Your search keyword '"Tao ZF"' showing total 11 results

1. Synthesis and in-vitro biological activity of macrocyclic urea Chk1 inhibitors.

Author

Li G, Tao ZF, Tong Y, Przytulinska MK, Kovar P, Merta P, Chen Z, Zhang H, Sowin T, Rosenberg SH, and Lin NH

Subjects

Cell Line, Tumor, Checkpoint Kinase 1, HeLa Cells, Humans, Macrocyclic Compounds pharmacology, Protein Kinase Inhibitors pharmacology, Structure-Activity Relationship, Urea pharmacology, Macrocyclic Compounds chemical synthesis, Protein Kinase Inhibitors chemical synthesis, Protein Kinases metabolism, Urea chemical synthesis

Abstract

A variety of macrocyclic urea compounds were prepared as potent Chk1 inhibitors by modifying the C5 position of the benzene ring of the macrocyclic urea with ether moieties, aliphatic carbon chains, amide and halides. Enzymatic activity less than 20nM was observed in 29 of 40 compounds. Compounds 14, 46d, and 48j provided the best overall results in the cellular assays as they abrogated doxorubicin-induced cell cycle arrest (IC(50)=3.31, 3.08, and 3.13microM) and enhanced doxorubicin cytotoxicity (IC(50)=0.54, 1.27, and 0.96microM) while displaying no single agent activity, respectively.

Published

2007

2. Macrocyclic ureas as potent and selective Chk1 inhibitors: an improved synthesis, kinome profiling, structure-activity relationships, and preliminary pharmacokinetics.

Author

Tao ZF, Chen Z, Bui MH, Kovar P, Johnson E, Bouska J, Zhang H, Rosenberg S, Sowin T, and Lin NH

Subjects

Animals, Catalysis, Checkpoint Kinase 1, HeLa Cells, Humans, Macrocyclic Compounds pharmacology, Mice, Protein Kinase Inhibitors pharmacology, Structure-Activity Relationship, Urea pharmacology, Macrocyclic Compounds chemical synthesis, Macrocyclic Compounds pharmacokinetics, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors pharmacokinetics, Protein Kinases pharmacokinetics, Protein Kinases physiology, Urea chemical synthesis, Urea pharmacokinetics

Abstract

A new series of potent macrocyclic urea-based Chk1 inhibitors are described. A detailed SAR study on the 4-position of the phenyl ring of the 14-member macrocyclic ureas 1a and d led to the identification of the potent Chk1 inhibitors 2, 5-7, 10, 13, 14, 19-21, 25, 27, and 31-34. These compounds significantly sensitize tumor cells to the DNA-damaging antitumor agent doxorubicin in a cell-based assay and efficiently abrogate the doxorubicin-induced G2/M and camptothecin-induced S checkpoints, indicating that the potent biological activities of these compounds are mechanism-based through Chk1 inhibition. Kinome profiling analysis of a representative macrocyclic urea 25 against a panel of 120 kinases indicates that these novel macrocyclic ureas are highly selective Chk1 inhibitors. Preliminary PK studies of 1a and b suggest that the 14-member macrocyclic inhibitors may possess better PK properties than their 15-member counterparts. An improved synthesis of 2 and 20 by using 2-(trimethylsilyl)ethoxycarbonyl (Teoc) to protect the amino group not only readily provided the desired compounds in pure form but also facilitated the scale up of potent compounds for various biological studies.

Published

2007

3. Discovery of 4'-(1,4-dihydro-indeno[1,2-c]pyrazol-3-yl)-benzonitriles and 4'-(1,4-dihydro-indeno[1,2-c]pyrazol-3-yl)-pyridine-2'-carbonitriles as potent checkpoint kinase 1 (Chk1) inhibitors.

Author

Tao ZF, Li G, Tong Y, Stewart KD, Chen Z, Bui MH, Merta P, Park C, Kovar P, Zhang H, Sham HL, Rosenberg SH, Sowin TJ, and Lin NH

Subjects

Checkpoint Kinase 1, Nitriles chemistry, Protein Kinase Inhibitors chemistry, Structure-Activity Relationship, Nitriles pharmacology, Protein Kinase Inhibitors pharmacology, Protein Kinases drug effects

Abstract

An extensive structure-activity relationship study of the 3-position of a series of tricyclic pyrazole-based Chk1 inhibitors is described. As a result, 4'-(1,4-dihydro-indeno[1,2-c]pyrazol-3-yl)-benzonitriles (4) and 4'-(1,4-dihydro-indeno[1,2-c]pyrazol-3-yl)-pyridine-2'-carbonitriles (29) emerged as new lead series. Compared with the original lead compound 2, these new leads fully retain the biological activity in both enzymatic inhibition and cell-based assays. More importantly, the new leads 4 and 29 exhibit favorable physicochemical properties such as lower molecular weight, lower Clog P, and the absence of a hydroxyl group. Furthermore, structure-activity relationship studies were performed at the 6- and 7-positions of 4, which led to the identification of ideal Chk1 inhibitors 49, 50, 51, and 55. These compounds not only potently inhibit Chk1 in an enzymatic assay but also significantly potentiate the cytotoxicity of DNA-damaging agents in cell-based assays while they show little single agent activity. A cell cycle analysis by FACS confirmed that these Chk1 inhibitors efficiently abrogate the G2/M and S checkpoints induced by DNA-damaging agent. The current work paved the way to the identification of several potent Chk1 inhibitors with good pharmacokinetics that are suitable for in vivo study with oral dosing.

Published

2007

4. Cyanopyridyl containing 1,4-dihydroindeno[1,2-c]pyrazoles as potent checkpoint kinase 1 inhibitors: improving oral biovailability.

Author

Tong Y, Przytulinska M, Tao ZF, Bouska J, Stewart KD, Park C, Li G, Claiborne A, Kovar P, Chen Z, Merta PJ, Bui MH, Olson A, Osterling D, Zhang H, Sham HL, Rosenberg SH, Sowin TJ, and Lin NH

Subjects

Administration, Oral, Animals, Checkpoint Kinase 1, Cyanides chemistry, Indenes chemistry, Inhibitory Concentration 50, Mice, Molecular Structure, Protein Kinase Inhibitors administration & dosage, Protein Kinase Inhibitors chemical synthesis, Pyrazoles administration & dosage, Pyrazoles chemical synthesis, Rats, Structure-Activity Relationship, Hydrogen chemistry, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors pharmacology, Protein Kinases metabolism, Pyrazoles chemistry, Pyrazoles pharmacology, Pyridines chemistry

Abstract

A series of 1,4-dihydroindeno[1,2-c]pyrazole compounds with a cyanopyridine moiety at the 3-position of the tricyclic pyrazole core was explored as potent CHK-1 inhibitors. The impact of substitutions at the 6 and/or 7-position of the core on pharmacokinetic properties was studied in detail. Compounds carrying a side chain with an ether linker at the 7-position and a terminal morpholino group, such as 29 and 30, exhibited much-improved oral biovailability in mice as compared to earlier generation inhibitors. These compounds also possessed desirable cellular activity in potentiating doxorubicin and will serve as valuable tool compounds for in vivo evaluation of CHK-1 inhibitors to sensitize DNA-damaging agents.

Published

2007

5. Design, synthesis, and biological activity of 5,10-dihydro-dibenzo[b,e][1,4]diazepin-11-one-based potent and selective Chk-1 inhibitors.

Author

Wang L, Sullivan GM, Hexamer LA, Hasvold LA, Thalji R, Przytulinska M, Tao ZF, Li G, Chen Z, Xiao Z, Gu WZ, Xue J, Bui MH, Merta P, Kovar P, Bouska JJ, Zhang H, Park C, Stewart KD, Sham HL, Sowin TJ, Rosenberg SH, and Lin NH

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Azepines chemistry, Azepines pharmacology, Benzodiazepinones chemistry, Benzodiazepinones pharmacology, Biological Availability, Camptothecin pharmacology, Cell Line, Tumor, Checkpoint Kinase 1, Crystallography, X-Ray, Doxorubicin pharmacology, Drug Design, Drug Synergism, Humans, Mice, Models, Molecular, Protein Binding, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors pharmacology, Protein Kinases chemistry, Structure-Activity Relationship, Antineoplastic Agents chemical synthesis, Azepines chemical synthesis, Benzodiazepinones chemical synthesis, Protein Kinase Inhibitors chemical synthesis, Protein Kinases metabolism

Abstract

A novel series of 5,10-dihydro-dibenzo[b,e][1,4]diazepin-11-ones have been synthesized as potent and selective checkpoint kinase 1 (Chk1) inhibitors via structure-based design. Aided by protein X-ray crystallography, medicinal chemistry efforts led to the identification of compound 46d, with potent enzymatic activity against Chk1 kinase. While maintaining a low cytotoxicity of its own, compound 46d exhibited a strong ability to abrogate G2 arrest and increased the cytotoxicity of camptothecin by 19-fold against SW620 cells. Pharmacokinetic studies revealed that it had a moderate bioavailabilty of 20% in mice. Two important binding interactions between compound 46b and Chk1 kinase, revealed by X-ray cocrystal structure, were hydrogen bonds between the hinge region and the amide bond of the core structure and a hydrogen bond between the methoxy group and Lys38 of the protein.

Published

2007

6. Synthesis and biological evaluation of 4'-(6,7-disubstituted-2,4-dihydro-indeno[1,2-c]pyrazol-3-yl)-biphenyl-4-ol as potent Chk1 inhibitors.

Author

Tao ZF, Li G, Tong Y, Chen Z, Merta P, Kovar P, Zhang H, Rosenberg SH, Sham HL, Sowin TJ, and Lin NH

Subjects

Checkpoint Kinase 1, Drug Evaluation, Preclinical, HeLa Cells, Humans, Protein Kinase Inhibitors chemistry, Pyrazoles chemistry, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors pharmacology, Protein Kinases drug effects, Pyrazoles chemical synthesis, Pyrazoles pharmacology

Abstract

A new series of potent tricyclic pyrazole-based Chk1 inhibitors are described. Analogues disubstituted on the 6- and 7-positions show improved Chk1 inhibition potency compared with analogues with a single substituent on either the 6- or 7-position. Based on the lead compound 4'-(6,7-dimethoxy-2,4-dihydro-indeno[1,2-c]pyrazol-3-yl)-biphenyl-4-ol (2), detailed SAR studies on the 6- and 7-positions were performed. 3'-morpholin-4'-yl-propoxy, pyridin-4'-ylmethoxy, pyridin-3'-ylmethoxy, 2'-(5''-ethyl-pyridin-2''-yl)-ethoxy, pyridin-2'-ylethoxy, (6'-methyl-pyridin-2'-yl)-propoxyethoxy, 2',3'-dihydroxyl-1'-yl-propoxy, and tetrahydro-furan-3'-yloxy have been identified as the best groups on the 6-position when the 7-position is substituted with methoxyl group. Pyridin-2'-ylmethoxy and pyridin-3'-ylmethoxy have been identified as the best substituents at the 7-position while the 6-position bearing methoxyl group. These compounds significantly potentiate the cytotoxicity of DNA-damaging antitumor agents in a cell-based assay and efficiently abrogate the doxorubicin-induced G2/M and the camptothecin-induced S checkpoints, suggesting that their potent biological activities are mechanism-based through Chk1 inhibition.

Published

2007

7. 1,4-Dihydroindeno[1,2-c]pyrazoles as potent checkpoint kinase 1 inhibitors: extended exploration on phenyl ring substitutions and preliminary ADME/PK studies.

Author

Tong Y, Claiborne A, Pyzytulinska M, Tao ZF, Stewart KD, Kovar P, Chen Z, Credo RB, Guan R, Merta PJ, Zhang H, Bouska J, Everitt EA, Murry BP, Hickman D, Stratton TJ, Wu J, Rosenberg SH, Sham HL, Sowin TJ, and Lin NH

Subjects

Animals, Antineoplastic Agents chemistry, Caco-2 Cells, Checkpoint Kinase 1, DNA Damage, Drug Design, Flow Cytometry, Humans, Inhibitory Concentration 50, Mice, Microsomes, Liver metabolism, Protein Kinase Inhibitors chemistry, Protein Kinases metabolism, Rats, Antineoplastic Agents pharmacokinetics, Chemistry, Pharmaceutical methods, Drug Screening Assays, Antitumor, Protein Kinase Inhibitors pharmacokinetics, Protein Kinases chemistry

Abstract

A study on substitutions at the four open positions on the phenyl ring of the 1,4-dihydroindeno[1,2-c]pyrazoles as potent CHK-1 inhibitors is described. Bis-substitution at both the 6- and 7-positions led to inhibitors with IC(50) values below 0.3nM. The compound with the best overall activities (36) was able to potentiate the anti-proliferative effect of doxorubicin in HeLa cells by at least 47-fold. Physicochemical, metabolic, and pharmacokinetic properties of selected inhibitors are also disclosed.

Published

2007

8. Structure-based design, synthesis, and biological evaluation of potent and selective macrocyclic checkpoint kinase 1 inhibitors.

Author

Tao ZF, Wang L, Stewart KD, Chen Z, Gu W, Bui MH, Merta P, Zhang H, Kovar P, Johnson E, Park C, Judge R, Rosenberg S, Sowin T, and Lin NH

Subjects

Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Camptothecin pharmacology, Cell Line, Tumor, Checkpoint Kinase 1, Crystallography, X-Ray, DNA Damage, Doxorubicin pharmacology, Drug Design, Drug Screening Assays, Antitumor, Drug Synergism, Humans, Macrocyclic Compounds chemistry, Macrocyclic Compounds pharmacology, Models, Molecular, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors pharmacology, Protein Kinases metabolism, Structure-Activity Relationship, Urea chemistry, Urea pharmacology, Antineoplastic Agents chemical synthesis, Macrocyclic Compounds chemical synthesis, Protein Kinase Inhibitors chemical synthesis, Protein Kinases chemistry, Urea analogs & derivatives, Urea chemical synthesis

Abstract

Based on the crystallographic analysis of a urea-checkpoint kinase 1 (Chk1) complex and molecular modeling, a class of macrocyclic Chk1 inhibitors were designed and their biological activities were evaluated. An efficient synthetic methodology for macrocyclic ureas was developed with Grubbs metathesis macrocyclization as the key step. The structure-activity relationship studies demonstrated that the macrocyclization retains full Chk1 inhibition activity and that the 4-position of the phenyl ring can tolerate a wide variety of substituents. These novel Chk1 inhibitors exhibit excellent selectivity over a panel of more than 70 kinases. Compounds 5b, 5c, 5f, 15, 16d, 17g, 17h, 17k, 18d, and 22 were identified as ideal Chk1 inhibitors, which showed little or no single-agent activity but significantly potentiate the cytotoxicities of the DNA-damaging antitumor agents doxorubicin and camptothecin. These novel Chk1 inhibitors abrogate the doxorubicin-induced G2 and camptothecin-induced S checkpoint arrests, confirming that their potent biological activities are mechanism-based through Chk1 inhibition.

Published

2007

9. Selective Chk1 inhibitors differentially sensitize p53-deficient cancer cells to cancer therapeutics.

Author

Chen Z, Xiao Z, Gu WZ, Xue J, Bui MH, Kovar P, Li G, Wang G, Tao ZF, Tong Y, Lin NH, Sham HL, Wang JY, Sowin TJ, Rosenberg SH, and Zhang H

Subjects

Antibodies pharmacology, Blotting, Western, CDC2 Protein Kinase immunology, CDC2 Protein Kinase metabolism, Camptothecin pharmacology, Caspases metabolism, Cell Cycle drug effects, Cell Line, Tumor, Cell Proliferation drug effects, Cell Proliferation radiation effects, Cell Survival drug effects, Cell Survival radiation effects, Checkpoint Kinase 1, DNA Damage, Dose-Response Relationship, Drug, Doxorubicin pharmacology, Drug Synergism, HeLa Cells, Humans, Molecular Structure, Neoplasms drug therapy, Neoplasms metabolism, Neoplasms pathology, Phosphorylation drug effects, Protein Kinase Inhibitors chemistry, Protein Kinases genetics, Protein Kinases immunology, Protein Serine-Threonine Kinases antagonists & inhibitors, Protein Serine-Threonine Kinases metabolism, RNA, Small Interfering genetics, Time Factors, Tumor Suppressor Protein p53 genetics, Urea chemistry, Urea pharmacology, cdc25 Phosphatases genetics, cdc25 Phosphatases metabolism, Protein Kinase Inhibitors pharmacology, Protein Kinases metabolism, Tumor Suppressor Protein p53 deficiency, Urea analogs & derivatives

Abstract

The majority of cancer therapeutics induces DNA damage to kill cells. Normal proliferating cells undergo cell cycle arrest in response to DNA damage, thus allowing DNA repair to protect the genome. DNA damage induced cell cycle arrest depends on an evolutionarily conserved signal transduction network in which the Chk1 kinase plays a critical role. In mammalian cells, the p53 and RB pathways further augment the cell cycle arrest response to prevent catastrophic cell death. Given the fact that most tumor cells suffer defects in the p53 and RB pathways, it is likely that tumor cells would depend more on the Chk1 kinase to maintain cell cycle arrest than would normal cells. Therefore Chk1 inhibition could be used to specifically sensitize tumor cells to DNA-damaging agents. We have previously shown that siRNA-mediated Chk1 knockdown abrogates DNA damage-induced checkpoints and potentiates the cytotoxicity of several DNA-damaging agents in p53-deficient cell lines. In this study, we have developed 2 potent and selective Chk1 inhibitors, A-690002 and A-641397, and shown that these compounds abrogate cell cycle checkpoints and potentiate the cytotoxicity of topoisomerase inhibitors and gamma-radiation in p53-deficient but not in p53-proficient cells of different tissue origins. These results indicate that it is feasible to achieve a therapeutic window with 1 or more Chk1 inhibitors in potentiation of cancer therapy based on the status of the p53 pathway in a wide spectrum of tumor types., (Copyright 2006 Wiley-Liss, Inc.)

Published

2006

10. Chk1 inhibitors for novel cancer treatment.

Author

Tao ZF and Lin NH

Subjects

Antineoplastic Agents chemical synthesis, Antineoplastic Agents therapeutic use, Checkpoint Kinase 1, Chemotherapy, Adjuvant methods, Clinical Trials, Phase I as Topic, Drug Synergism, Humans, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors therapeutic use, Protein Kinases drug effects, Antineoplastic Agents chemistry, Cell Cycle drug effects, DNA Damage drug effects, Protein Kinase Inhibitors chemistry, Protein Kinases metabolism

Abstract

Chemo- and radiotherapies that target DNA are the mainstay of cancer treatment. In response to DNA damage, cells are arrested in multiple checkpoints in the cell cycle to allow the damaged DNA to be repaired before progressing into mitosis. Normal cells are arrested in the G1 phase mediated by the p53 tumor suppressor, and p53-deficient cancer cells are arrested in the S or G2 phase. Checkpoint kinase 1 (Chk 1) is a serine / threonine protein kinase and a key mediator in the DNA damage-induced checkpoint network. When the G2 or S checkpoint is abrogated by the inhibition of Chk1, p53-deficient cancer cells undergo mitotic catastrophe and eventually apoptosis, whereas normal cells are still arrested in the G1 phase. Thus, Chk1 inhibitors can preferentially potentiate the efficacy of DNA damaging agents in cancer cells, and Chk1 is an attractive therapeutic target for cancer treatment, especially since approximately 50% of all human cancers are p53-deficient. This review discusses the rationale of Chk1 as an anticancer target, the structural basis for designing Chk1 inhibitors, and recently disclosed Chk1 inhibitors.

Published

2006

11. Synthesis and biological evaluation of 1-(2,4,5-trisubstituted phenyl)-3-(5-cyanopyrazin-2-yl)ureas as potent Chk1 kinase inhibitors.

Author

Li G, Hasvold LA, Tao ZF, Wang GT, Gwaltney SL 2nd, Patel J, Kovar P, Credo RB, Chen Z, Zhang H, Park C, Sham HL, Sowin T, Rosenberg SH, and Lin NH

Subjects

Antibiotics, Antineoplastic chemical synthesis, Checkpoint Kinase 1, Crystallography, X-Ray, Doxorubicin pharmacology, Humans, Inhibitory Concentration 50, Nitriles chemical synthesis, Nitriles pharmacology, Protein Kinase Inhibitors chemical synthesis, Protein Kinases metabolism, Pyrazines chemical synthesis, Pyrazines pharmacology, Tumor Cells, Cultured, Urea analogs & derivatives, Urea chemical synthesis, Urea pharmacology, Antibiotics, Antineoplastic pharmacology, Cell Cycle drug effects, Protein Kinase Inhibitors pharmacology, Protein Kinases drug effects

Abstract

Based on the X-ray crystallography of our lead compound 1-(5-chloro-2,4-dimethoxyphenyl)-3-(5-cyanopyrazin-2-yl)urea in the checkpoint kinase 1 (Chk1) enzyme, we modified R4, and to a lesser extent, R2, and R5 of the phenyl ring, and made a variety of N-aryl-N'-pyrazinylurea Chk1 inhibitors. Enzymatic activity less than 20 nM was observed in 15 of 41 compounds. Compound 8i provided the best overall results in the cellular assays as it abrogated doxorubicin-induced cell cycle arrest (IC50=1.7 microM) and enhanced doxorubicin cytotoxicity (IC50=0.44 microM) while displaying no single agent activity.

Published

2006