Your search keyword '"V. Petrauskas"' showing total 8 results

1. Heat Shock Protein 90 Inhibitor Effects on Pancreatic Cancer Cell Cultures

Author

Aistė Gulla, Hong Liang, Kęstutis Strupas, James R. Eshleman, Egidijus Kazlauskas, Daumantas Matulis, and V. Petrauskas

Subjects

Endocrinology, Diabetes and Metabolism, Lactams, Macrocyclic, Ganetespib, Antineoplastic Agents, Isoindoles, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Endocrinology, Heat shock protein, Cell Line, Tumor, Internal Medicine, medicine, Benzoquinones, Humans, Cell Culture Techniques, Three Dimensional, HSP90 Heat-Shock Proteins, Cell Proliferation, Adenosine Triphosphatases, Hepatology, biology, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Cell growth, Cancer, Isoxazoles, Resorcinols, Triptolide, Triazoles, medicine.disease, Hsp90, In vitro, Pancreatic Neoplasms, Rifabutin, Cell culture, 030220 oncology & carcinogenesis, Benzamides, biology.protein, Cancer research, 030211 gastroenterology & hepatology, Carcinoma, Pancreatic Ductal

Abstract

Objectives Pancreatic ductal adenocarcinoma is one of the deadliest cancers for which few curative therapies are available to date. Heat shock protein 90 (Hsp90) inhibitors have shown activity against numerous cancers in vitro; therefore, we tested whether they could be used to target pancreatic ductal adenocarcinoma. Methods Inhibitors of Hsp90 ATPase activity were applied on low-passage pancreatic cell line cultures (Panc10.05, Panc215, A6L) in a dose-response manner, and the inhibitor in vitro effect on cell growth was evaluated. Seven of novel Hsp90 inhibitors based on resorcinol fragment and 5 commercially available Hsp90 inhibitors (17-AAG, AT-13387, AUY-922, ganetespib, and rifabutin) as well as control compound triptolide were tested yielding IC50 values in 2- and 3-dimensional assays. Results The novel Hsp90 inhibitors exhibited strong effects on all 3 tested pancreatic cell line cultures (Panc10.05, Panc215, A6L) reaching the IC50 of 300 to 600 nM in 2- and 3-dimensional assays. Conclusions Novel Hsp90 inhibitors can be developed as antipancreatic cancer agents. Their chemical structures are simpler, and they are likely to exhibit lower side effects than the much more complex inhibitors used as controls.

Published

2021

2. Thiazide and other Cl-benzenesulfonamide-bearing clinical drug affinities for human carbonic anhydrases

Author

Daumantas Matulis, V. Petrauskas, Vilma Michailovienė, Lina Baranauskiene, and Lina Škiudaitė

Subjects

Biochemistry, Thiazides, chemistry.chemical_compound, Antibiotics, Catalytic Domain, Medicine and Health Sciences, Drug Interactions, Enzyme Inhibitors, Diuretics, Carbonic Anhydrases, chemistry.chemical_classification, Sulfonamides, Multidisciplinary, biology, Chemistry, Antimicrobials, Pharmaceutics, Drugs, Enzymes, Isoenzymes, Antihypertensive Drugs, carbonic anhydrase, thiazide, sulfonamide, Physical Sciences, Metolazone, Medicine, Chlorine, Research Article, Chemical Elements, Protein Binding, Gene isoform, Thermal shift assay, Bicarbonate, Science, Sulfonamide, Microbiology, Structure-Activity Relationship, Drug Therapy, Carbonic anhydrase, Microbial Control, Humans, Pharmacology, Biology and Life Sciences, Proteins, Isothermal titration calorimetry, Affinities, Enzyme, biology.protein, Enzymology

Abstract

Twelve carbonic anhydrase (CA) isoforms catalyze carbon dioxide hydration to bicarbonate and acid protons and are responsible for many biological functions in human body. Despite their vital functions, they are also responsible for, or implicated in, numerous ailments and diseases such as glaucoma, high altitude sickness, and cancer. Because CA isoforms are highly homologous, clinical drugs designed to inhibit enzymatic activity of a particular isoform, can also bind to others with similar affinity causing toxic side effects. In this study, the affinities of twelve CA isoforms have been determined for nineteen clinically used drugs used to treat hypertension related diseases, i.e. thiazides, indapamide, and metolazone. Their affinities were determined using a fluorescent thermal shift assay. Stopped flow assay and isothermal titration calorimetry were also employed on a subset of compounds and proteins to confirm inhibition of CA enzymatic activity and verify the quantitative agreement between different assays. The findings of this study showed that pharmaceuticals could bind to human CA isoforms with variable affinities and inhibit their catalytic activity, even though the drug was intended to interact with a different (non-CA) protein target. Relatively minor structural changes of the compounds may cause significant changes in affinity and selectivity for a particular CA isoform.

Published

2021

3. Protein-ligand binding volume determined from a single 2D NMR spectrum with increasing pressure

Author

V. Petrauskas, Gediminas Skvarnavičius, Christian Roumestand, Vilma Michailovienė, Zigmantas Toleikis, and Daumantas Matulis

Subjects

Magnetic Resonance Spectroscopy, Ligands, 010402 general chemistry, 01 natural sciences, protein-ligand binding volume, 2D NMR, pressure, Article, Enzyme catalysis, Carbonic anhydrase, 0103 physical sciences, Materials Chemistry, Physical and Theoretical Chemistry, 010304 chemical physics, biology, Chemistry, Proteins, Nuclear magnetic resonance spectroscopy, Ligand (biochemistry), Magnetic Resonance Imaging, 0104 chemical sciences, Surfaces, Coatings and Films, Volume (thermodynamics), biology.protein, Biophysics, Two-dimensional nuclear magnetic resonance spectroscopy, Heteronuclear single quantum coherence spectroscopy, Protein Binding, Protein ligand

Abstract

Proteins undergo changes in their partial volumes in numerous biological processes such as enzymatic catalysis, unfolding–refolding, and ligand binding. The change in the protein volume upon ligand binding—a parameter termed the protein–ligand binding volume—can be extensively studied by high-pressure NMR spectroscopy. In this study, we developed a method to determine the protein–ligand binding volume from a single two-dimensional (2D) 1H–15N heteronuclear single quantum coherence (HSQC) spectrum at different pressures, if the exchange between ligand-free and ligand-bound states of a protein is slow in the NMR time-scale. This approach required a significantly lower amount of protein and NMR time to determine the protein–ligand binding volume of two carbonic anhydrase isozymes upon binding their ligands. The proposed method can be used in other protein–ligand systems and expand the knowledge about protein volume changes upon small-molecule binding.

Published

2021

4. Inhibitor Binding to Carbonic Anhydrases by Fluorescent Thermal Shift Assay

Author

Matthew J. Todd, V. Petrauskas, Asta Zubrienė, and Daumantas Matulis

Subjects

chemistry.chemical_classification, Gene isoform, Thermal shift assay, chemistry, biology, Ligand, Carbonic anhydrase, Melting point, biology.protein, Biophysics, Fluorescence, Affinities, Sulfonamide

Abstract

In this chapter we describe the model that quantifies interactions between proteins and ligands applying the thermal shift assay. When combined with fluorescence-based measurements of protein thermal unfolding, this model forms the basis of the fluorescent thermal shift assay—a widely applicable and cost-effective technique to quantify ligand affinity towards proteins. Most ligands stabilize proteins against thermal denaturation and shift their melting points towards higher temperatures. Equations that relate the shift in protein melting temperature with the ligand concentration are presented. The assay has been used to determine affinities of various sulfonamide inhibitor binding to carbonic anhydrase isoforms. The results illustrate applicability and limitations of the fluorescent thermal shift assay.

Published

2019

5. Change in Volume Upon Inhibitor Binding to Carbonic Anhydrases by Fluorescent Pressure Shift Assay

Author

V. Petrauskas, Daumantas Matulis, and Gediminas Skvarnavičius

Subjects

Aqueous solution, Volume (thermodynamics), biology, Chemistry, Carbonic anhydrase, biology.protein, Biophysics, Fluorescence, Complement (complexity)

Abstract

High-pressure studies of protein–ligand system in aqueous solution provide volumetric information about the increase or decrease in compactness of the interacting counterparts. Volumetric parameters complement the thermodynamic picture of protein–ligand interaction. Here we describe fluorescent pressure shift assay—a technique that addresses volume-related parameters of protein–ligand system. Carbonic anhydrase (CA) and their ligands were useful objects that extended our knowledge about the applicability of this method.

Published

2019

6. Volume of Hsp90 Protein-Ligand Binding Determined by Fluorescent Pressure Shift Assay, Densitometry, and NMR

Author

Christian Roumestand, Vladimir A. Sirotkin, V. Petrauskas, Gediminas Skvarnavičius, Joana Smirnovienė, Daumantas Matulis, and Zigmantas Toleikis

Subjects

0301 basic medicine, 010402 general chemistry, Ligands, 01 natural sciences, Fluorescence, law.invention, 03 medical and health sciences, law, Heat shock protein, Materials Chemistry, Pressure, Humans, HSP90 Heat-Shock Proteins, Physical and Theoretical Chemistry, Enzyme Inhibitors, Nuclear Magnetic Resonance, Biomolecular, Adenosine Triphosphatases, Binding Sites, biology, Molecular Structure, Chemistry, Hsp90, 0104 chemical sciences, Surfaces, Coatings and Films, Crystallography, 030104 developmental biology, Solvation shell, Proteome, biology.protein, Recombinant DNA, Biophysics, Densitometry, Protein ligand

Abstract

Human heat shock protein 90 (Hsp90) is a key player in the homeostasis of the proteome and plays a role in numerous diseases, such as cancer. For the design of Hsp90 ATPase activity inhibitors, it is important to understand the relationship between an inhibitor structure and its inhibition potential. The volume of inhibitor binding is one of the most important such parameters that are rarely being studied. Here, the volumes of binding of several ligands to recombinant Hsp90 were obtained by three independent experimental techniques: fluorescent pressure shift assay, vibrating tube densitometry, and high-pressure NMR. Within the error range, all techniques provided similar volumetric parameters for the investigated protein-ligand systems. Protein-ligand binding volumes were negative, suggesting that the protein-ligand complex, together with its hydration shell, occupies less volume than the separate constituents with their hydration shells. Binding volumes of tightly binding, subnanomolar ligands were significantly more negative than those of weakly binding, millimolar ligands. The volumes of binding could be useful for designing inhibitors with desired recognition properties and further development as drugs.

Published

2016

7. Discovery and characterization of novel selective inhibitors of carbonic anhydrase IX

Author

J. Smirnoviene, S. Baksyte, A. Mickeviciute, Alexey Smirnov, Saulius Grazulis, V. Petrauskas, Audrius Zakšauskas, G. Milinaviciute, V. Morkunaite, David D. Timm, Povilas Norvaisas, Jelena Jachno, Jurgita Matuliene, Asta Zubriene, Lina Baranauskiene, Virginija Dudutiene, V. Pilipuityte, Vilma Petrikaite, Justina Kazokaite, Elena Manakova, A. Kasiliauskaite, J. Revuckiene, Edita Capkauskaite, John E. Ladbury, P. Gibieza, Vytautas Smirnovas, M. Kisonaite, Visvaldas Kairys, E. Ivanauskaite, V. Juozapaitiene, Daumantas Matulis, Egidijus Kazlauskas, Vilma Michailoviene, and D. Linge

Subjects

Stereochemistry, Protein Conformation, Kinetics, Plasma protein binding, Calorimetry, Crystallography, X-Ray, Catalysis, law.invention, Protein structure, Carbonic Anhydrase IV, law, Catalytic Domain, Neoplasms, Drug Discovery, Humans, Carbonic Anhydrase Inhibitors, Carbonic Anhydrases, Sulfonamides, biology, Chemistry, Active site, Benzene, Carbonic Anhydrase IX, Carbon Dioxide, Hydrogen-Ion Concentration, Recombinant Proteins, Drug Design, biology.protein, Recombinant DNA, Molecular Medicine, Thermodynamics, Selectivity, Crystallization, Protein Binding

Abstract

Human carbonic anhydrase IX (CA IX) is highly expressed in tumor tissues, and its selective inhibition provides a potential target for the treatment of numerous cancers. Development of potent, highly selective inhibitors against this target remains an unmet need in anticancer therapeutics. A series of fluorinated benzenesulfonamides with substituents on the benzene ring was designed and synthesized. Several of these exhibited a highly potent and selective inhibition profile against CA IX. Three fluorine atoms significantly increased the affinity by withdrawing electrons and lowering the pKa of the benzenesulfonamide group. The bulky ortho substituents, such as cyclooctyl or even cyclododecyl groups, fit into the hydrophobic pocket in the active site of CA IX but not CA II, as shown by the compound's co-crystal structure with chimeric CA IX. The strongest inhibitor of recombinant human CA IX's catalytic domain in human cells achieved an affinity of 50 pM. However, the high affinity diminished the selectivity. The most selective compound for CA IX exhibited 10 nM affinity. The compound that showed the best balance between affinity and selectivity bound with 1 nM affinity. The inhibitors described in this work provide the basis for novel anticancer therapeutics targeting CA IX.

Published

2014

8. Determination of the volume changes induced by ligand binding to heat shock protein 90 using high-pressure denaturation

Author

Daumantas Matulis, V. Petrauskas, P. Cimmperman, and Zigmantas Toleikis

Subjects

Thermal shift assay, Protein Denaturation, Lactams, Macrocyclic, Biophysics, Molecular Conformation, Plasma protein binding, Ligands, Biochemistry, Heat shock protein, Benzoquinones, Pressure, Denaturation (biochemistry), HSP90 Heat-Shock Proteins, Molecular Biology, Guanidine, Protein Unfolding, biology, Chemistry, Protein Stability, Cell Biology, Ligand (biochemistry), Binding constant, Hsp90, Crystallography, Volume (thermodynamics), biology.protein, Thermodynamics, Macrolides, Protein Binding

Abstract

The volume changes accompanying ligand binding to proteins are thermodynamically important and could be used in the design of compounds with specific binding properties. Measuring the volumetric properties could yield as much information as the enthalpic properties of binding. Pressure-based methods are significantly more laborious than temperature methods and are underused. Here we present a pressure shift assay (PressureFluor, analogous to the ThermoFluor thermal shift assay) that uses high pressure to denature proteins. The PressureFluor method was used to study the ligand binding thermodynamics of heat shock protein 90 (Hsp90). Ligands stabilize the protein against pressure denaturation, similar to the stabilization against temperature denaturation. The equations that relate the ligand dosing, protein concentration, and binding constant with the volumes and compressibilities of unfolding and binding are presented.

Published

2011