the issue of generic alternatives, which is highly affected by factors like therapeutic efficacy, cost effectiveness, aesthetic and elegant appearance and implementation of packaging number over the drug product. However, the community pharmacist professionals are also facing difficulty in making decision regarding selection and dispensing the most efficacious brand to the patients. In this regard, the initiation of recent approaches for the development of amenable drug products has led to evolve the concept of generating new avenues for achieving higher patient compliance. Hence, the objective of this study was to evaluate the quality attributes and make comparisons regarding different brands of Dexibuprofen available in market of Karachi, Pakistan. The study is based on evaluation of physical chemical parameters of five different brands. Moreover, a comparative dissolution profile of selected brands of Dexibuprofen was also performed by applying numerous approaches. DEX-1was selected as reference while DEX-2- DEX-5 was selected as test brands. Results of all the selected brands met all the compendial requirements. Interpretation of the entire aforementioned test was evaluated using model independent, model- dependent and one - way ANOVA. The work presented in this study has been designed to provide quality standard products easily accessible in Pakistani market.

Published

2018

6. Biowaiver studies of newly optimized meloxicam tablets

Author

Farya, Zafar, Sohail, Khan, Huma, Ali, Shabana N, Shah, Rabia, Bushra, Ghazala Raza, Naqvi, Kashif, Maroof, Maqsood Ahmed, Khan, and Zebun, Nisa

Subjects

Drug Liberation, Chemistry, Pharmaceutical, Drug Compounding, Anti-Inflammatory Agents, Non-Steroidal, Meloxicam, Tablets

Abstract

In this research work biowaiver studies of newly developed and optimized Meloxicam 7.5mg and 15mg water dispersible formulations were carried out at different dissolution media i.e. 0.1N HCl, phosphate buffer pH 4.5, pH 6.8, and pH 7.5 at 50 rpm. For this purpose reference (MA

Published

2018

7. Development and validation of RP- HPLC method with UV detection to determine and quantify dimenhydrinate in human plasma

Author

Zeb-Un-Nisa, Muhammad Harris, Shoaib, Syed Imran, Ali, Mehwish, Rizvi, Huma Ali, Ali, Rasheeda, Fatima, Maqsood Ahmed, Khan, and Sadia Suri, Kashif

Subjects

Chromatography, Reverse-Phase, Drug Stability, Limit of Detection, Dimenhydrinate, Liquid-Liquid Extraction, Temperature, Humans, Spectrophotometry, Ultraviolet, Reference Standards, Chromatography, High Pressure Liquid

Abstract

A simple, sensitive and rigorous method for estimation of dimenhydrinate in human plasma was searched and its validation was carried out. LLE (Liquid-Liquid extraction) of analyte with mixture of Hexane and ethyl acetate (1:1 v/v) was carried out for the preparation of Plasma Samples, Chromatographic elution of dimenhydrinate was conducted in human plasma and mobile phase with C-18 bonda Pack column (10μm; 250 × 4.6), using a mobile phase consisting a solution of ammonium bicarbonate in water and methanol at a flow rate of 0.5ml/minute with UV detection at 229 nm. The resolution of dimenhydrinate was well performed from plasma components. This method was validated and exhibited linearity with concentration range of 6 to 380ng/ml of dimenhydrinate in plasma. The Intra day precision was 89.2 to 96.89% and Inter day precision was 88.6% to 93.26%, the average recovery of dimenhydrinate was 97.02%. The efficacy of extraction was proved by above mentioned results. 2ng/ml and 6ng/ml, were appraised as the LOD and LOQ of dimenhydrinate, stability studies disclosed that dimenhydrinate exhibited stability in Plasma after Freezethaw cycles and upon -20°C storage, the method was developed well.

Published

2018

8. Incidence of drug interactions in intensive care units in tertiary care settings: Classification, facts and measures

Author

Hina, Hasnain, Huma, Ali, Farya, Zafar, Ali Akbar, Sial, Shazia, Alam, Anwar Ejaz, Beg, Rabia, Bushra, Mehwish, Rizvi, Maqsood Ahmed, Khan, Huma, Shareef, Ghazala R, Naqvi, and Anum, Tariq

Subjects

Male, Intensive Care Units, Time Factors, Tertiary Healthcare, Incidence, Polypharmacy, Humans, Drug Interactions, Female, Pakistan, Middle Aged, Classification

Abstract

Drug-drug interactions (DDIs) are extremely significant concern, particularly in sensitive population including pediatric and geriatric. Propensity for the development of DDIs is high in patients admitted at intensive care units (ICU). This study was conducted to evaluate the DDIs incidence, facts and measures in ICU. From a total of 150 cases studied for ICU patients, with the mean age of 56.37±12.45 years, 55.33% were male and the rest were female 44.66%. The demographic information like age, gender and main diagnosis details of study participants that were extracted from the patients' clinical record. A statistically significant association between the drug interaction and the number of drugs prescribed per prescription was observed (p0.0001). Concerning the onset of outcome, 52% of DDIs distinguished as delayed onset of effect (past 24 hours) and 35% were categorized as rapid onset (within 24 hours). Despite the facts regarding patient safety and minimizing DIs error, polypharmacy is still frequent in critically ill patients admitted in ICU attributed high risk of adverse reactions due to use of multiple interventions to treat severity of disease condition. Such studies may be used to develop an effective tool for the diagnosis and management of DDIs.

Published

2018

9. Empagliflozin: HPLC based analytical method development and application to pharmaceutical raw material and dosage form.

Author

Hanif, Anas M., Bushra, Rabia, Ismail, Nahlah Elkudssiah, Bano, Rahila, Abedin, Saima, Alam, Shazia, Khan, Maqsood Ahmed, and Arif, Hafiz Muhammad

Abstract

The current investigation is based on efficient method development for the quantification of empagliflozin in raw and pharmaceutical dosage forms, as no pharmacopoeial method for the drug is available so far. The developed analytical method was validated as per ICH guidelines. C18 column with mobile phase (pH 4.8) consisted of 0.1% trifluoroacetic acid solution and acetonitrile (70:30 v/v) was used for drug analysis. The calibration plot showed good linear regression (r2>0.999) over the concentration of 0.025-30 μg mL-1. The LOD and LOQ were found to be 0.020 μg mL-1 and 0.061 μg mL-1, respectively. The percentage recovery was estimated between 98.0 to 100.13%. Accuracy and precision data were found to be less than 2%, indicating the suitability of method for routine analysis in pharmaceutical industries. Moreover, the drug solution was found to be stable in refrigerator and ambient room temperature with mean % accuracy of >98%. Empagliflozin contents were also tested in both the raw API and marketed tablet brands using this newly developed method. The mean assay of raw empagliflozin and tablet brands were ranged from 99.29%±1.12 to 100.95%±1.69 and 97.18%±1.59 to 98.92%±1.00 respectively. Based on these findings, the present investigated approach is suitable for quantification of empagliflozin in raw and pharmaceutical dosage forms. [ABSTRACT FROM AUTHOR]

Published

2021

10. Development and validation of reverse phase HPLC method for determination of angiotensin receptor blocking agent irbesartan in plasma.

Author

Zeb-un-Nis, Ali, Syed Imran, Rizvi, Mehwish, Khan, Maqsood Ahmed, Sultan, Rafi Akhter, Fatima, Rasheeda, Shaheen, Najma, Zafar, Farya, Kashif, Sadia Suri, and Khatian, Najeeb

Abstract

A sensitive, reproducible and modest analytical procedure was developed and validated for evaluation of irbesartan in human plasma. LLE (Liquid-Liquid extraction) of the drug was carried out with acetonitrile (1:1 v/v). Chromatographic separation of irbesartan was conducted by the help of 4.0mm × 25cm column having L1 packing from plasma and mobile phase utilizing HPLC. The mobile phase comprise of phosphate buffer and acetonitrile in a ratio of 67:33 v/v. The flow rate was set at 1ml/minute and the detector at a wavelength of 220 nm. The resolution of irbesartan was well performed from plasma components. This method was validated and demonstrated linearity with a concentration range of 0.1to 6µg/ml of irbesartan in plasma. Intra-day, inter-day accuracy was found 89.33% to 96.37% while intra-day, inter-day precision was found within the limit of 0.02 and 2.15 respectively. The mean recovery of irbesartan was 97.28%. The efficacy of extraction was proved by above-mentioned results. In plasma, the 0.05 and 0.1µg/ml dilutions were exhibited as the LOD and LOQ of irbesartan. Stability studies disclosed that irbesartan showed stability at -20oC storage. [ABSTRACT FROM AUTHOR]

Published

2019

11. Formulation design, characterization and optimization of cinitapride (lmg) immediate release tablets using direct compression technology.

Author

Bushra, Rabia, Atta-ur-Rehman, Ghayas, Sana, Zafar, Farya, Ali, Huma, Shafiq, Yousra, Khalid, Farah, Khan, Maqsood Ahmed, Hanif, Anas, and Mustapha, Omer

Abstract

Cinitapride hydrogen tartarate is relatively a new prokinetic agent that widely prescribed for GERD and epigastric pain. Present study was aimed to develop and optimize cinitapride (1 mg) immediate release (IR) tablet formulation(s) by direct compression using central composite rotatable technique. Overall nine formulations (FC1-FC9) were generated by varying the composition of binder avicel PH 102 (XI) and superdisintegrant crospovidone (X2). The effect of interaction of excipients on hardness (Yl), friability (Y2), disintegration (Y3) and dissolution at 15 min (Y4) were analyzed by RSM plotting. On the basis of physico-chemical evaluation FC3, FC4 and FC6 were found to be the optimized formulations however; FC3 was selected to be the best trial owing to excellent drug release (100.17%) with least friability (0.14%). These IR tablets showed the release pattern similar to the Weibull model with r2 value of 0.978- 0.998. The dissimilarity (f1) and similarity indexes (f2) of FC3, FC4, FC6 with the marketed product were estimated to be 2.57 and 76.51, 4.51 and 64.46, 4.32 and 66.78 respectively. Trial optimized formulations were highly stable with the shelf lives of 58-64 months. So, keeping in view the results of present investigation, it is concluded that the technique of manufacturing and optimization is found to be excellent for developing immediate release cinitapride tablets. [ABSTRACT FROM AUTHOR]

Published

2018

12. Dexibuprofen: Statistical assessment of drug release kinetics and investigative quality perspective.

Author

Hanif, Anas M., Sial, Ali Akbar, Ali, Huma, Zafar, Farya, Baig, Mirza Tasawar, Bushra, Rabia, Khan, Maqsood Ahmed, Nawab, Amber, Mustapha, Omer, and Shafique, Shumaila

Abstract

Healthcare professionals including physicians and pharmacists have been trying since long to come across and work out regarding the issue of generic alternatives, which is highly affected by factors like therapeutic efficacy, cost effectiveness, aesthetic and elegant appearance and implementation of packaging number over the drug product. However, the community pharmacist professionals are also facing difficulty in making decision regarding selection and dispensing the most efficacious brand to the patients. In this regard, the initiation of recent approaches for the development of amenable drug products has led to evolve the concept of generating new avenues for achieving higher patient compliance. Hence, the objective of this study was to evaluate the quality attributes and make comparisons regarding different brands of Dexibuprofen available in market of Karachi, Pakistan. The study is based on evaluation of physical chemical parameters of five different brands. Moreover, a comparative dissolution profile of selected brands of Dexibuprofen was also performed by applying numerous approaches. DEX-1was selected as reference while DEX-2-DEX-5was selected as test brands. Results of all the selected brands met all the compendial requirements. Interpretation of the entire aforementioned test was evaluated using model independent, model- dependent and one – way ANOVA. The work presented in this study has been designed to provide quality standard products easily accessible in Pakistani market. [ABSTRACT FROM AUTHOR]

Published

2018

13. Biowaiver studies of newly optimized meloxicam tablets.

Author

Zafar, Farya, Khan, Sohail, Ali, Huma, Shah, Shabana N., Bushra, Rabia, Naqvi, Ghazala Raza, Maroof, Kashif, Khan, Maqsood Ahmed, and Nisa, Zeb un

Abstract

In this research work biowaiver studies of newly developed and optimized Meloxicam 7.5mg and 15mg water dispersible formulations were carried out at different dissolution media i.e. 0.1N HCl, phosphate buffer pH 4.5, pH 6.8, and pH 7.5 at 50 rpm. For this purpose reference (MA9 and MB9) and tests (MA2, MA4, MA6, MA7 and MA8 (15 mg) and MB2, MB4, MB6, MB7and MB8 (7.5 mg) formulations were compared. In vitro patterns were analyzed by using model-independent and model-dependent methods. Results indicated that all formulation at pH 0.1N HCl and phosphate buffer pH 4.5 followed Weibull model, while at pH 6.8 and pH 7.5 all formulations followed Hixson-Crowell model. Similarly results of model independent methods demonstrated that all the reference formulations were found to be similar with the tests formulations. Results indicated that Biowaiver could be granted to all the optimized water dispersible meloxicam formulations of both batches, so waiver for bioequivalence study can be allowed. [ABSTRACT FROM AUTHOR]

Published

2018

14. Incidence of drug interactions in intensive care units in tertiary care settings: Classification, facts and measures.

Author

Hasnain, Hina, Ali, Huma, Zafar, Farya, Sial, Ali Akbar, Alam, Shazia, Beg, Anwar Ejaz, Bushra, Rabia, Rizvi, Mehwish, Khan, Maqsood Ahmed, Shareef, Huma, Naqvi, Ghazala R., and Anum Tariq

Abstract

Drug-drug interactions (DDIs) are extremely significant concern, particularly in sensitive population including pediatric and geriatric. Propensity for the development of DDIs is high in patients admitted at intensive care units (ICU). This study was conducted to evaluate the DDIs incidence, facts and measures in ICU. From a total of 150 cases studied for ICU patients, with the mean age of 56.37±12.45 years, 55.33% were male and the rest were female 44.66%. The demographic information like age, gender and main diagnosis details of study participants that were extracted from the patients' clinical record. A statistically significant association between the drug interaction and the number of drugs prescribed per prescription was observed (p<0.0001). Concerning the onset of outcome, 52% of DDIs distinguished as delayed onset of effect (past 24 hours) and 35% were categorized as rapid onset (within 24 hours). Despite the facts regarding patient safety and minimizing DIs error, polypharmacy is still frequent in critically ill patients admitted in ICU attributed high risk of adverse reactions due to use of multiple interventions to treat severity of disease condition. Such studies may be used to develop an effective tool for the diagnosis and management of DDIs. [ABSTRACT FROM AUTHOR]

Published

2018

15. Development and validation of reverse phase HPLC method for determination of angiotensin receptor blocking agent irbesartan in plasma.

Author

Nisa Z, Ali SI, Rizvi M, Khan MA, Sultan RA, Fatima R, Shaheen N, Zafar F, Kashif SS, and Khatian N

Subjects

Angiotensin II Type 1 Receptor Blockers pharmacokinetics, Calibration, Chromatography, Reverse-Phase methods, Drug Stability, Humans, Irbesartan pharmacokinetics, Limit of Detection, Sensitivity and Specificity, Angiotensin II Type 1 Receptor Blockers blood, Chromatography, High Pressure Liquid methods, Irbesartan blood

Abstract

A sensitive, reproducible and modest analytical procedure was developed and validated for evaluation of irbesartan in human plasma. LLE (Liquid-Liquid extraction) of the drug was carried out with acetonitrile (1:1 v/v). Chromatographic separation of irbesartan was conducted by the help of 4.0mm × 25cm column having L1 packing from plasma and mobile phase utilizing HPLC. The mobile phase comprise of phosphate buffer and acetonitrile in a ratio of 67:33 v/v. The flow rate was set at 1ml/minute and the detector at a wavelength of 220 nm. The resolution of irbesartan was well performed from plasma components. This method was validated and demonstrated linearity with a concentration range of 0.1to 6μg/ml of irbesartan in plasma. Intra-day, inter-day accuracy was found 89.33% to 96.37% while intra-day, inter-day precision was found within the limit of 0.02 and 2.15 respectively. The mean recovery of irbesartan was 97.28%. The efficacy of extraction was proved by above-mentioned results. In plasma, the 0.05 and 0.1μg/ml dilutions were exhibited as the LOD and LOQ of irbesartan. Stability studies disclosed that irbesartan showed stability at -20°C storage.

Published

2019

16. Formulation design, characterization and optimization of cinitapride (1mg) immediate release tablets using direct compression technology.

Author

Bushra R, Rehman A, Ghayas S, Zafar F, Ali H, Shafiq Y, Khalid F, Khan MA, Hanif A, and Mustapha O

Subjects

Drug Compounding, Tablets, Benzamides chemical synthesis, Benzamides metabolism, Chemistry, Pharmaceutical methods, Compressive Strength, Drug Design

Abstract

Cinitapride hydrogen tartarate is relatively a new prokinetic agent that widely prescribed for GERD and epigastric pain. Present study was aimed to develop and optimize cinitapride (1 mg) immediate release (IR) tablet formulation(s) by direct compression using central composite rotatable technique. Overall nine formulations (FC1-FC9) were generated by varying the composition of binder avicel PH 102 (X1) and superdisintegrant crospovidone (X2). The effect of interaction of excipients on hardness (Y1), friability (Y2), disintegration (Y3) and dissolution at 15 min (Y4) were analyzed by RSM plotting. On the basis of physico-chemical evaluation FC3, FC4 and FC6 were found to be the optimized formulations however; FC3 was selected to be the best trial owing to excellent drug release (100.17%) with least friability (0.14%). These IR tablets showed the release pattern similar to the Weibull model with r2 value of 0.978-0.998. The dissimilarity (f1) and similarity indexes (f2) of FC3, FC4, FC6 with the marketed product were estimated to be 2.57 and 76.51, 4.51 and 64.46, 4.32 and 66.78 respectively. Trial optimized formulations were highly stable with the shelf lives of 58-64 months. So, keeping in view the results of present investigation, it is concluded that the technique of manufacturing and optimization is found to be excellent for developing immediate release cinitapride tablets.

Published

2018