Your search keyword '"Vasilevich NI"' showing total 16 results

1. Synthesis and antiamnesic activity of a series of N-acylprolyl-containing dipeptides

Author

Gudasheva, TA, primary, Voronina, TA, additional, Ostrovskaya, RU, additional, Rozantsev, GG, additional, Vasilevich, NI, additional, Trofimov, SS, additional, Kravchenko, EV, additional, Skoldinov, AP, additional, and Seredenin, SB, additional

Published

1996

2. Biological evaluation of 9-thioansamitocin P3.

Author

Vasilevich NI, Jiang H, Xiao H, Feng K, Jian C, Chen C, Li M, Chen Z, Pang L, Li X, Chestkov AV, Sun AH, Xu W, Fuselier JA, Coy DH, and Sun L

Subjects

Humans, Cell Line, Tumor, Cell Cycle, Cell Division, Antineoplastic Agents pharmacology, Antineoplastic Agents metabolism, Maytansine

Abstract

Highly cytotoxic maytansine derivatives are widely used in targeted tumor delivery. Structure-activity studies published earlier suggested the C9 carbinol to be a key element necessary to retain the potency. However, in 1984 a patent was published by Takeda in which the synthesis of 9-thioansamitocyn (AP3SH) was described and its activity in xenograft models was shown. In this article we summarize the results of an extended study of the anti-tumor properties of AP3SH. Like other maytansinoids, it induces apoptosis and arrests the cell cycle in the G2/M phase. It is metabolized in liver microsomes predominately by C3A4 isoform and doesn't inhibit any CYP isoforms except CYP3A4 (midazolam, IC50 7.84 μM). No hERG inhibition, CYP induction or mutagenicity in Ames tests were observed. AP3SH demonstrates high antiproliferative activity against 25 tumor cell lines and tumor growth inhibition in U937 xenograft model. Application of AP3SH as a cytotoxic payload in drug delivery system was demonstrated by us earlier., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Sun L. reports financial support was provided by Shenzhen Science and Technology Program. If there are other authors, they declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

3. The Suppressive Effect of Rebastinib on Triple-negative Breast Cancer Tumors Involves Multiple Mechanisms of Action.

Author

Feng K, Jian C, Xiao H, Jiang H, Yang J, Yang M, Sun A, Song W, Chestkov AV, Vasilevich NI, and Sun L

Subjects

Humans, Rats, Mice, Animals, Female, Pyrazoles therapeutic use, Cell Proliferation, Pyridines pharmacology, Cell Line, Tumor, Apoptosis, Xenograft Model Antitumor Assays, Triple Negative Breast Neoplasms drug therapy, Breast Neoplasms pathology

Abstract

Background/aim: High resistance of triple-negative breast cancer has prompted scientists to look for new targets susceptible to treatment. CDK16 has been suggested as a promising target whose inhibition can lead to tumor growth suppression. Rebastinib, a potent inhibitor of CDK16, has been reported to exhibit anti-tumor activity both in vitro and in vivo., Materials and Methods: The anticancer activity of rebastinib was studied in vitro using cell proliferation, cell cycle arrest and cell apoptosis assays and in vivo in xenograft tumor models using MDA-MB-231 and MDA-MB-468-derived tumors. The safety and drug-like properties of rebastinib were assessed using a panel of Absorption, Distribution, Metabolism, and Excretion (ADME) assays, Ames tests, human Ether-a-go-go Related Gene (hERG) experiments and pharmacokinetic studies in mice and rats., Results: Rebastinib demonstrates antitumor activity against breast cancer both in vitro and in vivo. However, the response of the tumor strongly depends on the type of triple-negative breast cancer. Rebastinib-induced cell cycle arrest was observed in G 0 /G 1 phase suggesting a more complex mechanism than just CDK16 inhibition. ADME and PK studies confirmed the drug-like properties and reasonable safety of rebastinib., Conclusion: Our studies confirmed rebastinib to be a promising drug candidate for breast cancer treatment with high oral bioavailability and reasonable safety. Our data suggest that the mechanism of action of rebastinib is not limited to CDK16 inhibition but also involves other pathways. This does not diminish the importance of rebastinib as a drug candidate, but reveals the presence of several mechanisms, suggesting a wider scope of possible applications., (Copyright © 2023 International Institute of Anticancer Research (Dr. George J. Delinasios), All rights reserved.)

Published

2023

4. General Ser/Thr Kinases Pharmacophore Approach for Selective Kinase Inhibitors Search as Exemplified by Design of Potent and Selective Aurora A Inhibitors.

Author

Vasilevich NI, Aksenova EA, Kazyulkin DN, and Afanasyev II

Subjects

Humans, Aurora Kinase A antagonists & inhibitors, Aurora Kinase A chemistry, Models, Molecular, Protein Kinase Inhibitors chemistry

Abstract

A general pharmachophore model for various types of Ser/Thr kinases was developed. Search for the molecules fitting to this pharmacophore among ASINEX proprietary library revealed a number of compounds, which were tested and appeared to possess some activity against several Ser/Thr kinases such as Aurora A, Aurora B and Haspin. The possibility of performing the fine-tuning of the general Ser/Thr pharmacophore to desired types of kinase to get active and selective inhibitors was exemplified by Aurora A kinase. As a result, several hits in 3-5 nm range of activity against Aurora A kinase with rather good selectivity and ADME properties were obtained., (© 2016 John Wiley & Sons A/S.)

Published

2016

5. Search for Potent and Selective Aurora A Inhibitors Based on General Ser/Thr Kinase Pharmacophore Model.

Author

Vasilevich NI, Tatarskiy VV, Aksenova EA, Kazyulkin DN, and Afanasyev II

Abstract

Based on the data for compounds known from the literature to be active against various types of Ser/Thr kinases, a general pharmachophore model for these types of kinases was developed. The search for the molecules fitting to this pharmacophore among the ASINEX proprietary library revealed a number of compounds, which were tested and appeared to possess some activity against Ser/Thr kinases such as Aurora A, Aurora B and Haspin. Our work on the optimization of these molecules against Aurora A kinase allowed us to achieve several hits in a 3-5 nM range of activity with rather good selectivity and Absorption, Distribution, Metabolism, and Excretion (ADME) properties, and cytotoxicity against 16 cancer cell lines. Thus, we showed the possibility to fine-tune the general Ser/Thr pharmacophore to design active and selective compounds against desired types of kinases.

Published

2016

6. A re-examination of the MDM2/p53 interaction leads to revised design criteria for novel inhibitors.

Author

Vasilevich NI, Afanasyev II, Kovalskiy DA, Genis DV, and Kochubey VS

Subjects

Cell Line drug effects, Drug Design, Drug Evaluation, Preclinical methods, Humans, Ligands, Molecular Targeted Therapy methods, Molecular Weight, Protein Conformation, Protein Interaction Domains and Motifs, Proto-Oncogene Proteins c-mdm2 chemistry, Proto-Oncogene Proteins c-mdm2 isolation & purification, Proto-Oncogene Proteins c-mdm2 metabolism, Small Molecule Libraries chemistry, Models, Molecular, Proto-Oncogene Proteins c-mdm2 antagonists & inhibitors, Small Molecule Libraries pharmacology, Tumor Suppressor Protein p53 metabolism

Abstract

The general model of epitope-type MDM2 inhibitor was developed based on the structural information on the complexes between MDM2 and various low molecular weight ligands found in the PDB database. Application of this model to our in-house library has led us to a new scaffold capable of interrupting protein-protein interactions. A synthetic library based on this and related scaffolds resulted in new classes of compounds that possess biochemical and cellular activity and good pharmacokinetic properties. We assume that such general approach to PPI inhibitors design may be useful for the development of inhibitors of various PPI types, including Bcl/XL., (© 2014 John Wiley & Sons A/S.)

Published

2014

7. Determination of flomoxef in human plasma by liquid chromatography/electrospray ionization tandem mass spectrometry.

Author

Kravtsova OY, Paramonov SA, Vasilevich NI, Kazyulkin DN, Vlasova E, and Engsig M

Subjects

Cephalosporins chemistry, Chromatography, Liquid, Drug Stability, Humans, Least-Squares Analysis, Reproducibility of Results, Sensitivity and Specificity, Cephalosporins blood, Spectrometry, Mass, Electrospray Ionization methods, Tandem Mass Spectrometry methods

Abstract

A specific, sensitive, rapid and reproducible method for the determination of flomoxef in human plasma using high-performance liquid chromatography-tandem mass spectrometry was developed and validated. Flomoxef was detected using an electrospay ionization method operated in negative-ion mode. Chromatographic separation was performed in gradient elution mode on a Luna® C18(2) column (3 μM, 20 × 4.0 mm) at a flow rate of 1 mL/min and runtime 3.5 min. The mobile phase consisted of acetonitrile and water containing 0.1% formic acid as additive. Extraction of flomoxef from plasma and precipitation of plasma proteins was performed with acetonitrile with an absolute recovery of 86.4 ± 1.6%. The calibration curve was linear with a correlation coefficient of 0.999 over the concentration range 10-5000 ng/mL and the lower limit of quantification was 10 ng/mL. The intra- and inter-day precisions were <11.8%, while the accuracy ranged from 99.6 to 109.0%. A stability study of flomoxef revealed that it could be successfully analyzed at 4 ºС over 24 h, but it was unstable in solutions at room temperature during short-term storage (4 h) and several freeze-thaw cycles., (Copyright © 2013 John Wiley & Sons, Ltd.)

Published

2013

8. Lessons from natural products chemistry can offer novel approaches for synthetic chemistry in drug discovery.

Author

Vasilevich NI, Kombarov RV, Genis DV, and Kirpichenok MA

Subjects

Biological Products chemistry, Pharmaceutical Preparations chemical synthesis, Pharmaceutical Preparations chemistry, Biological Products chemical synthesis, Drug Discovery methods

Published

2012

9. Propenylamide and propenylsulfonamide cephalosporins as a novel class of anti-MRSA beta-lactams.

Author

Pohlmann J, Vasilevich NI, Glushkov AI, Kellenberger L, Shapiro S, Caspers P, Page MG, and Danel F

Subjects

Anti-Bacterial Agents chemical synthesis, Anti-Bacterial Agents pharmacology, Cephalosporins chemical synthesis, Cephalosporins pharmacology, Methicillin-Resistant Staphylococcus aureus enzymology, Microbial Sensitivity Tests, Structure-Activity Relationship, beta-Lactams metabolism, Amides chemistry, Anti-Bacterial Agents chemistry, Cephalosporins chemistry, Methicillin-Resistant Staphylococcus aureus drug effects, beta-Lactams antagonists & inhibitors

Abstract

Novel C(3) propenylamide and propenylsulfonamide cephalosporins have been synthesized and tested for their ability to inhibit the penicillin-binding protein 2' (PBP2') from Staphylococcus epidermidis and the growth of a panel of clinically relevant bacterial species, including methicillin-resistant Staphylococcus aureus (MRSA). The most potent compounds inhibited the growth of MRSA strains with minimum inhibitory concentrations (MIC) as low as 1 microg/mL. The structure-activity relationship revealed the potential for further optimization of this new cephalosporin class., (Copyright 2010 Elsevier Ltd. All rights reserved.)

Published

2010

10. Potent, orally bioavailable, liver-selective stearoyl-CoA desaturase (SCD) inhibitors.

Author

Koltun DO, Zilbershtein TM, Migulin VA, Vasilevich NI, Parkhill EQ, Glushkov AI, McGregor MJ, Brunn SA, Chu N, Hao J, Mollova N, Leung K, Chisholm JW, and Zablocki J

Subjects

Acetamides chemistry, Administration, Oral, Animals, Cell Line, Tumor, Dose-Response Relationship, Drug, Fatty Acids chemistry, Humans, Inhibitory Concentration 50, Liver drug effects, Liver metabolism, Male, Microsomes metabolism, Rats, Rats, Sprague-Dawley, Stearoyl-CoA Desaturase chemistry, Sucrose chemistry, Triglycerides chemistry, Chemistry, Pharmaceutical methods, Liver enzymology, Stearoyl-CoA Desaturase antagonists & inhibitors

Abstract

Two structurally distinct series of SCD (Delta9 desaturase) inhibitors (1 and 2) have been previously reported by our group. In the present work, we merged the structural features of the two series. This led to the discovery of compound 5b (CVT-12,012) which is highly potent in a human cell-based (HEPG2) SCD assay (IC(50)=6nM). This compound has 78% oral bioavailability in rats and is preferentially distributed into liver (76 times vs plasma) with relatively low brain penetration. In a five-day study (sucrose fed rats) compound 5b significantly reduced SCD activity in a dose-dependent manner as determined by GC analysis of fatty acid composition in plasma and liver, and significantly reduced liver triglycerides versus the control group ( approximately 50%).

Published

2009

11. Orally bioavailable, liver-selective stearoyl-CoA desaturase (SCD) inhibitors.

Author

Koltun DO, Vasilevich NI, Parkhill EQ, Glushkov AI, Zilbershtein TM, Mayboroda EI, Boze MA, Cole AG, Henderson I, Zautke NA, Brunn SA, Chu N, Hao J, Mollova N, Leung K, Chisholm JW, and Zablocki J

Subjects

Administration, Oral, Animals, Benzyl Compounds chemical synthesis, Benzyl Compounds pharmacokinetics, Cell Line, Tumor, Dietary Carbohydrates metabolism, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacology, Humans, Microsomes, Liver metabolism, Pyrimidinones chemical synthesis, Pyrimidinones pharmacokinetics, Rats, Rats, Sprague-Dawley, Stearoyl-CoA Desaturase metabolism, Tissue Distribution, Benzyl Compounds chemistry, Enzyme Inhibitors chemistry, Pyrimidinones chemistry, Stearoyl-CoA Desaturase antagonists & inhibitors

Abstract

We discovered a structurally novel SCD (Delta9 desaturase) inhibitor 4a (CVT-11,563) that has 119 nM potency in a human cell-based (HEPG2) SCD assay and selectivity against Delta5 and Delta6 desaturases. This compound has 90% oral bioavailability (rat) and excellent plasma exposure (dAUC 935 ng h/mL). Additionally, 4a shows moderately selective liver distribution (three times vs plasma and adipose tissue) and relatively low brain penetration. In a five-day study (high sucrose diet, rat) compound 4a significantly reduced SCD activity as determined by GC analysis of fatty acid composition in plasma and liver. We describe the discovery of 4a from HTS hit 1 followed by scaffold replacement and SAR studies focused on DMPK properties.

Published

2009

12. Novel, potent, selective, and metabolically stable stearoyl-CoA desaturase (SCD) inhibitors.

Author

Koltun DO, Parkhill EQ, Vasilevich NI, Glushkov AI, Zilbershtein TM, Ivanov AV, Cole AG, Henderson I, Zautke NA, Brunn SA, Mollova N, Leung K, Chisholm JW, and Zablocki J

Subjects

Animals, Cell Line, Drug Evaluation, Preclinical, Enzyme Inhibitors metabolism, Enzyme Inhibitors pharmacology, Humans, Inhibitory Concentration 50, Microsomes metabolism, Pteridines metabolism, Pteridines pharmacology, Quinoxalines pharmacology, Rats, Stearoyl-CoA Desaturase metabolism, Structure-Activity Relationship, Enzyme Inhibitors chemistry, Pteridines chemistry, Quinoxalines chemistry, Stearoyl-CoA Desaturase antagonists & inhibitors

Abstract

We identified a series of structurally novel SCD (Delta9 desaturase) inhibitors via high-throughput screening and follow-up SAR studies. Modification of the central bicyclic scaffold has proven key to our potency optimization effort. The most potent analog (8g) had IC(50) value of 50 pM in a HEPG2 SCD assay and has been shown to be metabolically stable and selective against Delta5 and Delta6 desaturases.

Published

2009

13. Efficient synthesis of 5-substituted 2-aryl-6-cyanoindolizines via nucleophilic substitution reactions.

Author

Babaev EV, Vasilevich NI, and Ivushkina AS

Abstract

2-Aryl-6-cyano-7-methyl-5-indolizinones were successfully converted into 2-aryl-5-chloro-6-cyano-7-methylindolizines. The obtained 5-chloroindolizines readily underwent nucleophilic substitution at position 5 leading in high yields to novel 5-functionalised indolizines.

Published

2005

14. Examination of the 1,4-disubstituted azetidinone ring system as a template for combretastatin A-4 conformationally restricted analogue design.

Author

Sun L, Vasilevich NI, Fuselier JA, Hocart SJ, and Coy DH

Subjects

Animals, Antineoplastic Agents chemical synthesis, Antineoplastic Agents pharmacology, Cell Line, Tumor, Humans, Mice, Mice, Nude, Models, Molecular, Rats, Stilbenes chemical synthesis, Stilbenes pharmacology, Antineoplastic Agents chemistry, Azetidines chemistry, Stilbenes chemistry

Abstract

A series of novel 1,4-diaryl-2-azetidinones was prepared by stereospecific Staudinger reaction as conformationally restricted analogues of combretastatin A-4 because molecular modeling studies suggested close geometric similarities. They were evaluated for cytotoxicity against a number of human tumor and normal cell lines. Strong potencies were observed, with the best compounds exhibiting IC(50)'s of 25-74 nM against human neuroblastoma IMR 32 cell growth and a variety of other cell lines. Compounds inhibited tubulin polymerization with potencies commensurate with their cytotoxic activity and a more soluble anilino-containing analogue was very effective in inhibiting the growth of AR42J rat pancreatic tumors transplanted into in nude mice. Further studies on this interesting group of compounds as anti-cancer agents appear warranted.

Published

2004

15. Abilities of 3,4-diarylfuran-2-one analogs of combretastatin A-4 to inhibit both proliferation of tumor cell lines and growth of relevant tumors in nude mice.

Author

Sun L, Vasilevich NI, Fuselier JA, and Coy DH

Subjects

Animals, Antineoplastic Agents, Phytogenic toxicity, Cell Cycle drug effects, Cell Division drug effects, Cell Line, Tumor, Drug Screening Assays, Antitumor, Female, Furans toxicity, Growth Inhibitors pharmacology, Growth Inhibitors toxicity, Humans, Male, Mice, Mice, Nude, Stilbenes toxicity, Tubulin metabolism, Xenograft Model Antitumor Assays, Antineoplastic Agents, Phytogenic pharmacology, Furans pharmacology, Stilbenes pharmacology

Abstract

Background: Combretastatin A-4 (CA-4) and its analogs are potent inhibitors of tubulin polymerization and display strong inhibitory activity on both solid tumor and tumor cell growth. Since natural CA-4 is difficult to synthesize and also isomerizes to an inactive form quite readily, a recently reported new 3,4-diarylfuran-2-one-based series of CA-4 analogs was investigated, in the hope of bypassing some of these difficulties. These analogs appear to offer a valuable tool for CA-4 research because of their extremely facile synthesis from readily available starting materials., Materials and Methods: The CA-4 analogs were evaluated by MTT assay, cell cycle analysis, tubulin polymerization and tumor-inhibiting experiments., Results: Various benzene ring substitutions on the furan-2-one skeleton (analogs to the two aromatic rings on the CA-4 styrene skeleton) quickly demonstrated that the structure-activity relationships are quite similar to previously synthesized CA-4 analogs. The most interesting analog appears to be an anilino compound (NV-5-9) which was also quite soluble. Analog NV-5-9 was remarkably potent in all tested tumor cell lines and could strongly inhibit tubulin polymerization at doses as low as 1 mM. Further experiments with tumor-bearing mice indicated that NV-5-9 and other potent analogs (NV-4-82 and NV-4-86) were effective in treating human prostate PC-3 and SCLC NCI-H69 tumors at well below an oral MTD dose of around 200 mg/kg body weight. This suggests some bioavailability by this route., Conclusion: These data strongly support that NV-5-9 is extremely potent, readily synthesizable and apparently suitable for in vivo studies employing transplanted tumors.

Published

2004

16. [The use of the HPLC method for the quantitative determination of a peptide analog of piracetam with nootropic activity and its main metabolites].

Author

Boĭko SS, Zherdev VP, Gudasheva TA, Vasilevich NI, Ostrovskaia RU, Voronina TA, and Rozantsev GG

Subjects

Animals, Liver chemistry, Male, Nootropic Agents pharmacokinetics, Piracetam analysis, Piracetam pharmacokinetics, Rats, Spectrophotometry, Ultraviolet, Chromatography, High Pressure Liquid methods, Nootropic Agents analysis, Piracetam analogs & derivatives

Abstract

HPLC method has been developed for pharmacokinetic study of nootropic peptide analog of pyracetam GVS-111 and its main metabolites. In the model experiments on rats the enzymes of blood plasma were shown to metabolize GVS-111 during 1-h incubation with the formation of metabolite, phenylacetylproline. This suggests that in vivo experiments these blood plasma enzymes will also be actively involved in the metabolism of the compound tested. The liver tissue enzymes metabolized GVS-111 much slower.

Published

1996