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International Journal of Pharmaceutics | 2002

Evaluation of modified gum karaya as carrier for the dissolution enhancement of poorly water-soluble drug nimodipine

G. V Murali Mohan Babu; Ch. D. S. Prasad; K. V. Ramana Murthy

Modified gum karaya (MGK), a recently developed excipient was evaluated as carrier for dissolution enhancement of poorly soluble drug, nimodipine (NM). The advantages of MGK over the parent gum karaya (GK) were illustrated by differences in the in vitro dissolution profiles of respective solid mixtures prepared by co-grinding technique. The influence of process variable, such as polysaccharide concentration and method of preparation of solid mixture on dissolution rate was studied. Solubility studies were also performed to explain the differences in dissolution rate. Solid mixtures were characterized by differential scanning calorimetry (DSC), X-ray diffraction studies (XRD) and scanning electron microscopy (SEM). The dissolution rate of NM was increased as the MGK concentration increased and optimum ratio was found to be 1:9 w/w ratio (NM:MGK). It is found that method of preparation of solid mixtures was significantly effected the dissolution rate of NM from solid mixtures. The order of method of preparation in according to their Dissolution Efficiency is physical mixture < co-grinding mixture < swollen carrier mixture < kneading mixture (water as kneading agent) < kneading mixture (70% v/v ethanol as kneading agent) < solid dispersion. Though, the solid mixtures prepared by other methods like solid dispersion, swollen carrier mixture and kneading technique gave faster release, co-grinding mixture prepared in 1:9 w/w ratio (NM:MGK) was found to exhibit a significant improvement in dissolution rate without requiring addition of organic solvents or high temperatures for its preparation and the process is less cumbersome. Hence, co-grinding technique appears to be more easier and the most convenient method from a practical point of view.


Drug Development and Industrial Pharmacy | 2003

Nimesulide-Modified Gum Karaya Solid Mixtures: Preparation, Characterization, and Formulation Development

G. V Murali Mohan Babu; N Ravi Kumar; K Himasankar; A Seshasayana; K. V. Ramana Murthy

Abstract Solid mixtures of nimesulide (NS) and modified gum karaya (MGK) were prepared to improve the dissolution rate of NS. The effect of drug-carrier ratio on dissolution rate of NS was investigated by preparing the solid mixtures of different ratios by cogrinding method. Solid mixtures were also prepared by physical mixing, kneading, and solid dispersion techniques to study the influence of method of preparation. Differential Scanning Calorimetry (DSC), X-ray Diffraction (XRD), and equilibrium solubility studies were performed to explain the results of in vitro dissolution rate studies. It was clearly evident from the results that the NS dissolution rate was dependent on the concentration of MGK in the solid mixtures, and optimum weight ratio was found to be 1:4 (NS:MGK). Though the dissolution rate of NS from all solid mixtures prepared by different methods improved significantly, maximum improvement in dissolution rate was observed with solid dispersions. The order of methods basing on their effect on dissolution efficiency is solid dispersion>kneading>cogrinding> physical mixing>pure NS. Tablets of pure drug and solid mixtures (1:4 w/w, NS:MGK) were prepared. Though the best results from the dissolution test were obtained for the tablets containing solid dispersions, tablets containing cogrinding mixture were found to be suitable, from a practical point of view, for commercialization.


Indian Journal of Pharmaceutical Sciences | 2001

Controlled Release Of Dicolfenac Sodium By Gum Karaya – Chitosan Complex Coacervate : In Vivo Evaluation

G. V Murali Mohan Babu; K Himasankar; Cheruvu P. S Narayan; K. V. Ramana Murthy


Indian Journal of Pharmaceutical Sciences | 2002

Development of new controlled release formulation of flurbiprofen: In vitro - in vivo correlation

G. V Murali Mohan Babu; Ch. D. S. Prasad; K Himasankar; V. Gourishankar; N. Kishore Kumar; K. V. Ramana Murthy


Indian Journal of Pharmaceutical Sciences | 2002

Studies On Preparation And Evaluation Of Modified Form Of Gum Karaya

G. V Murali Mohan Babu; K Himasankar; B Janaki Ram; A Seshasayana; K. V. Ramana Murthy


Indian Journal of Pharmaceutical Sciences | 2002

Development of dissolution medium for a poorly water soluble drug, celecoxib

G. V Murali Mohan Babu; V Gouri Shankar; K. Hima Sankar; A Seshasayana; N. Kishore Kumar; K. V. Ramana Murthy


Indian Journal of Pharmaceutical Sciences | 2002

Studies on the solid dispersion systems of glipizide

K Himasankar; G. V Murali Mohan Babu; P. S. S Krishna Babu; Ch. D. S. Prasad; L Narasinga Rao; K. V. Ramana Murthy


Acta Pharmaceutica | 2001

Evaluation of gum karaya as a carrier in the design of oral controlled-release hydrophilic matrix systems

G. V Murali Mohan Babu; Ch. D. S. Prasad; K. Hima Sankar; Cheruvu P. S Narayan; K. V. Ramana Murthy


Indian drugs | 2002

Comparative studies on effect of some hydrophilic polymers onthe dissolution rate of a poorlywater soluble drug, meloxicam

N. Kishore Kumar; G. V Murali Mohan Babu; Ch. D. S. Prasad; K Himasankar; A Seshasayana; V. Ramana Murthy


Indian Journal of Pharmaceutical Sciences | 2002

Formulation And Evaluation Of Tablet Dosage Forms Of Nimodipine-Modified Gum Karaya Co-Grinding Mixtures

G. V Murali Mohan Babu; K Himasankar; N. Kishore Kumar; B Janaki Ram; A Seshasayana; K. V. Ramana Murthy

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