Ram S. Sakhare scite author profile

Ram S. Sakhare

5Publications

49Citation Statements Received

8Citation Statements Given

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Swami Ramanand Teerth Marathwada University

Publications

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Therapeutic approaches to drug targets in atherosclerosis

Jamkhande

Chandak

Dhawale

et al. 2014

Saudi Pharmaceutical Journal

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Non-communicable diseases such as cancer, atherosclerosis and diabetes are responsible for major social and health burden as millions of people are dying every year. Out of which, atherosclerosis is the leading cause of deaths worldwide. The lipid abnormality is one of the major modifiable risk factors for atherosclerosis. Both genetic and environmental components are associated with the development of atherosclerotic plaques. Immune and inflammatory mediators have a complex role in the initiation and progression of atherosclerosis. Understanding of all these processes will help to invent a range of new biomarkers and novel treatment modalities targeting various cellular events in acute and chronic inflammation that are accountable for atherosclerosis. Several biochemical pathways, receptors and enzymes are involved in the development of atherosclerosis that would be possible targets for improving strategies for disease diagnosis and management. Earlier anti-inflammatory or lipid-lowering treatments could be useful for alleviating morbidity and mortality of atherosclerotic cardiovascular diseases. However, novel drug targets like endoglin receptor, PPARα, squalene synthase, thyroid hormone analogues, scavenger receptor and thyroid hormone analogues are more powerful to control the process of atherosclerosis. Therefore, the review briefly focuses on different novel targets that act at the starting stage of the plaque form to the thrombus formation in the atherosclerosis.

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Marine bioactive agents: a short review on new marine antidiabetic compounds

Barde

Sakhare

Kanthale

et al. 2015

Asian Pacific Journal of Tropical Disease

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Development and Validation of Stability Indicating Assay Method for Simultaneous Estimation of Ilaprazole and Domperidone in Bulk and Solid Dosage Form by Uv-Spectroscopy

Sakhare¹,

Pekamwar²,

Dhamane³

et al. 2016

Int. Res. J. Pharm.

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A Simple, rapid, precise and accurate stability indicating UV-Spectrophotometric method was developed for simultaneous estimation of Ilaprazole (ILA) and Domperidone (DOM) in bulk and capsule formulation and validated as per ICH guidelines. The solvent used for this method was methanol. The λmax of ILA and DOM were found to be 306 and 288 nm respectively. The linearity for ILA and DOM was in the range of 1-6 μg/ml and 3-18 μg/ml, respectively with regression coefficient(r²) of 0.999 for both drugs. The % recovery was found to be in the range of 99.29-100.87% and 99.92-100.16% for ILA and DOM respectively. Percentage RSD for precision and accuracy of the method was found to be less than 2% .LOD values for ILA and DOM were found to be 0.0866 μg/ml and 0.4026 μg/ml respectively. LOQ values for ILA and DOM were found to be 0.2625 μg/ml and 1.241 μg/ml respectively. The Forced degradation study is validated as per ICH guidelines. The developed method is suitable for the analysis of tablet formulation for quality control purposes.

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Stability Indicating HPTLC Method for Simultaneous Estimation of Eperisone Hydrochloride and Diclofenac Sodium in Bulk and Solid Dosage Form

Sakhare¹,

Pekamwar²,

Dannak³

2016

Eurasian J Anal Chem

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RP-HPLC Method Development and Validation for the Estimation of Lansoprazole in Presence of Related Substances by QbD Approach

Gholve¹,

Sangshetti²,

Bhusnure³

et al. 2021

JPRI

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A rapid specific RP-HPLC method has been developed for the determination of Lansoprazole impurities in the drug substance. The control of pharmaceutical impurities is currently a critical issue in the pharmaceutical industry. The International Council for Harmonization (ICH) has formulated a workable guideline regarding the control of impurities. The objective of the recent study was to develop and validate a HPLC method for the quantitative determination of process-related impurities of Lansoprazole in pharmaceutical drug substance. Lansoprazole, 2-[[[3-methyl-4-(2,2,2-trifluoroethoxy)-2-pyridinyl] methyl]-sulfinyl]- 1H-benzimidazole is an proton pump inhibitor used in the management of gastric ulcers. Chromatographic identification of the impurities was carried out by response surface methodology, applying a three-level Box Behnken design with three center points. Three factors selected were a mobile phase, flow rate, column temperature. Evaluation of the main factor, their interaction, and the quadric effect on peak resolution were done on Waters Symmetry C8, 250 x 4.6mm, 5µm column is used for the development of the method. The mobile phase consists of buffer and acetonitrile. The flow rate of the mobile phase was 1.0 ml/min with gradient elution. The column temperature is ambient and the detection wavelength is 235 nm. The injection volume was 10 µL. The method was validated as per ICH guidelines for linearity in the range of 50-150 µg/ml and the LOD & LOQ values obtained were 0.437×10-4 and 0.1325×10-3 µg/ml respectively which specifies the method's sensitivity. The proposed method was successfully used to determine the Lansoprazole impurities in drug substances.

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Ram S. Sakhare

Therapeutic approaches to drug targets in atherosclerosis

Marine bioactive agents: a short review on new marine antidiabetic compounds

Development and Validation of Stability Indicating Assay Method for Simultaneous Estimation of Ilaprazole and Domperidone in Bulk and Solid Dosage Form by Uv-Spectroscopy

Stability Indicating HPTLC Method for Simultaneous Estimation of Eperisone Hydrochloride and Diclofenac Sodium in Bulk and Solid Dosage Form

RP-HPLC Method Development and Validation for the Estimation of Lansoprazole in Presence of Related Substances by QbD Approach

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