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8 results on '"Kuldeepak Sharma"'

2. List of contributors

Author

Muhammad Afzal, Mohit Agrawal, Muhammad Masood Ahmad, Fahad Al-Abbasi, Haider Ali, Kazi Asraf Ali, Sk Zeeshan Ali, Waleed Hassan Almalki, Hisham N. Altayb, Sami I. Alzarea, Kumar Anand, Muhammed Burak Ay, Shwetlana Bandyopadhy, Mirza Masroor Ali Beg, Rudranil Bhowmik, Mainak Chakraborty, Suparno Chakraborty, Raja Chakraverty, Priti Das, Siddhartha Das Pramanik, Debankini Dasgupta, Tanzeela Fazal, Srijon Gayen, Arijit Guha, Pratibha Gupta, Pallab Kanti Haldar, Salman Bakr I. Hosawi, Chowdhury Mobaswar Hossain, Sandipan Jana, Mohammed Kaleem, Samit Karmakar, Sanmoy Karmakar, Gauthaman Karunakaran, Rupinder Kaur, Imran Kazmi, Nurida Kemelbek Kyzy, Faez Iqbal Khan, Naushad Ahmad Khan, Ruqaiyah Khan, Chinnabonia Gopala Krishna, Amrita Kumari, Reshma Kumari, Aanchal Loshali, Arindam Maity, Muhammad Arshad Malik, Avishek Mandal, Pallab Mandal, Hindol Mazumdar, Tilekeeva Ulankul Muktarovna, Bibi Nazia Murtaza, Muhammad Shahid Nadeem, Himani Nautiyal, Muhammad Azhar Nisar, Kudaibergen Osmonaliev, Soupayan Pal, Parag Panday, Susmita Patra, Partha Pratim Das, Raisur Rahman, Khandekar Hussan Reza, Muhammad Naeem Riaz, Kalyan Roy, Sanhati Dutta Roy, Muhammad Zubair Saleem, Shakir Saleem, Kalyan Samanta, Nilanjan Sarkar, Mohammed Zahed Sarwar, Monalisha Sengupta, Md. Adil Shaharyar, Kuldeepak Sharma, Yogendra Singh, Ankush Sundriyal, Gayatri Thapa, Aziz Ud-din, Jafar Abdulla Mohamed Usman, and Ameeduzzafar Zafar

Published
2023
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3. Dietary vitamin D equilibrium in serum ameliorates direct bilirubin associated diabetes mellitus

Author

Lovro Žiberna, Kuldeepak Sharma, and Irena Zajc

Subjects
0301 basic medicine, medicine.medical_specialty, Cirrhosis, Bilirubin, medicine.medical_treatment, Toxicology, Liver disorder, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Insulin resistance, Diabetes mellitus, Internal medicine, medicine, Diabetes Mellitus, Humans, Vitamin D, business.industry, Insulin, General Medicine, medicine.disease, 030104 developmental biology, Endocrinology, chemistry, Liver, 030220 oncology & carcinogenesis, Dietary Supplements, Liver function, Insulin Resistance, business, Reactive Oxygen Species, TBIL, Heme Oxygenase-1
Abstract

Diabetes mellitus (DM), a non-communicable endocrine disease that is marked by a differing degree of tolerance to insulin and dysfunction. The connection between diabetes and liver failure important to doctors in general practice diabetologists and hepatologists. DM is linked with an elevated risk of hepatic consequences and mortality of liver cirrhosis patients. DM may facilitate to insult the liver by inducing inflammation and fibrosis by elevating mitochondrial oxidative stress. The conventional liver function indices are bilirubin including Indirect Bilirubin (IBil), Direct Bilirubin (DBil), and Total Bilirubin (TBil). DBil, IBil, and TBil, have diverse clinical implications as the standard index of liver disorder. An elevated level of DBil may suggest damage to the hepatic cell whereas TBil is within the normal range. Thus, increased liver enzymes are correlated with hepatic insulin resistance in healthy subjects. Notably, a significant correlation between DBil levels and Insulin resistance risk could indicate a connection between liver dysfunction and diabetes mellitus risk. Thus, our primary goal via the current review to examine the impact of dietary vitamin D (VitD) in serum mediated risk reduction of insulin resistance and further incidence of DM through inflammatory liver associated high DBil. Therefore, modifying these inflammatory pathways may be a therapeutic alternative approach for diabetes treatment.

Published
2020

4. Efficacy of NVC-422 in the treatment of dermatophytosis caused byTrichophyton mentagrophytesusing a guinea pig model

Author

Mahmoud A. Ghannoum, Amber J. Cirino, Mark L Anderson, Kuldeepak Sharma, Anthony R. Miller, Lu Wang, Lisa Long, Ron Najafi, and Bahram Memarzadeh

Subjects
education.field_of_study, biology, business.industry, Population, Dermatology, Antimicrobial, biology.organism_classification, Microbiology, Guinea pig, In vivo, Clinical endpoint, Medicine, Trichophyton, Epidermophyton, education, business, Microsporum
Abstract

Objectives Dermatophytes, belonging to genera including Trichophyton, Epidermophyton, and Microsporum, are the causative agents of superficial fungal infections, prevalences of which are estimated to be as high as 25% in the worldwide population. This study evaluated the activity of topical formulations of NVC-422 (sodium 2-[dichloroamino]-2-methylpropane-1-sulfonate), the lead compound in a new class of antimicrobials that consist of broad-spectrum, fast-acting, nonantibiotic antimicrobial molecules based on the endogenously produced N-chlorotaurines. Methods The antifungal efficacy of NVC-422 was investigated using a guinea pig model of infection with Trichophyton mentagrophytes. Infected guinea pigs were randomly assigned to four treatment and two control groups. The efficacy of the treatments was assessed clinically and mycologically at 72 hours after the final topical dose. Results The test compound 2% NVC-422 in 1% Noveon Gel demonstrated the highest level of clinical efficacy. Outcomes of treatment with all other test compounds differed significantly from outcomes in the untreated control group (P = 0.003, P = 0.029, P = 0.012, and P < 0.0001, respectively). Fungal elements were detectable in skin sections from untreated guinea pigs but not in skin sections obtained from any of the treatment groups. Conclusions Evaluation of the efficacy of NVC-422 in the treatment of dermatophytosis using an experimental guinea pig model showed that this compound possesses potent antifungal efficacy as measured by mycological and clinical endpoints. The highest degree of clinical and mycological efficacy was demonstrated by 2% NVC-422 in 1% Noveon Gel. These data show that NVC-422 has potent antifungal activity in vivo. Clinical evaluation of NVC-422 in the treatment of superficial infections caused by dermatophytes, including onychomycosis, is warranted.

Published
2013
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5. Possible mechanism of the cardio-renal protective effects of AVE-0991, a non-peptide Mas-receptor agonist, in diabetic rats

Author

Kuldeepak Sharma, Manjeet Singh, Kulwinder Singh, and Pyare Lal Sharma

Subjects
Blood Glucose, Agonist, Medicine (General), medicine.medical_specialty, Cardiotonic Agents, medicine.drug_class, Renal function, In Vitro Techniques, Kidney, Proto-Oncogene Mas, Blood Urea Nitrogen, Diabetes Mellitus, Experimental, Receptors, G-Protein-Coupled, R5-920, Endocrinology, Diastole, Proto-Oncogene Proteins, Internal medicine, Diabetes mellitus, Ventricular Pressure, Internal Medicine, medicine, Animals, Arterial Pressure, Rats, Wistar, Blood urea nitrogen, business.industry, Imidazoles, Streptozotocin, medicine.disease, Lipids, Rats, Proteinuria, Preload, Blood pressure, Creatinine, Ventricular pressure, Peptides, business, medicine.drug
Abstract

Hypothesis:This study was designed to investigate the cardio-renal protective effect of AVE-0991, a non-peptide Mas-receptor agonist, and A-779, a Mas-receptor antagonist, in diabetic rats.Materials and methods:Wistar rats treated with streptozotocin (50 mg/kg, i.p., once), developed diabetes mellitus after 1 week. After 8 weeks, myocardial functions were assessed by measuring left ventricular developed pressure (LVDP), rate of left ventricular pressure development (d p/d tmax), rate of left ventricular pressure decay (d p/d tmin) and left ventricular end diastolic pressure (LVEDP) on an isolated Langendorff’s heart preparation. Further, mean arterial blood pressure (MABP) was measured by using the tail-cuff method. Assessment of renal functions and lipid profile was carried out using a spectrophotometer.Results:The administration of streptozotocin to rats produced persistent hyperglycaemia, dyslipidaemia and hypertension which consequently produced cardiac and renal dysfunction in 8 weeks. AVE0991 treatment produced cardio-renal protective effects, as evidenced by a significant increase in LVDP, d p/d tmax, d p/d tminand a significant decrease in LVEDP, BUN, and protein urea. Further, AVE-0991 treatment for the first time has been shown to reduce dyslipidaemia and produced antihyperglycaemic activity in streptozotocin-treated rats. However, MABP and creatinine clearance remained unaffected with AVE-0991 treatment.Conclusions:AVE-0991 produced cardio-renal protection possibly by improving glucose and lipid metabolism in diabetic rats, independent of its blood pressure lowering action.

Published
2012
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6. Efficacy of NVC-422 in the treatment of dermatophytosis caused by Trichophyton mentagrophytes using a guinea pig model

Author

Mahmoud A, Ghannoum, Lisa, Long, Amber J, Cirino, Anthony R, Miller, Ron, Najafi, Lu, Wang, Kuldeepak, Sharma, Mark, Anderson, and Bahram, Memarzadeh

Subjects
Male, Random Allocation, Antifungal Agents, Tinea, Trichophyton, Taurine, Guinea Pigs, Animals, Gels
Abstract

Dermatophytes, belonging to genera including Trichophyton, Epidermophyton, and Microsporum, are the causative agents of superficial fungal infections, prevalences of which are estimated to be as high as 25% in the worldwide population. This study evaluated the activity of topical formulations of NVC-422 (sodium 2-[dichloroamino]-2-methylpropane-1-sulfonate), the lead compound in a new class of antimicrobials that consist of broad-spectrum, fast-acting, nonantibiotic antimicrobial molecules based on the endogenously produced N-chlorotaurines.The antifungal efficacy of NVC-422 was investigated using a guinea pig model of infection with Trichophyton mentagrophytes. Infected guinea pigs were randomly assigned to four treatment and two control groups. The efficacy of the treatments was assessed clinically and mycologically at 72 hours after the final topical dose.The test compound 2% NVC-422 in 1% Noveon Gel demonstrated the highest level of clinical efficacy. Outcomes of treatment with all other test compounds differed significantly from outcomes in the untreated control group (P = 0.003, P = 0.029, P = 0.012, and P0.0001, respectively). Fungal elements were detectable in skin sections from untreated guinea pigs but not in skin sections obtained from any of the treatment groups.Evaluation of the efficacy of NVC-422 in the treatment of dermatophytosis using an experimental guinea pig model showed that this compound possesses potent antifungal efficacy as measured by mycological and clinical endpoints. The highest degree of clinical and mycological efficacy was demonstrated by 2% NVC-422 in 1% Noveon Gel. These data show that NVC-422 has potent antifungal activity in vivo. Clinical evaluation of NVC-422 in the treatment of superficial infections caused by dermatophytes, including onychomycosis, is warranted.

Published
2013

8. Transdermal delivery of buprenorphine through cadaver skin

Author

Samir D. Roy, Eric J. Roos, and Kuldeepak Sharma

Subjects
Chemical Phenomena, Skin Absorption, Pharmaceutical Science, In Vitro Techniques, Administration, Cutaneous, Diffusion, chemistry.chemical_compound, Stratum corneum, medicine, Organic chemistry, Humans, Solubility, Chromatography, High Pressure Liquid, Transdermal, Chromatography, Ethanol, Chemistry, Physical, Free base, Permeation, Hydrogen-Ion Concentration, Lauric acid, Buprenorphine, Partition coefficient, medicine.anatomical_structure, chemistry, Spectrophotometry, Ultraviolet, Pharmaceutical Vehicles
Abstract

The skin permeation of buprenorphine base and HCl salt through cadaver skin was investigated. The octanol-water partition coefficient and solubilities of both buprenorphine free base and HCl salt were determined at 32 degrees C. As expected, buprenorphine free base was more lipophilic than its HCl salt and was practically insoluble in aqueous buffer at pH 8.7. The drug solubility decreased exponentially as the pH of the solution increased, whereas the permeability coefficient increased as the donor solution pH decreased. The skin flux of buprenorphine.HCl was significantly higher than that of the free base from propylene glycol/lauric acid vehicle mixtures. Buprenorphine base permeation through tape-stripped epidermis suggested that in addition to stratum corneum, viable epidermis presented a significant diffusion barrier because of the very low aqueous solubility of the free base observed. The mean steady-state skin fluxes of buprenorphine.HCl were 20.3 and 29.7 micrograms/cm2/h from propylene glycol:lauryl alcohol: ethanol (80:15:5) and propylene glycol: propylene glycol monolaurate: water (80:15:5) vehicle mixtures, respectively. The skin flux of buprenorphine.HCl from various monolithic matrix patches was also evaluated. When capric acid, lauric acid, and lauryl alcohol were separately incorporated into an adhesive matrix, the skin flux of buprenorphine.HCl was enhanced by a factor of 2 to 3.5. Finally, based on the total body clearance and minimum effective concentration of buprenorphine, a transdermal delivery rate of 2.5 micrograms/cm2/h from a 20-cm2 patch was estimated. The in vitro skin permeation data clearly suggest that transdermal delivery of buprenorphine is feasible to achieve a desired systemic analgesic effect.

Published
1994

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