Your search keyword '"Kasim K. Kabirov"' showing total 14 results

1. Data from A Novel l-Asparaginase with low l-Glutaminase Coactivity Is Highly Efficacious against Both T- and B-cell Acute Lymphoblastic Leukemias In Vivo

Author

Arnon Lavie, Pieter Van Vlierberghe, Yogen Saunthararajah, Bradley J. Merrill, Alexander V. Lyubimov, Kasim K. Kabirov, Michael J. Schlicht, Steven Goossens, Barbara De Moerloose, Veerle Mondelaers, Tim Lammens, Sofie Peirs, Andre Kajdacsy-Balla, Maarten C. Bosland, Dolores L. Mahmud, Annie Oh, Damiano Rondelli, Li Liu, Amanda M. Schalk, Michael Caffrey, Aleksandar Antanasijevic, Jenny Y. Zhang, Ying Su, and Hien Anh Nguyen

Abstract

Acute lymphoblastic leukemia (ALL) is the most common type of pediatric cancer, although about 4 of every 10 cases occur in adults. The enzyme drug l-asparaginase serves as a cornerstone of ALL therapy and exploits the asparagine dependency of ALL cells. In addition to hydrolyzing the amino acid l-asparagine, all FDA-approved l-asparaginases also have significant l-glutaminase coactivity. Since several reports suggest that l-glutamine depletion correlates with many of the side effects of these drugs, enzyme variants with reduced l-glutaminase coactivity might be clinically beneficial if their antileukemic activity would be preserved. Here we show that novel low l-glutaminase variants developed on the backbone of the FDA-approved Erwinia chrysanthemi l-asparaginase were highly efficacious against both T- and B-cell ALL, while displaying reduced acute toxicity features. These results support the development of a new generation of safer l-asparaginases without l-glutaminase activity for the treatment of human ALL.Significance: A new l-asparaginase–based therapy is less toxic compared with FDA-approved high l-glutaminase enzymes Cancer Res; 78(6); 1549–60. ©2018 AACR.

Published

2023

2. Protected graft copolymer-formulated fibroblast growth factors mitigate the lethality of partial body irradiation injury.

Author

Gerardo M Castillo, Akiko Nishimoto-Ashfield, Cynthia C Jones, Kasim K Kabirov, Alexander Zakharov, and Alexander V Lyubimov

Subjects

Medicine, Science

Abstract

We evaluated the mitigating effects of fibroblast growth factor 4 and 7 (FGF4 and FGF7, respectively) in comparison with long acting protected graft copolymer (PGC)-formulated FGF4 and 7 (PF4 and PF7, respectively) administered to C57BL/6J mice a day after exposure to LD50/30 (15.7 Gy) partial body irradiation (PBI) which targeted the gastrointestinal (GI) system. The PGC that we developed increased the bioavailability of FGF4 and FGF7 by 5- and 250-fold compared to without PGC, respectively, and also sustained a 24 hr presence in the blood after a single subcutaneous administration. The dose levels tested for mitigating effects on radiation injury were 3 mg/kg for the PF4 and PF7 and 1.5 mg each for their combination (PF4/7). Amifostine administered prior to PBI was used as a positive control. The PF4, PF7, or PF4/7 mitigated the radiation lethality in mice. The mitigating effect of PF4 and PF7 was similar to the positive control and PF7 was better than other mitigators tested. The plasma citrulline levels and hematology parameters were early markers of recovery and survival. GI permeability function appeared to be a late or full recovery indicator. The villus length and crypt number correlated with plasma citrulline level, indicating that it can act as a surrogate marker for these histology evaluations. The IL-18 concentrations in jejunum as early as day 4 and TPO levels in colon on day 10 following PBI showed statistically significant changes in irradiated versus non-irradiated mice which makes them potential biomarkers of radiation exposure. Other colon and jejunum cytokine levels are potentially useful but require larger numbers of samples than in the present study before their full utility can be realized.

Published

2017

3. High-loading Gα 13 -binding EXE peptide nanoparticles prevent thrombosis and protect mice from cardiac ischemia/reperfusion injury

Author

Chang Liu, Aiming Pang, Paola Leon Plata, Ying Liu, Can Wang, Ni Cheng, M. Keegan Delaney, Kasim K. Kabirov, Minyi Gu, Claire W Chang, Yujie Cui, Yaping Zhang, Aleksander V. Lyubimov, Asrar B. Malik, Randal A. Skidgel, Jalees Rehman, Yanyan Bai, Zhigang Hong, Xiaoping Du, and Alexander Zakharov

Subjects

0301 basic medicine, Aspirin, business.industry, Ischemia, General Medicine, 030204 cardiovascular system & hematology, Pharmacology, medicine.disease, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, P2Y12, Cangrelor, chemistry, In vivo, Hemostasis, Antithrombotic, medicine, business, Reperfusion injury, medicine.drug

Abstract

Inefficient delivery is a major obstacle to the development of peptide-based drugs targeting the intracellular compartment. We recently showed that selectively inhibiting integrin outside-in signaling using a peptide (mP6) derived from the Gα13-binding ExE motif within the integrin β3 cytoplasmic domain had antithrombotic effects. Here, we engineered lipid-stabilized, high-loading peptide nanoparticles (HLPN), in which a redesigned ExE peptide (M3mP6) constituted up to 70% of the total nanoparticle molarity, allowing efficient in vivo delivery. We observed that M3mP6 HLPN inhibited occlusive thrombosis more potently than a clopidogrel/aspirin combination without adverse effects on hemostasis in rodents. Furthermore, M3mP6 HLPN synergized with P2Y12 receptor inhibitors or the clopidogrel/aspirin combination in preventing thrombosis, without exacerbating hemorrhage. M3mP6 HLPN also inhibited intravascular coagulation more potently than the P2Y12 inhibitor cangrelor. Postischemia injection of M3mP6 HLPN protected the heart from myocardial ischemia-reperfusion injury in a mouse model. This study demonstrates an efficient in vivo peptide delivery strategy for a therapeutic that not only efficaciously prevented thrombosis with minimal bleeding risk but also protected from myocardial ischemia-reperfusion injury in mice.

Published

2020

4. A Novel <scp>l</scp>-Asparaginase with low <scp>l</scp>-Glutaminase Coactivity Is Highly Efficacious against Both T- and B-cell Acute Lymphoblastic Leukemias In Vivo

Author

Aleksander V. Lyubimov, Damiano Rondelli, Steven Goossens, Andre Kajdacsy-Balla, Pieter Van Vlierberghe, Bradley J. Merrill, Li Liu, Tim Lammens, Hien Anh Nguyen, Veerle Mondelaers, Aleksandar Antanasijevic, Sofie Peirs, Maarten C. Bosland, Michael J. Schlicht, Kasim K. Kabirov, Jenny Y. Zhang, Michael Caffrey, Annie Oh, Dolores Mahmud, Arnon Lavie, Yogen Saunthararajah, Ying Su, Barbara De Moerloose, and Amanda M. Schalk

Subjects

Male, 0301 basic medicine, Cancer Research, Asparaginase, Glutamine, Antineoplastic Agents, Mice, SCID, Pharmacology, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Glutaminase, In vivo, Cell Line, Tumor, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, Acute lymphocytic leukemia, Toxicity Tests, Acute, medicine, Animals, Humans, B cell, business.industry, Cancer, medicine.disease, Xenograft Model Antitumor Assays, Pediatric cancer, Recombinant Proteins, Acute toxicity, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Oncology, chemistry, 030220 oncology & carcinogenesis, Female, business

Abstract

Acute lymphoblastic leukemia (ALL) is the most common type of pediatric cancer, although about 4 of every 10 cases occur in adults. The enzyme drug l-asparaginase serves as a cornerstone of ALL therapy and exploits the asparagine dependency of ALL cells. In addition to hydrolyzing the amino acid l-asparagine, all FDA-approved l-asparaginases also have significant l-glutaminase coactivity. Since several reports suggest that l-glutamine depletion correlates with many of the side effects of these drugs, enzyme variants with reduced l-glutaminase coactivity might be clinically beneficial if their antileukemic activity would be preserved. Here we show that novel low l-glutaminase variants developed on the backbone of the FDA-approved Erwinia chrysanthemi l-asparaginase were highly efficacious against both T- and B-cell ALL, while displaying reduced acute toxicity features. These results support the development of a new generation of safer l-asparaginases without l-glutaminase activity for the treatment of human ALL. Significance: A new l-asparaginase–based therapy is less toxic compared with FDA-approved high l-glutaminase enzymes Cancer Res; 78(6); 1549–60. ©2018 AACR.

Published

2018

5. Oral toxicity and pharmacokinetic studies of SHetA2, a new chemopreventive agent, in rats and dogs

Author

Alexander Zakharov, Dejan Nikolic, Aryamitra Banerjee, Tomas Martin-Jimenez, Irina Mankovskaya, Lian Chen, Alexander V. Lyubimov, Izet M. Kapetanovic, Emmanuel Onua, Richard B. van Breemen, Doris M. Benbrook, Nancy Dinger, Marcia Pereira, Kasim K. Kabirov, and Carol J. Detrisac

Subjects

Male, No-observed-adverse-effect level, Health, Toxicology and Mutagenesis, Metabolite, Retinoic acid, Administration, Oral, Motor Activity, Pharmacology, Weight Gain, Toxicology, Rats, Sprague-Dawley, Eating, chemistry.chemical_compound, Dogs, Species Specificity, Pharmacokinetics, Adrenal Glands, Toxicity Tests, Animals, Anticarcinogenic Agents, Medicine, Chromans, No-Observed-Adverse-Effect Level, Chemical Health and Safety, business.industry, Prostate, Public Health, Environmental and Occupational Health, Thiones, Organ Size, General Medicine, Rats, Bioavailability, Lowest-observed-adverse-effect level, chemistry, Apoptosis, Area Under Curve, Toxicity, Female, business

Abstract

SHetA2 is a heteroarotinoid that has shown selective inhibition of cancer cell growth and an induction of apoptosis without activation of nuclear retinoic acid receptors. In the rat study, SHetA2 was administered in 1% aqueous methylcellulose/0.2% Tween 80 by oral gavage at 0, 100, 500, and 2,000 mg/kg/day for 28 days. The high-dose administration induced decreased activity in male rats, decreased body-weight gains and food consumption, and changes in organ weights. The major metabolite of SHetA2 in rat plasma was monohydroxy SHetA2, which was considerably higher than the parent compound after oral and intravenous administration. Pharmacokinetic analysis showed extremely low (1%) systemic bioavailability of SHetA2 for all doses tested. The dose of 2,000 mg/kg/day was considered as the lowest observed adverse effect level. The no observed adverse effect level (NOAEL) was 500 mg/kg/day. In the dog study, no toxicity of SHetA2 in 30% aqueous Solutol(®) HS 15 was observed in any tested dose groups (0, 100, 400, and 1,500 mg/kg/day). The major metabolite of SHetA2 in dog plasma was also monohydroxy SHetA2, which was equal to or lower than the parent compound after oral administration. SHetA2 levels in dog plasma were notably higher, when compared to levels in rat plasma. However, exposure was not dose proportional, as exemplified by a lack of proportional increase in maximum concentration or area under the plasma concentration-time curve with increasing dose. The NOAEL was not established and was considered to be above 1,500 mg/kg/day.

Published

2012

6. Effects of bacterial and presystemic nitroreductase metabolism of 2-chloro-5-nitro-N-phenylbenzamide on its mutagenicity and bioavailability

Author

Kasim K. Kabirov, Levy Kopelovich, Elena V. Kabirova, Robert Swezey, Carol E. Green, Laura Rasay, Izet M. Kapetanovic, and Aleksander V. Lyubimov

Subjects

Male, Salmonella typhimurium, Metabolite, Biological Availability, Estrogen receptor, Pharmacology, Toxicology, Article, Ames test, Rats, Sprague-Dawley, chemistry.chemical_compound, Nitroreductase, Dogs, Pharmacokinetics, Animals, Anilides, Amines, Biotransformation, Antagonist, General Medicine, Metabolism, Nitroreductases, Rats, Bioavailability, PPAR gamma, chemistry, Mutagens

Abstract

2-Chloro-5-nitro-N-phenylbenzamide (GW9662), a potent irreversible PPAR-γ antagonist, has shown promise as a cancer chemopreventive agent and is undergoing preclinical evaluations. Studies were initiated to assess its bacterial mutagenicity and pharmacokinetic profile in two animal species prior to subchronic oral toxicity evaluations and the results are reported here. GW9662 was mutagenic in both TA98 and TA100 bacterial strains with and without metabolic activation but was negative in the nitroreductase-deficient strains (TA98NR and TA100NR) also with and without metabolic activation, indicating that GW9662 mutagenicity is dependent on nitroreduction. The mutagenic activity was predominantly via a base-substitution mechanism. Following oral dosing in rats and dogs, the parent compound, GW9662, was virtually absent from plasma samples, but there was chromatographic evidence for the presence of metabolites in the plasma as a result of oral dosing. Metabolite identification studies showed that an amine metabolite ACPB (5-amino-2-chloro-N-phenylbenzamide), a product of nitro reduction, was the predominant species exhibiting large and persistent plasma levels. Thus systemic circulation of GW9662 has been attained largely in the form of its reduced metabolite, probably a product of gut bacterial metabolism. GW9662 was detectable in plasma of rats and dogs after intravenous dose albeit at low concentrations. Pharmacokinetic analysis following intravenous dosing in rats showed a rapid clearance and an extensive tissue distribution which could have accounted for the very low plasma levels. Of note, the amine metabolite was absent following intravenous dosing in both rats and dogs, confirming it being a product of presystemic metabolism. The potential utility of GW9662 as a chemopreventive agent, especially as an Estrogen Receptor-α (ER-α) inducer in an otherwise ER-α negative breast tissue, is of great interest. However, the results shown here suggest that additional animal toxicological and bioavailability studies are required to establish a role of GW9662 as a chemopreventive agent.

Published

2012

7. Assessment of oral toxicity and safety of 9-cis-UAB30, a potential chemopreventive agent, in rat and dog studies

Author

Matthew Lindeblad, Irina Mankovskaya, Kasim K. Kabirov, Nancy Dinger, Alexander V. Lyubimov, Robert Morrisey, Tomas Martin-Jimenez, and Izet M. Kapetanovic

Subjects

Male, No-observed-adverse-effect level, Drug-Related Side Effects and Adverse Reactions, Globulin, Health, Toxicology and Mutagenesis, Hyperglobulinemia, Administration, Oral, Naphthalenes, Pharmacology, Toxicology, Dogs, Species Specificity, Pharmacokinetics, medicine, Animals, Anticarcinogenic Agents, Hypoalbuminemia, Toxicity Tests, Chronic, Adverse effect, No-Observed-Adverse-Effect Level, Chemical Health and Safety, Dose-Response Relationship, Drug, biology, business.industry, Public Health, Environmental and Occupational Health, Organ Size, General Medicine, medicine.disease, Rats, Dose–response relationship, Organ Specificity, Toxicity, Fatty Acids, Unsaturated, biology.protein, Female, business

Abstract

9-cis-UAB30 is a potential chemopreventative agent that has been shown to be effective on many different types of tumors. The safety and toxicity of 9-cis-UAB30 had not been previously established. These studies were conducted to evaluate the potential toxicity and pharmacokinetics in a rodent and a nonrodent species for the purpose of investigational new drug submission. Oral gavage administration of 9-cis-UAB30 at the doses 0, 3, 15, and 100 mg/kg/day to CD® rats for 28 days showed a dose-dependent (although not dose-proportional) increase in plasma drug levels in week 4. The liver was the target organ for toxicity of 9-cis-UAB30. Hepatomegaly along with increases in serum aspartate-aminotransferase and alkaline-phosphatase levels were seen in rats. Moderate hypoalbuminemia and hyperglobulinemia resulted in a decreased albumin/globulin ratio. Histopathology revealed hepatocellular change consistent with hepatic glycogen deposition. Toxicity studies in dogs did not show treatment-related toxicity at doses as high as 100 mg/kg/day (highest dose tested) administered by capsules for 28 days. No effects on the central nervous system (functional observational battery in rats) or cardiovascular function (safety pharmacology study in telemeterized dogs) were seen. The no observed adverse effect level (NOAEL) in the rat studies was 3 mg/kg/day; however, the adverse effects seen in rats receiving 15 mg/kg/day (the least observed adverse effect level) was a slight, but statistically significant, elevation in fibrinogen and decrease in prothrombin time, which may be a sign of some tendency for increased blood coagulation. The NOAEL in the dog study was at least 100 mg/kg/day.

Published

2011

8. Assessment of oral toxicity and safety of pentamethylchromanol (PMCol), a potential chemopreventative agent, in rats and dogs

Author

Izet M. Kapetanovic, Matthew Lindeblad, Alexander V. Lyubimov, Irina Mankovskaya, Nancy Dinger, Carol J. Detrisac, Kasim K. Kabirov, and Alexander Zakharov

Subjects

Male, medicine.medical_specialty, Anemia, Administration, Oral, Toxicology, Article, Nephrotoxicity, Dogs, Oral administration, Internal medicine, Toxicity Tests, Animals, Anticarcinogenic Agents, Medicine, Dosing, Chromans, Adverse effect, Dose-Response Relationship, Drug, business.industry, Stomach, Organ Size, medicine.disease, Rats, Endocrinology, medicine.anatomical_structure, Toxicity, Female, Histopathology, Drug Screening Assays, Antitumor, business

Abstract

2,2,5,7,8-Pentamethyl-6-chromanol (PMCol) was administered by gavage in rats for 28 days at dose levels of 0, 100, 500, and 2000mg/kg/day. PMCol administration induced decreases in body weight gains and food consumption, hepatotoxicity (increased TBILI, ALB, ALT, TP; increased relative liver weights; increased T4 and TSH), nephrotoxicity (increased BUN and BUN/CREAT, histopathology lesions), effect on lipid metabolism (increased CHOL), anemia, increase in WBC counts (total and differential), coagulation (FBGN upward arrow and PT downward arrow) and hyperkeratosis of the nonglandular stomach in the 2000mg/kg/day dose group (in one or both sexes). In the 500mg/kg/day dose group, toxicity was seen to a lesser extent. In the 100mg/kg/day dose group, only increased CHOL (females) was observed. To assess the toxicity of PMCol in male dogs it was administered orally by capsule administration for 28 days at dose levels of 0, 50, 200 and 800mg/kg/day (four male dogs/dose group). PMCol treatment at 800mg/kg/day resulted in pronounced toxicity to the male dogs. Target organs of toxicity were liver and thymus. Treatment at 200mg/kg/day resulted in toxicity consistent with slight adverse effect on the liver only. The results of the safety pharmacology study indicate that doses of 0, 50, 200 and 800mg/kg administered orally did not have an effect on the QT interval, blood pressures and body temperatures following dosing over a 24-h recording period. Under the conditions of this study, the no-observed-adverse effect level (NOAEL) for daily oral administration of PMCol by gavage for 28 days to male rats was 100mg/kg/day and 50mg/kg in male dogs. In female rats, the NOAEL was not established due to statistically significant and biologically meaningful increases in CHOL level seen in the 100mg/kg/day dose group. The results of these studies indicated that administration of PMCol at higher dose levels resulted in severe toxicity in dogs and moderate toxicity in rats, however, administration at lower levels is considered to be less likely to result in toxicity following 28 days of exposure. Sex-related differences were seen in rats. Male rats appeared to have greater sensitivity to nephrotoxicity, while female animals had a greater incidence of hepatoxicity and changes in hematological parameters evaluated, especially at a dose of 500mg/kg/day, which correlated to the higher plasma drug levels in female rats. It appeared that dogs were generally more sensitive than rats to oral administration of PMCol. Further examination of the potential toxic effects of PMCol in longer term studies is required prior to understanding the full risks of PMCol administration as a chemopreventative agent.

Published

2010

9. In vitro assessment of P450 induction potential of novel chemopreventive agents SR13668, 9-cis-UAB30, and pentamethychromanol in primary cultures of human hepatocytes

Author

Kasim K. Kabirov, Jonathan P. Jackson, Izet M. Kapetanovic, and Alexander V. Lyubimov

Subjects

Drug, CYP2B6, media_common.quotation_subject, Carbazoles, Drug Evaluation, Preclinical, Naphthalenes, Pharmacology, Toxicology, Cytochrome P-450 Enzyme System, In vivo, Humans, RNA, Messenger, Chromans, Enzyme inducer, Cells, Cultured, media_common, chemistry.chemical_classification, Dose-Response Relationship, Drug, biology, CYP3A4, Reverse Transcriptase Polymerase Chain Reaction, CYP1A2, Cytochrome P450, General Medicine, Enzyme, chemistry, Enzyme Induction, Fatty Acids, Unsaturated, Hepatocytes, biology.protein

Abstract

Several compounds, including 2,10-dicarbethoxy-6-methoxy-5,7-dihydroindolo[2,3-b]carbazole (SR13668), (2E,4E,6Z,8E)-8-(3',4'-dihydro-1'(2'H)-napthalen-1'-ylidene)-3,7-dimethyl-2,4,6-octatrienoic acid (9-cis-UAB30), and 2,2,5,7,8-pentamethyl-6-chromanol (PMCol), were selected as promising chemopreventive agents and have entered preclinical trials for cancer prevention. The potential for adverse drug events resulting from interactions with other administered drugs, food components, or food additives presents an important question. Among the most important drug-drug interactions (DDI) is the potential of a new chemical entity (NCE) to induce cytochrome P450 enzymes (P450). Drug induction of P450 enzymes can lead to adverse drug interactions by increasing the metabolism of other drugs that are substrates for the induced isoform. Currently, sandwich cultured primary human hepatocytes are the standard for predicting human P450 enzyme induction in vitro as these cells retain the ability to respond to prototypical P450 inducers with the same specificity and potency exhibited in vivo. Therefore, a select panel of inducible P450 target genes (CYP1A2, CYP2B6, and CYP3A4) and their induction activity (measured by LC-MS/MS of respective marker substrate metabolites) were monitored in cultured hepatocytes following treatment with SR13668, 9-cis-UAB30, or PMCol to predict clinically significant drug-induced expression. The concentration ranges of the NCE used were selected to maximize the clinical relevance of these results. All responses were evaluated according to major prototypical P450 inducers (i.e., 3-methylcholanthrene, 3-MC; phenobarbital, PB; rifampicin, RIF) and increases > or = 40% of the respective positive control(s) were considered an indication of demonstrable induction. Herein, we report that there is low potential for DDI with SR13668 and PMCol due to enzyme induction of CYP1A2, CYP2B6, and CYP3A4 expression at the concentrations examined. Similarly, the study results suggested that 9-cis-UAB30 has low potential to induce CYP1A2 and CYP3A4 expression at the concentrations examined. However, 9-cis-UAB30 was shown to significantly induce CYP2B6 enzyme activity at 10 microM suggesting the potential for DDI as a result.

Published

2009

10. Direct determination of selenium in rat blood plasma by Zeeman atomic absorption spectrometry

Author

Izet M. Kapetanovic, Alexander V. Lyubimov, and Kasim K. Kabirov

Subjects

Male, Accuracy and precision, Chromatography, Dose-Response Relationship, Drug, Reducing agent, Chemistry, Spectrophotometry, Atomic, Analytical chemistry, chemistry.chemical_element, General Medicine, Plasma, Toxicology, Ascorbic acid, Rats, law.invention, Standard curve, Selenium, law, Standard addition, Animals, Female, Atomic absorption spectroscopy

Abstract

The method was developed to be applied for direct determination of selenium in rat plasma by graphite-furnace atomic absorption spectrometry with Zeeman background correction. Blood was obtained from CD® rats of both sexes 2 h after dosing in weeks 7 and 13 in order to acquire data on the levels of selenium in these animals during 13-week gavage administration of l -seleno-methylselenocysteine (SeMC), a new candidate chemopreventive agent under development. Application of the commonly used method of standard addition was found to be unsuitable to calculate the selenium content in rat plasma (within-run and between-run accuracy and precision parameters were less than 85%). Therefore, a new analytical method was developed. In this method, samples of rat plasma (50 μL) were diluted 10-fold with a reducing agent containing l -ascorbic acid, a modifier solution containing palladium chloride and Triton X-100. Samples were atomized in pyrolytically coated graphite tubes and peak height signals were measured. Selenium concentrations were determined by linear least squares regression analysis based on the standard curve generated in pooled rat blank plasma. Since selenium is normally present in plasma, a three-step approach was used to calculate selenium plasma levels. Initially selenium levels were determined based on the standard curve with selenium-spiked pool plasma. In the second step, background selenium levels in the pooled plasma were determined based on the same standard curve. In the third step, background level was added to the previously derived number. The relative errors were in the range from −4.6 to 11.4% (intra-day assay) and from −0.4 to 8.8% (inter-day assay) which proved good accuracy. The relative standard deviations were in the range from 1.88 to 4.70% (intra-day precision) and from 3.28 to 5.38% (inter-day precision). In rat plasma, the following dose-dependent selenium levels (mean ± S.D.) in males and females, respectively, were observed at 13 weeks: 655.5 ± 48.8 and 595.8 ± 43.9 ng/mL (control group), 927.9 ± 85.3 and 859.3 ± 164.3 ng/mL (0.4 mg/kg per day dose group), 1238.9 ± 182.4 and 1169.9 ± 112.6 ng/mL (0.8 mg/kg per day dose group), and 1476.5 ± 138.1 and 1320.1 ± 228.6 ng/mL (2.0 mg/kg per day dose group). No significant sex differences in selenium plasma levels were seen in the SeMC-treated groups. No significant differences in selenium plasma levels were seen between mean plasma levels at 7 and 13 weeks. The described method is simple, rapid, accurate, precise and can be easily applied in other laboratories for a large number of samples.

Published

2008

11. Combination treatment with bortezomib and thiostrepton is effective against tumor formation in mouse models of DEN/PB-induced liver carcinogenesis

Author

Aryamitra Banerjee, Jennifer A. Landolfi, Alexander V. Lyubimov, Andrei L. Gartel, Ming Wang, Kasim K. Kabirov, and Marianna Halasi

Subjects

Carcinoma, Hepatocellular, medicine.drug_class, Antibiotics, Biology, Pharmacology, Thiostrepton, Bortezomib, chemistry.chemical_compound, Mice, Antineoplastic Combined Chemotherapy Protocols, Carcinoma, medicine, Animals, Diethylnitrosamine, Molecular Biology, Extra Views, Liver Neoplasms, Cell Biology, medicine.disease, Boronic Acids, Disease Models, Animal, Cell Transformation, Neoplastic, chemistry, Liver, Apoptosis, Phenobarbital, Pyrazines, Cancer cell, Proteasome inhibitor, Liver cancer, Developmental Biology, medicine.drug

Abstract

Nanoparticle-encapsulated thiazole antibiotic, thiostrepton, has been shown to be an effective agent for inhibiting tumor growth in solid tumor models through the inhibition of proteasomal activity by the induction of apoptosis in cancer cells. Here, we show the efficacy of thiostrepton-micelles in inhibiting tumor growth in a DEN/PB-induced liver cancer model. We also demonstrate an enhanced anticancer effect of the combination treatment of thiostrepton with bortezomib, another proteasome inhibitor in this liver cancer model.

Published

2012

12. Abstract 4781: Analysis of a new chemopreventative agent SHetA2 and its metabolites in Beagle dog liver and plasma

Author

Irina Mankovskaya, Richard B. van Breemen, Doris M. Benbrook, Alexander V. Lyubimov, Alexander Zakharov, Dejan Nikolic, Kasim K. Kabirov, Izet M. Kapetanovic, and Lian Chen

Subjects

Cancer Research, chemistry.chemical_compound, Oncology, Chemistry, Metabolite, Toxicity, Glucuronidation, Pharmacology, Glucuronide, Tandem mass spectrometry, Beagle, High-performance liquid chromatography, Bioavailability

Abstract

Flexible heteroarotinoid SHetA2 {[(4-nitrophenyl)amino][2,2,4,4-tetramethylthiochroman-6-yl)amino] methanethione]} is a new candidate anticancer compound which is effective against a number of different types of tumors. We conducted preclinical safety and toxicity testing of SHetA2 in Beagle dogs with emphasis on determination of SHetA2 and its metabolites (especially GSH-conjugates) in liver. SHetA2 (in 30% aqueous Solutol® HS 15 to improve bioavailability) was administered orally to male and female Beagle dogs for 29 consecutive days. The dose levels of SHetA2 were 0 (control group 1), 100 (group 2), 400 (group 3), and 1500 (group 4) mg/kg/day. The liver and plasma samples were collected on day 29 at 2 hours after drug administration. SHetA2 and its metabolites levels were measured by high performance liquid chromatography and tandem mass spectrometry (LC/MS/MS) on Micromass Quattro micro API triple quadrupole mass-spectrometer. Metabolites formation was also confirmed by high-resolution accurate mass analysis on Waters SYNAPT time-of-flight (TOF) mass spectrometer. The following known metabolites of SHetA2 were quantified in liver (using the parent compound calibration curve): monohydroxy SHetA2 [SHetA2(O1)], dihydroxy SHetA2 [SHetA2(O2)], and GSH-conjugates of SHetA2 [SHetA2-GSH], monohydroxy SHetA2 [SHetA2(O1)-GSH], and dihydroxy SHetA2 [SHetA2(O2)-GSH]. Trihydroxy SHetA2 and its GSH-conjugate were below quantification level or not detected. The GSH-metabolites were of particular interest since conjugation with GSH may serve as a potential indicator of a compound toxicity. However, despite the relatively high levels of SHetA2-GSH-conjugate in dog liver, no drug-related mortality or clinical signs of toxicity were seen in any dose groups. We also found significant levels of several previously unknown metabolites - glucuronide conjugates of SHetA2, SHetA2(O1), and SHetA2(O2). These glucuronides were not reported in mouse and rat liver, in contrast to our dog study. The exact position of glucuronidation was not determined. It may represent a common N- or a rare case of S-glucuronidation for SHetA2, and, in addition, O-glucuronidation for oxidation products of SHetA2. The most abundant metabolites in liver were: glucuronide of SHetA2, SHetA2(O1) and its glucuronide, and GSH-conjugate of SHetA2 whose levels were at 29-80%, 16-31%, 14-39%, and 9-20%, respectively, of SHetA2 levels (2,600-14,000 ng/g; based on average values). Dihydroxy SHetA2 showed two major peaks: “SHetA2(O2)a” (mixture of SHetA2(O2) and its glucuronide conjugate) and “SHetA2(O2)b” (identity was not confirmed; requires additional experiments for its structure elucidation). In plasma, SHetA2(O1) was a major metabolite - 52-86 % of SHetA2 level (600-1,600 ng/mL). Glucuronide of SHetA2 was only at 7-13% of the parent compound. All GSH-conjugates were below quantification level or not detected in plasma. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 103rd Annual Meeting of the American Association for Cancer Research; 2012 Mar 31-Apr 4; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2012;72(8 Suppl):Abstract nr 4781. doi:1538-7445.AM2012-4781

Published

2012

13. High-loading Gα 13 -binding EXE peptide nanoparticles prevent thrombosis and protect mice from cardiac ischemia/reperfusion injury.

Author

Pang A, Cheng N, Cui Y, Bai Y, Hong Z, Delaney MK, Zhang Y, Chang C, Wang C, Liu C, Plata PL, Zakharov A, Kabirov K, Rehman J, Skidgel RA, Malik AB, Liu Y, Lyubimov A, Gu M, and Du X

Subjects

Animals, Ischemia, Mice, Peptides, Myocardial Reperfusion Injury drug therapy, Myocardial Reperfusion Injury prevention & control, Nanoparticles, Pharmaceutical Preparations, Thrombosis prevention & control

Abstract

Inefficient delivery is a major obstacle to the development of peptide-based drugs targeting the intracellular compartment. We recently showed that selectively inhibiting integrin outside-in signaling using a peptide (mP6) derived from the Gα 13 -binding ExE motif within the integrin β 3 cytoplasmic domain had antithrombotic effects. Here, we engineered lipid-stabilized, high-loading peptide nanoparticles (HLPN), in which a redesigned ExE peptide (M3mP6) constituted up to 70% of the total nanoparticle molarity, allowing efficient in vivo delivery. We observed that M3mP6 HLPN inhibited occlusive thrombosis more potently than a clopidogrel/aspirin combination without adverse effects on hemostasis in rodents. Furthermore, M3mP6 HLPN synergized with P2Y12 receptor inhibitors or the clopidogrel/aspirin combination in preventing thrombosis, without exacerbating hemorrhage. M3mP6 HLPN also inhibited intravascular coagulation more potently than the P2Y12 inhibitor cangrelor. Postischemia injection of M3mP6 HLPN protected the heart from myocardial ischemia-reperfusion injury in a mouse model. This study demonstrates an efficient in vivo peptide delivery strategy for a therapeutic that not only efficaciously prevented thrombosis with minimal bleeding risk but also protected from myocardial ischemia-reperfusion injury in mice., (Copyright © 2020 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.)

Published

2020

14. Combination treatment with bortezomib and thiostrepton is effective against tumor formation in mouse models of DEN/PB-induced liver carcinogenesis.

Author

Wang M, Halasi M, Kabirov K, Banerjee A, Landolfi J, Lyubimov AV, and Gartel AL

Subjects

Animals, Antineoplastic Combined Chemotherapy Protocols pharmacology, Boronic Acids pharmacology, Bortezomib, Carcinoma, Hepatocellular drug therapy, Carcinoma, Hepatocellular pathology, Cell Transformation, Neoplastic drug effects, Diethylnitrosamine, Disease Models, Animal, Liver drug effects, Liver pathology, Liver Neoplasms pathology, Mice, Phenobarbital, Pyrazines pharmacology, Thiostrepton pharmacology, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Boronic Acids therapeutic use, Cell Transformation, Neoplastic pathology, Liver Neoplasms drug therapy, Pyrazines therapeutic use, Thiostrepton therapeutic use

Abstract

Nanoparticle-encapsulated thiazole antibiotic, thiostrepton, has been shown to be an effective agent for inhibiting tumor growth in solid tumor models through the inhibition of proteasomal activity by the induction of apoptosis in cancer cells. Here, we show the efficacy of thiostrepton-micelles in inhibiting tumor growth in a DEN/PB-induced liver cancer model. We also demonstrate an enhanced anticancer effect of the combination treatment of thiostrepton with bortezomib, another proteasome inhibitor in this liver cancer model.

Published

2012