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3. Crystal structure of protein tyrosine phosphatase 1B in complex with an isothiazolidinone-containing inhibitor

Author

Douty, B., primary, Wayland, B., additional, Ala, P.J., additional, Bower, M.J., additional, Pruitt, J., additional, Bostrom, L., additional, Wei, M., additional, Klabe, R., additional, Gonneville, L., additional, Wynn, R., additional, Burn, T.C., additional, Liu, P.C.C., additional, Combs, A.P., additional, and Yue, E.W., additional

Published
2007
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4. Structural Basis for Inhibition of Protein Tyrosine Phosphatase 1B by Isothiazolidinone Heterocyclic Phosphonate Mimetics

Author

Ala, P.J., primary, Gonneville, L., additional, Hillman, M.C., additional, Becker-Pasha, M., additional, Wei, M., additional, Reid, B.G., additional, Klabe, R., additional, Yue, E.W., additional, Wayland, B., additional, Douty, B., additional, Combs, A.P., additional, Polam, P., additional, Wasserman, Z., additional, Bower, M., additional, Burn, T.C., additional, Hollis, G.F., additional, and Wynn, R., additional

Published
2006
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7. ChemInform Abstract: Preparation and Structure‐Activity Relationship of Novel P1/P1′‐ Substituted Cyclic Urea‐Based Human Immunodeficiency Virus Type‐1 Protease Inhibitors.

Author

NUGIEL, D. A., primary, JACOBS, K., additional, WORLEY, T., additional, PATEL, M., additional, KALTENBACH, R. F. III, additional, MEYER, D. T., additional, JADHAV, P. K., additional, DE LUCCA, G. V., additional, SMYSER, T. E., additional, KLABE, R. M., additional, BACHELER, L. T., additional, RAYNER, M. M., additional, and SEITZ, S. P., additional

Published
1996
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10. Structure-Based Design and Discovery of Protein Tyrosine Phosphatase Inhibitors Incorporating Novel Isothiazolidinone Heterocyclic Phosphotyrosine Mimetics

Author

Combs, A. P., Yue, E. W., Bower, M., Ala, P. J., Wayland, B., Douty, B., Takvorian, A., Polam, P., Wasserman, Z., Zhu, W., Crawley, M. L., Pruitt, J., Sparks, R., Glass, B., Modi, D., McLaughlin, E., Bostrom, L., Li, M., Galya, L., Blom, K., Hillman, M., Gonneville, L., Reid, B. G., Wei, M., Becker-Pasha, M., Klabe, R., Huber, R., Li, Y., Hollis, G., Burn, T. C., Wynn, R., Liu, P., and Metcalf, B.

Abstract

Structure-based design led to the discovery of novel (S)-isothiazolidinone ((S)-IZD) heterocyclic phosphotyrosine (pTyr) mimetics that when incorporated into dipeptides are exceptionally potent, competitive, and reversible inhibitors of protein tyrosine phosphatase 1B (PTP1B). The crystal structure of PTP1B in complex with our most potent inhibitor 12 revealed that the (S)-IZD heterocycle interacts extensively with the phosphate binding loop precisely as designed in silico. Our data provide strong evidence that the (S)-IZD is the most potent pTyr mimetic reported to date.

Published
2005

13. Inhibition of Clinically Relevant Mutant Variants of HIV-1 by Quinazolinone Non-Nucleoside Reverse Transcriptase Inhibitors

Author

Corbett, J. W., Ko, S. S., Rodgers, J. D., Gearhart, L. A., Magnus, N. A., Bacheler, L. T., Diamond, S., Jeffrey, S., Klabe, R. M., Cordova, B. C., Garber, S., Logue, K., Trainor, G. L., Anderson, P. S., and Erickson-Viitanen, S. K.

Abstract

A series of 4-alkenyl and 4-alkynyl-3,4-dihydro-4-(trifluoromethyl)-2-(1H)-quinazolinones were found to be potent non-nucleoside reverse transcriptase inhibitors (NNRTIs) of human immunodeficiency virus type-1 (HIV-1). The 4-alkenyl-3,4-dihydro-4-(trifluoromethyl)-2-(1H)-quinazolinones DPC 082 and DPC 083 and the 4-alkynyl-3,4-dihydro-4-(trifluoromethyl)-2-(1H)-quinazolinones DPC 961 and DPC 963 were found to exhibit low nanomolar potency toward wild-type RF virus (IC90 = 2.0, 2.1, 2.0, and 1.3 nM, respectively) and various single and many multiple amino acid substituted HIV-1 mutant viruses. The increased potency is combined with favorable plasma serum protein binding as demonstrated by improvements in the percent free drug in human plasma when compared to efavirenz:  3.0%, 2.0%, 1.5%, 2.8%, and 0.2−0.5% for DPC 082, DPC 083, DPC 961, DPC 963, and efavirenz, respectively.

Published
2000

16. Nonsymmetric P2/P2‘ Cyclic Urea HIV Protease Inhibitors. Structure−Activity Relationship, Bioavailability, and Resistance Profile of Monoindazole-Substituted P2 Analogues

Author

Lucca, G. V. De, Kim, U. T., Liang, J., Cordova, B., Klabe, R. M., Garber, S., Bacheler, L. T., Lam, G. N., Wright, M. R., Logue, K. A., Erickson-Viitanen, S., Ko, S. S., and Trainor, G. L.

Abstract

Using the structural information gathered from the X-ray structures of various cyclic urea/HIVPR complexes, we designed and synthesized many nonsymmetrical P2/P2‘-substituted cyclic urea analogues. Our efforts concentrated on using an indazole as one of the P2 substituents since this group imparted enzyme (Ki) potency as well as translation into excellent antiviral (IC90) potency. The second P2 substituent was used to adjust the physical and chemical properties in order to maximize oral bioavailability. Using this approach several very potent (IC90 11 nM) and orally bioavailable (F% 93−100%) compounds were discovered (21, 22). However, the resistance profiles of these compounds were inadequate, especially against the double (I84V/V82F) and ritonavir-selected mutant viruses. Further modification of the second P2 substituent in order to increase H-bonding interactions with the backbone atoms of residues Asp 29, Asp 30, and Gly 48 led to analogues with much better resistance profiles. However, these larger analogues were incompatible with the apparent molecular weight requirements for good oral bioavailability of the cyclic urea class of HIVPR inhibitors (MW < 610).

Published
1998

17. Cyclic HIV Protease Inhibitors:  Synthesis, Conformational Analysis, P2/P2‘ Structure−Activity Relationship, and Molecular Recognition of Cyclic Ureas

Author

Lam, P. Y. S., Ru, Y., Jadhav, P. K., Aldrich, P. E., DeLucca, G. V., Eyermann, C. J., Chang, C.-H., Emmett, G., Holler, E. R., Daneker, W. F., Li, L., Confalone, P. N., McHugh, R. J., Han, Q., Li, R., Markwalder, J. A., Seitz, S. P., Sharpe, T. R., Bacheler, L. T., Rayner, M. M., Klabe, R. M., Shum, L., Winslow, D. L., Kornhauser, D. M., Jackson, D. A., Erickson-Viitanen, S., and Hodge, C. N.

Abstract

High-resolution X-ray structures of the complexes of HIV-1 protease (HIV-1PR) with peptidomimetic inhibitors reveal the presence of a structural water molecule which is hydrogen bonded to both the mobile flaps of the enzyme and the two carbonyls flanking the transition-state mimic of the inhibitors. Using the structure−activity relationships of C2-symmetric diol inhibitors, computed-aided drug design tools, and first principles, we designed and synthesized a novel class of cyclic ureas that incorporates this structural water and preorganizes the side chain residues into optimum binding conformations. Conformational analysis suggested a preference for pseudodiaxial benzylic and pseudodiequatorial hydroxyl substituents and an enantiomeric preference for the RSSR stereochemistry. The X-ray and solution NMR structure of the complex of HIV-1PR and one such cyclic urea, DMP323, confirmed the displacement of the structural water. Additionally, the bound and “unbound” (small-molecule X-ray) ligands have similar conformations. The high degree of preorganization, the complementarity, and the entropic gain of water displacement are proposed to explain the high affinity of these small molecules for the enzyme. The small size probably contributes to the observed good oral bioavailability in animals. Extensive structure-based optimization of the side chains that fill the S2 and S2‘ pockets of the enzyme resulted in DMP323, which was studied in phase I clinical trials but found to suffer from variable pharmacokinetics in man. This report details the synthesis, conformational analysis, structure−activity relationships, and molecular recognition of this series of C2-symmetry HIV-1PR inhibitors. An initial series of cyclic ureas containing nonsymmetric P2/P2‘ is also discussed.

Published
1996

18. Preparation and Structure−Activity Relationship of Novel P1/P1‘-Substituted Cyclic Urea-Based Human Immunodeficiency Virus Type-1 Protease Inhibitors

Author

Nugiel, D. A., Jacobs, K., Worley, T., Patel, M., Kaltenbach, R. F., III, Meyer, D. T., Jadhav, P. K., Lucca, G. V. De, Smyser, T. E., Klabe, R. M., Bacheler, L. T., Rayner, M. M., and Seitz, S. P.

Abstract

A series of novel P1/P1‘-substituted cyclic urea-based HIV-1 protease inhibitors was prepared. Three different synthetic schemes were used to assemble these compounds. The first approach uses amino acid-based starting materials and was originally used to prepare DMP 323. The other two approaches use l-tartaric acid or l-mannitol as the starting material. The required four contiguous R,S,S,R centers of the cyclic urea scaffold are introduced using substrate control methodology. Each approach has specific advantages based on the desired P1/P1‘ substituent. Designing analogs based on the enzyme's natural substrates provided compounds with reduced activity. Attempts at exploiting hydrogen bond sites in the S1/S1‘ pocket, suggested by molecular modeling studies, were not fruitful. Several analogs had better binding affinity compared to our initial leads. Modulating the compound's physical properties led to a 10-fold improvement in translation resulting in better overall antiviral activity.

Published
1996

19. Stereoisomers of Cyclic Urea HIV-1 Protease Inhibitors:  Synthesis and Binding Affinities

Author

Kaltenbach, R. F., III, Nugiel, D. A., Lam, P. Y. S., Klabe, R. M., and Seitz, S. P.

Abstract

We have synthesized stereoisomers of cyclic urea HIV-1 protease inhibitors to study the effect of varying configurations on binding affinities. Four different synthetic approaches were used to prepare the desired cyclic urea stereoisomers. The original cyclic urea synthesis using amino acid starting materials was used to prepare three isomers. Three additional isomers were prepared by synthetic routes utilizing l-tartaric acid and d-sorbitol as chiral starting materials. A stereoselective hydroxyl inversion of the cyclic urea trans-diol was used to prepare three additional isomers. In all 9 of the 10 possible cyclic urea stereoisomers were prepared, and their binding affinities are described.

Published
1998

20. Design, Synthesis, and Evaluation of Tetrahydropyrimidinones as an Example of a General Approach to Nonpeptide HIV Protease Inhibitors

Author

Lucca, G. V. De, Liang, J., Aldrich, P. E., Calabrese, J., Cordova, B., Klabe, R. M., Rayner, M. M., and Chang, C.-H.

Abstract

Re-examination of the design of the cyclic urea class of HIV protease (HIVPR) inhibitors suggests a general approach to designing novel nonpeptide cyclic HIVPR inhibitors. This process involves the inversion of the stereochemical centers of the core transition-state isostere of the linear HIVPR inhibitors and cyclization of the resulting core using an appropriate cyclizing reagent. As an example, this process is applied to the diamino alcohol class of HIVPR inhibitors11 to give tetrahydropyrimidinones. Conformational analysis of the tetrahydropyrimidinones and modeling of its interaction with the active site of HIVPR suggested modifications which led to very potent inhibitors of HIVPR (24 with a Ki = 0.018 nM). The X-ray crystallographic structure of the complex of 24 with HIVPR confirms the analysis and modeling predictions. The example reported in this study and other examples that are cited indicate that this process may be generally applicable to other linear inhibitors.

Published
1997

21. Improved P1/P1‘ Substituents for Cyclic Urea Based HIV-1 Protease Inhibitors:  Synthesis, Structure−Activity Relationship, and X-ray Crystal Structure Analysis

Author

Nugiel, D. A., Jacobs, K., Cornelius, L., Chang, C.-H., Jadhav, P. K., Holler, E. R., Klabe, R. M., Bacheler, L. T., Cordova, B., Garber, S., Reid, C., Logue, K. A., Gorey-Feret, L. J., Lam, G. N., Erickson-Viitanen, S., and Seitz, S. P.

Abstract

We present several novel P1/P1‘ substituents that can replace the characteristic benzyl P1/P1‘ moiety of the cyclic urea based HIV protease inhibitor series. These substituents typically provide 5−10-fold improvements in binding affinity compared to the unsubstituted benzyl analogs. The best substituent was the 3,4-(ethylenedioxy)benzyl group. Proper balancing of the molecule's lipophilicity facilitated the transfer of this improved binding affinity into a superior cellular antiviral activity profile. Several analogs were evaluated further for protein binding and resistance liabilities. Compound 18 (IC90 = 8.7 nM) was chosen for oral bioavailability studies based on its log P and solubility profile. A 10 mg/kg dose in dogs provided modest bioavailability with Cmax = 0.22 μg/mL. X-ray crystallographic analysis of two analogs revealed several interesting features responsible for the 3,4-(ethylenedioxy)benzyl-substituted analog's potency:  (1) Comparing the two complexes revealed two distinct binding modes for each P1/P1‘ substituent; (2) The ethylenedioxy moieties are within 3.6 Å of Pro 81 providing additional van der Waals contacts missing from the parent structure; (3) The enzyme's Arg 8 side chain moves away from the P1 substituent to accommodate the increased steric volume while maintaining a favorable hydrogen bond distance between the para oxygen substituent and the guanidine NH.

Published
1997

30. Discovery of Potent and Selective Inhibitors of Wild-Type and Gatekeeper Mutant Fibroblast Growth Factor Receptor (FGFR) 2/3.

Author

Shvartsbart A, Roach JJ, Witten MR, Koblish H, Harris JJ, Covington M, Hess R, Lin L, Frascella M, Truong L, Leffet L, Conlen P, Beshad E, Klabe R, Katiyar K, Kaldon L, Young-Sciame R, He X, Petusky S, Chen KJ, Horsey A, Lei HT, Epling LB, Deller MC, Vechorkin O, and Yao W

Subjects
Animals, Rats, Signal Transduction, Structure-Activity Relationship, Neoplasms drug therapy, Protein Kinase Inhibitors chemistry, Receptors, Fibroblast Growth Factor antagonists & inhibitors, Receptors, Fibroblast Growth Factor chemistry, Receptors, Fibroblast Growth Factor drug effects
Abstract

Upregulation of the fibroblast growth factor receptor (FGFR) signaling pathway has been implicated in multiple cancer types, including cholangiocarcinoma and bladder cancer. Consequently, small molecule inhibition of FGFR has emerged as a promising therapy for patients suffering from these diseases. First-generation pan-FGFR inhibitors, while highly effective, suffer from several drawbacks. These include treatment-related hyperphosphatemia and significant loss of potency for the mutant kinases. Herein, we present the discovery and optimization of novel FGFR2/3 inhibitors that largely maintain potency for the common gatekeeper mutants and have excellent selectivity over FGFR1. A combination of meticulous structure-activity relationship (SAR) analysis, structure-based drug design, and medicinal chemistry rationale ultimately led to compound 29 , a potent and selective FGFR2/3 inhibitor with excellent in vitro absorption, distribution, metabolism, excretion (ADME), and pharmacokinetics in rat. A pharmacodynamic study of a closely related compound established that maximum inhibition of downstream ERK phosphorylation could be achieved with no significant effect on serum phosphate levels relative to vehicle.

Published
2022
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31. Discovery of Pemigatinib: A Potent and Selective Fibroblast Growth Factor Receptor (FGFR) Inhibitor.

Author

Wu L, Zhang C, He C, Qian D, Lu L, Sun Y, Xu M, Zhuo J, Liu PCC, Klabe R, Wynn R, Covington M, Gallagher K, Leffet L, Bowman K, Diamond S, Koblish H, Zhang Y, Soloviev M, Hollis G, Burn TC, Scherle P, Yeleswaram S, Huber R, and Yao W

Subjects
Dose-Response Relationship, Drug, Humans, Molecular Structure, Morpholines chemical synthesis, Morpholines chemistry, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors chemistry, Pyrimidines chemical synthesis, Pyrimidines chemistry, Pyrroles chemical synthesis, Pyrroles chemistry, Receptor, Fibroblast Growth Factor, Type 1 metabolism, Receptor, Fibroblast Growth Factor, Type 2 metabolism, Receptor, Fibroblast Growth Factor, Type 3 metabolism, Structure-Activity Relationship, United States, United States Food and Drug Administration, Drug Discovery, Morpholines pharmacology, Protein Kinase Inhibitors pharmacology, Pyrimidines pharmacology, Pyrroles pharmacology, Receptor, Fibroblast Growth Factor, Type 1 antagonists & inhibitors, Receptor, Fibroblast Growth Factor, Type 2 antagonists & inhibitors, Receptor, Fibroblast Growth Factor, Type 3 antagonists & inhibitors
Abstract

Aberrant activation of FGFR has been linked to the pathogenesis of many tumor types. Selective inhibition of FGFR has emerged as a promising approach for cancer treatment. Herein, we describe the discovery of compound 38 (INCB054828, pemigatinib), a highly potent and selective inhibitor of FGFR1, FGFR2, and FGFR3 with excellent physiochemical properties and pharmacokinetic profiles. Pemigatinib has received accelerated approval from the U.S. Food and Drug Administration for the treatment of adults with previously treated, unresectable locally advanced or metastatic cholangiocarcinoma with a FGFR2 fusion or other rearrangement. Additional clinical trials are ongoing to evaluate pemigatinib in patients with FGFR alterations.

Published
2021
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32. INCB054828 (pemigatinib), a potent and selective inhibitor of fibroblast growth factor receptors 1, 2, and 3, displays activity against genetically defined tumor models.

Author

Liu PCC, Koblish H, Wu L, Bowman K, Diamond S, DiMatteo D, Zhang Y, Hansbury M, Rupar M, Wen X, Collier P, Feldman P, Klabe R, Burke KA, Soloviev M, Gardiner C, He X, Volgina A, Covington M, Ruggeri B, Wynn R, Burn TC, Scherle P, Yeleswaram S, Yao W, Huber R, and Hollis G

Subjects
Administration, Oral, Animals, Cell Line, Tumor, Female, Half-Life, Humans, Mice, Mice, Inbred C57BL, Mice, Nude, Mice, SCID, Morpholines chemistry, Morpholines pharmacokinetics, Neoplasms pathology, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors pharmacokinetics, Pyrimidines chemistry, Pyrimidines pharmacokinetics, Pyrroles chemistry, Pyrroles pharmacokinetics, Rats, Rats, Nude, Receptor, Fibroblast Growth Factor, Type 1 metabolism, Receptor, Fibroblast Growth Factor, Type 2 metabolism, Receptor, Fibroblast Growth Factor, Type 3 metabolism, Xenograft Model Antitumor Assays, Morpholines therapeutic use, Neoplasms drug therapy, Protein Kinase Inhibitors therapeutic use, Pyrimidines therapeutic use, Pyrroles therapeutic use, Receptor, Fibroblast Growth Factor, Type 1 antagonists & inhibitors, Receptor, Fibroblast Growth Factor, Type 2 antagonists & inhibitors, Receptor, Fibroblast Growth Factor, Type 3 antagonists & inhibitors
Abstract

Alterations in fibroblast growth factor receptor (FGFR) genes have been identified as potential driver oncogenes. Pharmacological targeting of FGFRs may therefore provide therapeutic benefit to selected cancer patients, and proof-of-concept has been established in early clinical trials of FGFR inhibitors. Here, we present the molecular structure and preclinical characterization of INCB054828 (pemigatinib), a novel, selective inhibitor of FGFR 1, 2, and 3, currently in phase 2 clinical trials. INCB054828 pharmacokinetics and pharmacodynamics were investigated using cell lines and tumor models, and the antitumor effect of oral INCB054828 was investigated using xenograft tumor models with genetic alterations in FGFR1, 2, or 3. Enzymatic assays with recombinant human FGFR kinases showed potent inhibition of FGFR1, 2, and 3 by INCB054828 (half maximal inhibitory concentration [IC50] 0.4, 0.5, and 1.0 nM, respectively) with weaker activity against FGFR4 (IC50 30 nM). INCB054828 selectively inhibited growth of tumor cell lines with activation of FGFR signaling compared with cell lines lacking FGFR aberrations. The preclinical pharmacokinetic profile suggests target inhibition is achievable by INCB054828 in vivo with low oral doses. INCB054828 suppressed the growth of xenografted tumor models with FGFR1, 2, or 3 alterations as monotherapy, and the combination of INCB054828 with cisplatin provided significant benefit over either single agent, with an acceptable tolerability. The preclinical data presented for INCB054828, together with preliminary clinical observations, support continued investigation in patients with FGFR alterations, such as fusions and activating mutations., Competing Interests: Holly Koblish, Liangxing Wu, Kevin Bowman, Sharon Diamond, Darlise DiMatteo, Yue Zhang, Michael Hansbury, Mark Rupar, Xiaoming Wen, Paul Collier, Patricia Feldman, Ronald Klabe, Krista A. Burke, Maxim Soloviev, Christine Gardiner, Xin He, Alla Volgina, Maryanne Covington, Richard Wynn, Timothy C. Burn, Swamy Yeleswaram, Wenqing Yao are employees of Incyte Corporationand own Incyte stock. Phillip C. C. Liu, Bruce Ruggeri, Peggy Scherle, Reid Huber, and Gregory Hollis were employees of Incyte employees Corporation at the time of this work and own Incyte stock.Our commercial affiliation does not alter our adherence to PLOS ONE policies on sharing data and materials.

Published
2020
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33. Isothiazolidinone inhibitors of PTP1B containing imidazoles and imidazolines.

Author

Douty B, Wayland B, Ala PJ, Bower MJ, Pruitt J, Bostrom L, Wei M, Klabe R, Gonneville L, Wynn R, Burn TC, Liu PC, Combs AP, and Yue EW

Subjects
Crystallography, X-Ray, Drug Design, Enzyme Inhibitors chemical synthesis, Imidazoles chemical synthesis, Imidazolines chemical synthesis, Imidazolines chemistry, Imidazolines pharmacology, Models, Molecular, Structure-Activity Relationship, Thiazoles chemical synthesis, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Imidazoles chemistry, Imidazoles pharmacology, Protein Tyrosine Phosphatase, Non-Receptor Type 1 antagonists & inhibitors, Thiazoles chemistry, Thiazoles pharmacology
Abstract

The structure-based design and synthesis of isothiazolidinone (IZD) inhibitors of PTP1B containing imidazoles and imidazolines and their modification to interact with the B site of PTP1B are described here. The X-ray crystal structures of 3I and 4I complexed with PTP1B were solved and revealed the inhibitors are interacting extensively with the B site of the enzyme.

Published
2008
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34. High-throughput determination of mode of inhibition in lead identification and optimization.

Author

Wei M, Wynn R, Hollis G, Liao B, Margulis A, Reid BG, Klabe R, Liu PC, Becker-Pasha M, Rupar M, Burn TC, McCall DE, and Li Y

Subjects
Animals, Baculoviridae genetics, Binding Sites, Catalytic Domain, Cell Line, Combinatorial Chemistry Techniques, Drug Design, Drug Evaluation, Preclinical, Escherichia coli genetics, Histidine chemistry, Humans, Inhibitory Concentration 50, Kinetics, Ligands, Protein Binding, Protein Structure, Tertiary, Protein Tyrosine Phosphatase, Non-Receptor Type 1, Protein Tyrosine Phosphatases chemistry, Protein Tyrosine Phosphatases metabolism, Spodoptera cytology, Spodoptera metabolism, Adenosine Triphosphate antagonists & inhibitors, Protein Tyrosine Phosphatases antagonists & inhibitors, Receptors, G-Protein-Coupled antagonists & inhibitors
Abstract

After finishing the primary high-throughput screening, the screening team is often faced with thousands of hits to be evaluated further. Effective filtering of these hits is crucial in identifying leads. Mode of inhibition (MOI) study is extremely useful in validating whether the observed compound activity is specific to the biological target. In this article, the authors describe a high-throughput MOI determination method for evaluating thousands of compounds using an existing screening infrastructure. Based on enzyme or receptor kinetics theory, the authors developed the method by measuring the ratio of IC(50) or percent inhibition at 2 carefully chosen substrate or ligand concentrations to define an inhibitor as competitive, uncompetitive, or noncompetitive. This not only facilitates binning of HTS hits according to their MOI but also greatly expands HTS utility in support of the medicinal chemistry team's lead optimization practice. Three case studies are presented to demonstrate how the method was applied successfully in 3 discovery programs targeting either an enzyme or a G-protein-coupled receptor.

Published
2007
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35. Structural basis for inhibition of protein-tyrosine phosphatase 1B by isothiazolidinone heterocyclic phosphonate mimetics.

Author

Ala PJ, Gonneville L, Hillman MC, Becker-Pasha M, Wei M, Reid BG, Klabe R, Yue EW, Wayland B, Douty B, Polam P, Wasserman Z, Bower M, Combs AP, Burn TC, Hollis GF, and Wynn R

Subjects
Binding Sites, Catalytic Domain, Crystallography, X-Ray, Escherichia coli genetics, Humans, Hydrogen Bonding, Hydrolysis, Inhibitory Concentration 50, Kinetics, Models, Molecular, Molecular Structure, Protein Conformation drug effects, Protein Structure, Secondary, Protein Structure, Tertiary, Protein Tyrosine Phosphatase, Non-Receptor Type 1, Protein Tyrosine Phosphatases analysis, Protein Tyrosine Phosphatases isolation & purification, Structure-Activity Relationship, Substrate Specificity, Water chemistry, Molecular Mimicry, Organophosphonates pharmacology, Protein Tyrosine Phosphatases antagonists & inhibitors, Protein Tyrosine Phosphatases chemistry, Thiazoles pharmacology
Abstract

Crystal structures of protein-tyrosine phosphatase 1B in complex with compounds bearing a novel isothiazolidinone (IZD) heterocyclic phosphonate mimetic reveal that the heterocycle is highly complementary to the catalytic pocket of the protein. The heterocycle participates in an extensive network of hydrogen bonds with the backbone of the phosphate-binding loop, Phe(182) of the flap, and the side chain of Arg(221). When substituted with a phenol, the small inhibitor induces the closed conformation of the protein and displaces all waters in the catalytic pocket. Saturated IZD-containing peptides are more potent inhibitors than unsaturated analogs because the IZD heterocycle and phenyl ring directly attached to it bind in a nearly orthogonal orientation with respect to each other, a conformation that is close to the energy minimum of the saturated IZD-phenyl moiety. These results explain why the heterocycle is a potent phosphonate mimetic and an ideal starting point for designing small nonpeptidic inhibitors.

Published
2006
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36. Cellular pharmacology of D-d4FC, a nucleoside analogue active against drug-resistant HIV.

Author

Erickson-Viitanen S, Wu JT, Shi G, Unger S, King RW, Fish B, Klabe R, Geleziunas R, Gallagher K, Otto MJ, and Schinazi RF

Subjects
Cells, Cultured, Cytidine Triphosphate analogs & derivatives, Cytidine Triphosphate metabolism, Drug Interactions, HIV Protease Inhibitors pharmacology, HIV Reverse Transcriptase antagonists & inhibitors, HIV-1 physiology, Humans, Intracellular Membranes metabolism, Leukocytes, Mononuclear metabolism, Nucleosides chemistry, Nucleosides pharmacology, Phosphorylation drug effects, Phytohemagglutinins, Zalcitabine analogs & derivatives, Anti-HIV Agents pharmacology, Cytidine Triphosphate pharmacology, Drug Resistance, Viral, HIV-1 drug effects, Leukocytes, Mononuclear drug effects, Reverse Transcriptase Inhibitors pharmacology
Abstract

The backbone of effective highly active antiretroviral therapy regimens for the treatment of HIV infections currently contains at least two nucleosides. Among the features that influence the potency of each component of a regimen and the overall efficacy of the combination are the cellular uptake and bioconversion of nucleoside analogues to their active triphosphate form, and the extent of possible interactions in these steps that might occur when more than one nucleoside is used in a regimen. D-d4FC (Reverset), a new cytidine analogue with the ability to inhibit many nucleoside-resistant viral variants, was examined for these parameters. In phytohemaglutinin-stimulated human peripheral blood mononuclear cells, D-d4FC was taken up in a rapid (8 h to 50% maximal value), saturable (plateau above 10 microM parent nucleoside concentration) process, resulting in levels of D-d4FC triphosphate that should provide potent antiviral activity against a variety of virus genotypes. Based on measurement of antiviral effects in cell culture, additive and in some cases, synergistic interactions were observed with protease inhibitors, non-nucleoside reverse transcriptase inhibitors or other nucleosides, including cytidine analogues.

Published
2003
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37. DPC 817: a cytidine nucleoside analog with activity against zidovudine- and lamivudine-resistant viral variants.

Author

Schinazi RF, Mellors J, Bazmi H, Diamond S, Garber S, Gallagher K, Geleziunas R, Klabe R, Pierce M, Rayner M, Wu JT, Zhang H, Hammond J, Bacheler L, Manion DJ, Otto MJ, Stuyver L, Trainor G, Liotta DC, and Erickson-Viitanen S

Subjects
Animals, Anti-HIV Agents pharmacokinetics, Anti-HIV Agents pharmacology, Cytidine chemical synthesis, Cytidine pharmacokinetics, HIV Infections drug therapy, HIV Reverse Transcriptase drug effects, HIV-1 genetics, Humans, Lamivudine pharmacokinetics, Lamivudine pharmacology, Macaca mulatta, Nucleosides chemical synthesis, Nucleosides chemistry, Nucleosides pharmacokinetics, Nucleosides pharmacology, Reverse Transcriptase Inhibitors pharmacokinetics, Reverse Transcriptase Inhibitors pharmacology, Zalcitabine analogs & derivatives, Zalcitabine chemical synthesis, Zalcitabine pharmacokinetics, Zidovudine pharmacokinetics, Zidovudine pharmacology, Cytidine analogs & derivatives, Cytidine pharmacology, Drug Resistance, Viral, HIV-1 drug effects, Zalcitabine pharmacology
Abstract

Highly active antiretroviral therapy (HAART) is the standard treatment for infection with the human immunodeficiency virus (HIV). HAART regimens consist of protease inhibitors or nonnucleoside reverse transcriptase inhibitors combined with two or more nucleoside reverse transcriptase inhibitors (NRTIs). DPC 817, 2',3'-didehydro-2',3'-dideoxy-5-fluorocytidine (PSI 5582 D-D4FC) is a potent inhibitor of HIV type 1 replication in vitro. Importantly, DPC 817 retains activity against isolates harboring mutations in the reverse transcriptase gene that confer resistance to lamivudine (3TC) and zidovudine (AZT), which are frequent components of initial HAART regimens. DPC 817 combines this favorable resistance profile with rapid uptake and conversion to the active metabolite DPC 817-triphosphate, which has an intracellular half-life of 13 to 17 h. Pharmacokinetics in the rhesus monkey suggest low clearance of parent DPC 817 and a plasma half-life longer than that of either AZT or 3TC. Together, these properties suggest that DPC 817 may be useful as a component of HAART regimens in individuals with resistance to older NRTI agents.

Published
2002
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38. Drug design with a new transition state analog of the hydrated carbonyl: silicon-based inhibitors of the HIV protease.

Author

Chen CA, Sieburth SM, Glekas A, Hewitt GW, Trainor GL, Erickson-Viitanen S, Garber SS, Cordova B, Jeffry S, and Klabe RM

Subjects
Cells, Cultured, Humans, Models, Molecular, Drug Design, HIV Protease Inhibitors chemistry, HIV Protease Inhibitors pharmacology, HIV-1 drug effects, Organosilicon Compounds chemistry, Organosilicon Compounds pharmacology
Abstract

Background: Silicon is the element most similar to carbon, and bioactive organosilanes have therefore been of longstanding interest. Design of bioactive organosilanes has often involved a systematic replacement of a bioactive molecule's stable carbon atoms with silicon. Silanediols, which are best known as unstable precursors of the robust and ubiquitous silicone polymers, have the potential to mimic an unstable carbon, the hydrated carbonyl. As a bioisostere of the tetrahedral intermediate of amide hydrolysis, a silanediol could act as a transition state analog inhibitor of protease enzymes., Results: Silanediol analogs of a carbinol-based inhibitor of the HIV protease were prepared as single enantiomers, with up to six stereogenic centers. As inhibitors of this aspartic protease, the silanediols were nearly equivalent to both their carbinol analogs and indinavir, a current treatment for AIDS, with low nanomolar K(i) values. IC(90) data from a cell culture assay mirrored the K(i) data, demonstrating that the silanediols can also cross cell membranes and deliver their antiviral effects., Conclusions: In their first evaluation as inhibitors of an aspartic protease, silanediol peptidomimetics have been found to be nearly as potent as currently available pharmaceutical agents, in enzyme and cell protection assays. These neutral, cell-permeable transition state analogs therefore provide a novel foundation for the design of therapeutic agents.

Published
2001
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39. DPC 681 and DPC 684: potent, selective inhibitors of human immunodeficiency virus protease active against clinically relevant mutant variants.

Author

Kaltenbach RF 3rd, Trainor G, Getman D, Harris G, Garber S, Cordova B, Bacheler L, Jeffrey S, Logue K, Cawood P, Klabe R, Diamond S, Davies M, Saye J, Jona J, and Erickson-Viitanen S

Subjects
Administration, Oral, Animals, Blood Proteins metabolism, Dogs, Drug Resistance, Microbial, Female, Genotype, HIV Protease Inhibitors pharmacokinetics, Humans, Injections, Intravenous, Male, Protein Binding, Sulfonamides pharmacokinetics, HIV Infections virology, HIV Protease Inhibitors pharmacology, HIV-1 drug effects, Sulfonamides pharmacology
Abstract

Human immunodeficiency virus (HIV) protease inhibitors (PIs) are important components of many highly active antiretroviral therapy regimens. However, development of phenotypic and/or genotypic resistance can occur, including cross-resistance to other PIs. Development of resistance takes place because trough levels of free drug are inadequate to suppress preexisting resistant mutant variants and/or to inhibit de novo-generated resistant mutant variants. There is thus a need for new PIs, which are more potent against mutant variants of HIV and show higher levels of free drug at the trough. We have optimized a series of substituted sulfonamides and evaluated the inhibitors against laboratory strains and clinical isolates of HIV type 1 (HIV-1), including viruses with mutations in the protease gene. In addition, serum protein binding was determined to estimate total drug requirements for 90% suppression of virus replication (plasma IC(90)). Two compounds resulting from our studies, designated DPC 681 and DPC 684, are potent and selective inhibitors of HIV protease with IC(90)s for wild-type HIV-1 of 4 to 40 nM. DPC 681 and DPC 684 showed no loss in potency toward recombinant mutant HIVs with the D30N mutation and a fivefold or smaller loss in potency toward mutant variants with three to five amino acid substitutions. A panel of chimeric viruses constructed from clinical samples from patients who failed PI-containing regimens and containing 5 to 11 mutations, including positions 10, 32, 46, 47, 50, 54, 63, 71, 82, 84, and 90 had mean IC(50) values of <20 nM for DPC 681 and DPC 681, respectively. In contrast, marketed PIs had mean IC(50) values ranging from 200 nM (amprenavir) to >900 nM (nelfinavir).

Published
2001
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40. Synthesis and evaluation of novel quinolinones as HIV-1 reverse transcriptase inhibitors.

Author

Patel M, McHugh RJ Jr, Cordova BC, Klabe RM, Bacheler LT, Erickson-Viitanen S, and Rodgers JD

Subjects
Antiviral Agents chemical synthesis, Drug Resistance genetics, HIV-1 genetics, Humans, Inhibitory Concentration 50, Mutation genetics, Quinolones chemical synthesis, Antiviral Agents pharmacology, HIV Reverse Transcriptase antagonists & inhibitors, HIV-1 drug effects, Quinolones pharmacology
Abstract

A series of 4,4-disubstituted quinolinones was prepared and evaluated as HIV-1 reverse transcriptase inhibitors. The C-3 substituted compound 9h displayed improved antiviral activity against clinically significant single (K103N) and double (K103N/L100I) mutant viruses.

Published
2001
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41. Trifluoromethyl-containing 3-alkoxymethyl- and 3-aryloxymethyl-2-pyridinones are potent inhibitors of HIV-1 non-nucleoside reverse transcriptase.

Author

Corbett JW, Kresge KJ, Pan S, Cordova BC, Klabe RM, Rodgers JD, and Erickson-Viitanen SK

Subjects
Anti-HIV Agents pharmacology, Combinatorial Chemistry Techniques, Cytopathogenic Effect, Viral drug effects, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacology, Fluorine chemistry, HIV Reverse Transcriptase genetics, HIV-1 drug effects, HIV-1 genetics, Inhibitory Concentration 50, Mutation, Pyridones chemical synthesis, Structure-Activity Relationship, Anti-HIV Agents chemical synthesis, HIV Reverse Transcriptase antagonists & inhibitors, Pyridones pharmacology
Abstract

3-Alkoxymethyl- and 3-aryloxymethyl-2-pyridinones were synthesized and evaluated for activity as non-nucleoside reverse transcriptase inhibitors (NNRTIs) of HIV-1. It was found that several compounds were potent inhibitors of HIV-1 with the most potent compound 24 exhibiting an IC90 = 32 nM. Compound 24 also possessed a potent resistance profile as demonstrated by submicromolar IC90s against several clinically meaningful mutant virus strains.

Published
2001
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42. Does a diol cyclic urea inhibitor of HIV-1 protease bind tighter than its corresponding alcohol form? A study by free energy perturbation and continuum electrostatics calculations.

Author

Wang L, Duan Y, Stouten P, De Lucca GV, Klabe RM, and Kollman PA

Subjects
Azepines, Binding Sites, HIV Protease Inhibitors pharmacology, In Vitro Techniques, Models, Molecular, Static Electricity, Thermodynamics, Urea chemistry, Urea metabolism, Urea pharmacology, HIV Protease Inhibitors chemistry, HIV Protease Inhibitors metabolism, Urea analogs & derivatives
Abstract

The cyclic urea inhibitors of HIV-1 protease generally have two hydroxyl groups on the seven-membered ring. In this study, free energy perturbation and continuum electrostatic calculations were used to study the contributions of the two hydroxyl groups to the binding affinity and solubility of a cyclic urea inhibitor DMP323. The results indicated that the inhibitor with one hydroxyl group has better binding affinity and solubility than the inhibitor with two hydroxyl groups. Therefore, removal of one hydroxyl group from DMP323 may help to improve the properties of DMP323. This is also likely to be true for other cyclic urea inhibitors. The study also illustrated the difficulty in accurate modeling of the binding affinities of HIV-1 protease inhibitors, which involves many possible protonation states of the two catalytic aspartic acids in the active site of the enzyme.

Published
2001
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43. 3,3a-Dihydropyrano[4,3,2-de]quinazolin-2(1H)-ones are potent non-nucleoside reverse transcriptase inhibitors.

Author

Corbett JW, Pan S, Markwalder JA, Cordova BC, Klabe RM, Garber S, Rodgers JD, and Erickson-Viitanen SK

Subjects
Binding Sites, Combinatorial Chemistry Techniques, Drug Resistance, HIV Reverse Transcriptase genetics, Heterocyclic Compounds, 2-Ring chemical synthesis, Heterocyclic Compounds, 2-Ring pharmacology, Heterocyclic Compounds, 3-Ring chemical synthesis, Heterocyclic Compounds, 3-Ring pharmacology, Humans, Inhibitory Concentration 50, Models, Molecular, Point Mutation, Pyrans chemical synthesis, Quinazolines chemical synthesis, Reverse Transcriptase Inhibitors pharmacology, Structure-Activity Relationship, HIV Reverse Transcriptase antagonists & inhibitors, Pyrans pharmacology, Quinazolines pharmacology, Reverse Transcriptase Inhibitors chemical synthesis
Abstract

A series of unique 3,3a-dihydropyrano[4,3,2-de]quinazolin-2(1H)-ones and a 2a,5-dihydro-2H-thieno[4,3,2-de]quinazo-line-4(3H)-thione were found to be HIV-1 non-nucleoside reverse transcriptase inhibitors. One of these compounds, as the racemate, possessed an IC90 = 4.6 nM against wild-type virus in a whole cell antiviral assay and had an IC90 = 76 and 897 nM against the clinically significant K103N and K103N/L100I mutant viruses, respectively.

Published
2001
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44. Novel 2,2-dioxide-4,4-disubstituted-1,3-H-2,1,3-benzothiadiazines as non-nucleoside reverse transcriptase inhibitors.

Author

Corbett JW, Gearhart LA, Ko SS, Rodgers JD, Cordova BC, Klabe RM, and Erickson-Viitanen SK

Subjects
Benzothiadiazines pharmacology, HIV-1 enzymology, Humans, Molecular Structure, Reverse Transcriptase Inhibitors pharmacology, Benzothiadiazines chemical synthesis, Reverse Transcriptase Inhibitors chemical synthesis
Abstract

Benzothiadiazine non-nucleoside reverse transcriptase inhibitors (NNRTIs) of HIV have been synthesized via a novel process to afford active inhibitors, with the most potent compound exhibiting an IC90 = 180 nM in a whole cell assay. The 2,2-dioxide-1H-2,1,3-benzothiadiazine ring system was constructed in one step from 2-amino-5-chlorobenzonitrile.

Published
2000
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45. Expanded-spectrum nonnucleoside reverse transcriptase inhibitors inhibit clinically relevant mutant variants of human immunodeficiency virus type 1.

Author

Corbett JW, Ko SS, Rodgers JD, Jeffrey S, Bacheler LT, Klabe RM, Diamond S, Lai CM, Rabel SR, Saye JA, Adams SP, Trainor GL, Anderson PS, and Erickson-Viitanen SK

Subjects
Amino Acid Substitution genetics, Animals, Anti-HIV Agents pharmacokinetics, Blood Proteins metabolism, HIV-1 enzymology, Half-Life, Humans, Macaca mulatta, Male, Pan troglodytes, Protein Binding, Reverse Transcriptase Inhibitors pharmacokinetics, Stereoisomerism, Anti-HIV Agents pharmacology, HIV Reverse Transcriptase antagonists & inhibitors, HIV-1 drug effects, HIV-1 genetics, Mutation physiology, Reverse Transcriptase Inhibitors pharmacology
Abstract

A research program targeted toward the identification of expanded-spectrum nonnucleoside reverse transcriptase inhibitors which possess increased potency toward K103N-containing mutant human immunodeficiency virus (HIV) and which maintain pharmacokinetics consistent with once-a-day dosing has resulted in the identification of the 4-cyclopropylalkynyl-4-trifluoromethyl-3, 4-dihydro-2(1H)quinazolinones DPC 961 and DPC 963 and the 4-cyclopropylalkenyl-4-trifluoromethyl-3, 4-dihydro-2(1H)quinazolinones DPC 082 and DPC 083 for clinical development. DPC 961, DPC 963, DPC 082, and DPC 083 all exhibit low-nanomolar potency toward wild-type virus, K103N and L100I single-mutation variants, and many multiply amino acid-substituted HIV type 1 mutants. This high degree of potency is combined with a high degree of oral bioavailability, as demonstrated in rhesus monkeys and chimpanzees, and with plasma serum protein binding that can result in significant free levels of drug.

Published
1999
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46. Synthesis and evaluation of benzoxazinones as HIV-1 reverse transcriptase inhibitors. Analogs of Efavirenz (SUSTIVA).

Author

Patel M, McHugh RJ Jr, Cordova BC, Klabe RM, Erickson-Viitanen S, Trainor GL, and Ko SS

Subjects
Alkynes, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, Benzoxazines, Cyclopropanes, Drug Evaluation, Preclinical, HIV Reverse Transcriptase drug effects, Oxazines pharmacology, Reverse Transcriptase Inhibitors chemistry, Reverse Transcriptase Inhibitors pharmacology, Structure-Activity Relationship, Anti-HIV Agents chemical synthesis, Oxazines chemical synthesis, Oxazines chemistry, Reverse Transcriptase Inhibitors chemical synthesis
Abstract

Two series of benzoxazinones differing in the aromatic substitution pattern were prepared and evaluated as HIV-1 reverse transcriptase inhibitors. The 5-fluoro (5a-d) and 6-nitro (5e-h) substituted compounds displayed activity comparable or better than Efavirenz, the lead structure of the series.

Published
1999
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47. Unsymmetrical cyclic ureas as HIV-1 protease inhibitors: novel biaryl indazoles as P2/P2' substituents.

Author

Patel M, Rodgers JD, McHugh RJ Jr, Johnson BL, Cordova BC, Klabe RM, Bacheler LT, Erickson-Viitanen S, and Ko SS

Subjects
Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, HIV Protease drug effects, HIV Protease Inhibitors pharmacology, HIV-1 enzymology, Urea pharmacology, HIV Protease Inhibitors chemistry, Urea chemistry
Abstract

The preparation of unsymmetrical cyclic ureas bearing novel biaryl indazoles as P2/P2' substituents was undertaken, utilizing a Suzuki coupling reaction as the key step. Compound 6i was equipotent to the lead compound of the series SE063.

Published
1999
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48. Synthesis and evaluation of analogs of Efavirenz (SUSTIVA) as HIV-1 reverse transcriptase inhibitors.

Author

Patel M, Ko SS, McHugh RJ Jr, Markwalder JA, Srivastava AS, Cordova BC, Klabe RM, Erickson-Viitanen S, Trainor GL, and Seitz SP

Subjects
Alkynes, Anti-HIV Agents pharmacology, Benzoxazines, Cyclopropanes, Molecular Structure, Oxazines pharmacology, Reverse Transcriptase Inhibitors pharmacology, Structure-Activity Relationship, Anti-HIV Agents chemical synthesis, HIV-1, Oxazines chemical synthesis, Oxazines chemistry, Reverse Transcriptase Inhibitors chemical synthesis
Abstract

Efavirenz (SUSTIVA) is a potent non-nucleoside reverse transcriptase inhibitor. Due to the observation of breakthrough mutations of the reverse transcriptase enzyme during Efavirenz therapy, we sought to develop an optimized second generation series. To that end, SAR of the substituents on the aromatic ring was undertaken and the results are summarized here. The 5,6-difluoro (4f) and the 6-methoxy (4m) substituted benzoxazinones were determined to be equipotent, and as a result such substitution patterns will be incorporated in second generation scaffolds.

Published
1999
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49. Increased antiviral activity of cyclic urea HIV protease inhibitors by modifying the P1/P1' substituents.

Author

Kaltenbach RF 3rd, Klabe RM, Cordova BC, and Seitz SP

Subjects
Drug Design, HIV Protease Inhibitors chemistry, HIV Protease Inhibitors pharmacology, Structure-Activity Relationship, Urea chemical synthesis, Urea pharmacology, HIV Protease Inhibitors chemical synthesis, Urea analogs & derivatives
Abstract

A series of alkyl substituted P1/P1' analogs was prepared in an attempt to increase translation of the 3-aminoindazole class of HIV protease inhibitors. Increasing the lipophilicity of the P1/P1' residues dramatically improved translation of enzyme activity to antiviral activity in the whole cell assay.

Published
1999
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50. Thermodynamic linkage between the binding of protons and inhibitors to HIV-1 protease.

Author

Trylska J, Antosiewicz J, Geller M, Hodge CN, Klabe RM, Head MS, and Gilson MK

Subjects
Hydrogen-Ion Concentration, Kinetics, Magnetic Resonance Spectroscopy, Oligopeptides pharmacology, Thermodynamics, Urea antagonists & inhibitors, HIV Protease Inhibitors chemistry, Protons
Abstract

The aspartyl dyad of free HIV-1 protease has apparent pK(a)s of approximately 3 and approximately 6, but recent NMR studies indicate that the aspartyl dyad is fixed in the doubly protonated form over a wide pH range when cyclic urea inhibitors are bound, and in the monoprotonated form when the inhibitor KNI-272 is bound. We present computations and measurements related to these changes in protonation and to the thermodynamic linkage between protonation and inhibition. The Poisson-Boltzmann model of electrostatics is used to compute the apparent pK(a)s of the aspartyl dyad in the free enzyme and in complexes with four different inhibitors. The calculations are done with two parameter sets. One assigns epsilon = 4 to the solute interior and uses a detailed model of ionization; the other uses epsilon = 20 for the solute interior and a simplified representation of ionization. For the free enzyme, both parameter sets agree well with previously measured apparent pK(a)s of approximately 3 and approximately 6. However, the calculations with an internal dielectric constant of 4 reproduce the large pKa shifts upon binding of inhibitors, but the calculations with an internal dielectric constant of 20 do not. This observation has implications for the accurate calculation of pK(a)s in complex protein environments. Because binding of a cyclic urea inhibitor shifts the pK(a)s of the aspartyl dyad, changing the pH is expected to change its apparent binding affinity. However, we find experimentally that the affinity is independent of pH from 5.5 to 7.0. Possible explanations for this discrepancy are discussed.

Published
1999
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