Your search keyword '"Bantia S"' showing total 79 results

1. In vitro efficacy of forodesine and nelarabine (ara-G) in pediatric leukemia

Author

Homminga, I. (Irene), Zwaan, C.M. (Michel), Manz, C.Y. (Chantal), Parker, C. (Cynthia), Bantia, S. (Shanta), Smits, W.K., Higginbotham, F. (Fiona), Pieters, R. (Rob), Meijerink, J.P.P. (Jules), Homminga, I. (Irene), Zwaan, C.M. (Michel), Manz, C.Y. (Chantal), Parker, C. (Cynthia), Bantia, S. (Shanta), Smits, W.K., Higginbotham, F. (Fiona), Pieters, R. (Rob), and Meijerink, J.P.P. (Jules)

Abstract

Forodesine and nelarabine (the pro-drug of ara-G) are 2 nucleoside analogues with promising anti-leukemic activity. To better understand which pediatric patients might benefit from forodesine or nelarabine (ara-G) therapy, we investigated the in vitro sensitivity to these drugs in 96 diagnostic pediatric leukemia patient samples and the mRNA expression levels of different enzymes involved in nucleoside metabolism. Forodesine and ara-G cytotoxicities were higher in T-cell acute lymphoblastic leukemia (T-ALL) samples than in B-cell precursor (BCP)-ALL and acute myeloid leukemia (AML) samples. Resistance to forodesine did not preclude ara-G sensitivity and vice versa, indicating that both drugs rely on different resistance mechanisms. Differences in sensitivity could be partly explained by significantly higher accumulation of intra-cellular dGTP in forodesine-sensitive samples compared with resistant samples, and higher mRNA levels of dGK but not dCK. The mRNA levels of the transporters ENT1 and ENT2 were higher in ara-G-sensitive than -resistant samples. We conclude that especially T-ALL, but also BCP-ALL, pediatric patients may benefit from forodesine or nelarabine (ara-G) treatment.

Published

2011

2. OP0106 Effect of BCX4208 add-on therapy to allopurinol 300 mg on plasma hypoxanthine and xanthine concentrations in gout patients

Author

Bantia, S., primary, Parker, C., additional, Harman, L., additional, Papac, D., additional, and Hollister, A., additional

Published

2013

3. FRI0401 BCX4208, a novel enzyme inhibitor for chronic management of GOUT, shows a low risk of potential drug-drug interactions

Author

Bantia, S., primary, Harman, L., additional, Hollister, A., additional, and Pearson, P., additional

Published

2013

4. Discovery of Highly Potent Small Molecule Kallikrein Inhibitors

Author

Zhang, J., primary, Krishnan, R., additional, Arnold, C., additional, Mattsson, E., additional, Kilpatrick, J., additional, Bantia, S., additional, Dehghani, A., additional, Boudreaux, B., additional, Gupta, S., additional, Kotian, P.L., additional, Chand, P., additional, and Babu, Y.S., additional

Published

2006

5. Comparison of the Anti-Influenza Virus Activity of RWJ-270201 with Those of Oseltamivir and Zanamivir

Author

Bantia, S., primary, Parker, C. D., additional, Ananth, S. L., additional, Horn, L. L., additional, Andries, K., additional, Chand, P., additional, Kotian, P. L., additional, Dehghani, A., additional, El-Kattan, Y., additional, Lin, T., additional, Hutchison, T. L., additional, Montgomery, J. A., additional, Kellog, D. L., additional, and Babu, Y. S., additional

Published

2001

6. Guanidinobenzoic acid inhibitors of influenza virus neuraminidase 1 1Edited by R. Huber

Author

Sudbeck, E.A, primary, Jedrzejas, M.J, additional, Singh, S, additional, Brouillette, W.J, additional, Air, G.M, additional, Laver, W.G, additional, Babu, Y.S, additional, Bantia, S, additional, Chand, P, additional, Chu, N, additional, Montgomery, J.A, additional, Walsh, D.A, additional, and Luo, M, additional

Published

1997

7. Crystal structure of influenza virus neuraminidase with inhibitor 3,5-diguanidino-4-(N-acetylamino)benzoic acid

Author

Sudbeck, E. A., primary, Jedrzejas, M. J., additional, Singh, S., additional, Brouillette, W. J., additional, Air, G. M., additional, Laver, W. G., additional, Babu, Y. S., additional, Bantia, S., additional, Chand, P., additional, Chu, N., additional, Montgomery, J. A., additional, Walsh, D. A., additional, and Luo, M., additional

Published

1996

8. Fibrinogen Baltimore I: polymerization defect associated with a gamma 292Gly----Val (GGC----GTC) mutation

Author

Bantia, S, primary, Mane, SM, additional, Bell, WR, additional, and Dang, CV, additional

Published

1990

9. Polymerization defect of fibrinogen Baltimore III due to a gamma Asn308- ---Ile mutation

Author

Bantia, S, primary, Bell, WR, additional, and Dang, CV, additional

Published

1990

10. Syntheses and Neuraminidase Inhibitory Activity of Multisubstituted Cyclopentane Amide Derivatives

Author

Chand, P., Babu, Y. S., Bantia, S., Rowland, S., Dehghani, A., Kotian, P. L., Hutchison, T. L., Ali, S., Brouillette, W., El-Kattan, Y., and Lin, T.-H.

Abstract

In further studies aimed toward identifying effective and safe inhibitors of influenza neuraminidases, we synthesized a series of multisubstituted cyclopentane amide derivatives. Amides prepared were 14 examples of N-substituted alkyl or aralkyl types from primary amines, 13 examples of the N,N-disubstituted alkyl, aralkyl, or substituted-alkyl type from secondary amines, and 12 examples from cycloaliphatic or substituted cycloaliphatic secondary amines. These compounds bearing two chiral centers, at position-1 in the ring and position-1‘ in the side chain attached at position 3, were tested for their ability to inhibit A and B forms of influenza neuraminidase. The 1-ethylpropylamide, diethylamide, dipropylamide, and 4-morpholinylamide showed very good inhibitory activity (IC50 = 0.015−0.080 μM) vs the neuraminidase A form, but modest activity (IC50 = 3.0−9.2 μM) vs the neuraminidase B form. Since the parent amides bear two chiral centers (C-1 and C-1‘), three of the better inhibitors were tested at higher levels of diastereomeric purity. The diastereomers corresponding to the active forms of the 1-(ethyl)propylamide, the diethylamide, and the dipropylamide (all of the same configuration at the C-1‘ chiral center), and the diastereomer of the diethylamide representing the active form at both C-1‘ and C-1 were isolated or synthesized from precursors that were isolated as diastereomers. These diastereomers showed some improvement in neuraminidase inhibition over the parent diastereomeric mixtures. 1-Carboxy-1-hydroxy derivatives of the best active compounds, the diethylamide and the dipropylamide, were also prepared. These compounds were not as active as the compounds without the 1-hydroxy group. In an in vivo study, the C-1‘ active isomer of the diethylamide from the 1-carboxy series was tested in influenza-infected mice by oral and intranasal administration and found to be very effective only intranasally in preventing weight loss at doses as low as 0.1 (mg/kg)/day.

Published

2004

11. Systematic Structure-Based Design and Stereoselective Synthesis of Novel Multisubstituted Cyclopentane Derivatives with Potent Antiinfluenza Activity

Author

Chand, P., Kotian, P. L., Dehghani, A., El-Kattan, Y., Lin, T.-H., Hutchison, T. L., Babu, Y. S., Bantia, S., Elliott, A. J., and Montgomery, J. A.

Abstract

The design and synthesis of novel, orally active, potent, and selective inhibitors of influenza neuraminidase differing structurally from existing neuraminidase inhibitors are described. X-ray crystal structures of complexes of neuraminidase with known five- and six-membered ring inhibitors revealed that potent inhibition of the enzyme is determined by the relative positions of the interacting inhibitor substituents (carboxylate, glycerol, acetamido, hydroxyl) rather than by the absolute position of the central ring. This led us to design potential neuraminidase inhibitors in which the cyclopentane ring served as a scaffold for substituents (carboxylate, guanidino, acetamido, alkyl) that would interact with the four binding pockets of the neuraminidase active site at least as effectively as those of the established six-membered ring inhibitors such as DANA (2), zanamivir (3), and oseltamivir (4). A mixture of the isomers was prepared initially. Protein crystallography of inhibitor−enzyme complexes was used to screen mixtures of isomers in order to identify the most active stereoisomer. A synthetic route to the identified candidate 50 was developed, which featured (3 + 2) cycloaddition of 2-ethylbutyronitrile oxide to methyl (1S,4R)-4[(tert-butoxycarbonyl)amino]cyclopent-2-ene-1-carboxylate (43). Structures of the synthetic compounds were verified by NMR spectroscopy using nuclear Overhauser effect methodology. Two new neuraminidase inhibitors discovered in this work, 50 and 54, have IC50 values vs neuraminidase from influenza A and B of <1 and <10 nM, respectively. These IC50 values are comparable or superior to those for zanamivir and oseltamivir, agents recently approved by the FDA for treatment of influenza. The synthetic route used to prepare 50 and 54 was refined so that synthesis of pure active isomer 54, which has five chiral centers, required only seven steps from readily available intermediates. Further manipulation was required to prepare deoxy derivative 50. Because the activities of the two compounds are comparable and 54 [RWJ-270201 (BCX-1812)] is the easier to synthesize, it was selected for further clinical evaluation.

Published

2001

12. Purine nucleoside phosphorylase inhibitor BCX-1777 (Immucillin-H)-a novel potent and orally active immunosuppressive agent

Author

Bantia, S., Miller, P. J., Parker, C. D., Ananth, S. L., Horn, L. L., Kilpatrick, J. M., Morris, P. E., Hutchison, T. L., Montgomery, J. A., and Sandhu, J. S.

Published

2001

13. BCX-1812 (RWJ-270201):  Discovery of a Novel, Highly Potent, Orally Active, and Selective Influenza Neuraminidase Inhibitor through Structure-Based Drug Design

Author

Babu, Y. S., Chand, P., Bantia, S., Kotian, P., Dehghani, A., El-Kattan, Y., Lin, T.-H., Hutchison, T. L., Elliott, A. J., Parker, C. D., Ananth, S. L., Horn, L. L., Laver, G. W., and Montgomery, J. A.

Published

2000

14. Potent Inhibition of Influenza Sialidase by a Benzoic Acid Containing a 2-Pyrrolidinone Substituent

Author

Atigadda, V. R., Duarte, F., Ali, S. M., Babu, Y. S., Bantia, S., Chand, P., Chu, N., Montgomery, J. A., Walsh, D. A., Sudbeck, E. A., Finley, J., Luo, M., Air, G. M., Laver, G. W., and Brouillette, W. J.

Abstract

On the basis of the lead compound 4-(N-acetylamino)-3-guanidinobenzoic acid (BANA 113), which inhibits influenza A sialidase with a Ki of 2.5 μM, several novel aromatic inhibitors of influenza sialidases were designed. In this study the N-acetyl group of BANA 113 was replaced with a 2-pyrrolidinone ring, which was designed in part to offer opportunities for introduction of spatially directed side chains that could potentially interact with the 4-, 5-, and/or 6-subsites of sialidase. While the parent structure 1-(4-carboxy-2-guanidinophenyl)pyrrolidin-2-one (8) was only a modest inhibitor of sialidase, the introduction of a hydroxymethyl or bis(hydroxymethyl) substituent at the C5‘ position of the 2-pyrrolidinone ring resulted in inhibitors (9 and 12, respectively) with low micromolar activity. Crystal structures of these inhibitors in complex with sialidase demonstrated that the substituents at the 5‘-position of the 2-pyrrolidinone ring interact in the 4- and/or 5-subsites of the enzyme. Replacement of the guanidine in 12 with a hydrophobic 3-pentylamino group resulted in a large enhancement in binding to produce an inhibitor (14) with an IC50 of about 50 nM against influenza A sialidase, although the inhibition of influenza B sialidase was 2000-fold less. This represents the first reported example of a simple, achiral benzoic acid with potent (low nanomolar) activity as an inhibitor of influenza sialidase.

Published

1999

15. Design of benzoic acid inhibitors of influenza neuraminidase containing a cyclic substitution for the N-acetyl grouping

Author

Brouillette, W.J., Atigadda, V.R., Luo, M., Air, G.M., Babu, Y.S., and Bantia, S.

Published

1999

16. Discovery of highly potent small molecule kallikrein inhibitors

Author

Zhang, J., Kirshnan, R., Arnold, C.S., Mattsson, E., Kilpatrick, J.M., Bantia, S., Dehghani, A., Boudreaux, B., Gupta, S.N., Kotian, P.L., Chand, P., and Babu, Y.S.

Published

2007

17. Design and Synthesis of Benzoic Acid Derivatives as Influenza Neuraminidase Inhibitors Using Structure-Based Drug Design<SUP>1</SUP><BBR RID="jm970479eb00001">

Author

Chand, P., Babu, Y. S., Bantia, S., Chu, N., Cole, L. B., Kotian, P. L., Laver, W. G., Montgomery, J. A., Pathak, V. P., Petty, S. L., Shrout, D. P., Walsh, D. A., and Walsh, G. M.

Abstract

A series of 94 benzoic acid derivatives was synthesized and tested for its ability to inhibit influenza neuraminidase. The enzyme−inhibitor complex structure was determined by X-ray crystallographic analysis for compounds which inhibited the enzyme. The most potent compound tested in vitro, 5 (4-(acetylamino)-3-guanidinobenzoic acid), had an IC50 = 2.5 × 10^-6 M against N9 neuraminidase. Compound 5 was oriented in the active site of the neuraminidase in a manner that was not predicted from the reported active site binding of GANA (4) with neuraminidase. In a mouse model of influenza, 5 did not protect the mice from weight loss due to the influenza virus when dosed intranasally.

Published

1997

18. Guanidinobenzoic acid inhibitors of influenza virus neuraminidase 11Edited by R. Huber

Author

Sudbeck, E.A, Jedrzejas, M.J, Singh, S, Brouillette, W.J, Air, G.M, Laver, W.G, Babu, Y.S, Bantia, S, Chand, P, Chu, N, Montgomery, J.A, Walsh, D.A, and Luo, M

Abstract

The active site of influenza virus neuraminidase (NA) is formed by 11 universally conserved residues. A guanidino group incorporated into two unrelated NA inhibitors was previously reported to occupy different negatively charged sites in the NA active site. A new inhibitor containing two guanidino groups was synthesized in order to utilize both sites in an attempt to acquire a combined increase in affinity. The X-ray crystal structures of the complexes show that the expected increase in affinity could not be achieved even though the added guanidino group binds to the negatively charged site as designed. This suggests that the ligand affinity to the target protein is contributed both from ligand-protein interactions and solvation/conformation energy of the ligand.

Published

1997

19. Synthesis of a Potent Transition-State Inhibitor of 5‘-Deoxy-5‘-methylthioadenosine Phosphorylase

Author

Kamath, V. P., Ananth, S., Bantia, S., and Morris, P. E., Jr.

Abstract

Human 5‘-deoxy-5‘-methylthioadenosine phosphorylase (MTAP) participates in the purine salvage pathway to generate adenine and methylthioribose-1-phosphate, which in turn is converted into adenine nucleotides and methionine. Hence, inhibition of MTA phosphorylase may be an effective target in the design of potential antiproliferative agents. Presented herein is the synthesis of 2-(4-amino-5H-pyrrolo[3,2-d]pyrimidin-7-yl)-5-methylsulfanylmethylpyrrolidin-3,4-diol (1), a potent inhibitor of MTAP.

Published

2004

20. ChemInform Abstract: KINETICS OF DECARBOXYLATION OF THE TWO EPIMERS OF 5‐TERT‐BUTYL‐1‐METHYL‐2‐OXOCYCLOHEXANECARBOXLIC ACID: LACK OF STEREOELECTRONIC CONTROL IN β‐KETO ACID DECARBOXYLATION

Author

KAYSER, R. H., primary, BRAULT, M., additional, POLLACK, R. M., additional, BANTIA, S., additional, and SADOFF, S. F., additional

Published

1984

21. ChemInform Abstract: MODIFICATION OF AN ENZYME CARBOXYLATE RESIDUE IN THE INHIBITION OF 3‐OXO‐Δ5‐STEROID ISOMERASE BY (3S)‐SPIRO(5α‐ANDROSTANE‐3,2′‐OXIRANE)‐17β‐OL. IMPLICATIONS FOR THE MECHANISM OF ACTION

Author

BEVINS, C. L., primary, BANTIA, S., additional, POLLACK, R. M., additional, BOUNDS, P. L., additional, and KAYSER, R. H., additional

Published

1984

22. ChemInform Abstract: Kinetics and Mechanism of the Ketonization of a Conjugated Trienol.

Author

DZINGELESKI, G. D., primary, BANTIA, S., additional, BLOTNY, G., additional, and POLLACK, R. M., additional

Published

1988

23. ChemInform Abstract: Evidence for an Enol Intermediate in the 3-Oxo-Δ5-steroid Isomerase Catalyzed Isomerization of Δ5 Ketones.

Author

BANTIA, S., primary and POLLACK, R. M., additional

Published

1986

24. Synthesis and biological evaluation of Ribo 7-N/O/S pyrimidine 9-deaza C-nucleoside analogs as new antiviral agents for inhibiting HCV RNA-dependent RNA polymerases.

Author

Wu M, Vadlakonda S, El-Kattan Y, Ghosh A, Lin TH, Chambers-Wilson R, Cheng X, Bantia S, Kellogg-Yelder D, Chand P, Babu YS, and Kotian PL

Subjects

Humans, Nucleosides pharmacology, Hepacivirus, RNA-Dependent RNA Polymerase, Adenosine, Antiviral Agents, Pyrimidine Nucleosides pharmacology, Hepatitis C drug therapy

Abstract

Hepatitis C infection is caused by the bloodborne pathogen hepatitis C virus (HCV) and can lead to serious liver diseases and, ultimately, death if the treatment is ineffective. This work reports the synthesis and preclinical evaluation of 7 novel 9-O/N/S pyrimidine nucleosides, including compound 12, the triphosphate of known compound 7b. The nucleosides are 9-deaza modifications of adenosine and guanosine with β-2'-C-methyl substituent on the ribose. Within this series of compounds, a 9-deaza furopyrimidine analog of adenosine, compound 7b, showed high anti-HCV activity in vitro, good stability, low toxicity, and low genotoxicity when administrated in low doses, and an adequate pharmacokinetics profile. An improved synthesis of compound 7b compared to a previous study is also reported. Compound 12 was synthesized as a control to verify phosphorylation of 7b occurred in vivo., Competing Interests: Declaration of competing interest This research did not receive any specific grant from funding agencies in the public, commercial, or not-for-profit sectors. BioCryst Pharmaceuticals Inc funded all studies. The authors declare the follow-ing competing financial interest(s): All authors are employees/former employees of BioCryst Pharmaceuti-cals Inc. and may hold stock in the same., (Copyright © 2023 Elsevier Masson SAS. All rights reserved.)

Published

2024

25. Synthesis of novel azasugar-containing 2'β-C-Me 9-deaza nucleosides as potential anti-hepatitis C virus agents.

Author

Kotian PL, Wu M, Ghosh A, Polach KJ, El-Kattan Y, Kumar VS, Lin TH, Cheng X, Bantia S, Raman K, Chand P, and Babu YS

Subjects

Humans, Hepacivirus, Antiviral Agents, Nucleosides, Hepatitis C drug therapy

Abstract

As a part of our ongoing discovery efforts exploring azasugar as agents for treating various unmet medical needs, we prepared analogs of azasugar as potential anti-hepatitis C virus (HCV) agents. Herein we describe the synthesis of novel 2'β-C-Me 9-deazanucleoside azasugar analogs.

Published

2023

26. Purine nucleoside phosphorylase enables dual metabolic checkpoints that prevent T cell immunodeficiency and TLR7-associated autoimmunity.

Author

Abt ER, Rashid K, Le TM, Li S, Lee HR, Lok V, Li L, Creech AL, Labora AN, Mandl HK, Lam AK, Cho A, Rezek V, Wu N, Abril-Rodriguez G, Rosser EW, Mittelman SD, Hugo W, Mehrling T, Bantia S, Ribas A, Donahue TR, Crooks GM, Wu TT, and Radu CG

Subjects

Animals, Autoimmunity, Humans, Mice, Purine Nucleosides, T-Lymphocytes, Toll-Like Receptor 7, Immunologic Deficiency Syndromes, Purine-Nucleoside Phosphorylase genetics, Purine-Nucleoside Phosphorylase metabolism

Abstract

Purine nucleoside phosphorylase (PNP) enables the breakdown and recycling of guanine nucleosides. PNP insufficiency in humans is paradoxically associated with both immunodeficiency and autoimmunity, but the mechanistic basis for these outcomes is incompletely understood. Here, we identify two immune lineage-dependent consequences of PNP inactivation dictated by distinct gene interactions. During T cell development, PNP inactivation is synthetically lethal with downregulation of the dNTP triphosphohydrolase SAMHD1. This interaction requires deoxycytidine kinase activity and is antagonized by microenvironmental deoxycytidine. In B lymphocytes and macrophages, PNP regulates Toll-like receptor 7 signaling by controlling the levels of its (deoxy)guanosine nucleoside ligands. Overriding this regulatory mechanism promotes germinal center formation in the absence of exogenous antigen and accelerates disease in a mouse model of autoimmunity. This work reveals that one purine metabolism gene protects against immunodeficiency and autoimmunity via independent mechanisms operating in distinct immune lineages and identifies PNP as a potentially novel metabolic immune checkpoint.

Published

2022

27. Correction to: Treatment duration with immune-based therapies in Cancer: an enigma.

Author

Bantia S and Choradia N

Abstract

Following publication of the original article [1], the authors reported an error in the typesetting of their article. The first section of the main text was mistakenly included in the abstract.

Published

2019

28. Treatment duration with immune-based therapies in Cancer: an enigma.

Author

Bantia S and Choradia N

Subjects

Clinical Trials as Topic, Drug Administration Schedule, Humans, Immunotherapy, Neoplasms immunology, Antineoplastic Agents, Immunological administration & dosage, Neoplasms drug therapy

Abstract

Unlike chemotherapy treatments that target the tumor itself (rather nonspecifically), immune-based therapies attempt to harness the power of an individual patient's immune system to combat cancer. Similar to chemotherapeutic agents, the dosage and Administration section of labeling for all five currently approved PD-1/PD-L1 inhibitors (immunotherapy) recommends duration of treatment until disease progression or unacceptable toxicity. Overactivation or constitutive activation of the immune system with immune based therapies can lead to T-cell exhaustion and activation induced cell death (AICD) in T- and B-cells. Examples of immune exhaustion and T-cell depletion is noted in preclinical and clinical studies. Overactivation or constitutive activation leading to Immune exhaustion is a real phenomenon and of profound concern as immune cells are the true arsenal for control of the tumor growth. Designing trials rigorously to address the optimum treatment duration with immune based therapies is critical. By addressing this concern now, not only we may improve patient outcomes, but also gather a deeper understanding of the role and mechanisms of the immune system in the control of tumor growth.Chemotherapy and immune-based therapies provide antitumor effects through completely different mechanisms. Chemotherapeutic agents are cytotoxic in that they directly inhibit basic cellular mechanisms, killing both malignant and nonmalignant cells (hopefully with a preference for malignant cells), while immune based therapies wake-up the host immune system to recognize malignant cells and eliminate them.While there is a burgeoning excitement surrounding development of immune based therapies for the treatment of cancer, the optimal duration for these therapies need to be explored with equal fervor. Dosing for chemotherapy has been determined over years through large-scale prospective randomized trials to pinpoint the dose which maximizes therapeutic effect while minimizing side effects. Also, due to the mechanism of chemotherapeutic action, the duration of treatment with these agents is generally until disease progression or patient intolerance. However, experience with immune based therapies is limited, with current dosing and duration guidelines based primarily on initial trials required for approval of the agents. Since immune based therapies work by activating the body's own immune system, there is concern that overactivation or constitutive activation of the immune system may lead to immune exhaustion and depletion of effector T-cells thereby causing decreased anti-tumor effects and possible allowing for tumor progression.Similar to chemotherapeutic agents, the Dosage and Administration section of labeling for all five currently approved PD-1/PD-L1 inhibitors recommends duration of treatment until disease progression or unacceptable toxicity. However, since immune based therapies work with a completely different mechanism compared to chemotherapy, using the same therapy duration may not be the optimal approach.In exploring treatment duration with immune based therapies, we need to answer the following: (1) does indefinite treatment with immune based therapies exhaust the immune system counteracting its own mechanism of action leading to tumor progression and (2) how can clinical trials be designed to identify the optimal duration of immune-based therapy that prevents immune cell exhaustion but supports anti-tumor immunity.

Published

2018

29. BCX4430, a novel nucleoside analog, effectively treats yellow fever in a Hamster model.

Author

Julander JG, Bantia S, Taubenheim BR, Minning DM, Kotian P, Morrey JD, Smee DF, Sheridan WP, and Babu YS

Subjects

Adenine analogs & derivatives, Adenosine analogs & derivatives, Adenosine therapeutic use, Alanine Transaminase blood, Animals, Antibodies, Neutralizing blood, Antibodies, Viral blood, Cells, Cultured, Cricetinae, Disease Models, Animal, Female, Mesocricetus, Pyrrolidines, Treatment Outcome, Viral Plaque Assay, Viremia drug therapy, Viremia virology, Yellow Fever mortality, Yellow Fever virology, Antiviral Agents therapeutic use, Purine Nucleosides therapeutic use, Yellow Fever drug therapy, Yellow fever virus drug effects, Yellow fever virus immunology

Abstract

No effective antiviral therapies are currently available to treat disease after infection with yellow fever virus (YFV). A Syrian golden hamster model of yellow fever (YF) was used to characterize the effect of treatment with BCX4430, a novel adenosine nucleoside analog. Significant improvement in survival was observed after treatment with BCX4430 at 4 mg/kg of body weight per day dosed intraperitoneally (i.p.) twice daily (BID). Treatment with BCX4430 at 12.5 mg/kg/day administered i.p. BID for 7 days offered complete protection from mortality and also resulted in significant improvement of other YF disease parameters, including weight loss, serum alanine aminotransferase levels (6 days postinfection [dpi]), and viremia (4 dpi). In uninfected hamsters, BCX4430 at 200 mg/kg/day administered i.p. BID for 7 days was well tolerated and did not result in mortality or weight loss, suggesting a potentially wide therapeutic index. Treatment with BCX4430 at 12 mg/kg/day i.p. remained effective when administered once daily and for only 4 days. Moreover, BCX4430 dosed at 200 mg/kg/day i.p. BID for 7 days effectively treated YF, even when treatment was delayed up to 4 days after virus challenge, corresponding with peak viral titers in the liver and serum. BCX4430 treatment did not preclude a protective antibody response, as higher neutralizing antibody (nAb) concentrations corresponded with increasing delays of treatment initiation, and greater nAb responses resulted in the protection of animals from a secondary challenge with YFV. In summary, BCX4430 is highly active in a hamster model of YF, even when treatment is initiated at the peak of viral replication., (Copyright © 2014, American Society for Microbiology. All Rights Reserved.)

Published

2014

30. Protection against filovirus diseases by a novel broad-spectrum nucleoside analogue BCX4430.

Author

Warren TK, Wells J, Panchal RG, Stuthman KS, Garza NL, Van Tongeren SA, Dong L, Retterer CJ, Eaton BP, Pegoraro G, Honnold S, Bantia S, Kotian P, Chen X, Taubenheim BR, Welch LS, Minning DM, Babu YS, Sheridan WP, and Bavari S

Subjects

Adenine analogs & derivatives, Administration, Oral, Animals, Antiviral Agents administration & dosage, Antiviral Agents chemistry, Antiviral Agents pharmacokinetics, DNA-Directed RNA Polymerases antagonists & inhibitors, DNA-Directed RNA Polymerases metabolism, Disease Models, Animal, Ebolavirus drug effects, Filoviridae enzymology, Hemorrhagic Fever, Ebola prevention & control, Hemorrhagic Fever, Ebola virology, Humans, Injections, Intramuscular, Macaca fascicularis virology, Marburg Virus Disease prevention & control, Marburg Virus Disease virology, Marburgvirus drug effects, Purine Nucleosides administration & dosage, Purine Nucleosides chemistry, Purine Nucleosides pharmacokinetics, Pyrrolidines, RNA biosynthesis, Time Factors, Adenosine analogs & derivatives, Antiviral Agents pharmacology, Filoviridae drug effects, Filoviridae Infections prevention & control, Filoviridae Infections virology, Purine Nucleosides pharmacology

Abstract

Filoviruses are emerging pathogens and causative agents of viral haemorrhagic fever. Case fatality rates of filovirus disease outbreaks are among the highest reported for any human pathogen, exceeding 90% (ref. 1). Licensed therapeutic or vaccine products are not available to treat filovirus diseases. Candidate therapeutics previously shown to be efficacious in non-human primate disease models are based on virus-specific designs and have limited broad-spectrum antiviral potential. Here we show that BCX4430, a novel synthetic adenosine analogue, inhibits infection of distinct filoviruses in human cells. Biochemical, reporter-based and primer-extension assays indicate that BCX4430 inhibits viral RNA polymerase function, acting as a non-obligate RNA chain terminator. Post-exposure intramuscular administration of BCX4430 protects against Ebola virus and Marburg virus disease in rodent models. Most importantly, BCX4430 completely protects cynomolgus macaques from Marburg virus infection when administered as late as 48 hours after infection. In addition, BCX4430 exhibits broad-spectrum antiviral activity against numerous viruses, including bunyaviruses, arenaviruses, paramyxoviruses, coronaviruses and flaviviruses. This is the first report, to our knowledge, of non-human primate protection from filovirus disease by a synthetic drug-like small molecule. We provide additional pharmacological characterizations supporting the potential development of BCX4430 as a countermeasure against human filovirus diseases and other viral diseases representing major public health threats.

Published

2014

31. Preclinical and clinical evaluation of forodesine in pediatric and adult B-cell acute lymphoblastic leukemia.

Author

Balakrishnan K, Ravandi F, Bantia S, Franklin A, and Gandhi V

Subjects

Acute Disease, Adolescent, Adult, Apoptosis drug effects, Child, Child, Preschool, Deoxycytidine Kinase metabolism, Deoxyguanine Nucleotides metabolism, Female, Humans, Infant, Male, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma metabolism, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma pathology, Young Adult, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Purine Nucleosides pharmacology, Purine Nucleosides therapeutic use, Pyrimidinones pharmacology, Pyrimidinones therapeutic use

Abstract

Background: The discovery that purine nucleoside phosphorylase (PNP) deficiency leads to T-cell lymphopenia was the basis for introducing PNP inhibitors for T-cell leukemias. Forodesine is an orally bioavailable PNP inhibitor with picomolar potency. Because T lymphoblasts and indolent chronic lymphocytic leukemia (CLL) B cells inherently elicit favorable pharmacokinetics to accumulate deoxyguanosine triphosphate (dGTP), forodesine demonstrated promising activity in preclinical and clinical settings for patients with T-cell acute lymphoblastic leukemia (T-ALL) and B-cell CLL (B-CLL). However, the use of forodesine in B-cell ALL (B-ALL) is unknown., Patients and Methods: Leukemic blasts obtained from pediatric patients with de novo B-ALL (n = 10) were incubated with forodesine and deoxyguanosine (dGuo), and the biological end points of apoptosis, intracellular dGTP accumulation, and inhibition of RNA and DNA synthesis were measured. Additionally, adult patients with B-ALL (n = 2) were intravenously infused with 80 mg/m(2)/d daily for 5 days. After therapy, clinical response, toxicity, laboratory biomarkers including PNP enzyme inhibition, and plasma forodesine, dGuo, and intracellular dGTP levels were analyzed., Results: Our in vitro investigations demonstrated that forodesine treatment inhibited proliferation and induced modest apoptosis in de novo B-ALL lymphoblasts. There was time-dependent accumulation of dGTP and inhibition of RNA and DNA synthesis. During therapy, neither patient achieved a complete response (CR), but there was disease stabilization for several weeks in both patients. There was significant maintained inhibition of PNP enzyme in red blood cells, accumulation of forodesine and dGuo in plasma, and intracellular dGTP accumulation in both patients., Conclusion: Our preclinical and clinical investigations suggest that forodesine has activity in B-ALL. However, it needs to be either infused with dGuo or combined with established chemotherapeutic agents based on mechanistic rationale., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

32. Characterization of the binding affinities of peramivir and oseltamivir carboxylate to the neuraminidase enzyme.

Author

Bantia S, Upshaw R, and Babu YS

Subjects

Acids, Carbocyclic, Antiviral Agents pharmacology, Buffers, Drug Combinations, Drug Interactions, Drug Resistance, Viral drug effects, Enzyme Inhibitors pharmacology, Humans, Influenza, Human virology, Neuraminidase metabolism, Oseltamivir pharmacology, Protein Binding, Solutions, Spectrometry, Fluorescence, Viral Proteins metabolism, Cyclopentanes pharmacology, Guanidines pharmacology, Influenza A Virus, H1N1 Subtype drug effects, Influenza A Virus, H1N1 Subtype enzymology, Influenza, Human drug therapy, Neuraminidase antagonists & inhibitors, Oseltamivir analogs & derivatives, Viral Proteins antagonists & inhibitors

Abstract

With the continued threat of morbidity and mortality from influenza and the development of resistance to influenza antiviral drugs, there is increasing interest in new treatments, such as the investigational intravenous drug peramivir, and in combination treatments. In this study, we determined the impact of oseltamivir carboxylate on the binding affinity of peramivir/neuraminidase (NA) enzyme complex and vice versa. Influenza NA was incubated with peramivir and oseltamivir carboxylate alone and in combination. Dissociation rates of the enzyme-inhibitor complex measured in the presence of NA substrate for peramivir alone and the combination were similar, suggesting that peramivir competitively inhibits the neuraminidase enzyme and that oseltamivir carboxylate when added to peramivir does not impact the binding affinity of peramivir to the NA enzyme., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2011

33. In vitro efficacy of forodesine and nelarabine (ara-G) in pediatric leukemia.

Author

Homminga I, Zwaan CM, Manz CY, Parker C, Bantia S, Smits WK, Higginbotham F, Pieters R, and Meijerink JP

Subjects

Cell Line, Tumor, Child, Deoxycytidine Kinase genetics, Deoxyguanine Nucleotides metabolism, Drug Resistance, Neoplasm, Equilibrative Nucleoside Transporter 1 genetics, Equilibrative-Nucleoside Transporter 2 genetics, Gene Expression, Humans, In Vitro Techniques, Leukemia, Myeloid, Acute genetics, Leukemia, Myeloid, Acute metabolism, Leukemia, Prolymphocytic, B-Cell genetics, Leukemia, Prolymphocytic, B-Cell metabolism, Phosphotransferases (Alcohol Group Acceptor) genetics, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma genetics, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma metabolism, Purines metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, RNA, Neoplasm genetics, RNA, Neoplasm metabolism, Antineoplastic Agents therapeutic use, Arabinonucleosides therapeutic use, Leukemia, Myeloid, Acute drug therapy, Leukemia, Prolymphocytic, B-Cell drug therapy, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Prodrugs therapeutic use, Purine Nucleosides therapeutic use, Pyrimidinones therapeutic use

Abstract

Forodesine and nelarabine (the pro-drug of ara-G) are 2 nucleoside analogues with promising anti-leukemic activity. To better understand which pediatric patients might benefit from forodesine or nelarabine (ara-G) therapy, we investigated the in vitro sensitivity to these drugs in 96 diagnostic pediatric leukemia patient samples and the mRNA expression levels of different enzymes involved in nucleoside metabolism. Forodesine and ara-G cytotoxicities were higher in T-cell acute lymphoblastic leukemia (T-ALL) samples than in B-cell precursor (BCP)-ALL and acute myeloid leukemia (AML) samples. Resistance to forodesine did not preclude ara-G sensitivity and vice versa, indicating that both drugs rely on different resistance mechanisms. Differences in sensitivity could be partly explained by significantly higher accumulation of intracellular dGTP in forodesine-sensitive samples compared with resistant samples, and higher mRNA levels of dGK but not dCK. The mRNA levels of the transporters ENT1 and ENT2 were higher in ara-G-sensitive than -resistant samples. We conclude that especially T-ALL, but also BCP-ALL, pediatric patients may benefit from forodesine or nelarabine (ara-G) treatment.

Published

2011

34. A single intramuscular injection of neuraminidase inhibitor peramivir demonstrates antiviral activity against novel pandemic A/California/04/2009 (H1N1) influenza virus infection in mice.

Author

Bantia S, Kellogg D, Parker C, Upshaw R, Ilyushina NA, and Babu YS

Subjects

Acids, Carbocyclic, Animals, Body Weight, Disease Models, Animal, Female, Injections, Intramuscular, Mice, Mice, Inbred BALB C, Orthomyxoviridae Infections mortality, Orthomyxoviridae Infections pathology, Orthomyxoviridae Infections virology, Rodent Diseases drug therapy, Rodent Diseases mortality, Rodent Diseases pathology, Rodent Diseases virology, Survival Analysis, Antiviral Agents administration & dosage, Cyclopentanes administration & dosage, Guanidines administration & dosage, Influenza A Virus, H1N1 Subtype drug effects, Orthomyxoviridae Infections drug therapy

Abstract

New and emerging influenza virus strains, such as the pandemic influenza A (H1N1) virus require constant vigilance for antiviral drug sensitivity and resistance. Efficacy of intramuscularly (IM) administered neuraminidase (NA) inhibitor, peramivir, was evaluated in mice infected with recently isolated pandemic A/California/04/2009 (H1N1, swine origin, mouse adapted) influenza virus. A single IM injection of peramivir (four dose groups), given 1h prior to inoculation, significantly reduced weight loss (p < 0.001) and mortality (p < 0.05) in mice infected with LD90 dose of pandemic A/California/04/2009 (H1N1) influenza virus compared to vehicle group. There was 20% survival in the vehicle-treated group, whereas in the peramivir-treated groups, survival increased in a dose-dependent manner with 60, 60, 90 and 100% survivors for the 1, 3, 10, and 30 mg/kg doses, respectively. Weight loss on day 4 in the vehicle-treated group was 3.4 gm, and in the peramivir-treated groups was 2.1, 1.5, 1.8 and 1.8 g for the 1, 3, 10 and 30 mg/kg dose groups, respectively. In the treatment model, peramivir given 24h after infection as a single IM injection at 50mg/kg dose, showed significant protection against lethality and weight loss. There was 13% survival in the vehicle-treated group while in the peramivir-treated group at 24, 48, and 72 h post infection, survival was 100, 40, and 50%, respectively. Survival in the oseltamivir groups (10 mg/kg/d twice a day, orally for 5 days) was 90, 30 and 20% at 24, 48 and 72 h, respectively. These data demonstrate efficacy of parenterally administered peramivir against the recently isolated pandemic influenza virus in murine infection models., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2011

35. Combination of peramivir and rimantadine demonstrate synergistic antiviral effects in sub-lethal influenza A (H3N2) virus mouse model.

Author

Bantia S, Kellogg D, Parker CD, and Babu YS

Subjects

Acids, Carbocyclic, Animals, Disease Models, Animal, Dose-Response Relationship, Drug, Drug Administration Routes, Drug Administration Schedule, Drug Synergism, Female, Mice, Mice, Inbred BALB C, Orthomyxoviridae Infections mortality, Survival Rate, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Cyclopentanes pharmacology, Cyclopentanes therapeutic use, Guanidines pharmacology, Guanidines therapeutic use, Influenza A Virus, H3N2 Subtype drug effects, Orthomyxoviridae Infections drug therapy, Rimantadine pharmacology, Rimantadine therapeutic use, Weight Loss drug effects

Abstract

Efficacy of combination of the intramuscularly administered neuraminidase (NA) inhibitor, peramivir, and the orally administered M2 ion channel blocker, rimantadine was evaluated in mouse influenza A/Victoria/3/75 (H3N2) model. Mice were challenged with a sub-lethal virus dose (0-40% mortality in placebo group) and changes in body weights were analyzed by three-dimensional effect analysis to assess mode of drug interactions. Compounds were administered in a 5-day treatment course starting 1h before viral inoculation. The peramivir and rimantadine doses ranged from 0.3-3 mg/kg/d and 5-30 mg/kg/d, respectively. The maximum mean weight loss of 5.19 g was observed in the vehicle-infected group on day 10. In the 1 and 3 mg/kg/d peramivir monotherapy groups, the weight losses were 4.3 and 3.55 g, respectively. In the rimantadine monotherapy group, the weight losses were 3.43, 2.1, and 1.64 g for the 5, 10, and 30 mg/kg/d groups, respectively. Combination of 1mg/kg/d peramivir with 5 and 10 mg/kg/d rimantadine produced weight losses of 1.69 and 0.69 (p<0.05 vs. vehicle and individual agent), respectively, whereas the combination of 3.0 mg/kg/d peramivir with 10 and 30 mg/kg/d rimantadine did not show any weight loss (p<0.05 vs. vehicle and individual agent). The three-dimensional analysis of the weight loss for the majority of the drug combinations of peramivir and rimantadine tested demonstrated synergistic antiviral effects., (Copyright © 2010 Elsevier B.V. All rights reserved.)

Published

2010

36. Phase 2 and pharmacodynamic study of oral forodesine in patients with advanced, fludarabine-treated chronic lymphocytic leukemia.

Author

Balakrishnan K, Verma D, O'Brien S, Kilpatrick JM, Chen Y, Tyler BF, Bickel S, Bantia S, Keating MJ, Kantarjian H, Gandhi V, and Ravandi F

Subjects

Administration, Oral, Aged, Antineoplastic Agents administration & dosage, Apoptosis drug effects, Drug Administration Schedule, Drug Therapy, Combination, Enzyme Inhibitors blood, Female, Follow-Up Studies, Humans, Leukemia, Lymphocytic, Chronic, B-Cell metabolism, Lymphocyte Count, Lymphocytes cytology, Lymphocytes drug effects, Male, Middle Aged, Phosphoric Monoester Hydrolases metabolism, Purine Nucleosides blood, Purine-Nucleoside Phosphorylase antagonists & inhibitors, Purine-Nucleoside Phosphorylase metabolism, Pyrimidinones blood, Severity of Illness Index, Vidarabine administration & dosage, Enzyme Inhibitors administration & dosage, Enzyme Inhibitors pharmacokinetics, Leukemia, Lymphocytic, Chronic, B-Cell drug therapy, Purine Nucleosides administration & dosage, Purine Nucleosides pharmacokinetics, Pyrimidinones administration & dosage, Pyrimidinones pharmacokinetics, Vidarabine analogs & derivatives

Abstract

Forodesine is a new and potent purine nucleoside phosphorylase (PNP) inhibitor. Patients with chronic lymphocytic leukemia (CLL) with primary resistance to fludarabine-based therapy or with progressive disease were eligible for oral forodesine (200 mg/d) for up to 24 weeks. Eight patients with median lymphocyte count of 35.9 x 10(9)/L and median serum beta2 microglobulin level of 6.45 mg/L were treated. Six had Rai stage III to IV and were previously heavily treated (median prior therapy = 5). Two had transient decrease in lymphocyte count to normal, whereas in 5, disease progressed. Adverse events were mild. Steady-state level of forodesine ranged from 200 to 1300 nM and did not reach desired 2 microM level. PNP inhibition ranged from 57% to 89% and steady-state 2'-deoxyguanosine (dGuo) concentration median was 1.8 microM. Intracellular deoxyguanosine triphosphate (dGTP) increase was very modest, from median of 6 microM to 10 microM. Compared with in vivo, in vitro incubations of CLL lymphocytes with 10 or 20 microM dGuo and forodesine (2 microM) resulted in accumulation of higher levels of dGTP (40-250 microM) which resulted in increase in apoptosis. Forodesine has biologic activity in CLL; pharmacodynamic parameters suggest that an alternate dosing schedule and/or higher doses to achieve greater intracellular dGTP may be beneficial in this patient population.

Published

2010

37. Potent orally bioavailable purine nucleoside phosphorylase inhibitor BCX-4208 induces apoptosis in B- and T-lymphocytes--a novel treatment approach for autoimmune diseases, organ transplantation and hematologic malignancies.

Author

Bantia S, Parker C, Upshaw R, Cunningham A, Kotian P, Kilpatrick JM, Morris P, Chand P, and Babu YS

Subjects

Administration, Oral, B-Lymphocytes immunology, B-Lymphocytes metabolism, B-Lymphocytes pathology, Cell Proliferation drug effects, Cells, Cultured, Deoxyguanosine genetics, Deoxyguanosine metabolism, Enzyme Inhibitors pharmacology, Graft Rejection drug therapy, Graft Rejection immunology, Hematologic Neoplasms drug therapy, Hematologic Neoplasms immunology, Humans, Lymphocyte Culture Test, Mixed, Organ Transplantation, Psoriasis immunology, Purine-Nucleoside Phosphorylase antagonists & inhibitors, T-Lymphocytes immunology, T-Lymphocytes metabolism, T-Lymphocytes pathology, Apoptosis drug effects, B-Lymphocytes drug effects, Enzyme Inhibitors therapeutic use, Psoriasis drug therapy, T-Lymphocytes drug effects

Abstract

The profound suppression of T-cell immunity seen in purine nucleoside phosphorylase (PNP; EC 2.4.2.1) deficient patients supports potential application of inhibitors of PNP in the therapy of T-cell mediated diseases. BCX-4208 is a novel potent transition state analog inhibitor of human PNP with an IC(50) of 0.5 nM. PNP inhibition leads to elevation of dGuo which is converted to dGTP mainly in lymphocytes causing imbalance in deoxynucleotide (dNTP) pools and cell apoptosis. In in vitro studies, neither BCX-4208 nor dGuo alone inhibits proliferation of lymphocytes. BCX-4208 in the presence of 10 microM deoxyguanosine (dGuo) inhibits lymphocyte proliferation induced by MLR, IL-2 or Con A with IC(50)s of 0.159, 0.26 and 0.73 microM, respectively. The IC(50) for dGuo in the presence of 1 microM BCX-4208 for the IL-2 stimulated lymphocytes was 3.12 microM. dGTP in human lymphocytes is elevated and a 3-5 fold increase in dGTP results in 50% inhibition after in vitro exposure to BCX-4208 and dGuo. Flow cytometric analyses of human lymphocytes using annexin V staining reveal that BCX-4208 in the presence of dGuo induces cellular apoptosis in T-cells (CD3+), B-cells (CD20+, CD19+) and NK (CD56+) cells. BCX-4208 is orally bioavailable in mice and elevates plasma dGuo levels to 3.7 microM (predose levels<0.004 microM), similar to levels seen in PNP-deficient patients and levels needed to cause apoptosis in T and B-cells. These data support the evaluation of BCX-4208 in the treatment of T-cell and B-cell mediated diseases. BCX-4208 is currently undergoing early clinical investigation in psoriasis and gout., (2010 Elsevier B.V. All rights reserved.)

Published

2010

38. Forodesine has high antitumor activity in chronic lymphocytic leukemia and activates p53-independent mitochondrial apoptosis by induction of p73 and BIM.

Author

Alonso R, López-Guerra M, Upshaw R, Bantia S, Smal C, Bontemps F, Manz C, Mehrling T, Villamor N, Campo E, Montserrat E, and Colomer D

Subjects

Antibodies, Monoclonal administration & dosage, Antibodies, Monoclonal, Murine-Derived, Antineoplastic Agents pharmacology, Antineoplastic Combined Chemotherapy Protocols pharmacology, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Apoptosis physiology, Apoptosis Regulatory Proteins metabolism, Bcl-2-Like Protein 11, Bendamustine Hydrochloride, Cyclophosphamide administration & dosage, DNA-Binding Proteins metabolism, Dose-Response Relationship, Drug, Drug Evaluation, Preclinical, Gene Expression Regulation, Leukemic drug effects, Humans, Leukemia, Lymphocytic, Chronic, B-Cell drug therapy, Leukemia, Lymphocytic, Chronic, B-Cell genetics, Membrane Proteins metabolism, Mitochondria metabolism, Mitochondria physiology, Nitrogen Mustard Compounds administration & dosage, Nuclear Proteins metabolism, Proto-Oncogene Proteins metabolism, Purine Nucleosides administration & dosage, Purine Nucleosides therapeutic use, Pyrimidinones administration & dosage, Pyrimidinones therapeutic use, Rituximab, Tumor Cells, Cultured, Tumor Protein p73, Tumor Suppressor Protein p53 metabolism, Tumor Suppressor Proteins metabolism, Vidarabine administration & dosage, Vidarabine analogs & derivatives, Apoptosis drug effects, Apoptosis Regulatory Proteins genetics, DNA-Binding Proteins genetics, Leukemia, Lymphocytic, Chronic, B-Cell pathology, Membrane Proteins genetics, Nuclear Proteins genetics, Proto-Oncogene Proteins genetics, Purine Nucleosides pharmacology, Pyrimidinones pharmacology, Tumor Suppressor Protein p53 physiology, Tumor Suppressor Proteins genetics

Abstract

Chronic lymphocytic leukemia (CLL) is an incurable disease derived from the monoclonal expansion of CD5(+) B lymphocytes. High expression levels of ZAP-70 or CD38 and deletions of 17p13 (TP53) and 11q22-q23 (ATM) are associated with poorer overall survival and shorter time to disease progression. DNA damage and p53 play a pivotal role in apoptosis induction in response to conventional chemotherapy, because deletions of ATM or p53 identify CLL patients with resistance to treatment. Forodesine is a transition-state inhibitor of the purine nucleoside phosphorylase with antileukemic activity. We show that forodesine is highly cytotoxic as single agent or in combination with bendamustine and rituximab in primary leukemic cells from CLL patients regardless of CD38/ZAP-70 expression and p53 or ATM deletion. Forodesine activates the mitochondrial apoptotic pathway by decreasing the levels of antiapoptotic MCL-1 protein and induction of proapoptotic BIM protein. Forodesine induces transcriptional up-regulation of p73, a p53-related protein able to overcome the resistance to apoptosis of CLL cells lacking functional p53. Remarkably, no differences in these apoptotic markers were observed based on p53 or ATM status. In conclusion, forodesine induces apoptosis of CLL cells bypassing the DNA-damage/ATM/p53 pathway and might represent a novel chemotherapeutic approach that deserves clinical investigation.

Published

2009

39. Design, parallel synthesis, and crystal structures of biphenyl antithrombotics as selective inhibitors of tissue factor FVIIa complex. Part 1: Exploration of S2 pocket pharmacophores.

Author

Kotian PL, Krishnan R, Rowland S, El-Kattan Y, Saini SK, Upshaw R, Bantia S, Arnold S, Babu YS, and Chand P

Subjects

Binding Sites, Catalytic Domain, Crystallography, X-Ray, Inhibitory Concentration 50, Models, Molecular, Molecular Structure, Structure-Activity Relationship, Anticoagulants chemistry, Anticoagulants pharmacology, Biphenyl Compounds chemistry, Biphenyl Compounds pharmacology, Blood Coagulation drug effects, Drug Design, Factor VIIa antagonists & inhibitors

Abstract

Factor VIIa (FVIIa), a serine protease enzyme, coupled with tissue factor (TF) plays an important role in a number of thrombosis-related disorders. Inhibition of TF x FVIIa occurs early in the coagulation cascade and might provide some safety advantages over other related enzymes. We report here a novel series of substituted biphenyl derivatives that are highly potent and selective TF x FVIIa inhibitors. Parallel synthesis coupled with structure-based drug design allowed us to explore the S2 pocket of the enzyme active site. A number of compounds with IC(50) value of <10 nM were synthesized. The X-ray crystal structures of some of these compounds complexed with TF x FVIIa were determined and results were applied to design the next round of inhibitors. All the potent inhibitors were tested for inhibition against a panel of related enzymes and selectivity of 17,600 over thrombin, 450 over trypsin, 685 over FXa, and 76 over plasmin was achieved. Two groups, vinyl 36b and 2-furan 36ab, were identified as the optimum binding substituents on the phenyl ring in the S2 pocket. Compounds with these two substituents are the most potent compounds in this series with good selectivity over related serine proteases. These compounds will be further explored for structure-activity relationship.

Published

2009

40. Probing the S2 site of factor VIIa to generate potent and selective inhibitors: the structure of BCX-3607 in complex with tissue factor-factor VIIa.

Author

Krishnan R, Kotian PL, Chand P, Bantia S, Rowland S, and Babu YS

Subjects

Binding Sites, Crystallography, X-Ray, Drug Design, Humans, In Vitro Techniques, Models, Molecular, Molecular Structure, Multiprotein Complexes chemistry, Factor VIIa antagonists & inhibitors, Factor VIIa chemistry, Pyridines chemistry, Pyridines pharmacology, Thromboplastin chemistry

Abstract

Factor VIIa (FVIIa) is a trypsin-like serine protease in the coagulation cascade. Its complex with tissue factor (TF) triggers the extrinsic pathway of the coagulation cascade, generating a blood clot. Research programs at several centers now recognize the important roles played by TF and FVIIa in both the thrombotic and inflammatory processes associated with cardiovascular diseases. Therefore, inhibition of the TF-FVIIa complex is seen as a promising target that is key to the development of clinical candidates for various cardiovascular applications. The crystal structure of the TF-FVIIa enzyme complex has been analyzed in order to design and synthesize small-molecule inhibitors. Using structure-based drug design (SBDD), a new series of inhibitors have been discovered that demonstrate high potency against the TF-FVIIa complex while maintaining substantial selectivity versus other closely related serine proteases such as trypsin, thrombin, factor Xa and plasmin.

Published

2007

41. The antithrombotic and anti-inflammatory effects of BCX-3607, a small molecule tissue factor/factor VIIa inhibitor.

Author

Arnold CS, Parker C, Upshaw R, Prydz H, Chand P, Kotian P, Bantia S, and Babu YS

Subjects

Animals, Atherosclerosis drug therapy, Blotting, Northern, Cells, Cultured, Disease Models, Animal, Dose-Response Relationship, Drug, Endothelium, Vascular metabolism, Endotoxemia pathology, Humans, Inflammation, Interleukin-6 metabolism, Interleukin-8 metabolism, Keratinocytes metabolism, Lipopolysaccharides metabolism, Male, Mice, Models, Biological, Models, Chemical, Prothrombin Time, RNA, Messenger metabolism, Rats, Rats, Sprague-Dawley, Sepsis, Time Factors, Anti-Inflammatory Agents pharmacology, Factor VIIa antagonists & inhibitors, Fibrinolytic Agents pharmacology, Pyridines pharmacology, Thromboplastin antagonists & inhibitors

Abstract

Tissue factor (TF) is a transmembrane glycoprotein that binds its zymogen cofactor, Factor VIIa (FVIIa) on the cell surface. Together (TF/FVIIa) they activate Factor X (FX) and Factor IX (FIX) and start the extrinsic pathway of blood coagulation. As such, the TF/FVIIa complex plays an important role in normal physiology as well as in thrombotic diseases such as unstable angina (UA), disseminated intravascular coagulation (DIC), and deep vein thrombosis (DVT). In addition to its function as an initiator of coagulation, TF/FVIIa plays an important role in inflammation. Expression of TF on the cell surface and its appearance as a soluble molecule are characteristic features of acute and chronic inflammation in conditions such as sepsis and atherosclerosis. Here we demonstrate that BCX-3607, a small molecule potent inhibitor of TF/FVIIa, reduces thrombus weight in an animal model of DVT. BCX-3607 also decreases the level of interleukin-6 (IL-6) in a LPS-stimulated mouse model of endotoxemia. Additionally, in vitro studies indicate that BCX-3607 blocks the generation of TF/FVIIa-induced IL-8 mRNA in human keratinocytes and reduces the TF/FVIIa-mediated generation of IL-6 and IL-8 in human umbilical vein endothelial cells (HUVEC). Therefore, BCX-3607 might block the TF/FVIIa-mediated coagulation and inflammation associated with pathological conditions.

Published

2006

42. An efficient synthesis of acyclic N7- and N9-adenine nucleosides via alkylation with secondary carbon electrophiles to introduce versatile functional groups at the C-1 position of acyclic moiety.

Author

Kotian PL, Kumar VS, Lin TH, El-Kattan Y, Ghosh A, Wu M, Cheng X, Bantia S, Babu YS, and Chand P

Subjects

Adenine chemistry, Alkylation, Antiviral Agents chemical synthesis, Antiviral Agents pharmacology, Microbial Sensitivity Tests, Molecular Structure, Nucleosides chemistry, Adenine analogs & derivatives, Adenine chemical synthesis, Carbon chemistry, Nucleosides chemical synthesis

Abstract

The introduction of versatile functional groups, allyl and ester, at the C-1 position of the acyclic chain in acyclic adenine nucleosides was achieved for the first time directly by alkylation of adenine and N6-potected adenine. Thus, the C-1'-substituted N9-adenine acyclic nucleoside, adenine-9-yl-pent-4-enoic acid ethyl ester (11), was prepared by direct alkylation of adenine with 2-bromopent-4-enoic acid ethyl ester (6), while the corresponding N7-regioisomer, 2-[6-(dimethylaminomethyleneamino)-purin-7-yl]-pent-4-enoic acid ethyl ester (10), was obtained in one step by the coupling of N, N-dimethyl-N'- (9H-purin-6-yl)-formamidine (9) with 2-bromopent-4-enoic acid ethyl ester (6). The functional groups, ester and allyl, were converted to the desired hydroxymethyl and hydroxyethyl groups, and subsequently to phosphonomethyl derivatives and corresponding pyrophosphorylphosphonates.

Published

2006

43. Anti-influenza virus activity of peramivir in mice with single intramuscular injection.

Author

Bantia S, Arnold CS, Parker CD, Upshaw R, and Chand P

Subjects

Acids, Carbocyclic, Animals, Antiviral Agents administration & dosage, Antiviral Agents chemistry, Cyclopentanes administration & dosage, Cyclopentanes chemistry, Disease Models, Animal, Drug Evaluation, Preclinical, Female, Guanidines administration & dosage, Guanidines chemistry, Injections, Intramuscular, Mice, Neuraminidase administration & dosage, Antiviral Agents therapeutic use, Cyclopentanes therapeutic use, Guanidines therapeutic use, Influenza A Virus, H1N1 Subtype, Neuraminidase antagonists & inhibitors, Neuraminidase therapeutic use, Orthomyxoviridae Infections drug therapy

Abstract

In the event of an influenza outbreak, antivirals including the neuraminidase (NA) inhibitors, peramivir, oseltamivir, and zanamivir may provide valuable benefit when vaccine production is delayed, limited, or cannot be used. Here we demonstrate the efficacy of a single intramuscular injection of peramivir in the mouse influenza model. Peramivir potently inhibits the neuraminidase enzyme N9 from H1N9 virus in vitro with a 50% inhibitory concentration (IC(50)) of 1.3+/-0.4 nM. On-site dissociation studies indicate that peramivir remains tightly bound to N9 NA (t(1/2)>24h), whereas, zanamivir and oseltamivir carboxylate dissociated rapidly from the enzyme (t(1/2)=1.25 h). A single intramuscular injection of peramivir (10mg/kg) significantly reduces weight loss and mortality in mice infected with influenza A/H1N1, while oseltamivir demonstrates no efficacy by the same treatment regimen. This may be due to tight binding of peramivir to the N1 NA enzymes similar to that observed for N9 enzyme. Additional efficacy studies indicate that a single injection of peramivir (2-20mg/kg) was comparable to a q.d.x 5 day course of orally administered oseltamivir (2-20mg/kg/day) in preventing lethality in H3N2 and H1N1 influenza models. A single intramuscular injection of peramivir may successfully treat influenza infections and provide an alternate option to oseltamivir during an influenza outbreak.

Published

2006

44. A proof-of-principle pharmacokinetic, pharmacodynamic, and clinical study with purine nucleoside phosphorylase inhibitor immucillin-H (BCX-1777, forodesine).

Author

Gandhi V, Kilpatrick JM, Plunkett W, Ayres M, Harman L, Du M, Bantia S, Davisson J, Wierda WG, Faderl S, Kantarjian H, and Thomas D

Subjects

Adult, Aged, Deoxyguanine Nucleotides metabolism, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacokinetics, Enzyme Inhibitors pharmacology, Female, Humans, Leukemia, Lymphoid pathology, Leukemia, Lymphoid urine, Male, Middle Aged, Molecular Structure, Purine Nucleosides, Purine-Nucleoside Phosphorylase metabolism, Pyrimidinones adverse effects, Pyrimidinones chemistry, Pyrroles adverse effects, Pyrroles chemistry, Treatment Outcome, Leukemia, Lymphoid drug therapy, Purine-Nucleoside Phosphorylase antagonists & inhibitors, Pyrimidinones pharmacokinetics, Pyrimidinones pharmacology, Pyrroles pharmacokinetics, Pyrroles pharmacology

Abstract

The discovery of purine nucleoside phosphorylase (PNP) deficiency and T lymphocytopenia suggested that inhibition of this enzyme could serve as a therapeutic target. Inhibitors of PNP failed until structure-based synthesis of immucillin-H (BCX-1777, forodesine), a transition-state analog of PNP. The picomolar potency for PNP, T cell-selective cytotoxicity, and animal studies provided the rationale for use of forodesine in T-cell malignancies. Five patients were treated with an intravenous infusion of forodesine (40 mg/m2) on day 1; treatment continued on day 2; forodesine was administered every 12 hours for an additional 8 doses. Plasma and cellular pharmacokinetics and pharmaco-dynamics were investigated. Median peak level of forodesine (5.4 microM) was achieved at the end of infusion. This level was sufficient to increase plasma 2'-deoxyguanosine (dGuo) concentrations in all patients. Intracellular deoxyguanosine triphosphate (dGTP) increased by 2- to 40-fold in 4 of 5 patients (8 of 9 courses) and correlated with antileukemia activity in 4 patients. However, objective responses were not observed. This was the first clinical study in humans to demonstrate the plasma pharmacokinetics and the pharmacodynamic effectiveness of the PNP inhibitor, forodesine; however, regrowth of leukemia cells in the blood and marrow after course 1 suggested that a different therapeutic schedule should be considered for future studies.

Published

2005

45. Comparison of the anti-influenza virus activity of cyclopentane derivatives with oseltamivir and zanamivir in vivo.

Author

Chand P, Bantia S, Kotian PL, El-Kattan Y, Lin TH, and Babu YS

Subjects

Acetamides pharmacology, Acids, Carbocyclic, Administration, Intranasal, Administration, Oral, Animals, Antiviral Agents administration & dosage, Antiviral Agents pharmacology, Cyclopentanes pharmacology, Dose-Response Relationship, Drug, Guanidines, Mice, Orthomyxoviridae Infections drug therapy, Oseltamivir, Pyrans, Sialic Acids pharmacology, Structure-Activity Relationship, Survival Rate, Treatment Outcome, Zanamivir, Antiviral Agents chemical synthesis, Cyclopentanes administration & dosage, Cyclopentanes chemical synthesis, Orthomyxoviridae drug effects

Abstract

Cyclopentane derivatives, designated as BCX-1812, BCX-1827, BCX-1898, and BCX-1923, were tested in parallel with oseltamivir carboxylate and zanamivir for the in vivo activity in mice infected with A/Turkey/Mas/76 X A/Beijing/32/92 (H6N2) influenza virus. The compounds were tested orally and intranasally at different dose levels. BCX-1812, BCX-1827, and BCX-1923 showed more than 50% protection at 1mg/kg/day dose level on oral treatment. The intranasal treatment was 100% effective even at 0.01 mg/kg/day for all four compounds. On comparison with oseltamivir carboxylate and zanamivir, these four cyclopentane derivatives have shown equal or better efficacies. The synthesis of two new compounds, BCX-1898 and BCX-1923, is also described.

Published

2005

46. Synthesis and inhibitory activity of benzoic acid and pyridine derivatives on influenza neuraminidase.

Author

Chand P, Kotian PL, Morris PE, Bantia S, Walsh DA, and Babu YS

Subjects

Benzoates chemistry, Crystallography, X-Ray, Models, Molecular, Molecular Conformation, Pyridines chemistry, Structure-Activity Relationship, Benzoates chemical synthesis, Benzoates pharmacology, Neuraminidase antagonists & inhibitors, Orthomyxoviridae enzymology, Pyridines chemical synthesis, Pyridines pharmacology

Abstract

Based upon the activity and X-ray crystallographic studies of tri-substituted benzene derivatives containing carboxylic acid, acetamido and guanidine groups, we investigated the effect of the fourth substituent to fulfill the fourth pocket of neuraminidase enzyme. The groups selected as fourth substituents were hydroxymethyl, hydroxyethyl, oxime and amino. These tetra-substituted benzene derivatives were synthesized and evaluated for neuraminidase inhibitory activity. All these compounds were found to have poorer IC(50) values than the tri-substituted compounds. Further, benzene ring was replaced by pyridine ring and di, tri and tetra-substituted pyridine derivatives were synthesized. The activity of the pyridine derivatives was comparable to benzene derivatives. The fourth substituent seems to disturb the binding of the other three substituents, so the activity is reduced as compared to tri-substituted benzene and pyridine derivatives.

Published

2005

47. Synthesis of N6-substituted 9-[3-(phosphonomethoxy)propyl]adenine derivatives as possible antiviral agents.

Author

El-Kattan Y, Lin TH, Wu M, Kumar VS, Kotian PL, Ghosh A, Cheng X, Bantia S, Babu YS, and Chand P

Subjects

Adenine analogs & derivatives, Adenine pharmacology, Antiviral Agents pharmacology, Hepacivirus drug effects, Humans, Organophosphonates pharmacology, Prodrugs pharmacology, Adenine chemical synthesis, Antiviral Agents chemical synthesis, Hepacivirus growth & development, Organophosphonates chemical synthesis, Prodrugs chemical synthesis, Virus Replication drug effects

Abstract

A number of N6-substituted 9-[3-(phosphonomethoxy)propyl]adenine derivatives having hydroxymethyl at C-1' position were prepared from the appropriate 6-chloroadenine derivative. The syntheses of the corresponding prodrugs of these compounds are also reported. These compounds showed poor activity against HCV in replicon assay.

Published

2005

48. Synthesis of 9-[1-(substituted)-2-(phosphonomethoxy)ethyl]adenine derivatives as possible antiviral agents.

Author

Wu M, El-Kattan Y, Lin TH, Ghosh A, Kumar VS, Kotian PL, Cheng X, Bantia S, Babu YS, and Chand P

Subjects

Adenine analogs & derivatives, Adenine pharmacology, Antiviral Agents pharmacology, Hepacivirus drug effects, Humans, Organophosphonates pharmacology, Prodrugs pharmacology, Adenine chemical synthesis, Antiviral Agents chemical synthesis, Hepacivirus growth & development, Organophosphonates chemical synthesis, Prodrugs chemical synthesis, Virus Replication drug effects

Abstract

Various C-1'-substituted acyclic N9 adenine nucleosides were prepared from 9-[(1-hydroxymethyl)(3-monomethoxytrityloxy)propyl]-N6-monomethoxytrityladenine. The hydroxymethyl was modified to the phosphonomethoxy derivative, and the 3-monomethoxytrityloxy was converted to hydroxyl, methoxy, azido, and amino. Other substituents, such as ethyl and ea-hydroxyethyl were also prepared. The resulting phosphonomethoxy derivatives were converted to prodrugs.

Published

2005

49. Purine nucleoside phosphorylase inhibitors in T-cell malignancies.

Author

Bantia S and Kilpatrick JM

Subjects

Animals, Cell Proliferation drug effects, Humans, Leukemia, T-Cell enzymology, Leukemia, T-Cell immunology, Lymphoma, T-Cell enzymology, Lymphoma, T-Cell immunology, T-Lymphocytes drug effects, T-Lymphocytes immunology, Antineoplastic Agents therapeutic use, Enzyme Inhibitors therapeutic use, Leukemia, T-Cell drug therapy, Lymphoma, T-Cell drug therapy, Purine-Nucleoside Phosphorylase antagonists & inhibitors

Abstract

Purine nucleoside phosphorylase (PNP)-deficient children exhibit profound impairment in the T-cell component of their immune systems, but have normal B-cell function. This rare condition provides a model for the development of specific inhibitors of PNP, which should enable selective suppression of T-cell function that may be useful in the treatment of T-cell-mediated diseases. BCX-1777 (BioCryst Pharmaceuticals Inc) is a rationally designed, potent transition-state analog inhibitor of PNP. This review provides a summary of in vitro and in vivo inhibition studies of T-cells by BCX-1777, and the role in this process of plasma deoxyguanosine (dGuo) and intracellular deoxyguanosine triphosphate (dGTP). Preliminary data from a phase I clinical trial of BCX-1777 in patients with T-cell malignancy demonstrated antileukemic activity which can be correlated to an increase in plasma dGuo and intracellular dGTP. This is consistent with results observed in cell cultures, animal studies and PNP-deficient patients. Clinical trials with BCX-1777 have demonstrated that inhibition of PNP leads to T-cell-selective suppression, confirming PNP to be a promising target for the treatment of T-cell-mediated diseases.

Published

2004

50. Mechanism of inhibition of T-acute lymphoblastic leukemia cells by PNP inhibitor--BCX-1777.

Author

Bantia S, Ananth SL, Parker CD, Horn LL, and Upshaw R

Subjects

Apoptosis drug effects, Cell Division drug effects, Cell Line, Culture Media, HIV Reverse Transcriptase antagonists & inhibitors, Half-Life, Humans, Lamivudine pharmacology, Lymphocytes drug effects, Lymphocytes metabolism, Purine Nucleosides, Reverse Transcriptase Inhibitors pharmacology, Stavudine pharmacology, Leukemia-Lymphoma, Adult T-Cell drug therapy, Purine-Nucleoside Phosphorylase antagonists & inhibitors, Pyrimidinones pharmacology, Pyrroles pharmacology

Abstract

Purine nucleoside phosphorylase (PNP) deficiency in humans produces a relatively selective depletion of T cells. BCX-1777 is a potent inhibitor of PNP. BCX-1777 in the presence of deoxyguanosine (dGuo) inhibits the proliferation of CEM-SS [T-acute lymphoblastic leukemia (T-ALL)] cells with an IC(50)=0.015 microM. This inhibition by BCX-1777 and dGuo is accompanied by elevation of dGTP (154-fold) and dATP (8-fold). Deoxycytidine (dCyt) completely and lamivudine (3TC) partially reverse this inhibition caused by BCX-1777 and dGuo. dNTP analysis of these samples indicates that, in the presence of dCyt, where complete reversal of inhibition is observed, dGTP and dATP pools revert back to the control levels. In samples containing 3TC, where partial reversal of inhibition was observed, dGTP decreased from 154-fold to 38-fold and dATP levels further increased from 8-fold to 30-fold compared to the control sample. In CEM-SS cells, inhibition of proliferation by BCX-1777 and dGuo is not due to accumulation of dATP because in the presence of 3TC, where reversal of inhibition is observed, dATP levels are further increased. These studies clearly indicate that inhibition of T cells is due to accumulation of dGTP resulting in cell death with characteristics of apoptosis. The half-life of dGTP in CEM-SS cells is 18 h, which is longer than that observed in human lymphocytes (4 h), suggesting that the nucleotidase level in CEM-SS cells is lower than in human lymphocytes. A 154-fold accumulation of dGTP in CEM-SS cells in the presence of BCX-1777 and dGuo compared to a 15-fold accumulation of dGTP in human lymphocytes suggests that kinase level is higher in CEM-SS cells compared to human lymphocytes. High kinase and low nucleotidase levels make CEM-SS cells more sensitive to inhibition by BCX-1777 and dGuo than human lymphocytes. Currently, BCX-1777 is in phase I/II clinical trial for the treatment of T cell malignancies.

Published

2003