Your search keyword '"Amrita Kamath"' showing total 34 results

1. The HER2-directed antibody-drug conjugate DHES0815A in advanced and/or metastatic breast cancer: preclinical characterization and phase 1 trial results

Author

Gail D. Lewis, Guangmin Li, Jun Guo, Shang-Fan Yu, Carter T. Fields, Genee Lee, Donglu Zhang, Peter S. Dragovich, Thomas Pillow, BinQing Wei, Jack Sadowsky, Douglas Leipold, Tim Wilson, Amrita Kamath, Michael Mamounas, M. Violet Lee, Ola Saad, Voleak Choeurng, Alexander Ungewickell, Sharareh Monemi, Lisa Crocker, Kevin Kalinsky, Shanu Modi, Kyung Hae Jung, Erika Hamilton, Patricia LoRusso, Ian Krop, Melissa M. Schutten, Renee Commerford, Mark X. Sliwkowski, and Eunpi Cho

Subjects

Science

Abstract

Abstract Approved antibody-drug conjugates (ADCs) for HER2-positive breast cancer include trastuzumab emtansine and trastuzumab deruxtecan. To develop a differentiated HER2 ADC, we chose an antibody that does not compete with trastuzumab or pertuzumab for binding, conjugated to a reduced potency PBD (pyrrolobenzodiazepine) dimer payload. PBDs are potent cytotoxic agents that alkylate and cross-link DNA. In our study, the PBD dimer is modified to alkylate, but not cross-link DNA. This HER2 ADC, DHES0815A, demonstrates in vivo efficacy in models of HER2-positive and HER2-low cancers and is well-tolerated in cynomolgus monkey safety studies. Mechanisms of action include induction of DNA damage and apoptosis, activity in non-dividing cells, and bystander activity. A dose-escalation study (ClinicalTrials.gov: NCT03451162) in patients with HER2-positive metastatic breast cancer, with the primary objective of evaluating the safety and tolerability of DHES0815A and secondary objectives of characterizing the pharmacokinetics, objective response rate, duration of response, and formation of anti-DHES0815A antibodies, is reported herein. Despite early signs of anti-tumor activity, patients at higher doses develop persistent, non-resolvable dermal, ocular, and pulmonary toxicities, which led to early termination of the phase 1 trial.

Published

2024

2. Identification and characterization of an octameric PEG-protein conjugate system for intravitreal long-acting delivery to the back of the eye.

Author

Whitney Shatz, Philip E Hass, Nikhil Peer, Maciej T Paluch, Craig Blanchette, Guanghui Han, Wendy Sandoval, Ashley Morando, Kelly M Loyet, Vladimir Bantseev, Helen Booler, Susan Crowell, Amrita Kamath, Justin M Scheer, and Robert F Kelley

Subjects

Medicine, Science

Abstract

Innovative protein engineering and chemical conjugation technologies have yielded an impressive number of drug candidates in clinical development including >80 antibody drug conjugates, >60 bispecific antibodies, >35 Fc-fusion proteins and >10 immuno-cytokines. Despite these innovations, technological advances are needed to address unmet medical needs with new pharmacological mechanisms. Age-related eye diseases are among the most common causes of blindness and poor vision in the world. Many such diseases affect the back of the eye, where the inaccessibility of the site of action necessitates therapeutic delivery via intravitreal (IVT) injection. Treatments administered via this route typically have vitreal half-lives

Published

2019

3. A homogeneous high-DAR antibody–drug conjugate platform combining THIOMAB antibodies and XTEN polypeptides

Author

Neelie Zacharias, Vladimir N. Podust, Kimberly K. Kajihara, Douglas Leipold, Geoffrey Del Rosario, Desiree Thayer, Emily Dong, Maciej Paluch, David Fischer, Kai Zheng, Corinna Lei, Jintang He, Carl Ng, Dian Su, Luna Liu, Shabkhaiz Masih, William Sawyer, Jeff Tinianow, Jan Marik, Victor Yip, Guangmin Li, Josefa Chuh, J. Hiroshi Morisaki, Summer Park, Bing Zheng, Hilda Hernandez-Barry, Kelly M. Loyet, Min Xu, Katherine R. Kozak, Gail Lewis Phillips, Ben-Quan Shen, Cong Wu, Keyang Xu, Shang-Fan Yu, Amrita Kamath, Rebecca K. Rowntree, Dorothea Reilly, Thomas Pillow, Andrew Polson, Volker Schellenberger, Wouter L. W. Hazenbos, and Jack Sadowsky

Subjects

General Chemistry

Abstract

The antibody-drug conjugate (ADC) is a well-validated modality for the cell-specific delivery of small molecules with impact expanding rapidly beyond their originally-intended purpose of treating cancer. However, antibody-mediated delivery (AMD) remains inefficient, limiting its applicability to targeting highly potent payloads to cells with high antigen expression. Maximizing the number of payloads delivered per antibody is one key way in which delivery efficiency can be improved, although this has been challenging to carry out; with few exceptions, increasing the drug-to-antibody ratio (DAR) above ∼4 typically destroys the biophysical properties and

Published

2022

4. Abstract LB242: Characterizing the fate<tissue distribution and excretion route> of cancer vaccine lipoplex-RNA following intravenous injection of 14C-DOTMA-lipoplex-mRNA in mice

Author

Victor Yip, Gillie Roth, Elizabeth Torres, Sara Wichner, Craig Blanchette, Amrita Kamath, and Ben-Quan Shen

Subjects

Cancer Research, Oncology

Abstract

Messenger RNA (mRNA) has emerged as a new class of therapeutic agent delivered by a carrier lipoplex (LPX) to elicit an immune-response for treating various diseases, including cancers. However, the PK and tissue distribution of the components is not well characterized given its therapeutic novelty and structural complexity. As such, this study aimed to characterize the distribution and metabolic fate of LPX-mRNA using a radiolabeled DOTMA, a component of the LPX-mRNA therapeutic, to aid the development of this anti-cancer agent. To track the fate of LPX-mRNA, DOTMA was first radiolabeled with [14C] through chemical synthesis (14C-DOTMA, and then mixed with DOPE and mRNA at a specific ratio to form 14C-DOTMA-LPX-mRNA (14C-LPX-mRNA)). The plasma protein binding and blood cell partitioning for both 14C-LPX-mRNA and 14C-DOTMA alone were assessed in vitro. Moreover, the in vivo biodistribution and elimination of both 14C-molecules were characterized following a single intravenous (IV) injection in mice up to 12 weeks.The in-vitro assays showed the 14C-DOTMA and the 14C-LPX-mRNA were highly associated with plasma proteins and blood cell as the complexes were spun down at a much higher level as compared to in PBS solution (~5% and ~60% plasma proteins bound and ~60% and ~80% blood cell partitioned in 14C-DOTMA and the 14C-LPX-mRNA, respectively). Following in-vivo dosing in mice, plasma radioactivity of both test molecules showed a biphasic elimination profile with a rapid phase of decrease during the first 3 days followed by a prolonged exposure phase. The radioactivity in the whole blood and plasma displayed similar profiles but had minimal partitioning to blood cells, differing from the in-vitro data. We hypothesized that, both drug substances began to associate with plasma proteins/blood cells, then quickly distributed to the tissues and eliminated from the systemic circulation. Among all tissues analyzed, the liver and spleen showed the highest radioactivity levels where the 14C-LPX-mRNA peaked within the day while 14C-DOTMA peaked at 3-weeks-after-dose, followed by a long persistency. Lower levels of distribution and persistence of radioactivity were also observed in other tissues. The route of elimination is mainly through the biliary-fecal route with minimal contribution from the renal route for 14C-LPX-mRNA. 14C-LPX-mRNA achieved mass balance at 8-weeks after dose where ~70% was eliminated through feces, 3% through urine and ~20% remaining in tissues. 14C-DOTMA animals have an under-recovery of about 40-50% in radioactivity due to animals’ low intake of food and water which caused a severe reduction in animals’ weight. In summary, this study fully characterized the fate of the 14C-DOTMA and the 14C-LPX-mRNA in vitro and in vivo in mice. Our data demonstrated that the LPX-mRNA (by tracking DOTMA) mainly distributed to the spleen and liver with a long persistency, consistent with previous study showing the spleen as the major tissue for mRNA distribution. However, the LPX’s elimination profile (duration/persistency) is likely very different from that of mRNA. The ongoing work is to track the fate of mRNA component in LPX-mRNA, which could provide more insight on the correlation of DOTMA and mRNA, and help the development of this novel therapeutic modality. Citation Format: Victor Yip, Gillie Roth, Elizabeth Torres, Sara Wichner, Craig Blanchette, Amrita Kamath, Ben-Quan Shen. Characterizing the fate of cancer vaccine lipoplex-RNA following intravenous injection of 14C-DOTMA-lipoplex-mRNA in mice [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 2 (Clinical Trials and Late-Breaking Research); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(8_Suppl):Abstract nr LB242.

Published

2023

5. Anti-Lymphocyte Antigen 6 Complex, Locus E

Author

Victor, Yip, Isabel, Figueroa, Brandon, Latifi, Shab, Masih, Carl, Ng, Doug, Leipold, Amrita, Kamath, and Ben-Quan, Shen

Subjects

Immunoconjugates, Metabolic Clearance Rate, GPI-Linked Proteins, Xenograft Model Antitumor Assays, Rats, Macaca fascicularis, Mice, Antineoplastic Agents, Immunological, Cell Line, Tumor, Neoplasms, Alpha-Globulins, Antigens, Surface, Animals, Humans, Female, Tissue Distribution

Abstract

Anti-Ly6E

Published

2020

6. Nonclinical toxicology development of a novel antibody antibiotic conjugate for treating invasive Staphylococcus Aureus infections

Author

Nicola J, Stagg, Paula, Katavolos, Kirsten, Achilles Poon, Shelly, Zhong, Nina, Ljumanovic, Amrita, Kamath, Hao, Cai, Montserrat, Carrasco-Triguero, and Wendy, Halpern

Subjects

Male, Pharmacology, Mutagenicity Tests, Immunotoxins, Globulins, Staphylococcal Infections, Toxicology, Spermatozoa, Rats, Rats, Sprague-Dawley, Macaca fascicularis, Drug Delivery Systems, Cardiovascular Diseases, Cell Wall, Testis, Animals, Administration, Intravenous, Female, Nervous System Diseases

Abstract

Invasive Staphylococcus aureus (S. aureus) infections are a leading cause of death and not effectively treated with prolonged standard of care antibiotics. A novel THIOMAB™ antibody antibiotic conjugate (TAC) was developed that uses a bacterial-wall specific antibody to deliver the antibiotic (dmDNA31, a rifamycin analogue) to bacteria to minimize toxicities typically seen with prolonged use of traditional antibiotics. The TAC nonclinical toxicology package included repeat dose rat and cynomolgus monkey toxicology studies for 8 weekly intravenous (IV) doses, a 7-day daily repeat dose IV toxicology study of dmDNA31 and an assessment of genotoxicity, cardiovascular toxicity, neurotoxicity and sperm parameters. TAC and dmDNA31 were well tolerated in rats and monkeys, and there was no evidence of genotoxicity, cardiovascular toxicity or neurotoxicity. Non-adverse findings were observed and included blue discoloration in skin, blood, etc. due to the blue color of dmDNA31, increased globulin due to the high doses of antibodies, and abnormal sperm morphology of small heads in male rats with no histopathology correlate in testis. This is an example of antibody-mediated delivery of an antibiotic that has the potential to offer a more effective way of eradicating infection while providing a better safety profile compared to traditional antibiotics.

Published

2022

7. Attachment Site Cysteine Thiol pK

Author

Breanna S, Vollmar, Binqing, Wei, Rachana, Ohri, Jianhui, Zhou, Jintang, He, Shang-Fan, Yu, Douglas, Leipold, Ely, Cosino, Sharon, Yee, Aimee, Fourie-O'Donohue, Guangmin, Li, Gail L, Phillips, Katherine R, Kozak, Amrita, Kamath, Keyang, Xu, Genee, Lee, Greg A, Lazar, and Hans K, Erickson

Subjects

Maleimides, Models, Molecular, Benzodiazepines, Immunoconjugates, Drug Stability, Protein Conformation, Mutation, Pyrroles, Cysteine

Abstract

The incorporation of cysteines into antibodies by mutagenesis allows for the direct conjugation of small molecules to specific sites on the antibody via disulfide bonds. The stability of the disulfide bond linkage between the small molecule and the antibody is highly dependent on the location of the engineered cysteine in either the heavy chain (HC) or the light chain (LC) of the antibody. Here, we explore the basis for this site-dependent stability. We evaluated the in vivo efficacy and pharmacokinetics of five different cysteine mutants of trastuzumab conjugated to a pyrrolobenzodiazepine (PBD) via disulfide bonds. A significant correlation was observed between disulfide stability and efficacy for the conjugates. We hypothesized that the observed site-dependent stability of the disulfide-linked conjugates could be due to differences in the attachment site cysteine thiol pK

Published

2017

8. Metabolism of 5-Isopropyl-6-(5-methyl-1,3,4-oxadiazol-2-yl)-N-(2-methyl-1H-pyrrolo[2,3-b]pyridin-5-yl)pyrrolo[2,1-f][1,2,4]triazin-4-amine (BMS-645737): Identification of an UnusualN-Acetylglucosamine Conjugate in the Cynomolgus Monkey

Author

John E. Leet, Ravindra W. Tejwani, Louis J. Lombardo, Yueping Zhang, Benjamin M. Johnson, Xiaohong Liu, Rajeev S. Bhide, Donna D. Wei, Ligang Qian, Yue-Zhong Shu, and Amrita Kamath

Subjects

Glycosylation, Magnetic Resonance Spectroscopy, Stereochemistry, Carboxylic acid, Glucuronidation, Pharmaceutical Science, Mice, Inbred Strains, Hydroxylation, Acetylglucosamine, Rats, Sprague-Dawley, Mice, chemistry.chemical_compound, Dogs, Cytochrome P-450 Enzyme System, Biotransformation, Tandem Mass Spectrometry, Animals, Bile, Humans, Moiety, Pyrroles, Mercapturic acid, Protein Kinase Inhibitors, Pharmacology, chemistry.chemical_classification, Molecular Structure, Triazines, Aromatic amine, Vascular Endothelial Growth Factor Receptor-2, Recombinant Proteins, Rats, Macaca fascicularis, chemistry, Dihydroxylation, Hepatocytes, Microsomes, Liver, Metabolic Networks and Pathways

Abstract

5-Isopropyl-6-(5-methyl-1,3,4-oxadiazol-2-yl)-N-(2-methyl-1H-pyrrolo[2,3-b]pyridin-5-yl)pyrrolo[2,1-f][1,2,4]triazin-4-amine (BMS-645737) is a potent and selective vascular endothelial growth factor receptor-2 antagonist. In this study, liquid chromatography/tandem mass spectrometry and NMR were used to investigate the biotransformation of BMS-645737 in vitro and in the cynomolgus monkey, dog, mouse, and rat. Metabolic pathways for BMS-645737 included multistep processes involving both oxidation and conjugation reactions. For example, the 2-methyl-1H-pyrrolo moiety underwent cytochrome P450-catalyzed hydroxylation followed by oxidation to a carboxylic acid and then conjugation with taurine. Alternatively, the 5-methyl-1,3,4-oxadiazol-2-yl moiety was metabolized by hydroxylation and then conjugation with sulfate. The pyridin-5-yl group underwent direct glucuronidation in hepatocytes (dog, monkey, human) and conjugation with N-acetylglucosamine in the monkey. Conjugation with glutathione and processing along the mercapturic acid pathway was a minor metabolic pathway in vivo, although BMS-645737 did not form conjugates in the presence of glutathione-supplemented liver microsomes. Other minor biotransformation pathways included oxidative dehydrogenation, dihydroxylation, and hydrolytic opening of the oxadiazole ring followed by either deacetylation or hydrolysis of the resulting diacyl hydrazide. Whereas previous studies have shown the formation of N-acetylglucosamine conjugates of alcohols, arylamines, and other small molecules, this report describes the biotransformation of a heterocyclic aromatic amine via direct conjugation with N-acetylglucosamine.

Published

2008

9. Discovery of Pyrrolopyridine−Pyridone Based Inhibitors of Met Kinase: Synthesis, X-ray Crystallographic Analysis, and Biological Activities

Author

Robert J. Schmidt, Benjamin J. Henley, Celia D’Arienzo, Jonathan Lippy, John S. Sack, Yueping Zhang, Yongmi An, John T. Hunt, Amrita Kamath, John S. Tokarski, Barri Wautlet, Veeraswamy Manne, Dianlin Xie, Punit Marathe, Donna D. Wei, Louis J. Lombardo, Kyoung S. Kim, Robert Jeyaseelan, David K. Williams, Joseph Fargnoli, Liping Zhang, Yaquan Zhang, Johnni Gullo-Brown, Zhen-Wei Cai, George L. Trainor, and Robert M. Borzilleri

Subjects

Male, Pyridones, medicine.drug_class, Stereochemistry, Antineoplastic Agents, Carboxamide, Crystallography, X-Ray, Inhibitory Concentration 50, Mice, Structure-Activity Relationship, Cell Line, Tumor, Proto-Oncogene Proteins, Drug Discovery, medicine, Animals, Humans, Transferase, Structure–activity relationship, Receptors, Growth Factor, Binding site, Protein Kinase Inhibitors, Cell Proliferation, chemistry.chemical_classification, Mice, Inbred BALB C, Kinase, Phosphotransferases, Proto-Oncogene Proteins c-met, Vascular Endothelial Growth Factor Receptor-2, Enzyme, fms-Like Tyrosine Kinase 3, Biochemistry, chemistry, Microsomes, Liver, Molecular Medicine, Signal transduction

Abstract

Conformationally constrained 2-pyridone analogue 2 is a potent Met kinase inhibitor with an IC50 value of 1.8 nM. Further SAR of the 2-pyridone based inhibitors of Met kinase led to potent 4-pyridone and pyridine N-oxide inhibitors such as 3 and 4. The X-ray crystallographic data of the inhibitor 2 bound to the ATP binding site of Met kinase protein provided insight into the binding modes of these inhibitors, and the SAR of this series of analogues was rationalized. Many of these analogues showed potent antiproliferative activities against the Met dependent GTL-16 gastric carcinoma cell line. Compound 2 also inhibited Flt-3 and VEGFR-2 kinases with IC50 values of 4 and 27 nM, respectively. It possesses a favorable pharmacokinetic profile in mice and demonstrates significant in vivo antitumor activity in the GTL-16 human gastric carcinoma xenograft model.

Published

2008

10. Discovery of orally active pyrrolopyridine- and aminopyridine-based Met kinase inhibitors

Author

Amrita Kamath, Yongmi An, John T. Hunt, Punit Marathe, Veeraswamy Manne, Zhen-Wei Cai, Donna D. Wei, John S. Sack, Robert J. Schmidt, Yueping Zhang, Robert M. Borzilleri, Kyoung S. Kim, Cornelius Lyndon A M, Gretchen M. Schroeder, David K. Williams, Xiao-Tao Chen, Joseph Fargnoli, Louis J. Lombardo, and John S. Tokarski

Subjects

Clinical Biochemistry, Aminopyridines, Pharmaceutical Science, Pharmacology, Biochemistry, Receptor tyrosine kinase, Mice, Structure-Activity Relationship, Stomach Neoplasms, In vivo, Drug Discovery, Animals, Humans, Urea, Pyrroles, Kinase activity, Protein Kinase Inhibitors, Molecular Biology, chemistry.chemical_classification, biology, Kinase, Chemistry, Organic Chemistry, Proto-Oncogene Proteins c-met, Xenograft Model Antitumor Assays, In vitro, Enzyme, Enzyme inhibitor, biology.protein, Molecular Medicine, Signal transduction

Abstract

A series of acylurea analogs derived from pyrrolopyridine and aminopyridine scaffolds were identified as potent inhibitors of Met kinase activity. The SAR at various positions of the two kinase scaffolds was investigated. These studies led to the discovery of compounds 3b and 20b, which demonstrated favorable pharmacokinetic properties in mice and significant antitumor activity in a human gastric carcinoma xenograft model.

Published

2008

11. Discovery and preclinical studies of 5-isopropyl-6-(5-methyl-1,3,4-oxadiazol-2-yl)-N-(2-methyl-1H-pyrrolo[2,3-b]pyridin-5-yl)pyrrolo[2,1-f][1,2,4]triazin-4-amine (BMS-645737), an in vivo active potent VEGFR-2 inhibitor

Author

Ligang Qian, Carl Thibeault, Amrita Kamath, Barri Wautlet, Alain Martel, George L. Trainor, Punit Marathe, Celia D’Arienzo, Benjamin J. Henley, Steven Mortillo, Donna D. Wei, Robert Jeyaseelan, Ravindra W. Tejwani, John T. Hunt, Louis J. Lombardo, Rejean Ruel, Yueping Zhang, Zhen-Wei Cai, Joseph Fargnoli, Arvind Mathur, Alexandre L'Heureux, Joel C. Barrish, Rajeev S. Bhide, and George M. Derbin

Subjects

ERG1 Potassium Channel, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Angiogenesis Inhibitors, Biochemistry, Chemical synthesis, Cell Line, Inhibitory Concentration 50, Mice, Structure-Activity Relationship, Growth factor receptor, In vivo, Drug Discovery, Animals, Humans, Pyrroles, Molecular Biology, Mice, Inbred BALB C, Bicyclic molecule, biology, Triazines, Chemistry, Organic Chemistry, Protein-Tyrosine Kinases, Vascular Endothelial Growth Factor Receptor-2, Xenograft Model Antitumor Assays, Ether-A-Go-Go Potassium Channels, In vitro, Enzyme inhibitor, Drug Design, biology.protein, Cytochrome P-450 CYP3A Inhibitors, Molecular Medicine, Tyrosine kinase, Isopropyl

Abstract

We report herein a series of substituted N-(1H-pyrrolo[2,3-b]pyridin-5-yl)pyrrolo[2,1-f][1,2,4]triazin-4-amines as inhibitors of vascular endothelial growth factor receptor-2 tyrosine kinase. Through structure–activity relationship studies, biochemical potency, pharmacokinetics, and kinase selectivity were optimized to afford BMS-645737 (13), a compound with good preclinical in vivo activity against human tumor xenograft models.

Published

2008

12. Preclinical discovery of ixabepilone, a highly active antineoplastic agent

Author

Francis Y. Lee, Richard Smykla, Robert M. Borzilleri, Craig R. Fairchild, Gregory D. Vite, Amrita Kamath, and Robert Kramer

Subjects

Male, Cancer Research, Epothilones, Combination therapy, Antineoplastic Agents, Pharmacology, Epothilone, Toxicology, Tubulin binding, Capecitabine, Mice, chemistry.chemical_compound, Tubulin, In vivo, Cell Line, Tumor, Neoplasms, medicine, Animals, Humans, Pharmacology (medical), Sorangium cellulosum, Clinical Trials as Topic, biology, Ixabepilone, Blood Proteins, biology.organism_classification, Xenograft Model Antitumor Assays, Tubulin Modulators, Oncology, chemistry, Drug Resistance, Neoplasm, Female, Taxoids, Drug Screening Assays, Antitumor, Protein Binding, medicine.drug

Abstract

The epothilones and their analogs constitute a novel class of antineoplastic agents, produced by the myxobacterium Sorangium cellulosum. These antimicrotubule agents act in a similar manner to taxanes, stabilizing microtubules and resulting in arrested tumor cell division and apoptosis. Unlike taxanes, however, epothilones and their analogs are macrolide antibiotics, with a distinct tubulin binding mode and reduced susceptibility to a range of common tumor resistance mechanisms that limit the effectiveness of taxanes and anthracyclines. While natural epothilones A and B show potent antineoplastic activity in vitro, these effects were not seen in preclinical in vivo models due to their poor metabolic stability and unfavorable pharmacokinetics. A range of epothilone analogs was synthesized, therefore, with the aim of identifying those with more favorable characteristics. Here, we describe the preclinical characterization and selection of ixabepilone, a semi-synthetic epothilone B analog, among many other epothilone analogs. Ixabepilone demonstrated superior preclinical characteristics, including high metabolic stability, low plasma protein binding and low susceptibility to multidrug resistance protein-mediated efflux, all of which were predictive of potent in vivo cell-killing activity. Ixabepilone also demonstrated in vivo antitumor activity in a range of human tumor models, several of which displayed resistance to commonly used agents such as anthracyclines and taxanes. These favorable preclinical characteristics have since translated to the clinic. Ixabepilone has shown promising phase II clinical efficacy and acceptable tolerability in a wide range of cancers, including heavily pretreated and drug-resistant tumors. Based on these results, a randomized phase III trial was conducted in anthracycline-pretreated or resistant and taxane-resistant metastatic breast cancer to evaluate ixabepilone in combination with capecitabine. Ixabepilone combination therapy showed significantly superior progression-free survival and tumor responses over capecitabine alone.

Published

2008

13. Discovery of Brivanib Alaninate ((S)-((R)-1-(4-(4-Fluoro-2-methyl-1H-indol-5-yloxy)-5-methylpyrrolo[2,1-f][1,2,4]triazin-6-yloxy)propan-2-yl)2-aminopropanoate), A Novel Prodrug of Dual Vascular Endothelial Growth Factor Receptor-2 and Fibroblast Growth Factor Receptor-1 Kinase Inhibitor (BMS-540215)

Author

Celia D’Arienzo, Daniel W. Kukral, Stephanie Barbosa, Steve Mortillo, John T. Hunt, Lawrence Wu, Punit Marathe, George M. Derbin, Joseph Fargnoli, Yong-Zheng Zhang, Robert M. Borzilleri, Joel C. Barrish, Zhongping Shi, Jeffrey A. Robl, Robert Jeyaseelan, Rajeev S. Bhide, Ligang Qian, Donna D. Wei, Junying Fan, Amrita Kamath, Xiaoping Zheng, Zhen-Wei Cai, Louis J. Lombardo, and Barri Wautlet

Subjects

biology, Chemistry, Stereochemistry, Fibroblast growth factor receptor 1, Kinase insert domain receptor, Prodrug, Chemical synthesis, stomatognathic diseases, chemistry.chemical_compound, Brivanib alaninate, Growth factor receptor, In vivo, Enzyme inhibitor, Drug Discovery, biology.protein, Molecular Medicine

Abstract

A series of amino acid ester prodrugs of the dual VEGFR-2/FGFR-1 kinase inhibitor 1 (BMS-540215) was prepared in an effort to improve the aqueous solubility and oral bioavailability of the parent compound. These prodrugs were evaluated for their ability to liberate parent drug 1 in in vitro and in vivo systems. The l-alanine prodrug 8 (also known as brivanib alaninate/BMS-582664) was selected as a development candidate and is presently in phase II clinical trials.

Published

2008

14. Discovery and SAR of 2-amino-5-(thioaryl)thiazoles as potent and selective Itk inhibitors

Author

Joel C. Barrish, David J. Shuster, Chunjian Liu, Kim W. McIntyre, Tai-An Lin, Amrita Kamath, Becky Penhallow, Kathleen D. O'Day, Steven B. Kanner, Joseph A. Furch, John H. Dodd, Steven H. Spergel, Hongjian Zhang, James Lin, Robert V. Moquin, Arthur M. Doweyko, John Wityak, Punit Marathe, Jagabandhu Das, and Chen Yi Hung

Subjects

Clinical Biochemistry, Pharmaceutical Science, Sulfides, Biochemistry, Jurkat cells, Jurkat Cells, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Aminothiazole, In vivo, Drug Discovery, Hypersensitivity, Animals, Humans, Enzyme Inhibitors, Molecular Biology, Cells, Cultured, chemistry.chemical_classification, biology, Organic Chemistry, Pneumonia, Protein-Tyrosine Kinases, Small molecule, Asthma, In vitro, Thiazoles, Ovalbumin, Enzyme, chemistry, Enzyme inhibitor, biology.protein, Molecular Medicine

Abstract

A series of structurally novel aminothiazole based small molecule inhibitors of Itk were prepared to elucidate their structure-activity relationships (SARs), selectivity, and cell activity in inhibiting IL-2 secretion in a Jurkat T-cell assay. Compound 3 is identified as a potent and selective Itk inhibitor which inhibits anti-TCR antibody induced IL-2 production in mice in vivo and was previously reported to reduce lung inflammation in a mouse model of ovalbumin induced allergy/asthma.

Published

2006

15. Design, Synthesis, and Evaluation of Orally Active 4-(2,4-Difluoro-5-(methoxycarbamoyl)phenylamino)pyrrolo[2,1-f][1,2,4]triazines as Dual Vascular Endothelial Growth Factor Receptor-2 and Fibroblast Growth Factor Receptor-1 Inhibitors

Author

Joseph Fargnoli, Daniel W. Kukral, Steve Mortillo, Viral Vyas, John S. Tokarski, John T. Hunt, Robert M. Borzilleri, Rajeev S. Bhide, Robert Jeyaseelan, Louis J. Lombardo, Amrita Kamath, Xiaoping Zheng, Ligang Qian, Barri Wautlet, Zhen-Wei Cai, Joel C. Barrish, Aberra Fura, and Christopher D. Ellis

Subjects

Male, Models, Molecular, Stereochemistry, Administration, Oral, Biological Availability, Mice, Nude, Antineoplastic Agents, In Vitro Techniques, Hydroxamic Acids, Fibroblast growth factor, Chemical synthesis, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Growth factor receptor, Drug Discovery, Animals, Humans, Pyrroles, Receptor, Fibroblast Growth Factor, Type 1, Cell Proliferation, Mice, Inbred BALB C, Oxadiazoles, Hydroxamic acid, Triazines, Fibroblast growth factor receptor 1, Receptor Protein-Tyrosine Kinases, Kinase insert domain receptor, Blood Proteins, Receptors, Fibroblast Growth Factor, Vascular Endothelial Growth Factor Receptor-2, Xenograft Model Antitumor Assays, chemistry, Drug Design, Microsomes, Liver, Molecular Medicine, Human umbilical vein endothelial cell, Endothelium, Vascular, Tyrosine kinase, Protein Binding

Abstract

A series of substituted 4-(2,4-difluoro-5-(methoxycarbamoyl)phenylamino)pyrrolo[2,1-f][1,2,4]triazines was identified as potent and selective inhibitors of the tyrosine kinase activity of the growth factor receptors VEGFR-2 (Flk-1, KDR) and FGFR-1. The enzyme kinetics associated with the VEGFR-2 inhibition of compound 50 (K(i) = 52 +/- 3 nM) confirmed that the pyrrolo[2,1-f][1,2,4]triazine analogues are competitive with ATP. Several analogues demonstrated low-nanomolar inhibition of VEGF- and FGF-dependent human umbilical vein endothelial cell (HUVEC) proliferation. Replacement of the C6-ester substituent of the pyrrolo[2,1-f][1,2,4]triazine core with heterocyclic bioisosteres, such as substituted 1,3,5-oxadiazoles, afforded compounds with excellent oral bioavailability in mice (i.e., 50 F(po) = 79%). Significant antitumor efficacy was observed with compounds 44, 49, and 50 against established L2987 human lung carcinoma xenografts implanted in athymic mice. A full account of the synthesis, structure-activity relationships, pharmacology, and pharmacokinetic properties of analogues within the series is presented.

Published

2005

16. Preclinical pharmacokinetics and oral bioavailability of BMS-310705, a novel epothilone B analog

Author

Francis Y. Lee, Yueping Zhang, Amrita Kamath, Ming Chang, and Punit Marathe

Subjects

Male, Cancer Research, education, Administration, Oral, Biological Availability, Mice, Nude, Pharmacology, Toxicology, Permeability, Polyethylene Glycols, Rats, Sprague-Dawley, Mice, Epothilone B Analog, Dogs, Cytochrome P-450 Enzyme System, Pharmacokinetics, Oral administration, Preclinical pharmacokinetics, Animals, Cytochrome P-450 CYP3A, Humans, Tissue Distribution, Pharmacology (medical), Chemistry, digestive, oral, and skin physiology, In vitro, Rats, Bioavailability, stomatognathic diseases, Oncology, Epothilone B, Epothilones, Microsomes, Liver, Female, Caco-2 Cells, Pharmaceutical Vehicles, In vivo pharmacokinetics

Abstract

BMS-310705, a novel semisynthetic derivative of epothilone B, is a tubulin-polymerization agent currently in phase I clinical trials for anticancer therapy. The in vitro and in vivo pharmacokinetics and oral bioavailability of BMS-310705 were investigated in mice, rats, and dogs. In addition, comparison of the pharmacokinetics of BMS-310705 using various formulations was conducted in rats.The permeability of BMS-310705 was evaluated in Caco-2 cells, an in vitro model of the human intestinal epithelium. Human liver microsomes were used to determine the cytochrome P450 enzymes involved in the metabolism of BMS-310705. Plasma protein binding of BMS-310705 was determined in mouse, rat, dog, and humans. BMS-310705 was administered to female nude mice as single doses of 5 mg/kg intravenously or 15 mg/kg orally. Male Sprague-Dawley rats were treated with single doses of BMS-310705 either intraarterially (2 mg/kg) or orally (8 mg/kg). The effect of Cremophor on the pharmacokinetics of BMS-310705 was evaluated in rats using various formulations with and without Cremophor. Male dogs were treated with 0.5 mg/kg intravenously or 1 mg/kg orally in a crossover study design.Systemic clearance of BMS-310705 was high in mice (152 ml/min/kg), rats (39 ml/min/kg), and dogs (25.7 ml/min/kg). The volume of distribution (Vss) in mice, rats, and dogs was 38, 54, and 4.7 l/kg, respectively, and greater than total body water. BMS-310705 showed moderate binding to plasma proteins in all four species tested. The clearance in humans may be intermediate to high based on both allometric scaling using parameters obtained from three species, and in vitro human liver microsomal stability data. In rats, the presence of Cremophor in the formulation resulted in a significant increase in exposure compared to buffered vehicles not containing Cremophor. Inhibition of p-glycoprotein and/or CYP3A4 by Cremophor may be responsible for this phenomenon, and studies in Caco-2 cells and human liver microsomes suggested that BMS-310705 may be a substrate for both p-glycoprotein and CYP3A4. The oral bioavailability of BMS-310705 in pH buffered formulations was 21% in mice, 34% in rats and 40% in dogs.In summary, BMS-310705 is cleared rapidly and distributes extensively in mice, rats, and dogs. The presence of Cremophor in the formulation could significantly increase exposure in rats, possibly due to interactions with p-glycoprotein and/or CYP3A4. Oral bioavailability using formulations not containing Cremophor were found to be adequate, suggesting potential for development of BMS-310705 as an oral anticancer drug.

Published

2005

17. Effect of Fruit Juices on the Oral Bioavailability of Fexofenadine in Rats

Author

Saeho Chong, Amrita Kamath, Ming Yao, and Yueping Zhang

Subjects

Male, Citrus, ATP Binding Cassette Transporter, Subfamily B, Administration, Oral, Biological Availability, Organic Anion Transporters, Pharmaceutical Science, Pharmacology, Intestinal absorption, Beverages, Rats, Sprague-Dawley, Food-Drug Interactions, Pharmacokinetics, Oral administration, medicine, Animals, Orange juice, Fexofenadine, biology, Chemistry, Rats, Bioavailability, Organic anion-transporting polypeptide, Intestinal Absorption, Area Under Curve, Fruit, Malus, Histamine H1 Antagonists, biology.protein, Ketoconazole, Terfenadine, medicine.drug

Abstract

Fexofenadine has been identified as a substrate for both the efflux transporter, P-glycoprotein (P-gp), as well as the influx transporter, organic anion transporting polypeptide (OATP). Clinical studies in humans showed that fruit juices reduced the oral bioavailability of fexofenadine by preferentially inhibiting OATP over P-gp. The objective of this study was to investigate the effects of fruit juices on the oral absorption of fexofenadine in rats to establish a preclinical fruit juice-drug interaction model. In rats, fexofenadine was excreted unchanged in the urine, bile, and gastrointestinal tract, indicating minimal metabolism, making it an ideal probe to study transport processes. Coadministration of fexofenadine with ketoconazole, a P-gp inhibitor, increased the oral exposure of fexofenadine by 187%. In contrast, coadministration of fexofenadine with orange juice or apple juice to rats decreased the oral exposure of fexofenadine by 31 and 22%, respectively. Increasing the quantity of orange or apple juice administered further decreased the oral exposure of fexofenadine, by 40 and 28%, respectively. This reduction in fexofenadine bioavailability was moderate compared to that seen in humans. These findings suggest that in rats fruit juices may also preferentially inhibit OATP rather than P-gp-mediated transport in fexofenadine oral absorption, albeit to a lesser extent than observed in humans. This fruit juice--drug interaction rat model may be useful in prediction of potential food--drug interactions in humans for drug candidates.

Published

2005

18. Discovery of N-(2-Chloro-6-methyl- phenyl)-2-(6-(4-(2-hydroxyethyl)- piperazin-1-yl)-2-methylpyrimidin-4- ylamino)thiazole-5-carboxamide (BMS-354825), a Dual Src/Abl Kinase Inhibitor with Potent Antitumor Activity in Preclinical Assays

Author

John Wityak, Amrita Kamath, Louis J. Lombardo, Ping Chen, John T. Hunt, Ivan Inigo, Stephen Castaneda, Joel C. Barrish, Herbert E. Klei, Robert J. Schmidt, John S. Tokarski, Sidney Pitt, Derek J. Norris, Francis Y. Lee, Jagabandhu Das, Craig Fairchild, Kathy A. Johnston, Punit Marathe, Robert M. Borzilleri, Cornelius Lyndon A M, Suhong Pang, Mei-Li Wen, Russell Peterson, Gary L. Schieven, Kamelia Behnia, David Kan, and Arthur M. Doweyko

Subjects

Stereochemistry, medicine.drug_class, Dasatinib, Antineoplastic Agents, Carboxamide, Pharmacology, Rats, Sprague-Dawley, Mice, chemistry.chemical_compound, Adenosine Triphosphate, hemic and lymphatic diseases, Drug Discovery, medicine, Animals, Humans, Enzyme Inhibitors, Proto-Oncogene Proteins c-abl, Thiazole, ABL, biology, Chemistry, medicine.disease, Rats, Thiazoles, Pyrimidines, src-Family Kinases, Enzyme inhibitor, biology.protein, Molecular Medicine, K562 Cells, Chronic myelogenous leukemia, Proto-oncogene tyrosine-protein kinase Src, K562 cells, medicine.drug

Abstract

A series of substituted 2-(aminopyridyl)- and 2-(aminopyrimidinyl)thiazole-5-carboxamides was identified as potent Src/Abl kinase inhibitors with excellent antiproliferative activity against hematological and solid tumor cell lines. Compound 13 was orally active in a K562 xenograft model of chronic myelogenous leukemia (CML), demonstrating complete tumor regressions and low toxicity at multiple dose levels. On the basis of its robust in vivo activity and favorable pharmacokinetic profile, 13 was selected for additional characterization for oncology indications.

Published

2004

19. P-glycoprotein plays a role in the oral absorption of BMS-387032, a potent cyclin-dependent kinase 2 inhibitor, in rats

Author

Amrita Kamath, Ming Chang, Saeho Chong, and Punit Marathe

Subjects

Cyclin-Dependent Kinase Inhibitor p21, Male, Cancer Research, medicine.medical_specialty, Biological Availability, Cell Cycle Proteins, Photoaffinity Labels, Pharmacology, Toxicology, Absorption, Rats, Sprague-Dawley, Excretion, Mice, Dogs, Oral administration, Internal medicine, medicine, Animals, Humans, Pharmacology (medical), ATP Binding Cassette Transporter, Subfamily B, Member 1, Oxazoles, P-glycoprotein, biology, Kinase, digestive, oral, and skin physiology, Brain, Rats, Bioavailability, Thiazoles, stomatognathic diseases, Endocrinology, Oncology, Knockout mouse, Microsomes, Liver, biology.protein, Microsome, Efflux, Caco-2 Cells

Abstract

BMS-387032, a novel cyclin-dependent kinase 2 inhibitor, is currently in phase I clinical trials for anticancer therapy. The oral bioavailability of BMS-387032 has been found to be about 31% in rats. Absorption and first-pass metabolism were evaluated as possible reasons for the incomplete oral bioavailability in rats. Male Sprague-Dawley rats were given single doses of BMS-387032 intraarterially (9.1 mg/kg), orally (9.1 mg/kg), or intraportally (10 mg/kg). The routes of excretion of BMS-387032 after intravenous dosing were investigated in bile-duct-cannulated rats. The rate of metabolism of BMS-387032 was investigated in liver microsomes. The permeability of BMS-387032 was evaluated using Caco-2 cells, an in vitro model of the intestinal epithelium. To determine if BMS-387032 was a P-glycoprotein substrate, brain uptake studies were conducted in P-glycoprotein knockout versus wildtype mice. The exposure in rats after an intraportal dose was similar to that after an intraarterial dose, indicating that absorption may play a greater role than liver first-pass metabolism in the low oral bioavailability seen in rats. After an intravenous dose, the percent of dose excreted unchanged in the urine and bile over a 9-h period was 28% and 11%, respectively. In vitro studies in rat liver microsomes showed low rates of metabolism of BMS-387032. The Caco-2 cell permeability of BMS-387032 was

Published

2004

20. Discovery of Aminothiazole Inhibitors of Cyclin-Dependent Kinase 2: Synthesis, X-ray Crystallographic Analysis, and Biological Activities

Author

Rawlins David B, Kevin R. Webster, Michael A. Poss, Chieh Ying Chang, Roberta Batorsky, Craig R. Fairchild, Toomas Mitt, Weifang Shan, Kristen A. Kellar, Hai Yun Xiao, John S. Tokarski, John T. Hunt, Francis Y. Lee, Janet G. Mulheron, Kyoung S. Kim, Nikola P. Pavletich, David Bol, Amrita Kamath, John S. Sack, Urvashi V. Roongta, Zhen Wei Cai, Isia Bursuker, Raj N. Misra, William G. Humphreys, Songfeng Lu, Wen Ching Han, Punit Marathe, S. David Kimball, Hong Zhu, and Ligang Qian

Subjects

Male, Models, Molecular, Stereochemistry, Benzeneacetamides, Antineoplastic Agents, Protein Serine-Threonine Kinases, Crystallography, X-Ray, Retinoblastoma Protein, Chemical synthesis, Histones, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Aminothiazole, Cyclin E, Drug Discovery, CDC2-CDC28 Kinases, Tumor Cells, Cultured, Animals, Combinatorial Chemistry Techniques, Humans, Structure–activity relationship, Enzyme Inhibitors, Phosphorylation, Protein kinase A, Oxazoles, Oxazole, Mice, Inbred BALB C, biology, Cell Cycle, Cyclin-Dependent Kinase 2, Cyclin-dependent kinase 2, Active site, DNA Polymerase I, Cyclin-Dependent Kinases, Thiazoles, chemistry, Mice, Inbred DBA, Enzyme inhibitor, biology.protein, Molecular Medicine, Female, Drug Screening Assays, Antitumor, Protein Binding

Abstract

High throughput screening identified 2-acetamido-thiazolylthio acetic ester 1 as an inhibitor of cyclin-dependent kinase 2 (CDK2). Because this compound is inactive in cells and unstable in plasma, we have stabilized it to metabolic hydrolysis by replacing the ester moiety with a 5-ethyl-substituted oxazole as in compound 14. Combinatorial and parallel synthesis provided a rapid analysis of the structure-activity relationship (SAR) for these inhibitors of CDK2, and over 100 analogues with IC(50) values in the 1-10 nM range were rapidly prepared. The X-ray crystallographic data of the inhibitors bound to the active site of CDK2 protein provided insight into the binding modes of these inhibitors, and the SAR of this series of analogues was rationalized. Many of these analogues displayed potent and broad spectrum antiproliferative activity across a panel of tumor cell lines in vitro. In addition, A2780 ovarian carcinoma cells undergo rapid apoptosis following exposure to CDK2 inhibitors of this class. Mechanism of action studies have confirmed that the phosphorylation of CDK2 substrates such as RB, histone H1, and DNA polymerase alpha (p70 subunit) is reduced in the presence of compound 14. Further optimization led to compounds such as water soluble 45, which possesses a favorable pharmacokinetic profile in mice and demonstrates significant antitumor activity in vivo in several murine and human models, including an engineered murine mammary tumor that overexpresses cyclin E, the coactivator of CDK2.

Published

2002

21. Discovery of N-(4-(2-amino-3-chloropyridin-4-yloxy)-3-fluorophenyl)-4-ethoxy-1-(4-fluorophenyl)-2-oxo-1,2-dihydropyridine-3-carboxamide (BMS-777607), a selective and orally efficacious inhibitor of the Met kinase superfamily

Author

John S. Tokarski, Barri Wautlet, Amrita Kamath, Xiao-Tao Chen, Robert Jeyaseelan, Yingru Zhang, Joseph Fargnoli, Guoxiang Shen, Kyoung S. Kim, David K. Williams, Yongmi An, John T. Hunt, Jun Dai, Kevin Stefanski, Veeraswamy Manne, Simone Oppenheimer, Ashok Kumar Gupta, Louis J. Lombardo, Gretchen M. Schroeder, George L. Trainor, Robert M. Borzilleri, Robert J. Schmidt, Benjamin J. Henley, Jonathan Lippy, Johnni Gullo-Brown, Zhen-Wei Cai, Yueping Zhang, Donna D. Wei, Cornelius Lyndon A M, Cheryl M. Clark, and John S. Sack

Subjects

Models, Molecular, Dihydropyridines, medicine.drug_class, Stereochemistry, Pyridones, Administration, Oral, Aminopyridines, Mice, Nude, Carboxamide, Antineoplastic Agents, Crystallography, X-Ray, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Dogs, Oral administration, In vivo, Cell Line, Tumor, Drug Discovery, medicine, Potency, Animals, Humans, biology, Kinase, Dihydropyridine, Proto-Oncogene Proteins c-met, Xenograft Model Antitumor Assays, Rats, chemistry, Solubility, Enzyme inhibitor, Lactam, biology.protein, Molecular Medicine, medicine.drug

Abstract

Substituted N-(4-(2-aminopyridin-4-yloxy)-3-fluoro-phenyl)-1-(4-fluorophenyl)-2-oxo-1,2-dihydropyridine-3-carboxamides were identified as potent and selective Met kinase inhibitors. Substitution of the pyridine 3-position gave improved enzyme potency, while substitution of the pyridone 4-position led to improved aqueous solubility and kinase selectivity. Analogue 10 demonstrated complete tumor stasis in a Met-dependent GTL-16 human gastric carcinoma xenograft model following oral administration. Because of its excellent in vivo efficacy and favorable pharmacokinetic and preclinical safety profiles, 10 has been advanced into phase I clinical trials.

Published

2009

22. Preclinical pharmacokinetics and in vitro metabolism of brivanib (BMS-540215), a potent VEGFR2 inhibitor and its alanine ester prodrug brivanib alaninate

Author

Amrita Kamath, Punit Marathe, Rajeev S. Bhide, Yueping Zhang, Celia D’Arienzo, and Joseph Fargnoli

Subjects

Male, Cancer Research, Drug Evaluation, Preclinical, Administration, Oral, Biological Availability, Mice, Nude, Antineoplastic Agents, Pharmacology, Toxicology, chemistry.chemical_compound, Mice, Dogs, Pharmacokinetics, Oral administration, In vivo, Preclinical pharmacokinetics, Animals, Humans, Pharmacology (medical), Prodrugs, Pyrroles, Tissue Distribution, Alanine, Mice, Inbred BALB C, Dose-Response Relationship, Drug, Chemistry, Triazines, Brain, Prodrug, Vascular Endothelial Growth Factor Receptor-2, Xenograft Model Antitumor Assays, In vitro, Rats, Macaca fascicularis, Brivanib alaninate, Oncology, Solubility, Injections, Intravenous, Female, Caco-2 Cells

Abstract

Brivanib alaninate is a prodrug of brivanib (BMS-540215), a potent oral VEGFR-2 inhibitor and is currently in development for the treatment of hepatocellular and colon carcinomas. In vitro and in vivo studies were conducted to characterize the preclinical pharmacokinetics and disposition of brivanib and brivanib alaninate, and antitumor efficacy in mice bearing human xenografts.In vitro studies were conducted in liver and intestinal fractions, plasma and Caco-2 cells to assess the metabolic stability. Pharmacokinetics of brivanib were determined in preclinical species after administration of single intravenous or oral doses of both brivanib and brivanib alaninate. The antitumor efficacy was assessed at equimolar doses in nude mice bearing human tumor xenografts. Human efficacious dose was predicted based on projected human pharmacokinetic parameters and exposure at efficacious doses in the mouse efficacy models.In vitro and in vivo studies indicated that brivanib alaninate was efficiently converted to brivanib. Brivanib showed good brain penetration in rats consistent with its high intrinsic permeability and lack of active efflux in Caco-2 cells. The oral bioavailability of brivanib varied among species (22-88%) and showed dissolution rate-limited absorption even when combined with organic co-solvents. Administration of brivanib as brivanib alaninate allowed completely aqueous vehicles, and an improvement in the oral bioavailability (55-97%) was observed. The clearance of brivanib in humans is anticipated to be low to intermediate (hepatic extraction ratio0.7), while its volume of distribution is expected to be high. The minimum efficacious dose of brivanib alaninate was determined to be 60 mg/kg per day.Brivanib alaninate is rapidly and efficiently converted to the parent, brivanib, as demonstrated both in vitro and in vivo and offers an excellent mode to deliver brivanib orally.

Published

2008

23. Discovery of brivanib alaninate ((S)-((R)-1-(4-(4-fluoro-2-methyl-1H-indol-5-yloxy)-5-methylpyrrolo[2,1-f][1,2,4]triazin-6-yloxy)propan-2-yl)2-aminopropanoate), a novel prodrug of dual vascular endothelial growth factor receptor-2 and fibroblast growth factor receptor-1 kinase inhibitor (BMS-540215)

Author

Zhen-wei, Cai, Yongzheng, Zhang, Robert M, Borzilleri, Ligang, Qian, Stephanie, Barbosa, Donna, Wei, Xiaoping, Zheng, Lawrence, Wu, Junying, Fan, Zhongping, Shi, Barri S, Wautlet, Steve, Mortillo, Robert, Jeyaseelan, Daniel W, Kukral, Amrita, Kamath, Punit, Marathe, Celia, D'Arienzo, George, Derbin, Joel C, Barrish, Jeffrey A, Robl, John T, Hunt, Louis J, Lombardo, Joseph, Fargnoli, and Rajeev S, Bhide

Subjects

Lung Neoplasms, Drug Evaluation, Preclinical, Administration, Oral, Biological Availability, Mice, Clinical Trials, Phase II as Topic, Microsomes, Animals, Humans, Prodrugs, Pyrroles, Receptor, Fibroblast Growth Factor, Type 1, Protein Kinase Inhibitors, Cell Proliferation, Alanine, Molecular Structure, Triazines, Carcinoma, Water, Stereoisomerism, Vascular Endothelial Growth Factor Receptor-2, Xenograft Model Antitumor Assays, Intestines, Liver, Solubility, Drug Design

Abstract

A series of amino acid ester prodrugs of the dual VEGFR-2/FGFR-1 kinase inhibitor 1 (BMS-540215) was prepared in an effort to improve the aqueous solubility and oral bioavailability of the parent compound. These prodrugs were evaluated for their ability to liberate parent drug 1 in in vitro and in vivo systems. The l-alanine prodrug 8 (also known as brivanib alaninate/BMS-582664) was selected as a development candidate and is presently in phase II clinical trials.

Published

2008

24. Synthesis, SAR, and Evaluation of 4-[2,4-Difluoro-5-(cyclopropylcarbamoyl)phenylamino]pyrrolo[2,1-f][1,2,4]triazine-based VEGFR-2 kinase inhibitors

Author

Joseph Fargnoli, Amrita Kamath, Louis J. Lombardo, Robert M. Borzilleri, Zhen-Wei Cai, John T. Hunt, Robert Jeyaseelan, John S. Tokarski, Barri Wautlet, Benjamin J. Henley, Steven Mortillo, Donna D. Wei, Rajeev S. Bhide, and Ligang Qian

Subjects

Cyclopropanes, Lung Neoplasms, Stereochemistry, medicine.drug_class, Clinical Biochemistry, Pharmaceutical Science, Mice, Nude, Carboxamide, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Cell Line, Tumor, Drug Discovery, medicine, Animals, Cytochrome P-450 Enzyme Inhibitors, Humans, Pyrroles, Kinase activity, Molecular Biology, Protein Kinase Inhibitors, Triazine, chemistry.chemical_classification, Oxadiazoles, biology, Kinase, Triazines, Organic Chemistry, Aromatic amine, Endothelial Cells, Vascular Endothelial Growth Factor Receptor-2, Xenograft Model Antitumor Assays, Enzyme, chemistry, Enzyme inhibitor, biology.protein, Molecular Medicine

Abstract

Introduction of the 2,4-difluoro-5-(cyclopropylcarbamoyl)phenylamino group at the C-4 position of the pyrrolo[2,1-f][1,2,4] triazine scaffold led to the discovery of a novel sub-series of inhibitors of VEGFR-2 kinase activity. Subsequent SAR studies on the 1,3,5-oxadiazole ring appended to the C-6 position of this new sub-family of pyrrolotriazines resulted in the identification of low nanomolar inhibitors of VEGFR-2. Antitumor efficacy was observed with compound 37 against L2987 human lung carcinoma xenografts in athymic mice.

Published

2007

25. Modulation of tight junctions does not predict oral absorption of hydrophilic compounds: use of Caco-2 and Calu-3 cells

Author

Anthony M. Marino, Saeho Chong, Sandra A. Dando, Richard Morrison, Amrita Kamath, and Neil Mathias

Subjects

Absorption (pharmacology), Cell Membrane Permeability, Tight junction, Chemistry, digestive, oral, and skin physiology, Organic Chemistry, Mouth Mucosa, Epithelial Cells, Cell biology, Absorption, Tight Junctions, Pharmaceutical Preparations, Permeability (electromagnetism), Caco-2, Cell culture, Paracellular transport, Drug Discovery, Monolayer, Molecular Medicine, Humans, Calcium, Caco-2 Cells, Relative permeability

Abstract

Permeability estimates using Caco-2 cells do not accurately predict the absorption of hydrophilic drugs that are primarily absorbed via the paracellular pathway. The objective of this study was to investigate whether modulation of tight junctions would help differentiation of paracellularly absorbed compounds. Tight junctions in Caco-2 cell monolayers were manipulated using calcium depletion approaches to decrease the transepithelial electrical resistance (TEER) of the monolayers, and permeability of hydrophilic compounds were measured under these conditions. Permeability of these compounds were also measured in Calu-3 cells, which have tighter junctions than Caco-2 cells. Calcium depletion loosened the tight junctions of Caco-2 cells to varying levels as measured by the decrease in TEER values of the monolayers. While the absolute permeability of all the model compounds increased as the tight junctions were loosened, the ratios of their permeability relative to mannitol permeability were similar. The permeability of these compounds in the tighter Calu-3 cells were also found to be similar to each other. Altering the tight junctions of Caco-2 cells to obtain leakier cell monolayers, or using a cell line with tighter junctions like Calu-3 cells, did not improve differentiation between well absorbed and poorly absorbed hydrophilic drugs. Mere manipulation of the tight junctions to increase or decrease transepithelial electrical resistance does not appear to be a viable approach to predict human absorption for hydrophilic compounds that are primarily absorbed via the paracellular pathway.

Published

2007

26. Correction to N-(Cycloalkylamino)acyl-2-aminothiazole Inhibitors of Cyclin-Dependent Kinase 2. N-[5-[[[5-(1,1-Dimethylethyl)-2-oxazolyl]methyl]thio]-2-thiazolyl]-4-piperidinecarboxamide (BMS-387032), a Highly Efficacious and Selective Antitumor Agent

Author

Hai Yun Xiao, Sunanda A. Ranadive, Kristen A. Kellar, Roberta Batorsky, Urvashi V. Roongta, John T. Hunt, Amrita Kamath, Rulin Zhao, Ligang Qian, Mark S. Bednarz, Kevin R. Webster, Francis Y.F. Lee, Syed Z. Ahmed, Weifang Shan, Nikola P. Pavletich, Kyoung Soo Kim, Stephanie Barbosa, Punit Marathe, John S. Sack, Raj N. Misra, Wen Ching Han, Janet G. Mulheron, S. David Kimball, Tokarski John S, Bang Chi Chen, David B. Rawlins, and Songfeng Lu

Subjects

Antitumor activity, biology, Chemistry, Stereochemistry, Drug Discovery, Cyclin-dependent kinase 2, 2-aminothiazole, biology.protein, Molecular Medicine, Thio

Published

2015

27. Discovery and evaluation of N-cyclopropyl- 2,4-difluoro-5-((2-(pyridin-2-ylamino)thiazol-5- ylmethyl)amino)benzamide (BMS-605541), a selective and orally efficacious inhibitor of vascular endothelial growth factor receptor-2

Author

Robert Jeyaseelan, Steve Mortillo, Joseph Fargnoli, Rajeev S. Bhide, Ligang Qian, George M. Derbin, John T. Hunt, Punit Marathe, Louis J. Lombardo, Amrita Kamath, Xiaoping Zheng, John S. Tokarski, Daniel W. Kukral, Robert M. Borzilleri, Barri Wautlet, Joel C. Barrish, and Celia D’Arienzo

Subjects

Models, Molecular, Umbilical Veins, Stereochemistry, Administration, Oral, Aminopyridines, Mice, Nude, Angiogenesis Inhibitors, In Vitro Techniques, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Non-competitive inhibition, Growth factor receptor, Aminothiazole, Drug Discovery, Animals, Humans, Kinase activity, Benzamide, Cell Proliferation, Binding Sites, biology, Chemistry, Endothelial Cells, Kinase insert domain receptor, Vascular Endothelial Growth Factor Receptor-2, Xenograft Model Antitumor Assays, Rats, Vascular endothelial growth factor, Macaca fascicularis, Thiazoles, Enzyme inhibitor, biology.protein, Molecular Medicine, Endothelium, Vascular

Abstract

Substituted 3-((2-(pyridin-2-ylamino)thiazol-5-ylmethyl)amino)benzamides were identified as potent and selective inhibitors of vascular endothelial growth factor receptor-2 (VEGFR-2) kinase activity. The enzyme kinetics associated with the VEGFR-2 inhibition of 14 (Ki = 49 ± 9 nM) confirmed that the aminothiazole-based analogues are competitive with ATP. Analogue 14 demonstrated excellent kinase selectivity, favorable pharmacokinetic properties in multiple species, and robust in vivo efficacy in human lung and colon carcinoma xenograft models.

Published

2006

28. Discovery and preclinical studies of (R)-1-(4-(4-fluoro-2-methyl-1H-indol-5-yloxy)-5- methylpyrrolo[2,1-f][1,2,4]triazin-6-yloxy)propan- 2-ol (BMS-540215), an in vivo active potent VEGFR-2 inhibitor

Author

Steven Mortillo, Donna D. Wei, Daniel W. Kukral, Viral Vyas, Arvind Mathur, Stephanie Barbosa, Laurence I. Wu, John T. Hunt, Zhen-Wei Cai, Soong-Hoon Kim, Robert Jeyaseelan, Kenneth J. Leavitt, Sam T. Chao, Joseph Fargnoli, Joel C. Barrish, Ligang Qian, Amrita Kamath, Punit Marathe, Xiaoping Zheng, Barri Wautlet, Yong-Zheng Zhang, Leslie Leith, Louis J. Lombardo, Celia D’Arienzo, George M. Derbin, Rajeev S. Bhide, Robert M. Borzilleri, and Aberra Fura

Subjects

Stereochemistry, Transplantation, Heterologous, Mice, Nude, Angiogenesis Inhibitors, chemistry.chemical_compound, Mice, Structure-Activity Relationship, In vivo, Cell Line, Tumor, Drug Discovery, Structure–activity relationship, Animals, Humans, Prodrugs, Pyrroles, Triazine, Mice, Inbred BALB C, Alanine, Triazines, Stereoisomerism, Prodrug, Vascular Endothelial Growth Factor Receptor-2, In vitro, Brivanib alaninate, chemistry, Alkoxy group, Molecular Medicine, Drug Screening Assays, Antitumor, Neoplasm Transplantation, Methyl group

Abstract

A series of substituted 4-(4-fluoro-1H-indol-5-yloxy)pyrrolo[2,1-f][1,2,4]triazine-based inhibitors of vascular endothelial growth factor receptor-2 kinase is reported. Structure-activity relationship studies revealed that a methyl group at the 5-position and a substituted alkoxy group at the 6-position of the pyrrolo[2,1-f][1,2,4]triazine core gave potent compounds. Biochemical potency, kinase selectivity, and pharmacokinetics of the series were optimized and in vitro safety liabilities were minimized to afford BMS-540215 (12), which demonstrated robust preclinical in vivo activity in human tumor xenograft models. The l-alanine prodrug of 12, BMS-582664 (21), is currently under evaluation in clinical trials for the treatment of solid tumors.

Published

2006

29. Multiple pathways are involved in the oral absorption of BMS-262084, a tryptase inhibitor, in rats: role of paracellular transport, binding to trypsin, and P-glycoprotein efflux

Author

Shih-Jung Lan, Richard A. Morrison, Timothy W. Harper, Amrita Kamath, Anthony M. Marino, and Saeho Chong

Subjects

Serine Proteinase Inhibitors, Trypsin inhibitor, education, Pharmaceutical Science, Administration, Oral, Biological Availability, Pharmacology, Intestinal absorption, Piperazines, Tight Junctions, Rats, Sprague-Dawley, medicine, Animals, Humans, Hypoglycemic Agents, Insulin, Aprotinin, Trypsin, ATP Binding Cassette Transporter, Subfamily B, Member 1, Tight junction, Dose-Response Relationship, Drug, Chemistry, digestive, oral, and skin physiology, Serine Endopeptidases, Dipeptides, Intestinal epithelium, Rats, stomatognathic diseases, Dipeptide transport, Injections, Intra-Arterial, Intestinal Absorption, Paracellular transport, Azetidines, Tryptases, Caco-2 Cells, medicine.drug, Protein Binding

Abstract

BMS-262084 is a potent and selective beta-lactam tryptase inhibitor with therapeutic potential for treating asthma. The oral bioavailability of BMS-262084 was low in rats (4% at a dose of 0.5 mg/kg) due to poor absorption. BMS-262084 was excreted mainly unchanged in the urine, suggesting minimal metabolism in rats. The objective of this study was to investigate the mechanisms of oral absorption of BMS-262084 in rats. Modulation of intestinal tight junctions, binding to trypsin, and involvement of the intestinal dipeptide transport system and P-glycoprotein (P-gp) in the absorption of BMS-262084 were examined. Coadministration of BMS-262084 with SQ-29852, a substrate of the intestinal dipeptide transport system, did not change the oral absorption of BMS-262084. An increase in the dose of BMS-262084 from 0.5 to 50 mg/kg resulted in a 3.7-fold increase in its oral absorption. Inulin absorption was enhanced upon coadministration with BMS-262084, suggesting the opening of tight junctions in the intestinal epithelium. Coadministration of aprotinin, a trypsin inhibitor, increased the oral absorption of BMS-262084 several fold. In vitro, using Caco-2 cells, BMS-262084 appeared to be a P-gp substrate, with an efflux ratio of 14. These results suggest that absorption of BMS-262084 is mediated by several concurrent mechanisms. At higher doses of BMS-262084, increased absorption may be primarily due to opening of tight junctions in the intestinal epithelium and consequent absorption via the paracellular pathway, while at lower doses, binding to trypsin may contribute to limiting its absorption. P-gp efflux may also play a role in influencing the absorption of BMS-262084. The intestinal dipeptide transporter system does not appear to be involved in the absorption of BMS-262084.

Published

2005

30. Selective Itk inhibitors block T-cell activation and murine lung inflammation

Author

Steven B. Kanner, Steven H. Spergel, Kim W. McIntyre, Robert M. Townsend, Gena S. Whitney, Robert V. Moquin, David J. Shuster, Joel C. Barrish, Juan J. Perez-Villar, Chunjian Liu, Amrita Kamath, Loran Killar, John H. Dodd, Jagabandhu Das, Xiao Xia Yang, John Wityak, Chen Yi Hung, Jennifer Postelnek, Tai-An Lin, Kathleen D. O'Day, Joseph A. Furch, Hongjian Zhang, Punit Marathe, Becky Penhallow, Arthur M. Doweyko, and James Lin

Subjects

T cell, T-Lymphocytes, Receptors, Antigen, T-Cell, Biology, Lymphocyte Activation, Biochemistry, Jurkat cells, chemistry.chemical_compound, Jurkat Cells, Mice, Cell Line, Tumor, medicine, Respiratory Hypersensitivity, Animals, Humans, Kinase activity, Enzyme Inhibitors, Receptor, Lung, Gene knockout, Mice, Inbred BALB C, Kinase, T-cell receptor, Anti-Inflammatory Agents, Non-Steroidal, Tyrosine phosphorylation, Protein-Tyrosine Kinases, medicine.anatomical_structure, chemistry, Cancer research, Interleukin-2, Immunosuppressive Agents

Abstract

Nonreceptor protein tyrosine kinases including Lck, ZAP-70, and Itk play essential roles in T-cell receptor (TCR) signaling. Gene knockout studies have revealed that mice lacking these individual kinases exhibit various degrees of immunodeficiency; however, highly selective small molecule inhibitors of these kinases as potential immunosuppressive agents have not been identified. Here we discovered two novel compounds, BMS-488516 and BMS-509744, that potently and selectively inhibit Itk kinase activity. The compounds reduce TCR-induced functions including PLCgamma1 tyrosine phosphorylation, calcium mobilization, IL-2 secretion, and T-cell proliferation in vitro in both human and mouse cells. The inhibitors suppress the production of IL-2 induced by anti-TCR antibody administered to mice. BMS-509744 also significantly diminishes lung inflammation in a mouse model of ovalbumin-induced allergy/asthma. Our findings represent the first description of selective inhibitors to probe human Itk function and its associated pathway, and support the hypothesis that Itk is a therapeutic target for immunosuppressive and inflammatory diseases.

Published

2004

31. N-(cycloalkylamino)acyl-2-aminothiazole inhibitors of cyclin-dependent kinase 2. N-[5-[[[5-(1,1-dimethylethyl)-2-oxazolyl]methyl]thio]-2-thiazolyl]-4- piperidinecarboxamide (BMS-387032), a highly efficacious and selective antitumor agent

Author

Weifang Shan, Hai-Yun Xiao, Kyoung S. Kim, Songfeng Lu, Francis Y. Lee, Roberta Batorsky, John S. Sack, John T. Hunt, Raj N. Misra, Rawlins David B, Kevin R. Webster, Amrita Kamath, Sunanda A. Ranadive, S. David Kimball, Urvashi V. Roongta, Kristen A. Kellar, Stephanie Barbosa, Syed Z. Ahmed, Rulin Zhao, Janet G. Mulheron, Wen-Ching Han, John S. Tokarski, Mark S. Bednarz, Nikola P. Pavletich, Ligang Qian, Punit Marathe, and Bang-Chi Chen

Subjects

Models, Molecular, Low protein, Stereochemistry, Transplantation, Heterologous, Thio, Antineoplastic Agents, In Vitro Techniques, Crystallography, X-Ray, Retinoblastoma Protein, Mice, Structure-Activity Relationship, Dogs, Drug Stability, Cell Line, Tumor, Drug Discovery, Cyclin E, CDC2-CDC28 Kinases, Structure–activity relationship, Animals, Humans, Phosphorylation, Oxazoles, Cyclin-dependent kinase 1, biology, Cell-Free System, Molecular Structure, Kinase, Chemistry, Cyclin-dependent kinase 2, Cyclin-Dependent Kinase 2, Rats, Transplantation, Thiazoles, Enzyme inhibitor, biology.protein, Microsomes, Liver, Molecular Medicine, Drug Screening Assays, Antitumor, Neoplasm Transplantation

Abstract

N-Acyl-2-aminothiazoles with nonaromatic acyl side chains containing a basic amine were found to be potent, selective inhibitors of CDK2/cycE which exhibit antitumor activity in mice. In particular, compound 21 [N-[5-[[[5-(1,1-dimethylethyl)-2-oxazolyl]methyl]thio]-2-thiazolyl]-4-piperidinecarboxamide, BMS-387032], has been identified as an ATP-competitive and CDK2-selective inhibitor which has been selected to enter Phase 1 human clinical trials as an antitumor agent. In a cell-free enzyme assay, 21 showed a CDK2/cycE IC(50) = 48 nM and was 10- and 20-fold selective over CDK1/cycB and CDK4/cycD, respectively. It was also highly selective over a panel of 12 unrelated kinases. Antiproliferative activity was established in an A2780 cellular cytotoxicity assay in which 21 showed an IC(50) = 95 nM. Metabolism and pharmacokinetic studies showed that 21 exhibited a plasma half-life of 5-7 h in three species and moderately low protein binding in both mouse (69%) and human (63%) serum. Dosed orally to mouse, rat, and dog, 21 showed 100%, 31%, and 28% bioavailability, respectively. As an antitumor agent in mice, 21 administered at its maximum-tolerated dose exhibited a clearly superior efficacy profile when compared to flavopiridol in both an ip/ip P388 murine tumor model and in a s.c./i.p. A2780 human ovarian carcinoma xenograft model.

Published

2004

32. Discovery of N-(4-(2-Amino-3-chloropyridin-4-yloxy)-3-fluorophenyl)-4-ethoxy-1-(4-fluorophenyl)-2-oxo-1,2-dihydropyridine-3-carboxamide (BMS-777607), a Selective and Orally Efficacious Inhibitor of the Met Kinase Superfamily.

Author

Gretchen M. Schroeder, Yongmi An, Zhen-Wei Cai, Xiao-Tao Chen, Cheryl Clark, Lyndon A. M. Cornelius, Jun Dai, Johnni Gullo-Brown, Ashok Gupta, Benjamin Henley, John T. Hunt, Robert Jeyaseelan, Amrita Kamath, Kyoung Kim, Jonathan Lippy, Louis J. Lombardo, Veeraswamy Manne, Simone Oppenheimer, John S. Sack, and Robert J. Schmidt

Published

2009

33. Discovery of Pyrrolopyridine−Pyridone Based Inhibitors of Met Kinase: Synthesis, X-ray Crystallographic Analysis, and Biological Activities.

Author

Kyoung Soon Kim, Liping Zhang, Robert Schmidt, Zhen-Wei Cai, Donna Wei, David K. Williams, Louis J. Lombardo, George L. Trainor, Dianlin Xie, Yaquan Zhang, Yongmi An, John S. Sack, John S. Tokarski, Celia Darienzo, Amrita Kamath, Punit Marathe, Yueping Zhang, Jonathan Lippy, Robert Jeyaseelan Sr., and Barri Wautlet

Published

2008

34. Correction to N-(Cycloalkylamino)acyl-2-aminothiazole Inhibitorsof Cyclin-Dependent Kinase 2. N-[5-[[[5-(1,1-Dimethylethyl)-2-oxazolyl]methyl]thio]-2-thiazolyl]-4-piperidinecarboxamide(BMS-387032), a Highly Efficacious and Selective Antitumor Agent.

Author

Raj N. Misra, Hai-yun Xiao, Kyoung S. Kim, Songfeng Lu, Wen-Ching Han, Stephanie A. Barbosa, John T. Hunt, David B. Rawlins, Weifang Shan, Syed Z. Ahmed, Ligang Qian, Bang-Chi Chen, Rulin Zhao, Mark S. Bednarz, Kristen A. Kellar, Janet G. Mulheron, Roberta Batorsky, Urvashi Roongta, Amrita Kamath, and Punit Marathe

Published

2015