Your search keyword '"Reddy, E. Premkumar"' showing total 22 results

1. Novel induction of CD40 expression by tumor cells with RAS/RAF/PI3K pathway inhibition augments response to checkpoint blockade.

Author

Yan C, Saleh N, Yang J, Nebhan CA, Vilgelm AE, Reddy EP, Roland JT, Johnson DB, Chen SC, Shattuck-Brandt RL, Ayers GD, and Richmond A

Subjects

Animals, Female, Glycine pharmacology, Humans, Male, Melanoma metabolism, Mice, Phosphatidylinositol 3-Kinases drug effects, Protein Kinase Inhibitors pharmacology, Signal Transduction drug effects, Signal Transduction physiology, Xenograft Model Antitumor Assays, raf Kinases antagonists & inhibitors, Antineoplastic Agents pharmacology, CD40 Antigens biosynthesis, Glycine analogs & derivatives, Immune Checkpoint Inhibitors pharmacology, Melanoma pathology, Sulfones pharmacology, ras Proteins antagonists & inhibitors

Abstract

Background: While immune checkpoint blockade (ICB) is the current first-line treatment for metastatic melanoma, it is effective for ~ 52% of patients and has dangerous side effects. The objective here was to identify the feasibility and mechanism of RAS/RAF/PI3K pathway inhibition in melanoma to sensitize tumors to ICB therapy., Methods: Rigosertib (RGS) is a non-ATP-competitive small molecule RAS mimetic. RGS monotherapy or in combination therapy with ICB were investigated using immunocompetent mouse models of BRAF wt and BRAF mut melanoma and analyzed in reference to patient data., Results: RGS treatment (300 mg/kg) was well tolerated in mice and resulted in ~ 50% inhibition of tumor growth as monotherapy and ~ 70% inhibition in combination with αPD1 + αCTLA4. RGS-induced tumor growth inhibition depends on CD40 upregulation in melanoma cells followed by immunogenic cell death, leading to enriched dendritic cells and activated T cells in the tumor microenvironment. The RGS-initiated tumor suppression was partially reversed by either knockdown of CD40 expression in melanoma cells or depletion of CD8 + cytotoxic T cells. Treatment with either dabrafenib and trametinib or with RGS, increased CD40 + SOX10 + melanoma cells in the tumors of melanoma patients and patient-derived xenografts. High CD40 expression level correlates with beneficial T-cell responses and better survival in a TCGA dataset from melanoma patients. Expression of CD40 by melanoma cells is associated with therapeutic response to RAF/MEK inhibition and ICB., Conclusions: Our data support the therapeutic use of RGS + αPD1 + αCTLA4 in RAS/RAF/PI3K pathway-activated melanomas and point to the need for clinical trials of RGS + ICB for melanoma patients who do not respond to ICB alone., Trial Registration: NCT01205815 (Sept 17, 2010).

Published

2021

2. A Contaminant Impurity, Not Rigosertib, Is a Tubulin Binding Agent.

Author

Baker SJ, Cosenza SC, Athuluri-Divakar S, Reddy MVR, Vasquez-Del Carpio R, Jain R, Aggarwal AK, and Reddy EP

Subjects

Drug Contamination, Drug Resistance, Neoplasm, Glycine pharmacology, Humans, Lung Neoplasms drug therapy, Lung Neoplasms metabolism, Mutation, Tubulin chemistry, Tubulin genetics, Tumor Cells, Cultured, Antineoplastic Agents pharmacology, Cell Proliferation, Glycine analogs & derivatives, Lung Neoplasms pathology, Sulfones pharmacology, Tubulin metabolism

Abstract

Rigosertib is a styryl benzyl sulfone that inhibits growth of tumor cells and acts as a RAS mimetic by binding to Ras binding domains of RAS effectors. A recent study attributed rigosertib's mechanism of action to microtubule binding. In that study, rigosertib was obtained from a commercial vendor. We compared the purity of clinical-grade and commercially sourced rigosertib and found that commercially sourced rigosertib contains approximately 5% ON01500, a potent inhibitor of tubulin polymerization. Clinical-grade rigosertib, which is free of this impurity, does not exhibit tubulin-binding activity. Cell lines expressing mutant β-tubulin have also been reported to be resistant to rigosertib. However, our study showed that these cells failed to proliferate in the presence of rigosertib at concentrations that are lethal to wild-type cells. Rigosertib induced a senescence-like phenotype in the small percentage of surviving cells, which could be incorrectly scored as resistant using short-term cultures., Competing Interests: Declaration of Interests E.P.R. is an equity holder, board member, and paid consultant of Onconova Therapeutics. S.J.B. is a paid consultant of Onconova Therapeutics. M.V.R.R. and S.C.C. are stockholders and paid consultants of Onconova Therapeutics, Inc. M.V.R.R. and E.P.R. are named inventors on pending and/or issued patents filed by Temple University., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

3. Drugging the 'undruggable' cancer targets.

Author

Dang CV, Reddy EP, Shokat KM, and Soucek L

Subjects

Drug Discovery, Humans, NF-kappa B, Oncogene Proteins, Fusion, Proto-Oncogene Proteins c-myb, Proto-Oncogene Proteins c-myc, Receptors, Androgen, ras Proteins, Antineoplastic Agents pharmacology, Antineoplastic Agents therapeutic use, Molecular Targeted Therapy, Neoplasms drug therapy

Abstract

The term 'undruggable' was coined to describe proteins that could not be targeted pharmacologically. However, progress is being made to 'drug' many of these targets, and therefore more appropriate terms might be 'difficult to drug' or 'yet to be drugged'. Many desirable targets in cancer fall into this category, including the RAS and MYC oncogenes, and pharmacologically targeting these intractable proteins is now a key challenge in cancer research that requires innovation and the development of new technologies. In this Viewpoint article, we asked four scientists working in this field for their opinions on the most crucial advances, as well as the challenges and what the future holds for this important area of research.

Published

2017

4. Dual Targeting of CDK4 and ARK5 Using a Novel Kinase Inhibitor ON123300 Exerts Potent Anticancer Activity against Multiple Myeloma.

Author

Perumal D, Kuo PY, Leshchenko VV, Jiang Z, Divakar SK, Cho HJ, Chari A, Brody J, Reddy MV, Zhang W, Reddy EP, Jagannath S, and Parekh S

Subjects

Animals, Apoptosis drug effects, Cell Line, Tumor, Cell Proliferation drug effects, Cyclin-Dependent Kinase 4 physiology, Gene Expression Profiling, Humans, Mice, Multiple Myeloma pathology, Protein Kinases physiology, Repressor Proteins physiology, Sirtuin 1 physiology, Xenograft Model Antitumor Assays, Antineoplastic Agents pharmacology, Cyclin-Dependent Kinase 4 antagonists & inhibitors, Multiple Myeloma drug therapy, Protein Kinase Inhibitors pharmacology, Pyridones pharmacology, Pyrimidines pharmacology, Repressor Proteins antagonists & inhibitors

Abstract

Multiple myeloma is a fatal plasma cell neoplasm accounting for over 10,000 deaths in the United States each year. Despite new therapies, multiple myeloma remains incurable, and patients ultimately develop drug resistance and succumb to the disease. The response to selective CDK4/6 inhibitors has been modest in multiple myeloma, potentially because of incomplete targeting of other critical myeloma oncogenic kinases. As a substantial number of multiple myeloma cell lines and primary samples were found to express AMPK-related protein kinase 5(ARK5), a member of the AMPK family associated with tumor growth and invasion, we examined whether dual inhibition of CDK4 and ARK5 kinases using ON123300 results in a better therapeutic outcome. Treatment of multiple myeloma cell lines and primary samples with ON123300 in vitro resulted in rapid induction of cell-cycle arrest followed by apoptosis. ON123300-mediated ARK5 inhibition or ARK5-specific siRNAs resulted in the inhibition of the mTOR/S6K pathway and upregulation of the AMPK kinase cascade. AMPK upregulation resulted in increased SIRT1 levels and destabilization of steady-state MYC protein. Furthermore, ON123300 was very effective in inhibiting tumor growth in mouse xenograft assays. In addition, multiple myeloma cells sensitive to ON123300 were found to have a unique genomic signature that can guide the clinical development of ON123300. Our study provides preclinical evidence that ON123300 is unique in simultaneously inhibiting key oncogenic pathways in multiple myeloma and supports further development of ARK5 inhibition as a therapeutic approach in multiple myeloma., (©2016 American Association for Cancer Research.)

Published

2016

5. Preclinical pharmacological evaluation of a novel multiple kinase inhibitor, ON123300, in brain tumor models.

Author

Zhang X, Lv H, Zhou Q, Elkholi R, Chipuk JE, Reddy MV, Reddy EP, and Gallo JM

Subjects

Animals, Antineoplastic Agents administration & dosage, Antineoplastic Agents pharmacokinetics, Brain Neoplasms drug therapy, Brain Neoplasms pathology, Cell Line, Tumor, Disease Models, Animal, Drug Evaluation, Preclinical, Humans, Mice, Phosphatidylinositol 3-Kinases metabolism, Phosphorylation, Protein Kinase Inhibitors administration & dosage, Protein Kinase Inhibitors pharmacokinetics, Proto-Oncogene Proteins c-akt metabolism, Pyridones administration & dosage, Pyridones pharmacokinetics, Pyrimidines administration & dosage, Pyrimidines pharmacokinetics, Signal Transduction drug effects, Xenograft Model Antitumor Assays, Antineoplastic Agents pharmacology, Brain Neoplasms metabolism, Protein Kinase Inhibitors pharmacology, Pyridones pharmacology, Pyrimidines pharmacology

Abstract

ON123300 is a low molecular weight multikinase inhibitor identified through a series of screens that supported further analyses for brain tumor chemotherapy. Biochemical assays indicated that ON123300 was a strong inhibitor of Ark5 and CDK4, as well as growth factor receptor tyrosine kinases such as β-type platelet-derived growth factor receptor (PDGFRβ). ON123300 inhibited U87 glioma cell proliferation with an IC(50) 3.4 ± 0.1 μmol/L and reduced phosphorylation of Akt, yet it also unexpectedly induced Erk activation, both in a dose- and time-dependent manner that subsequently was attributed to relieving Akt-mediated C-Raf S259 inactivation and activating a p70S6K-initiated PI3K-negative feedback loop. Cotreatment with the EGFR inhibitor gefitinib produced synergistic cytotoxic effects. Pursuant to the in vitro studies, in vivo pharmacokinetic and pharmacodynamic studies of ON123300 were completed in mice bearing intracerebral U87 tumors following intravenous doses of 5 and 25 mg/kg alone, and also at the higher dose concurrently with gefitinib. ON123300 showed high brain and brain tumor accumulation based on brain partition coefficient values of at least 2.5. Consistent with the in vitro studies, single agent ON123300 caused a dose-dependent suppression of phosphorylation of Akt as well as activation of Erk in brain tumors, whereas addition of gefitinib to the ON123300 regimen significantly enhanced p-Akt inhibition and prevented Erk activation. In summary, ON123300 demonstrated favorable pharmacokinetic characteristics, and future development for brain tumor therapy would require use of combinations, such as gefitinib, that mitigate its Erk activation and enhance its activity.

Published

2014

6. Discovery of 8-cyclopentyl-2-[4-(4-methyl-piperazin-1-yl)-phenylamino]-7-oxo-7,8-dihydro-pyrido[2,3-d]pyrimidine-6-carbonitrile (7x) as a potent inhibitor of cyclin-dependent kinase 4 (CDK4) and AMPK-related kinase 5 (ARK5).

Author

Reddy MV, Akula B, Cosenza SC, Athuluridivakar S, Mallireddigari MR, Pallela VR, Billa VK, Subbaiah DR, Bharathi EV, Vasquez-Del Carpio R, Padgaonkar A, Baker SJ, and Reddy EP

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Apoptosis drug effects, Cell Cycle drug effects, Cell Line, Tumor, Drug Screening Assays, Antitumor, Female, Heterografts, Humans, Mice, Mice, Nude, Molecular Docking Simulation, Neoplasm Transplantation, Protein Kinases, Pyridines chemistry, Pyridines pharmacology, Pyrimidines chemistry, Pyrimidines pharmacology, Structure-Activity Relationship, Antineoplastic Agents chemical synthesis, Cyclin-Dependent Kinase 4 antagonists & inhibitors, Pyridines chemical synthesis, Pyrimidines chemical synthesis, Repressor Proteins antagonists & inhibitors

Abstract

The success of imatinib, a BCR-ABL inhibitor for the treatment of chronic myelogenous leukemia, has created a great impetus for the development of additional kinase inhibitors as therapeutic agents. However, the complexity of cancer has led to recent interest in polypharmacological approaches for developing multikinase inhibitors with low toxicity profiles. With this goal in mind, we analyzed more than 150 novel cyano pyridopyrimidine compounds and identified structure-activity relationship trends that can be exploited in the design of potent kinase inhibitors. One compound, 8-cyclopentyl-2-[4-(4-methyl-piperazin-1-yl)-phenylamino]-7-oxo-7,8-dihydro-pyrido[2,3-d]pyrimidine-6-carbonitrile (7x), was found to be the most active, inducing apoptosis of tumor cells at a concentration of approximately 30-100 nM. In vitro kinase profiling revealed that 7x is a multikinase inhibitor with potent inhibitory activity against the CDK4/CYCLIN D1 and ARK5 kinases. Here, we report the synthesis, structure-activity relationship, kinase inhibitory profile, in vitro cytotoxicity, and in vivo tumor regression studies by this lead compound.

Published

2014

7. Design, synthesis, and biological evaluation of (E)-N-aryl-2-arylethenesulfonamide analogues as potent and orally bioavailable microtubule-targeted anticancer agents.

Author

Reddy MV, Mallireddigari MR, Pallela VR, Cosenza SC, Billa VK, Akula B, Subbaiah DR, Bharathi EV, Padgaonkar A, Lv H, Gallo JM, and Reddy EP

Subjects

Administration, Oral, Animals, Antineoplastic Agents chemical synthesis, Antineoplastic Agents pharmacokinetics, Biological Availability, Blood-Brain Barrier metabolism, Cell Cycle Checkpoints drug effects, Cell Line, Tumor, Cell Survival drug effects, Drug Resistance, Neoplasm drug effects, HCT116 Cells, Humans, K562 Cells, MCF-7 Cells, Mice, Mice, Nude, Microtubules metabolism, Neoplasms metabolism, Neoplasms pathology, Polymerization drug effects, Sulfonamides chemical synthesis, Sulfonamides pharmacokinetics, Tubulin metabolism, Tumor Burden drug effects, Antineoplastic Agents pharmacology, Drug Design, Microtubules drug effects, Neoplasms drug therapy, Sulfonamides pharmacology, Xenograft Model Antitumor Assays

Abstract

A series of novel (E)-N-aryl-2-arylethenesulfonamides (6) were synthesized and evaluated for their anticancer activity. Some of the compounds in this series showed potent cytotoxicity against a wide spectrum of cancer cell-lines (IC50 values ranging from 5 to 10 nM) including all drug resistant cell-lines. Nude mice xenograft assays with compound (E)-N-(3-amino-4-methoxyphenyl)-2-(2',4',6'-trimethoxyphenyl)ethenesulfonamide (6t) showed dramatic reduction in tumor size, indicating their in vivo potential as anticancer agents. A preliminary drug development study with compound 6t is predicted to have increased blood-brain barrier permeability relative to many clinically used antimitotic agents. Mechanistic studies indicate that 6t and some other analogues disrupted microtubule formation, formation of mitotic spindles, and arrest of cells in mitotic phase. Compound 6t inhibited purified tubulin polymerization in vitro and in vivo and circumvented drug resistance mediated by P-glycoprotein. Compound 6t specifically competed with colchicine binding to tubulin and with similar avidity as podophylltoxin, indicating its binding site on tubulin.

Published

2013

8. Hydrothiolation of benzyl mercaptan to arylacetylene: application to the synthesis of (E) and (Z)-isomers of ON 01910·Na (Rigosertib®), a phase III clinical stage anti-cancer agent.

Author

Pallela VR, Mallireddigari MR, Cosenza SC, Akula B, Subbaiah DR, Reddy EP, and Reddy MV

Subjects

Alkynes chemical synthesis, Alkynes chemistry, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Cell Line, Tumor, Cell Survival drug effects, Clinical Trials, Phase III as Topic, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Glycine chemical synthesis, Glycine chemistry, Glycine pharmacology, Humans, K562 Cells, Molecular Structure, Stereoisomerism, Structure-Activity Relationship, Sulfones chemical synthesis, Sulfones chemistry, Alkynes pharmacology, Antineoplastic Agents pharmacology, Glycine analogs & derivatives, Sulfhydryl Compounds chemistry, Sulfones pharmacology

Abstract

A stereoselective and efficient method for free radical addition of benzyl thiol to aryl acetylene in the presence of Et3B-hexane has been developed for the synthesis of (Z) and (E)-styryl benzyl sulfides where base catalyzed hydrothiolations have failed. The scope of this reaction was successfully extended for the synthesis of (E)-ON 01910·Na, a phase III clinical stage anti-cancer agent and its inactive geometrical isomer (Z)-ON 01910·Na. It is interesting to note that all the E-isomers synthesized have shown better cytotoxicity profile on cancer cells compared to the Z-isomers.

Published

2013

9. Determination of the glucuronide metabolite of ON 013100, a benzylstyrylsulfone antineoplastic drug, in colon cancer cells using LC/MS/MS.

Author

Cho SY, Cosenza SC, Pallela V, Panda G, Reddy MV, Reddy EP, and Roboz J

Subjects

Antineoplastic Agents analysis, Antineoplastic Agents pharmacology, Benzyl Compounds analysis, Benzyl Compounds pharmacology, Cell Line, Tumor, Chromatography, High Pressure Liquid, Colonic Neoplasms drug therapy, Drug Resistance, Neoplasm, Glucuronides chemistry, Glucuronides metabolism, Humans, Kinetics, Limit of Detection, Metabolic Detoxication, Phase I, Molecular Weight, Protein Kinase Inhibitors analysis, Protein Kinase Inhibitors pharmacology, Spectrometry, Mass, Electrospray Ionization, Stereoisomerism, Styrenes analysis, Styrenes pharmacology, Sulfones, Tandem Mass Spectrometry, Antineoplastic Agents metabolism, Benzyl Compounds metabolism, Colonic Neoplasms metabolism, Glucuronides analysis, Protein Kinase Inhibitors metabolism, Styrenes metabolism

Abstract

ON 013100, (E)-2,4,6-trimethoxystyryl-3-hydroxy-4-methoxybenzyl sulfone, is a potent kinase inhibitor whose phosphate form is in Phase I clinical trials in lymphoma and acute lymphoid leukemia. The objectives were to: (a) investigate the possible presence of the glucuronide metabolite of the drug in two representative colon cancer cell lines, a drug resistant (colo-205) and a drug sensitive (colo-320); (b) quantify the glucuronide metabolite and the unchanged drug in the cells after treatment with ON 013100. The glucuronide was synthesized and a selective LC/MS/MS method was developed and validated for the characterization and quantification of the metabolite. The glucuronide metabolite (570.6 Da) was found in the drug-resistant cells upon a 1h incubation with ON 013100 (20 μg/ml). After treatment with the drug, the concentration of the metabolite gradually decreased from 0.84 μg/ml at 0 h through 0.21 μg/ml at 6h to below detection limit of 8.0 ng/ml at 9 h. No glucuronide metabolite was detected in the drug-sensitive cells. The concentrations of intact ON 013100 in the drug-resistant cells gradually decreased from 0.41 μg/ml (0 h) to 0.06 μg/ml (9 h). The corresponding concentrations of the intact drug in the drug-sensitive cells were from 2.88 μg/ml to 0.94 μg/ml., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2013

10. Integrated pharmacokinetic-driven approach to screen candidate anticancer drugs for brain tumor chemotherapy.

Author

Lv H, Zhang X, Sharma J, Reddy MV, Reddy EP, and Gallo JM

Subjects

Animals, Antineoplastic Agents therapeutic use, Blood-Brain Barrier, Brain metabolism, Humans, Male, Mice, Mice, Inbred ICR, Protein Binding, Antineoplastic Agents pharmacokinetics, Brain Neoplasms drug therapy, Drug Discovery

Abstract

The goal of the study was to develop an effective screening strategy to select new agents for brain tumor chemotherapy from a series of low molecular weight anticancer agents [ON123x] by the combined use of in silico, in vitro cytotoxicity, and in vitro ADME profiling studies. The results of these studies were cast into a pipeline of tier 1 and tier 2 procedures that resulted in the identification of ON123300 as the lead compound. Of the 154 ON123xx compounds, 13 met tier 1 screening criteria based on physicochemical properties [i.e., MW < 450 Da, predicted log P between 2 and 3.5] and in vitro glioma cell cytotoxicity [i.e., IC50 < 10 μM] and were further tested in tier 2 assays. The tier 2 profiling studies consisted of metabolic stability, MDCK-MDR1 cell permeability and plasma and brain protein binding that were combined to globally assess whether favorable pharmacokinetic properties and brain penetration could be achieved in vivo. In vivo cassette dosing studies were conducted in mice for 12 compounds that permitted examination of in vitro/in vivo relationships that confirmed the suitability of the in vitro assays. A parameter derived from the in vitro assays accurately predicted the extent of drug accumulation in the brain based on the area under the drug concentration-time curve in brain measured in the cassette dosing study (r (2) = 0.920). Overall, the current studies demonstrated the value of an integrated pharmacokinetic-driven approach to identify potentially efficacious agents for brain tumor chemotherapy.

Published

2013

11. Screening candidate anticancer drugs for brain tumor chemotherapy: pharmacokinetic-driven approach for a series of (E)-N-(substituted aryl)-3-(substituted phenyl)propenamide analogues.

Author

Lv H, Wang F, Reddy MV, Zhou Q, Zhang X, Reddy EP, and Gallo JM

Subjects

Amides pharmacology, Animals, Antineoplastic Agents pharmacology, Blood Proteins metabolism, Brain Neoplasms drug therapy, Cell Line, Cell Survival drug effects, Computer Simulation, Dogs, Drug Screening Assays, Antitumor, Male, Mice, Mice, Inbred ICR, Mice, Nude, Models, Biological, Amides pharmacokinetics, Antineoplastic Agents pharmacokinetics, Brain Neoplasms metabolism

Abstract

A pharmacokinetic [PK]-driven screening process was implemented to select new agents for brain tumor chemotherapy from a series of low molecular weight anticancer agents [ON27x] that consisted of 141 compounds. The screening procedures involved a combination of in silico, in vitro and in vivo mouse studies that were cast into a pipeline of tier 1 and tier 2 failures that resulted in a final investigation of 2 analogues in brain tumor-bearing mice. Tier 1 failures included agents with a molecular weight of > 450 Da, a predicted log P (log P) of either <2 or > 3.5, and a cytotoxicity IC(50) value of > 2 uM. Next, 18 compounds underwent cassette dosing studies in normal mice that identified compounds with high systemic clearance, and low blood-brain barrier [BBB] penetration. These indices along with a derived parameter, referred to as the brain exposure index, comprised tier 2 failures that led to the administration of 2 compounds [ON27570, ON27740] as single agents [discrete dosing] to mice bearing intracerebral tumors. Comparison of ON27570's resultant PK parameters to those obtained in the cassette dosing format suggested a drug-drug interaction most likely at the level of BBB transport, and prompted the use of the in vitro MDCK-MDR1 transport model to help assess the nature of the discrepancy. Overall, the approach was able to identify candidate compounds with suitable PK characteristics yet further revisions to the method, such as the use of in vitro metabolism and transport assays, may improve the PK-directed approach to identify efficacious agents for brain tumor chemotherapy.

Published

2012

12. Preclinical pharmacokinetic and pharmacodynamic evaluation of novel anticancer agents, ON01910.Na (Rigosertib, Estybon™) and ON013105, for brain tumor chemotherapy.

Author

Nuthalapati S, Zhou Q, Guo P, Lv H, Cosenza S, Reddy MV, Reddy EP, and Gallo JM

Subjects

Animals, Antineoplastic Agents pharmacokinetics, Antineoplastic Agents pharmacology, Chromatography, Liquid, Drug Evaluation, Preclinical, Mice, Tandem Mass Spectrometry, Antineoplastic Agents therapeutic use, Brain Neoplasms drug therapy

Abstract

Purpose: To evaluate a mitotic inhibitor, ON01910.Na, as a potential chemotherapeutic agent for brain tumors using a series of PK/PD studies, which led to the evaluation of its structural analog, ON013105, a prodrug of the more lipophilic product, ON013100., Methods: Systemic PK characterization of ON01910 and ON013105 was completed in healthy mice. Using an orthotopic U87 glioma mouse model, brain and brain tumor distribution under steady-state conditions were evaluated for ON01910.Na and ON013105/ON013100; anticancer potential following a multiple-dose schedule of 250 mg/kg/day IP for 7 days was evaluated for ON01910.Na., Results: ON01910 exhibited low brain and brain tumor distribution with quasi-steady-state brain/plasma (Css(brain)/Css(plasma)) and brain tumor/plasma (Css(brain tumor)/Css(plasma)) concentration ratios of 0.03 ± 0.02 and 0.14 ± 0.08, respectively. Significant antiangiogenic potential and antiproliferative capacity of ON01910 in the intracerebral model was absent. ON013100 showed high brain and brain tumor penetration with Css(brain)/Css(plasma) and Css(brain tumor)/Css(plasma) ratios of 0.92 ± 0.26 and 1.35 ± 0.40, respectively; its prodrug ON013105 showed negligible brain and brain tumor penetration., Conclusions: ON013105, not ON01910.Na, was identified as a potential anticancer drug candidate for further investigation in brain tumor chemotherapy based on the properties of ON013100.

Published

2012

13. (Z)-1-aryl-3-arylamino-2-propen-1-ones, highly active stimulators of tubulin polymerization: synthesis, structure-activity relationship (SAR), tubulin polymerization, and cell growth inhibition studies.

Author

Reddy MV, Akula B, Cosenza SC, Lee CM, Mallireddigari MR, Pallela VR, Subbaiah DR, Udofa A, and Reddy EP

Subjects

Alkenes chemistry, Alkenes pharmacology, Aminophenols chemistry, Aminophenols pharmacology, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Apoptosis drug effects, Cell Division drug effects, Cell Line, Tumor, Cell Proliferation drug effects, Drug Resistance, Multiple, Drug Resistance, Neoplasm, Drug Screening Assays, Antitumor, G2 Phase drug effects, Humans, Microtubules drug effects, Microtubules ultrastructure, Polymerization, Spindle Apparatus drug effects, Spindle Apparatus ultrastructure, Stereoisomerism, Structure-Activity Relationship, Tubulin Modulators chemistry, Tubulin Modulators pharmacology, Alkenes chemical synthesis, Aminophenols chemical synthesis, Antineoplastic Agents chemical synthesis, Tubulin metabolism, Tubulin Modulators chemical synthesis

Abstract

Tubulin, the major structural component of microtubules, is a target for the development of anticancer agents. A series of (Z)-1-aryl-3-arylamino-2-propen-1-one (10) were synthesized and evaluated for antiproliferative activity in cell-based assay. The most active compound (Z)-1-(2-bromo-3,4,5-trimethoxyphenyl)-3-(3-hydroxy-4-methoxyphenylamino)prop-2-en-1-one (10ae) was tested in 20 tumor cell lines including multidrug resistant phenotype and was found to induce apoptosis in all these cell lines with similar GI(50) values. Flow cytometry studies showed that 10ae arrested the cells in G2/M phase of cell cycle. In addition to G2/M block, these compounds caused microtubule stabilization like paclitaxel and induced apoptosis via activation of the caspase family. The observations made in this investigation demonstrate that (Z)-1-Aryl-3-arylamino-2-propen-1-one (10) represents a new class of microtubule-stabilizing agents.

Published

2012

14. Application of a liquid chromatography-tandem mass spectrometry (LC/MS/MS) method to the pharmacokinetics of ON01910 in brain tumor-bearing mice.

Author

Nuthalapati S, Guo P, Zhou Q, Reddy MV, Reddy EP, and Gallo JM

Subjects

Animals, Brain Neoplasms metabolism, Calibration, Glycine pharmacokinetics, Limit of Detection, Mice, Reproducibility of Results, Antineoplastic Agents pharmacokinetics, Brain Neoplasms drug therapy, Chromatography, Liquid methods, Glycine analogs & derivatives, Sulfones pharmacokinetics, Tandem Mass Spectrometry methods

Abstract

ON01910 is a small molecular weight benzyl styryl sulfone currently under investigation as a novel anticancer agent. The purpose of the investigation was to develop a sensitive and reproducible liquid chromatography-tandem mass spectrometry (LC/MS/MS) method to quantitate levels of ON01910 in small amounts of five biological matrices; mouse plasma, feces, urine, normal brain and brain tumor. For all matrices, protein precipitation sample preparation was used that led to linear calibration curves with coefficients of determination greater than 0.99. The lower limit of quantitation (LLOQ) for all matrices was 5 ng/ml except that for mouse urine which was 10 ng/ml. The calibration standard curves were reproducible for all matrices with inter- and intra-day variability in precision and accuracy being less than 15% at all quality control concentrations except for the LLOQ in mouse plasma for which the accuracy was within 17%. The assay was successfully applied to characterize the systemic pharmacokinetics of ON01910 as well as its disposition in brain and brain tumor in mice. ON01910 exhibited a clearance of 3.61±0.85 l/h/kg and a half life of 8.66±3.30 h at 50 mg/kg dose given I.V., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2011

15. Discovery of a clinical stage multi-kinase inhibitor sodium (E)-2-{2-methoxy-5-[(2',4',6'-trimethoxystyrylsulfonyl)methyl]phenylamino}acetate (ON 01910.Na): synthesis, structure-activity relationship, and biological activity.

Author

Reddy MV, Venkatapuram P, Mallireddigari MR, Pallela VR, Cosenza SC, Robell KA, Akula B, Hoffman BS, and Reddy EP

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Apoptosis, Biological Availability, Cell Line, Tumor, Drug Resistance, Multiple, Drug Resistance, Neoplasm, Drug Screening Assays, Antitumor, Female, Glycine chemical synthesis, Glycine chemistry, Glycine pharmacology, Humans, Mice, Mice, Nude, Neoplasm Transplantation, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors pharmacology, Stereoisomerism, Structure-Activity Relationship, Sulfones chemistry, Sulfones pharmacology, Transplantation, Heterologous, Antineoplastic Agents chemical synthesis, Glycine analogs & derivatives, Protein Kinase Inhibitors chemical synthesis, Sulfones chemical synthesis

Abstract

Cyclin D proteins are elevated in many cancer cells, and targeted deletion of cyclin D1 gene in the mammary tissues protects mice from breast cancer. Accordingly, there is an increasing awareness of this novel nonenzymatic target for cancer therapeutics. We have developed novel, nonalkylating styrylbenzylsulfones that induce cell death in wide variety of cancer cells without affecting the proliferation and survival of normal cells. The development of derivatized styrylbenzylsulfones followed logically from a tumor cell cytotoxicity screen performed in our laboratory that did not have an a priori target profile. Modifications of some of the precursor molecules led to lead optimization with regard to tumor cell cytotoxicity. In this report we describe the synthesis and structure-activity relationships of novel, nonalkylating (E)-styrylbenzylsulfones and the development of the novel anticancer agent sodium (E)-2-{2-methoxy-5-[(2',4',6'-trimethoxystyrylsulfonyl)methyl]phenylamino}acetate (ON 01910.Na), which is in phase III trials for myelodysplastic syndromes (MDS) associated with aberrant expression of cyclin D proteins.

Published

2011

16. Design, synthesis, and biological evaluation of (E)-styrylbenzylsulfones as novel anticancer agents.

Author

Reddy MV, Mallireddigari MR, Cosenza SC, Pallela VR, Iqbal NM, Robell KA, Kang AD, and Reddy EP

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Cell Line, Tumor, Drug Design, Drug Resistance, Neoplasm, Drug Screening Assays, Antitumor, Female, Humans, Mice, Mice, Nude, Rats, Stereoisomerism, Structure-Activity Relationship, Styrenes chemistry, Styrenes pharmacology, Sulfones chemistry, Sulfones pharmacology, Toxicity Tests, Antineoplastic Agents chemical synthesis, Styrenes chemical synthesis, Sulfones chemical synthesis

Abstract

Cell cycle progression is regulated by cyclins and cyclin-dependent kinases, which are formed at specific stages of the cell cycle and regulate the G1/S and G2/M phase transitions, employing a series of "checkpoints" governed by phosphorylation of their substrates. Tumor development is associated with the loss of these checkpoint controls, and this provides an approach for the development of therapeutic agents that can specifically target tumor cells. Here, we describe the synthesis and SAR of a novel group of cytotoxic molecules that selectively induce growth arrest of normal cells in the G1 phase while inducing a mitotic arrest of tumor cells resulting in selective killing of tumor cell populations with little or no effect on normal cell viability. The broad spectrum of antitumor activity in vitro and xenograft models, lack of in vivo toxicity, and drug resistance suggest potential for use of these agents in cancer therapy.

Published

2008

17. Endodermal differentiation of murine embryonic carcinoma cells by retinoic acid requires JLP, a JNK-scaffolding protein.

Author

Kashef K, Xu H, Reddy EP, and Dhanasekaran DN

Subjects

Animals, Cell Line, Tumor, GTP-Binding Protein alpha Subunits, G12-G13 metabolism, Mice, Signal Transduction drug effects, Adaptor Proteins, Signal Transducing metabolism, Antineoplastic Agents pharmacology, Carcinoma, Embryonal metabolism, Cell Differentiation drug effects, Endoderm metabolism, Models, Biological, Pluripotent Stem Cells metabolism, Tretinoin pharmacology

Abstract

Retinoic acid (RA) is a morphogen that induces endodermal differentiation of murine P19 embryonic carcinoma cells. RA-induced differentiation of P19 cells has been used as a model system to define the differentiation programs of pluripotent stem cells. Using this system it has been shown that G alpha13--the alpha-subunit of the heterotrimeric G protein G13--and its activation of JNK-module are critically required for the endodermal differentiation of P19 cells. However, the mechanism through which G alpha13 is linked to JNK-module is unknown. Here, we report that RA stimulates the expression of JNK-interacting leucine zipper protein (JLP), a newly identified JNK-scaffolding protein and its critical role in RA-mediated endodermal differentiation. Our results indicate that there is a physical association between JLP and G alpha13 in RA-stimulated P19 cells. More interestingly, silencing JLP abrogates RA-mediated endodermal differentiation of P19 cells analogous to the effects seen with the silencing of G alpha13 or JNK. Therefore, our studies presented here identify for the first time, a novel role for a newly identified scaffolding protein in RA-mediated endodermal differentiation, providing a new signaling conduit to transmit signals from RA to JNK module., (2006 Wiley-Liss, Inc.)

Published

2006

18. ON01910, a non-ATP-competitive small molecule inhibitor of Plk1, is a potent anticancer agent.

Author

Gumireddy K, Reddy MV, Cosenza SC, Boominathan R, Baker SJ, Papathi N, Jiang J, Holland J, and Reddy EP

Subjects

Adenosine Triphosphate metabolism, Animals, Antineoplastic Agents chemistry, Antineoplastic Agents metabolism, Antineoplastic Agents toxicity, Apoptosis, Cell Cycle physiology, Cell Cycle Proteins genetics, Cell Line, Tumor, Dose-Response Relationship, Drug, Female, Humans, Mice, Mice, Nude, Molecular Structure, Neoplasms, Experimental metabolism, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors metabolism, Protein Kinase Inhibitors toxicity, Protein Kinases genetics, Protein Serine-Threonine Kinases, Proto-Oncogene Proteins genetics, Spindle Apparatus metabolism, Polo-Like Kinase 1, Antineoplastic Agents pharmacology, Cell Cycle Proteins metabolism, Protein Kinase Inhibitors pharmacology, Protein Kinases metabolism, Proto-Oncogene Proteins metabolism, Spindle Apparatus drug effects

Abstract

Elevated expression of polo-like kinase1 (Plk1) has been reported in many human tumors, and inhibition of Plk1 activity results in their mitotic arrest and apoptosis. Here we describe the profile of ON01910, a small molecule inhibitor of Plk1 activity, which induces mitotic arrest of tumor cells characterized by spindle abnormalities leading to their apoptosis. This compound was not ATP-competitive, but competed for the substrate binding site of the enzyme. In vivo, this compound did not exhibit hematotoxicity, liver damage, or neurotoxicity, and was a potent inhibitor of tumor growth in a variety of xenograft nude mouse models. ON01910 showed strong synergy with several chemotherapeutic agents, often inducing complete regression of tumors.

Published

2005

19. A non-ATP-competitive inhibitor of BCR-ABL overrides imatinib resistance.

Author

Gumireddy K, Baker SJ, Cosenza SC, John P, Kang AD, Robell KA, Reddy MV, and Reddy EP

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents therapeutic use, Benzamides, Benzene Derivatives chemistry, Benzene Derivatives therapeutic use, Cell Death, Female, Fusion Proteins, bcr-abl, Humans, Imatinib Mesylate, K562 Cells, Leukemia, Myelogenous, Chronic, BCR-ABL Positive drug therapy, Mice, Mice, Nude, Molecular Structure, Mutation, Piperazines chemistry, Piperazines therapeutic use, Protein-Tyrosine Kinases genetics, Pyrimidines chemistry, Pyrimidines therapeutic use, Recombinant Proteins genetics, Recombinant Proteins metabolism, Adenosine Triphosphate metabolism, Antineoplastic Agents metabolism, Benzene Derivatives metabolism, Drug Resistance, Neoplasm, Piperazines metabolism, Protein-Tyrosine Kinases antagonists & inhibitors, Protein-Tyrosine Kinases metabolism, Pyrimidines metabolism

Abstract

Imatinib, which is an inhibitor of the BCR-ABL tyrosine kinase, has been a remarkable success for the treatment of Philadelphia chromosome-positive (Ph+) chronic myelogenous leukemias (CMLs). However, a significant proportion of patients chronically treated with imatinib develop resistance because of the acquisition of mutations in the kinase domain of BCR-ABL. Mutations occur at residues directly implicated in imatinib binding or, more commonly, at residues important for the ability of the kinase to adopt the specific closed (inactive) conformation to which imatinib binds. In our quest to develop new BCR-ABL inhibitors, we chose to target regions outside the ATP-binding site of this enzyme because these compounds offer the potential to be unaffected by mutations that make CML cells resistant to imatinib. Here we describe the activity of one compound, ON012380, that can specifically inhibit BCR-ABL and induce cell death of Ph+ CML cells at a concentration of <10 nM. Kinetic studies demonstrate that this compound is not ATP-competitive but is substrate-competitive and works synergistically with imatinib in wild-type BCR-ABL inhibition. More importantly, ON012380 was found to induce apoptosis of all of the known imatinib-resistant mutants at concentrations of <10 nM concentration in vitro and cause regression of leukemias induced by i.v. injection of 32Dcl3 cells expressing the imatinib-resistant BCR-ABL isoform T315I. Daily i.v. dosing for up to 3 weeks with a >100 mg/kg concentration of this agent is well tolerated in rodents, without any hematotoxicity.

Published

2005

20. Synthesis of new coumarin 3-(N-aryl) sulfonamides and their anticancer activity.

Author

Reddy NS, Mallireddigari MR, Cosenza S, Gumireddy K, Bell SC, Reddy EP, and Reddy MV

Subjects

Antineoplastic Agents chemistry, Antineoplastic Agents toxicity, Cell Line, Tumor, Coumarins chemical synthesis, Coumarins toxicity, Humans, K562 Cells, Molecular Conformation, Molecular Structure, Sulfonamides chemistry, Antineoplastic Agents chemical synthesis, Cell Survival drug effects, Sulfonamides chemical synthesis, Sulfonamides toxicity

Abstract

Synthesis of coumarin 3-(N-aryl) sulfonamides was accomplished either by Knoevenagel condensation of anilinosulfonylacetic acids with suitable salicylaldehydes or by the reaction of methyl anilinosulfonylacetates with substituted salicylaldehydes in presence of a catalytic amount of a base. All the compounds tested for antiproliferative activity in different cancer cell lines have shown GI(50) values less than 100 microM.

Published

2004

21. Identification and characterisation of a novel heat shock protein 90 inhibitor ONO4140.

Author

Eachkoti, Rafiqa, Reddy, M.V. Ramana, Lieu, Yen K., Cosenza, Stephen C., and Reddy, E. PremKumar

Subjects

*PROTEIN analysis, *ANTINEOPLASTIC agents, *APOPTOSIS, *PROTEINS, *TUMORS

Abstract

Abstract: Heat shock protein (Hsp) 90 is a key component of the super-chaperone complex that maintains functionally active conformation of various client proteins. Many of these client proteins regulate important nodal points in multiple signalling pathways that promote cancer cell growth and survival. Inhibitors of Hsp90, therefore, have the potential of functioning as anti-cancer agents with pleiotropic effects. Identification of novel Hsp90 inhibitors with more favourable pharmacological properties is a priority in cancer therapy. To achieve this goal, we screened a compound library using a biochemical assay based on refolding of denatured firefly luciferase. The assay revealed high sensitivity, reliability and reproducibility with a Z-factor of 0.81±0.17. Six Hsp90 inhibitory compounds identified by this screening with IC50 values between 1.0 and 6μM were further characterised for anti-proliferative activity by Cell Titer-Blue Cell Viability Assay using multiple tumour cell lines. Of particular interest was ONO4140 with lowest GI50 values in three different cancer cell lines viz; DU-145, BT-474 and K562 cell lines. This study also revealed that short-term exposure of tumour cells with ONO4140 is sufficient to inhibit the catalytic activity of Hsp90, evaluated through disruption of Hsp90-p23 association by immunoprecipitation. This short term exposure appears to initiate events like degradation of Hsp90 client proteins such as ErbB2/Her-2 and Akt with concomitant inhibition of survival signalling leading to the apoptotic death of tumour cells as seen by western blotting and Caspase Glow-3,7 assay. The study also reveals that apoptosis following Hsp90 inhibition with ONO4140 occurs via Caspase9–Caspase3 intrinsic apoptotic pathway, a process that is likely triggered by inactivation of Akt. In conclusion, we have identified a novel class of synthetic compounds which show potent Hsp90 inhibitory action in preclinical studies. The discovery of this novel class of synthetic Hsp90 inhibitors with simple chemical backbone allows us to conduct further structural modifications to improve their potency and pharmacokinetic properties for use in cancer therapy. [Copyright &y& Elsevier]

Published

2014

22. Design, synthesis and evaluation of (E)-α-benzylthio chalcones as novel inhibitors of BCR-ABL kinase

Author

Reddy, M.V. Ramana, Pallela, Venkat R., Cosenza, Stephen C., Mallireddigari, Muralidhar R., Patti, Revathi, Bonagura, Marie, Truongcao, May, Akula, Balaiah, Jatiani, Shashidhar S., and Reddy, E. Premkumar

Subjects

*DRUG design, *ORGANIC synthesis, *STRUCTURE-activity relationship in pharmacology, *CHRONIC myeloid leukemia, *ANTINEOPLASTIC agents, *IMATINIB, *ENZYME inhibitors

Abstract

Abstract: Novel (E)-α-benzylthio chalcones are reported with preliminary in vitro activity data indicating that several of them are potent inhibitors (comparable to imatinib, the reference compound) of BCR-ABL phosphorylation in leukemic K562 cells, known to express high levels of BCR-ABL. The ability of such compounds to significantly inhibit K562 cell proliferation suggests that this scaffold could be a promising lead for the development of anticancer agents that are able to block BCR-ABL phosphorylation in leukemic cells. [Copyright &y& Elsevier]

Published

2010