Your search keyword '"Saša Vukmirović"' showing total 4 results

1. Plasma Distribution of Methotrexate and Its Polyglutamates in Pediatric Acute Lymphoblastic Leukemia: Preliminary Insights

Author

Hani Al-Salami, Momir Mikov, Slavica Lazarević, Ivana Rajšić, Svetlana Goločorbin-Kon, Saša Vukmirović, Armin Mooranian, and Maja Đanić

Subjects

Male, Antimetabolites, Antineoplastic, Clinical chemistry, Pharmacology, 03 medical and health sciences, Plasma, 0302 clinical medicine, Pediatric Acute Lymphoblastic Leukemia, medicine, Distribution (pharmacology), Humans, Pharmacology (medical), Prospective Studies, Child, Active metabolite, 030304 developmental biology, 0303 health sciences, Total plasma, Polyglutamate, business.industry, Precursor Cell Lymphoblastic Leukemia-Lymphoma, 3. Good health, Discontinuation, Methotrexate, Polyglutamic Acid, 030220 oncology & carcinogenesis, business, medicine.drug, Chromatography, Liquid

Abstract

High-dose methotrexate (HD-MTX) is the mainstream therapy of current acute lymphoblastic leukemia (ALL) regimens, but frequent intra- and interindividual differences in the clinical response to HD-MTX lead to chemotherapeutic interruption or discontinuation. The exact mechanism of transport across the cell membrane and the disposition of active methotrexate metabolites—methotrexate polyglutamates (MTXPGs)—are not well described in the literature. The aim of this study was to gain more insight into the plasma distribution of methotrexate and MTXPGs in pediatric patients with ALL and to clarify the obscure pathways of MTXPGs. We prospectively measured the concentrations of MTXPG1–7 in plasma samples from three male pediatric patients treated with HD-MTX and leucovorin rescue according to the IC-BFM 2009 protocol using liquid chromatography–mass spectrometry (LC-MS). Blood samples were obtained at 24, 36, 42, and 48 h after the start of HD-MTX treatment. Noticeable plasma concentrations of MTXPGs with a 2.2-fold interpatient variability were detected. The highest interindividual variability in total plasma MTXPG concentration was observed at 36 h, and ranged from 13.78 to 30.82 μmol/L. Among all patients, the predominant polyglutamate types in relation to the total plasma MTXPG concentration at each time point were MTXPG3 (16.71–30.02%) and MTXPG5 (26.23–38.60%), while MTXPG7 was the least abundant MTXPG (3.22–5.02%). The presence of MTXPGs in plasma of patients with ALL could be related to the action of ABC efflux transporters on blood cells and hepatocytes resulting from the administration of high doses of methotrexate. This study may not draw definitive conclusions, but it does reduce uncertainty about the dynamics of methotrexate and its active metabolites, which may be of vital importance for achieving a clinical response.

Published

2021

2. High-Loading Dose of Microencapsulated Gliclazide Formulation Exerted a Hypoglycaemic Effect on Type 1 Diabetic Rats and Incorporation of a Primary Deconjugated Bile Acid, Diminished the Hypoglycaemic Antidiabetic Effect

Author

Boris Milijašević, Jelena Calasan, Saša Vukmirović, Hani Al-Salami, Mladena Lalić-Popović, Momir Mikov, and Svetlana Goločorbin-Kon

Subjects

Blood Glucose, Male, medicine.medical_specialty, Clinical chemistry, medicine.drug_class, Drug Compounding, medicine.medical_treatment, Cholic Acid, Absorption (skin), Pharmacology, 030226 pharmacology & pharmacy, Diabetes Mellitus, Experimental, Bile Acids and Salts, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Oral administration, Internal medicine, Diabetes mellitus, medicine, Animals, Hypoglycemic Agents, Drug Interactions, Pharmacology (medical), Gliclazide, Bile acid, business.industry, Insulin, Cholic acid, medicine.disease, Rats, 3. Good health, Diabetes Mellitus, Type 1, Endocrinology, chemistry, 030220 oncology & carcinogenesis, business, medicine.drug

Abstract

Gliclazide is a drug commonly used in type 2 diabetes mellitus. Recently, gliclazide has shown desirable pharmacological effects such as immunoregulatory and anti-clotting effects, which suggests potential applications in type 1 diabetes mellitus (T1DM). Gliclazide has variable absorption after oral administration, and thus using targeted-delivery techniques, such as microencapsulation, may optimise gliclazide absorption and potential applications in T1DM. Bile acids such as cholic acid have shown microcapsule-stabilising and controlled-release effects, and thus their incorporation into gliclazide microcapsules may further optimise gliclazide release, absorption and antidiabetic effects. Accordingly, this study aimed to examine the hypoglycaemic effects of gliclazide microcapsules with and without cholic acid, in a rat model of T1DM. Thirty-five alloxan-induced T1DM rats were randomly divided into five equal groups and gavaged a single dose of empty microcapsules, gliclazide, gliclazide microcapsules, gliclazide-cholic acid or gliclazide-cholic acid microcapsules. Blood samples were collected over 10 h post-dose and analysed for blood glucose and gliclazide serum concentrations. Gliclazide microcapsules exerted a hypoglycaemic effect in the diabetic rats, and cholic acid incorporation diminished the hypoglycaemic effects, which suggests the lack of synergistic effects between gliclazide and cholic acid. In addition, neither microencapsulation nor cholic acid incorporation optimised gliclazide absorption which suggests that hypoglycaemic effects of gliclazide are independent of its absorption and serum concentrations. This also suggests that hypoglycaemic effects of gliclazide may be associated with gut-metabolic activation rather than gut-targeted delivery and systemic absorption. Gliclazide microcapsules exerted hypoglycaemic effects in T1DM rats independent of insulin and thus may have potentials in treatment of T1DM.

Published

2017

3. Effect of rat pretreatment with aqueous solutions of stevioside and bile acids on the action of certain cardioactive drugs

Author

Aleksandar Rašković, Momir Mikov, Velibor Vasović, Mihalj Poša, Vida Jakovljevic, and Saša Vukmirović

Subjects

Male, medicine.medical_specialty, Epinephrine, medicine.drug_class, medicine.medical_treatment, Pharmacology, Antiarrhythmic agent, Bile Acids and Salts, Electrocardiography, Glucosides, Heart Conduction System, Heart Rate, Internal medicine, Heart rate, medicine, Animals, Drug Interactions, Pharmacology (medical), Stevioside, Rats, Wistar, Metoprolol, Bile acid, Chemistry, Cardiovascular Agents, Cholic Acids, Heart, Rats, Solutions, Endocrinology, Verapamil, Sweetening Agents, Toxicity, Diterpenes, Kaurane, medicine.drug

Abstract

The interaction of aqueous solutions of stevioside and bile acids with cardioactive drugs was studied in rats by registering changes in their electrocardiograms (ECG). Wistar rats of both sexes received daily doses of 20 mg/kg (i.p.) of an aqueous solution of stevioside or physiological solution (controls), then were narcotized with urethane and connected to the ECG apparatus for the first recording. The jugular vein was prepared and connected to an infusion pump to administer one of the drugs: adrenaline (0.1 mg/ml), verapamil (2.5 mg/ml) or metoprolol (1 mg/ml) to rats in both groups, while recording their ECGs. In the second part of the study, the animals were treated in the same way but instead of the stevioside solution received a single dose of 4 mg/kg of monoketocholic acid methyl ester (ME) or sodium salt of the same bile acid (MKHNa), 30 minutes before cardioactive drug infusion. The infusion rate of cardioactive drugs was 0.2 ml/min, except for verapamil (0.1 ml/min). The events observed on ECG recordings were the first myocardial reaction to drug infusion, the second longer-lasting reaction (observed as more extended extrasystoles, decrease in intensity of the QRS complex, or changes in heart rate frequency), and toxicity effect. In the control animals, adrenaline induced a decrease in heart rate frequency at a dose of 0.094 mg/kg, while with stevioside-pretreated rats this effect appeared significantly earlier (at a dose of 0.018 mg/kg). No toxic effect of adrenaline was observed, either in control or stevioside-pretreated group. Bile acids caused no changes in myocardial reaction to adrenaline. Only in the group of animals that received MKHNa, a significant decrease in the QRS complex was observed. Finally, the infusion of stevioside to intact animals at doses of 45 and 55 mg/kg caused no significant changes in the ECG patterns. The myocardial reaction to metoprolol remained unchanged in rats of all groups when compared with controls except for a mild decrease in heart rate frequency. Stevioside induced/produced a significant increase in myocardial sensitivity to verapamil, but no toxic effect was observed in any of the cases. A similar conclusion also holds for the interaction with MKHNa, whereas ME caused an increase in the toxicity of verapamil.

Published

2006

4. Influence of bile acid derivates on tramadol analgesic effect in mice

Author

Velibor Vasović, Ivan Mikov, M. Pjevic, Momir Mikov, Saša Vukmirović, and Vida Jakovljevic

Subjects

Male, medicine.drug_class, Sodium, Analgesic, chemistry.chemical_element, Administration, Oral, Mice, Inbred Strains, Absorption (skin), Pharmacology, Injections, Intramuscular, Route of administration, Mice, Oral administration, medicine, Animals, Pharmacology (medical), Tramadol, Pain Measurement, Bile acid, Cholic Acids, Metabolism, Analgesics, Opioid, chemistry, medicine.drug

Abstract

Influence of two newly synthesized bile acids derivates, namely sodium salt of monoketocholic acid MKH-Na and methyl ester of monoketocholic acid MKH-Me on tramadol (12.5 mg/kg oral and intramuscular) analgesic effect was examined in this research. Analgesic effect was measured by antinociceptive hot plate method. Interaction was estimated by detection of changes in analgesic effect of tramadol combined with bile acids (subcutaneous administration of 4 mg/kg 20 min before tramadol) compared to analgesic effect of the same dose of tramadol given alone. Hydrosoluble sodium salt of monoketocholic acid did not show interaction with tramadol, regardless of the route of administration of tramadol. However, methyl ester of monoketocholic acid increased the analgesic effect of tramadol when it was given intramuscularly. After oral administration of tramadol, methyl ester of monoketocholic acid decreased the analgesic effect of tramadol. According to the time point when interaction reached statistically significant difference, it can be presumed that after intramuscular administration of tramadol, methyl ester of monoketocholic acid increases tramadol absorption and transport to brain and in that way increases its analgesic effect. The analgesic effect of tramadol after oral administration was decreased, which could be explained by the induction of tramadol metabolism in the liver, but should be examined in more details.

Published

2011