Your search keyword '"Elvin D, de Araujo"' showing total 17 results

1. Phenotypic Screening of Histone Deacetylase (HDAC) Inhibitors against Schistosoma mansoni

Author

Muhammad Murtaza Hassan, Abootaleb Sedighi, Olasunkanmi O. Olaoye, Cécile Häberli, Annika Merz, Elizabeth Ramos‐Morales, Elvin D. de Araujo, Christophe Romier, Manfred Jung, Jennifer Keiser, and Patrick T. Gunning

Subjects

Pharmacology, Organic Chemistry, Schistosoma mansoni, Biochemistry, Histone Deacetylases, Praziquantel, Histone Deacetylase Inhibitors, Isoenzymes, Repressor Proteins, Drug Discovery, Molecular Medicine, Animals, Humans, Schistosomiasis, General Pharmacology, Toxicology and Pharmaceutics

Abstract

Schistosomiasis is a prevalent yet neglected tropical parasitic disease caused by the Schistosoma genus of blood flukes. Praziquantel is the only currently available treatment, hence drug resistance poses a major threat. Recently, histone deacetylase 8 (HDAC8) selective inhibitors have been proposed as a viable treatment for schistosomiasis. Herein, we report the phenotypic screening of a focused library of small molecules of varying HDAC isozyme-inhibition profiles, including eight HDAC8 inhibitors with10-fold selectivity in comparable functional inhibition assays and IC

Published

2022

2. Sensitive Detection of Broad-Spectrum Bacteria with Small-Molecule Fluorescent Excimer Chemosensors

Author

Aaron D. Cabral, Daniel Nino, Nafiseh Rafiei, Krimo Toutah, Patrick T. Gunning, Tudor B. Radu, Elvin D. de Araujo, Bronte I. Murcar-Evans, Joshua N. Milstein, and Dziyana Kraskouskaya

Subjects

Bioengineering, 02 engineering and technology, 01 natural sciences, Flow cytometry, chemistry.chemical_compound, Cyclen, Cyclam, medicine, Fluorescence microscope, Animals, Humans, Mode of action, Instrumentation, Fluorescent Dyes, Fluid Flow and Transfer Processes, Bacteria, biology, medicine.diagnostic_test, Process Chemistry and Technology, 010401 analytical chemistry, 021001 nanoscience & nanotechnology, biology.organism_classification, Fluorescence, Small molecule, 0104 chemical sciences, 3. Good health, Zinc, Microscopy, Fluorescence, chemistry, Biophysics, 0210 nano-technology

Abstract

Antibiotic resistance is a major problem for world health, triggered by the unnecessary usage of broad-spectrum antibiotics on purportedly infected patients. Current clinical standards require lengthy protocols for the detection of bacterial species in sterile physiological fluids. In this work, a class of small-molecule fluorescent chemosensors termed ProxyPhos was shown to be capable of rapid, sensitive, and facile detection of broad-spectrum bacteria. The sensors act via a turn-on fluorescent excimer mechanism, where close-proximity binding of multiple sensor units amplifies a red shift emission signal. ProxyPhos sensors were able to detect down to 10 CFUs of model strains by flow cytometry assays and showed selectivity over mammalian cells in a bacterial coculture through fluorescence microscopy. The studies reveal that the zinc(II)-chelates cyclen and cyclam are novel and effective binding units for the detection of both Gram-negative and Gram-positive bacterial strains. Mode of action studies revealed that the chemosensors detect Gram-negative and Gram-positive strains with two distinct mechanisms. Preliminary studies applying ProxyPhos sensors to sterile physiological fluids (cerebrospinal fluid) in flow cytometry assays were successful. The results suggest that ProxyPhos sensors can be developed as a rapid, inexpensive, and robust tool for the "yes-no" detection of broad-spectrum bacteria in sterile fluids.

Published

2020

3. Emerging mechanisms of targeted protein degradation by molecular glues

Author

Geordon A, Frere, Elvin D, de Araujo, and Patrick T, Gunning

Subjects

Proteome, Ubiquitin-Protein Ligases, Proteolysis, Humans, Ligands, Protein Binding

Abstract

Targeted protein degradation has emerged as a transformative therapeutic modality for the treatment of human diseases. The clinical successes of approved protein degraders like lenalidomide and thalidomide in cancers and immune disorders, combined with the recent clinical debut of investigational heterobifunctional degraders, have demonstrated the potential of this pharmacological approach to expand the druggable proteome and improve patient outcomes. Molecular glue degraders are a class of protein degraders that operate by recruiting target proteins to cellular degradation machinery via noncanonical protein-protein interactions, inducing the destruction of the target protein. While heterobifunctional degraders consist of two distinct protein-binding moieties connected by a linker, molecular glue degraders contain a single pharmacophore and are thus more synthetically accessible, ligand-efficient, and often possess more drug-like physicochemical properties. In this chapter, we will explore the history of the field-from its conception to the recently accelerating discovery of novel glue degrader mechanisms-and contemplate its trajectory towards rational design with the emergence of new methods for protein quantification and high-throughput assays to screen for novel degraders.

Published

2022

4. Discovery of HDAC6-Selective Inhibitor NN-390 with

Author

Nabanita, Nawar, Shazreh, Bukhari, Ashley A, Adile, Yujin, Suk, Pimyupa, Manaswiyoungkul, Krimo, Toutah, Olasunkanmi O, Olaoye, Yasir S, Raouf, Abootaleb, Sedighi, Harsimran Kaur, Garcha, Muhammad Murtaza, Hassan, William, Gwynne, Johan, Israelian, Tudor B, Radu, Mulu, Geletu, Ayah, Abdeldayem, Justyna M, Gawel, Aaron D, Cabral, Chitra, Venugopal, Elvin D, de Araujo, Sheila K, Singh, and Patrick T, Gunning

Subjects

Models, Molecular, Brain Neoplasms, Cell Survival, Antineoplastic Agents, Histone Deacetylase 6, Histone Deacetylase Inhibitors, Molecular Docking Simulation, Structure-Activity Relationship, Cell Line, Tumor, Drug Discovery, Neoplastic Stem Cells, Humans, Computer Simulation, Drug Screening Assays, Antitumor, Medulloblastoma

Abstract

Histone deacetylase 6 (HDAC6) has been targeted in clinical studies for anticancer effects due to its role in oncogenic transformation and metastasis. Through a second-generation structure-activity relationship (SAR) study, the design, and biological evaluation of the selective HDAC6 inhibitor

Published

2022

5. Unique Molecular Interaction with the Histone Deacetylase 6 Catalytic Tunnel: Crystallographic and Biological Characterization of a Model Chemotype

Author

Andrew E. Shouksmith, Abootaleb Sedighi, Yasir S. Raouf, Niyati Kachhiyapatel, Ayah Abdeldayem, Paris R. Watson, Krimo Toutah, Olasunkanmi O. Olaoye, David W. Christianson, Patrick T. Gunning, Shazreh Bukhari, Pimyupa Manaswiyoungkul, Justyna M. Gawel, Aaron D. Cabral, Johan Israelian, Muhammad Murtaza Hassan, Nabanita Nawar, Fettah Erdogan, Elvin D. de Araujo, Tudor B. Radu, and Mulu Geletu

Subjects

Male, Histone Deacetylase 6, Hydroxamic Acids, Isozyme, Article, 03 medical and health sciences, Residue (chemistry), Structure-Activity Relationship, 0302 clinical medicine, Catalytic Domain, Cell Line, Tumor, Drug Discovery, Animals, Humans, Structural motif, Zebrafish, IC50, 030304 developmental biology, Cell Proliferation, 0303 health sciences, Mice, Inbred BALB C, Sulfonamides, biology, Molecular Structure, Chemistry, Hydrogen bond, HDAC6, Zebrafish Proteins, biology.organism_classification, 3. Good health, Histone Deacetylase Inhibitors, Molecular Docking Simulation, 030220 oncology & carcinogenesis, Biophysics, Molecular Medicine, Pharmacophore, Protein Binding

Abstract

Histone deacetylase 6 (HDAC6) is involved in multiple regulatory processes, ranging from cellular stress to intracellular transport. Inhibition of aberrant HDAC6 activity in several cancers and neurological diseases has been shown to be efficacious in both preclinical and clinical studies. While selective HDAC6 targeting has been pursued as an alternative to pan-HDAC drugs, identifying truly selective molecular templates has not been trivial. Herein, we report a structure-activity relationship study yielding TO-317, which potently binds HDAC6 catalytic domain 2 (Ki = 0.7 nM) and inhibits the enzyme function (IC50 = 2 nM). TO-317 exhibits 158-fold selectivity for HDAC6 over other HDAC isozymes by binding the catalytic Zn2+ and, uniquely, making a never seen before direct hydrogen bond with the Zn2+ coordinating residue, His614. This novel structural motif targeting the second-sphere His614 interaction, observed in a 1.84 A resolution crystal structure with drHDAC6 from zebrafish, can provide new pharmacophores for identifying enthalpically driven, high-affinity, HDAC6-selective inhibitors.

Published

2021

6. Development of HDAC Inhibitors Exhibiting Therapeutic Potential in T-Cell Prolymphocytic Leukemia

Author

Patrick T. Gunning, Yasir S. Raouf, Muhammad Murtaza Hassan, Jana von Jan, Aleksandr Ianevski, Muzaffar N. Bhatti, Justyna M. Gawel, Mulu Geletu, Pimyupa Manaswiyoungkul, Nabanita Nawar, Elvin D. de Araujo, Helena Sorger, Olasunkanmi O. Olaoye, Tero Aittokallio, Oliver H. Krämer, Marco Herling, Sanna Timonen, Ayah Abdeldayem, Krimo Toutah, Tudor B. Radu, Richard Moriggl, Shazreh Bukhari, Johan Israelian, Heidi A. Neubauer, Satu Mustjoki, Andrew E. Shouksmith, Abootaleb Sedighi, Computational Systems Medicine, TRIMM - Translational Immunology Research Program, Institute for Molecular Medicine Finland, Helsinki Institute for Information Technology, Tero Aittokallio / Principal Investigator, Bioinformatics, HUS Comprehensive Cancer Center, Department of Clinical Chemistry and Hematology, and Clinicum

Subjects

Male, Pyrrolidines, medicine.medical_treatment, TUBULIN, Apoptosis, SUBEROYLANILIDE HYDROXAMIC ACID, Histone Deacetylase 6, Hydroxamic Acids, 01 natural sciences, Targeted therapy, Mice, chemistry.chemical_compound, Drug Discovery, para-Aminobenzoates, Bendamustine Hydrochloride, Prolymphocytic leukemia, RICOLINOSTAT, Sulfonamides, 0303 health sciences, Molecular Structure, Chemistry, Drug Synergism, 3. Good health, Molecular Docking Simulation, Molecular Medicine, medicine.drug, Bendamustine, ACCURATE DOCKING, EXPRESSION, 3122 Cancers, BORTEZOMIB, Antineoplastic Agents, BCL-2 INHIBITOR, Article, Structure-Activity Relationship, 03 medical and health sciences, HISTONE DEACETYLASE INHIBITOR, Cell Line, Tumor, medicine, Animals, Humans, Epigenetics, COMBINATION, 030304 developmental biology, Venetoclax, HDAC6, Bridged Bicyclo Compounds, Heterocyclic, medicine.disease, 0104 chemical sciences, Histone Deacetylase Inhibitors, MODEL, 010404 medicinal & biomolecular chemistry, Leukemia, Prolymphocytic, T-Cell, Cancer research, T-cell prolymphocytic leukemia, Histone deacetylase

Abstract

Epigenetic targeting has emerged as an efficacious therapy for hematological cancers. The rare and incurable T-cell prolymphocytic leukemia (T-PLL) is known for its aggressive clinical course. Current epigenetic agents such as histone deacetylase (HDAC) inhibitors are increasingly used for targeted therapy. Through a structure-activity relationship (SAR) study, we developed an HDAC6 inhibitor KT-531, which exhibited higher potency in T-PLL compared to other hematological cancers. KT-531 displayed strong HDAC6 inhibitory potency and selectivity, on-target biological activity, and a safe therapeutic window in nontransformed cell lines. In primary T-PLL patient cells, where HDAC6 was found to be overexpressed, KT-531 exhibited strong biological responses, and safety in healthy donor samples. Notably, combination studies in T-PLL patient samples demonstrated KT-531 synergizes with approved cancer drugs, bendamustine, idasanutlin, and venetoclax. Our work suggests HDAC inhibition in T-PLL could afford sufficient therapeutic windows to achieve durable remission either as standalone or in combination with targeted drugs.

Published

2021

7. Characterization of Conformationally Constrained Benzanilide Scaffolds for Potent and Selective HDAC8 Targeting

Author

Muhammad Murtaza Hassan, Yasir S. Raouf, Pimyupa Manaswiyoungkul, Aaron D. Cabral, Abootaleb Sedighi, Rabia Altintas, Fettah Erdogan, Patrick T. Gunning, Giovanni Ganda, David W.J. Armstrong, Olasunkanmi O. Olaoye, Elvin D. de Araujo, Johan Israelian, Fabrizio Angeles, and Nabanita Nawar

Subjects

01 natural sciences, Histone Deacetylases, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, Catalytic Domain, Drug Discovery, Humans, Anilides, IC50, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Gene knockdown, biology, Benzanilide, HDAC8, Combinatorial chemistry, In vitro, 0104 chemical sciences, 3. Good health, Histone Deacetylase Inhibitors, Molecular Docking Simulation, Repressor Proteins, 010404 medicinal & biomolecular chemistry, Enzyme, Histone, chemistry, Drug Design, biology.protein, Molecular Medicine, Selectivity

Abstract

Histone deacetylases (HDACs) are an attractive therapeutic target for a variety of human diseases. Currently, all four FDA-approved HDAC-targeting drugs are nonselective, pan-HDAC inhibitors, exhibiting adverse side effects at therapeutic doses. Although selective HDAC inhibition has been proposed to mitigate toxicity, the targeted catalytic domains are highly conserved. Herein, we describe a series of rationally designed, conformationally constrained, benzanilide foldamers which selectively bind the catalytic tunnel of HDAC8. The series includes benzanilides, MMH371, MMH409, and MMH410, which exhibit potent in vitro HDAC8 activity (IC50 = 66, 23, and 66 nM, respectively) and up to 410-fold selectivity for HDAC8 over the next targeted HDAC. Experimental and computational analyses of the benzanilide structure docked with human HDAC8 enzyme showed the adoption of a low-energy L-shaped conformer that favors HDAC8 selectivity. The conformationally constrained HDAC8 inhibitors present an alternative biological probe for further determining the clinical utility and safety of pharmacological knockdown of HDAC8 in diseased cells.

Published

2020

8. A functional in vitro assay for screening inhibitors of STAT5B phosphorylation

Author

Diana Sina, Pimyupa Manaswiyoungkul, Karen Yuen, Patrick T. Gunning, Fettah Erdogan, Elvin D. de Araujo, Gary Tin, Abdul K. Qadree, and Krimo Toutah

Subjects

Clinical Biochemistry, Pharmaceutical Science, Ligands, SH2 domain, 01 natural sciences, stat, Analytical Chemistry, Western blot, Drug Discovery, STAT5 Transcription Factor, medicine, Humans, Phosphorylation, Proto-Oncogene Proteins c-abl, Protein Kinase Inhibitors, Spectroscopy, ABL, medicine.diagnostic_test, 010405 organic chemistry, Chemistry, Kinase, 010401 analytical chemistry, Reproducibility of Results, High-Throughput Screening Assays, 0104 chemical sciences, Cell biology, Kinetics, STAT protein, Tyrosine kinase

Abstract

Inhibition of STAT phosphorylation is recognized as a viable therapeutic strategy for disrupting tumorigenesis. Constitutive STAT phosphorylation is found with high frequency in a number of primary tumor types, while non-cancer cells exhibit low basal activity, providing an exploitable therapeutic window. STAT activation involves phosphorylation of the SH2 domain by a number of tyrosine kinases followed by STAT dimerization and translocation to the nucleus. By blocking the cognate binding site, STAT SH2-domain inhibitors can impede kinase-mediated de novo STAT phosphorylation. Assessing for inhibitors of STAT phosphorylation has previously been conducted exclusively in cellulo using Western blot analysis. However, while providing useful in cellulo efficacy, it is not possible to conclude that inhibition is due to a direct blockade of STAT protein. Here we developed a functional assay that directly reports the blockade of phosphorylation as a result of inhibitor interaction with STAT proteins. We have optimized reaction conditions for the functional assay and validated the assay against known STAT5B ligands, including peptides and small molecule inhibitors. As part of the study, we have also identified several sites of STAT5B phosphorylation by Abl kinase. This assay will serve to delineate the functional mechanism of STAT binders in vitro and deconvolute the mechanism of phospho-STAT inhibition observed in Western blot analysis.

Published

2019

9. Pharmacologic inhibition of STAT5 in acute myeloid leukemia

Author

Ji Sung Park, Gary Tin, Elizabeth Heyes, Anna Orlova, Bettina Wingelhofer, Abbarna A. Cumaraswamy, Dávid Bajusz, Florian Grebien, Barbara Maurer, Charles-Hugues Lardeau, Elvin D. de Araujo, Patrick T. Gunning, Irina Sadovnik, György M. Keserű, Angelika Berger-Becvar, Frank Ruge, Patricia Freund, Stefan Kubicek, Peter Valent, Richard Moriggl, and Siawash Ahmar

Subjects

0301 basic medicine, Cancer Research, Myeloid, Article, Cell Line, 03 medical and health sciences, Cell Line, Tumor, hemic and lymphatic diseases, Nitriles, STAT5 Transcription Factor, medicine, Animals, Humans, STAT5, Cell Proliferation, biology, Terpenes, business.industry, food and beverages, Myeloid leukemia, Drug Synergism, Hematology, Protein-Tyrosine Kinases, medicine.disease, Leukemia, Myeloid, Acute, Leukemia, Haematopoiesis, Pyrimidines, 030104 developmental biology, medicine.anatomical_structure, fms-Like Tyrosine Kinase 3, Oncology, PCAF, Fms-Like Tyrosine Kinase 3, Cancer research, biology.protein, Pyrazoles, business, Tyrosine kinase

Abstract

The transcription factor STAT5 is an essential downstream mediator of many tyrosine kinases (TKs), particularly in hematopoietic cancers. STAT5 is activated by FLT3-ITD, which is a constitutively active TK driving the pathogenesis of acute myeloid leukemia (AML). Since STAT5 is a critical mediator of diverse malignant properties of AML cells, direct targeting of STAT5 is of significant clinical value. Here, we describe the development and preclinical evaluation of a novel, potent STAT5 SH2 domain inhibitor, AC-4–130, which can efficiently block pathological levels of STAT5 activity in AML. AC-4–130 directly binds to STAT5 and disrupts STAT5 activation, dimerization, nuclear translocation, and STAT5-dependent gene transcription. Notably, AC-4–130 substantially impaired the proliferation and clonogenic growth of human AML cell lines and primary FLT3-ITD+ AML patient cells in vitro and in vivo. Furthermore, AC-4–130 synergistically increased the cytotoxicity of the JAK1/2 inhibitor Ruxolitinib and the p300/pCAF inhibitor Garcinol. Overall, the synergistic effects of AC-4–130 with TK inhibitors (TKIs) as well as emerging treatment strategies provide new therapeutic opportunities for leukemia and potentially other cancers.

Published

2018

10. PTG-0861: A novel HDAC6-selective inhibitor as a therapeutic strategy in acute myeloid leukaemia

Author

Abootaleb Sedighi, Yasir S. Raouf, Diana Sina, Krimo Toutah, Johan Israelian, Andrew E. Shouksmith, Patrick T. Gunning, Shazreh Bukhari, Elvin D. de Araujo, Olasunkanmi O. Olaoye, Aaron D. Cabral, Nabanita Nawar, Tudor B. Radu, Justyna M. Gawel, and Pimyupa Manaswiyoungkul

Subjects

Male, Druggability, Antineoplastic Agents, Apoptosis, Histone Deacetylase 6, Hydroxamic Acids, 01 natural sciences, 03 medical and health sciences, Mice, Structure-Activity Relationship, Catalytic Domain, Cell Line, Tumor, Drug Discovery, Animals, Humans, Epigenetics, Cytotoxicity, 030304 developmental biology, Pharmacology, 0303 health sciences, Molecular Structure, 010405 organic chemistry, Chemistry, Organic Chemistry, General Medicine, HDAC6, 3. Good health, 0104 chemical sciences, Histone Deacetylase Inhibitors, Molecular Docking Simulation, Leukemia, Myeloid, Acute, Acetylation, Cell culture, Cancer cell, Benzamides, Cancer research, Histone deacetylase, Protein Binding

Abstract

Dysregulated Histone Deacetylase (HDAC) activity across multiple human pathologies have highlighted this family of epigenetic enzymes as critical druggable targets, amenable to small molecule intervention. While efficacious, current approaches using non-selective HDAC inhibitors (HDACi) have been shown to cause a range of undesirable clinical toxicities. To circumvent this, recent efforts have focused on the design of highly selective HDACi as a novel therapeutic strategy. Beyond roles in regulating transcription, the unique HDAC6 (with two catalytic domains) regulates the deacetylation of α -tubulin; promoting growth factor-controlled cell motility, cell division, and metastatic hallmarks. Recent studies have linked aberrant HDAC6 function in various hematological cancers including acute myeloid leukaemia and multiple myeloma. Herein, we report the discovery, in vitro characterization, and biological evaluation of PTG-0861 (JG-265), a novel HDAC6-selective inhibitor with strong isozyme-selectivity (∼36× ) and low nanomolar potency (IC50 = 5.92 nM) against HDAC6. This selectivity profile was rationalized via in silico docking studies and also observed in cellulo through cellular target engagement. Moreover, PTG-0861 achieved relevant potency against several blood cancer cell lines (e.g. MV4-11, MM1S), whilst showing limited cytotoxicity against non-malignant cells (e.g. NHF, HUVEC) and CD-1 mice. In examining compound stability and cellular permeability, PTG-0861 revealed a promising in vitro pharmacokinetic (PK) profile. Altogether, in this study we identified a novel and potent HDAC6-selective inhibitor (∼4× more selective than current clinical standards – citarinostat, ricolinostat), which achieves cellular target engagement, efficacy in hematological cancer cells with a promising safety profile and in vitro PK.

Published

2020

11. Optimization of a high-throughput fluorescence polarization assay for STAT5B DNA binding domain-targeting inhibitors

Author

Fettah Erdogan, Aaron D. Cabral, Patrick T. Gunning, Elvin D. de Araujo, Pimyupa Manaswiyoungkul, and Olasunkanmi O. Olaoye

Subjects

Clinical Biochemistry, Oligonucleotides, Pharmaceutical Science, STAT5B, Fluorescence Polarization, Analytical Chemistry, 03 medical and health sciences, 0302 clinical medicine, Protein Domains, Drug Discovery, STAT5 Transcription Factor, Humans, Spectroscopy, 030304 developmental biology, 0303 health sciences, Chemistry, Oligonucleotide, food and beverages, DNA-binding domain, DNA, Small molecule, In vitro, High-Throughput Screening Assays, DNA-Binding Proteins, 030220 oncology & carcinogenesis, Biophysics, Phosphorylation, Fluorescence anisotropy, Proto-oncogene tyrosine-protein kinase Src

Abstract

Signal transducer and activator of transcription 5B (STAT5B) is constitutively activated in multiple cancers as a result of hyperactivating mutations or dysregulation of upstream effectors. Therapeutic strategies have predominantly targeted the Src homology 2 (SH2) domain to inhibit STAT phosphorylation, a prerequisite for STAT5B transcriptional activation. An alternative approach for STAT5B pharmacologic inhibition involves targeting the DNA-binding domain (DBD). However, this strategy remains relatively unexplored and is further hindered by the lack of a high-throughput in vitro engagement assay. Herein, we present the development and optimization of a STAT5B DBD fluorescence polarization (FP) assay, which facilitates rapid screening of small molecules targeting the STAT5B DBD though displacement of a fluorescently labelled oligonucleotide. The assay can generate a complete DNA-binding profile in 10 min, with signal stability up to 2 h, and minimal changes under a range of conditions including 10 % (v/v) glycerol, 15 % (v/v) DMSO, 1 mM NaCl, 0.02 % (w/v) BSA, and 1 mM EDTA. This assay is compatible with both unphosphorylated and phosphorylated STAT5B and demonstrates suitability for high-throughput screening with a Z′ factor of 0.68 ± 0.07 and a signal to noise ratio of 6.7 ± 0.84.

Published

2019

12. Strategies for over-expression and purification of recombinant full length STAT5B in Escherichia coli

Author

Elvin D. de Araujo, Patrick T. Gunning, and Mulu Geletu

Subjects

0301 basic medicine, Thermal shift assay, 030102 biochemistry & molecular biology, Recombinant Fusion Proteins, Gene Expression, STAT5B, Biology, medicine.disease_cause, law.invention, Blot, 03 medical and health sciences, 030104 developmental biology, Solubility, Biochemistry, Osmolyte, law, Escherichia coli, STAT5 Transcription Factor, Recombinant DNA, medicine, STAT protein, Humans, Transcription factor, Biotechnology

Abstract

STAT5B, a ubiquitious transcription factor, has been implicated in the onset and progression of several cancers. Since the inhibition of STAT activity holds significant therapeutic potential, there is a need to develop high-throughput biophysical screening platforms to rapidly identify high affinity binders of STATs. Biophysical assays would benefit from the efficient and cost-effective production of high purity, full-length STAT proteins. Herein, we have sampled a large region of protein expression and purification space that has substantially increased recombinant STAT5B protein yields from Escherichia coli. The identity of STAT5B was confirmed by Western blotting analysis, while the results of a fluorescence polarization assay indicated that the purified protein is correctly folded and functional. A thermal shift assay was employed to assess the effect of various osmolytes on the stability of the protein. The protein expression conditions identified in this study allowed for more efficient and higher recovery of soluble STAT5B protein, which will enable a broad range of biophysical studies and facilitate high-throughput STAT5B drug screening.

Published

2017

13. Identification and Characterization of AES-135, a Hydroxamic Acid-Based HDAC Inhibitor That Prolongs Survival in an Orthotopic Mouse Model of Pancreatic Cancer

Author

Mulu Geletu, Angelika Berger-Becvar, Ashley A. Adile, William L. Heaton, Stephen F. Konieczny, Justyna M. Gawel, Patrick T. Gunning, Andrew E. Shouksmith, Melissa L. Fishel, Sheila K. Singh, Thomas O'Hare, Michael W. Deininger, H. Artee Luchman, David Bakhshinyan, Michelle Grimard, Chitra Venugopal, Yasir S. Raouf, Fenil Shah, Samuel Weiss, and Elvin D. de Araujo

Subjects

Combination therapy, Hydrocarbons, Fluorinated, Apoptosis, Hydroxamic Acids, 01 natural sciences, Article, 03 medical and health sciences, chemistry.chemical_compound, Mice, In vivo, Pancreatic cancer, Cell Line, Tumor, Drug Discovery, medicine, Animals, Humans, Survival rate, 030304 developmental biology, Cell Proliferation, 0303 health sciences, Sulfonamides, Hydroxamic acid, Chemistry, HDAC11, HDAC6, medicine.disease, Coculture Techniques, 3. Good health, 0104 chemical sciences, Histone Deacetylase Inhibitors, Pancreatic Neoplasms, 010404 medicinal & biomolecular chemistry, Disease Models, Animal, Benzamides, Cancer research, Molecular Medicine, Histone deacetylase

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is an aggressive, incurable cancer with a 20% 1 year survival rate. While standard-of-care therapy can prolong life in a small fraction of cases, PDAC is inherently resistant to current treatments, and novel therapies are urgently required. Histone deacetylase (HDAC) inhibitors are effective in killing pancreatic cancer cells in in vitro PDAC studies, and although there are a few clinical studies investigating combination therapy including HDAC inhibitors, no HDAC drug or combination therapy with an HDAC drug has been approved for the treatment of PDAC. We developed an inhibitor of HDACs, AES-135, that exhibits nanomolar inhibitory activity against HDAC3, HDAC6, and HDAC11 in biochemical assays. In a three-dimensional coculture model, AES-135 kills low-passage patient-derived tumor spheroids selectively over surrounding cancer-associated fibroblasts and has excellent pharmacokinetic properties in vivo. In an orthotopic murine model of pancreatic cancer, AES-135 prolongs survival significantly, therefore representing a candidate for further preclinical testing.

Published

2019

14. ProxyPhos sensors for the detection of negatively charged membranes

Author

Angelika Berger-Becvar, Elvin D. de Araujo, Angel Lai, Bronte I. Murcar-Evans, Krimo Toutah, Dziyana Kraskouskaya, Patrick T. Gunning, Aaron D. Cabral, and Peter M. Macdonald

Subjects

0301 basic medicine, Cardiolipins, Phosphatidic Acids, Apoptosis, Phosphatidylserines, 010402 general chemistry, 01 natural sciences, Biochemistry, Analytical Chemistry, Flow cytometry, 03 medical and health sciences, chemistry.chemical_compound, Cell Line, Tumor, Electrochemistry, Cardiolipin, medicine, Environmental Chemistry, Humans, Spectroscopy, Phospholipids, Phospholipidosis, Phosphatidylglycerol, Membranes, medicine.diagnostic_test, Vesicle, Phosphatidylglycerols, Phosphatidic acid, Phosphatidylserine, 0104 chemical sciences, 030104 developmental biology, Membrane, chemistry

Abstract

Membrane-embedded negatively charged phospholipids (MENCP) can be used as biomarkers for a range of biological processes, including early detection of apoptosis in animal cells, drug-induced phospholipidosis, and selective detection of bacterial over animal cells. Currently, several technologies for the detection of apoptosis and bacterial cells are based on the recognition of MENCPs, including the AnnexinV stain and PSVue™ probes. As probes, these technologies have limitations, the most significant of which is the need for washing the unbound probe away to achieve optimal signal. In contrast, a turn-on chemosensor selective for MENCP would address this shortcoming, and allow for a more rapid protocol for the detection of apoptosis, bacteria and for other relevant applications. In this work, the aim was to explore whether ProxyPhos chemosensors, previously reported by our group for the detection of proximally phosphorylated peptides and proteins, could be re-purposed for the detection of MENCPs. Six lead ProxyPhos sensors were screened against synthetic vesicles containing biologically relevant negatively charged phospholipids including phosphatidic acid (PA), phosphatidylglycerol (PG), cardiolipin (CL) and phosphatidylserine (PS). Through these screens, ProxyPhos sensors exhibiting high selectivity for the detection of MENCPs over zwitterionic lipids were identified. Particular selectivity was observed for PA and CL. Sensitivity of the lead sensors for MENCPs was suitable for the detection of apoptosis: ProxyPhos detected vesicles containing as little as 2.5% PS and detected camptothecin-induced apoptosis in mammalian cells in flow cytometry experiments. The results suggest that ProxyPhos sensors can be used for the detection of MENCPs in synthetic vesicles and live mammalian cells.

Published

2017

15. Regulating the Master Regulator: Controlling Ubiquitination by Thinking Outside the Active Site

Author

Stacey-Lynn, Paiva, Sara R, da Silva, Elvin D, de Araujo, and Patrick T, Gunning

Subjects

Allosteric Regulation, Deubiquitinating Enzymes, Ubiquitin, Catalytic Domain, Ubiquitin-Protein Ligases, Ubiquitin-Conjugating Enzymes, Ubiquitination, Humans, Ubiquitin-Activating Enzymes, Enzyme Inhibitors, Protein Processing, Post-Translational, Thalidomide

Abstract

The labeling of proteins with ubiquitin/ubiquitin-like (Ubl) proteins is crucial for several physiological processes and in the onset of various diseases. Recently, targeting ubiquitin protein labeling has shifted toward the use of allosteric mechanisms over classical activity-based approaches. Allosteric enzyme regulation offers the potential for greater selectivity and has demonstrated less susceptibility to acquired resistance often associated with active site inhibitors. Furthermore, the isoform diversity among E1 activating, E2 conjugating, E3 ligase, and deubiquitinating (DUB) enzymes offers an ideal platform for modulating activity via allostery. Herein, we have reviewed allosteric inhibitors of the ubiquitin E1-E2-E3 and DUB enzymatic cascade developed over the past decade with a focus on their mechanisms of action. We have highlighted the advantages as well as the challenges associated with designing allosteric modulators of the ubiquitin labeling machinery, and the future promise in targeting these systems using allosteric approaches.

Published

2017

16. Disarming an electrophilic warhead: Retaining potency in Tyrosine Kinase Inhibitor (TKI)-resistant CML lines, while circumventing pharmacokinetic liabilities

Author

Patrick T. Gunning, Ami B. Patel, Andrew E. Shouksmith, Nadeem A. Vellore, David A. Rosa, Ping-Shan Lai, Rodolfo F. Gómez-Biagi, Thomas O'Hare, Michael W. Deininger, Ji Sung Park, William L. Heaton, Anna M. Eiring, Daniel P. Ball, Ahmed Ali, and Elvin D. de Araujo

Subjects

0301 basic medicine, STAT3 Transcription Factor, medicine.drug_class, Biological Availability, Antineoplastic Agents, Pharmacology, Biochemistry, Tyrosine-kinase inhibitor, Article, 03 medical and health sciences, chemistry.chemical_compound, Mice, Structure-Activity Relationship, 0302 clinical medicine, In vivo, Cell Line, Tumor, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, Drug Discovery, medicine, para-Aminobenzoates, Structure–activity relationship, Animals, Humans, STAT1, General Pharmacology, Toxicology and Pharmaceutics, STAT3, Protein Kinase Inhibitors, Cell Proliferation, Sulfonamides, Hydroxamic acid, biology, Dose-Response Relationship, Drug, Molecular Structure, Cell growth, Organic Chemistry, Myeloid leukemia, Neoplasms, Experimental, 3. Good health, 030104 developmental biology, chemistry, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, biology.protein, Molecular Medicine, Drug Screening Assays, Antitumor

Abstract

Pharmacologic blockade of the activation of signal transducer and activator of transcription 3 (STAT3) in tyrosine kinase inhibitor (TKI)-resistant chronic myeloid leukemia (CML) cell lines characterized by kinase-independent resistance was shown to re-sensitize CML cells to TKI therapy, suggesting that STAT3 inhibitors in combination with TKIs are an effective combinatorial therapeutic for the treatment of CML. Benzoic acid- and hydroxamic acid-based STAT3 inhibitors SH-4-054 and SH-5-007, developed previously in our laboratory, demonstrated promising activity against these resistant CML cell lines. However, pharmacokinetic studies in murine models (CD-1 mice) revealed that both SH-4-054 and SH-5-007 are susceptible to glutathione conjugation at the para position of the pentafluorophenyl group via nucleophilic aromatic substitution (SN Ar). To determine whether the electrophilicity of the pentafluorophenyl sulfonamide could be tempered, an in-depth structure-activity relationship (SAR) study of the SH-4-054 scaffold was conducted. These studies revealed that AM-1-124, possessing a 2,3,5,6-tetrafluorophenylsulfonamide group, retained STAT3 protein affinity (Ki =15 μm), as well as selectivity over STAT1 (Ki >250 μm). Moreover, in both hepatocytes and in in vivo pharmacokinetic studies (CD-1 mice), AM-1-124 was found to be dramatically more stable than SH-4-054 (t1/2 =1.42 h cf. 10 min, respectively). AM-1-124 is a promising STAT3-targeting inhibitor with demonstrated bioavailability, suitable for evaluation in preclinical cancer models.

Published

2016

17. Successful development and use of a thermodynamic stability screen for optimizing the yield of nucleotide binding domains

Author

Elvin D. de Araujo and Voula Kanelis

Subjects

chemistry.chemical_classification, Binding Sites, Inward-rectifier potassium ion channel, Protein subunit, Hydrolysis, GTPase, Ligand (biochemistry), Sulfonylurea Receptors, Protein Structure, Tertiary, DNA-Binding Proteins, Adenosine Triphosphate, chemistry, Biochemistry, KATP Channels, Osmolyte, Mutation, Sulfonylurea receptor, Humans, Thermodynamics, Nucleotide, Chemical stability, Nuclear Magnetic Resonance, Biomolecular, Biotechnology

Abstract

ATP sensitive potassium (KATP) channels consist of four copies of a pore-forming inward rectifying potassium channel (Kir6.1 or Kir6.2) and four copies of a sulfonylurea receptor (SUR1, SUR2A, or SUR2B). SUR proteins are members of the ATP-binding cassette superfamily of proteins. Binding of ATP to the Kir6.x subunit mediates channel inhibition, whereas MgATP binding and hydrolysis at the SUR NBDs results in channel opening. Mutations in SUR1 and SUR2A NBDs cause diseases of insulin secretion and cardiac disorders, respectively, underlying the importance of studying the NBDs. Although purification of SUR2A NBD1 in a soluble form is possible, the lack of long-term sample stability of the protein in a concentrated form has precluded detailed studies of the protein aimed at gaining a molecular-level understanding of how SUR mutations cause disease. Here we use a convenient and cost-effective thermodynamic screening method to probe stabilizing conditions for SUR2A NBD1. Results from the screen are used to alter the purification protocol to allow for significantly increased yields of the purified protein. In addition, the screen provides strategies for long-term storage of NBD1 and generating NBD1 samples at high concentrations suitable for NMR studies. NMR spectra of NBD1 with MgAMP-PNP are of higher quality compared to using MgATP, indicating that MgAMP-PNP be used as the ligand in future NMR studies. The screen presented here can be expanded to using different additives and can be employed to enhance purification yields, sample life times, and storage of other low stability nucleotide binding domains, such as GTPases.

Published

2014