Novel Inhibitor of Rho Kinase 2013

Abstract

The arising critical implications of Rho kinase signaling in cardiovascular diseases have been attracting attention in the pharmacological potential of Rho kinase inhibitors.

We identified a novel inhibitor of Rho kinase (2-(1H-indazole-5-yl)amino-4-methoxy-6-piperazino triazine; DW 1865) and characterized its effects in biochemical, cellular, tissue and animal based assays. DW 1865 potently inhibited the kinase activity of both Rho kinase 1 and Rho kinase 2 in vitro, and behaved as an ATP-competitive inhibitor.


Interestingly, DW1865 was 10 times more potent in inhibiting Rho kinase activities than fasudil as a selective Rho kinase inhibitor.


The activity of DW1865 was shown to be highly selective for Rho kinase in the panel assay of 13 other kinases.


In the isolated vascular tissue study,
DW1865 exerted vasorelaxation in phenylephrine- or
5-hydroxytriptamine-induced contraction in a concentration-dependent manner manner.


In spontaneously hypertensive rats, administration of DW1865 caused a significant and dose-related reduction in blood pressure. Furthermore, DW1865 blocked angiotensin II-induced stress fiber formation and cellular hypertrophy in rat heart-derived H9c2 cells.


Taken together, these results suggest that DW1865 is a highly selective and potent Rho kinase inhibitor that will alleviate the pathophysiological actions of Rho kinase such as stress fiber formation, cellular hypertrophy, and hypertension.

 

---

Graphical abstract

Keywords

• Rho kinase;
• Hypertrophy;
• Hypertension;
• Cardiovascular effect

Cu-Mediated N-Arylation of I)ndazoles 2004

Cupric acetate-mediated N-arylation with aryl boronic acids proceeded regioselectively to form the N-2-substituted derivatives.

 

Abstract

 

 

 

A N-derivatized 3-dimethylaminopropyloxypyrazole library was prepared using solution-phase parallel synthesis.

 

The library was designed using physicochemical constraints designed to remove non-membrane-permeable molecules.

 

 

Cupric acetate-mediated N-arylation with aryl boronic acids proceeded regioselectively to form the N-2-substituted derivatives. The presence of the 3-dimethylaminopropyloxy group was found to completely control the regioselectivity of the arylation. Presence of a dimethylaminoethyloxy or dimethylaminobutyloxy group gave a lesser degree of regioselectivity. The scope of the method as applied to library synthesis is discussed.

 

 

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• 

  Synthesis and Biological Evaluation of the 1-Arylpyrazole Class of σ₁ Receptor Antagonists: Identification of 4-{2-[5-Methyl-1-(naphthalen-2-yl)-1H-pyrazol-3-yloxy]ethyl}morpholine (S1RA, E-52862)

  José Luis Díaz, Rosa Cuberes, Joana Berrocal, Montserrat Contijoch, Ute Christmann, Ariadna Fernández, Adriana Port, Jörg Holenz, Helmut Buschmann, Christian Laggner, Maria Teresa Serafini, Javier Burgueño, Daniel Zamanillo, Manuel Merlos, José Miguel Vela, and Carmen Almansa
  Journal of Medicinal Chemistry2012 55 (19), 8211-8224

  • Synthesis and Biological Evaluation of the 1-Arylpyrazole Class of σ₁ Receptor Antagonists: Identification of 4-{2-[5-Methyl-1-(naphthalen-2-yl)-1H-pyrazol-3-yloxy]ethyl}morpholine (S1RA, E-52862)

    José LuisDíaz, RosaCuberes, JoanaBerrocal, MontserratContijoch, UteChristmann, AriadnaFernández, AdrianaPort, JörgHolenz, HelmutBuschmann, ChristianLaggner, Maria TeresaSerafini, JavierBurgueño, DanielZamanillo, ManuelMerlos, José MiguelVela, and CarmenAlmansa
    Journal of Medicinal Chemistry2012 55 (19), 8211-8224
    The synthesis and pharmacological activity of a new series of 1-arylpyrazoles as potent σ1 receptor (σ1R) antagonists are reported. The new compounds were evaluated in vitro in human σ1R and guinea pig σ2 receptor (σ2R) binding assays. The nature of the ...
    
    Abstract | Full Text HTML | PDF | PDF w/ Links
• 

  Transmetalation of Unsaturated Carbon Nucleophiles from Boron-Containing Species to the Mid to Late d-Block Metals of Relevance to Catalytic C−X Coupling Reactions (X = C, F, N, O, Pb, S, Se, Te)

  David V. Partyka
  Chemical Reviews2011 111 (3), 1529-1595

  • Transmetalation of Unsaturated Carbon Nucleophiles from Boron-Containing Species to the Mid to Late d-Block Metals of Relevance to Catalytic C−X Coupling Reactions (X = C, F, N, O, Pb, S, Se, Te)

    David V.Partyka
    Chemical Reviews2011 111 (3), 1529-1595
    Abstract | Full Text HTML | PDF | PDF w/ Links
• 

  Three-Component, One-Pot Reaction for the Combinatorial Synthesis of 1,3,4-Substituted Pyrazoles

  Fuchun Xie, Gang Cheng, and Youhong Hu
  Journal of Combinatorial Chemistry2006 8 (3), 286-288

  • Three-Component, One-Pot Reaction for the Combinatorial Synthesis of 1,3,4-Substituted Pyrazoles

    FuchunXie, GangCheng, and YouhongHu
    Journal of Combinatorial Chemistry2006 8 (3), 286-288
    Abstract | Full Text HTML | PDF | PDF w/ Links
• 

  Comprehensive Survey of Combinatorial Library Synthesis:  2004

  Roland E. Dolle
  Journal of Combinatorial Chemistry2005 7 (6), 739-798

  • Comprehensive Survey of Combinatorial Library Synthesis:  2004

    Roland E.Dolle
    Journal of Combinatorial Chemistry2005 7 (6), 739-798
    Abstract | Full Text HTML | PDF | PDF w/ Links
• 

  Cu(OAc)₂-Catalyzed N-Arylations of Sulfoximines with Aryl Boronic Acids

  Christian Moessner and Carsten Bolm
  Organic Letters2005 7 (13), 2667-2669

シグナル創薬分子

シグナル創薬のターゲット：　mTOR

 

http://www.cstj.co.jp/reference/pathway/mTor.php

 

 

 

mTORは、細胞の栄養状態を反映し、蛋白合成、細胞増殖、血管新生、免疫などを制御する。mTOR阻害剤は、ステントの再狭窄防止、抗癌剤、免疫抑制剤として実用化されている。

• エベロリムスは、臓器移植後の免疫抑制剤、腎細胞癌、乳癌の治療薬として認可されている。また冠動脈ステントの再狭窄防止剤として用いられている。
• シロリムス, テムシロリムス, ゾタロリムスなども臨床応用されている。

 

 

文献：

1. ^ Cafferkey et al.: Mol Cell Biol. 1993; 13(10), 6012-23. Dominant missense mutations in a novel yeast protein related to mammalian phosphatidylinositol 3-kinase and VPS34 abrogate rapamycin cytotoxicity.
2. ^ Helliwell et al.: Mol Biol Cell. 1994; 5(1), 105-18. TOR1 and TOR2 are structurally and functionally similar but not identical phosphatidylinositol kinase homologues in yeast.
3. ^ Sabers et al.: J Biol Chem. 1995; 270(2), 815-22. Isolation of a protein target of the FKBP12-rapamycin complex in mammalian cells.

外部リンク[編集]

• mTOR シグナル伝達

ROCK, Rho-kinase

Graphical abstract

Rho-kinase inhibitors developed recently,

classified as isoquinolines, pyridines, indazoles,

pyrazoles or others, are promising candidates

for the treatment of CNS disorders,

cardiovascular diseases, cancer and so on.

 

 

 

Keywords

• RhoA;
• Rho kinase;
• Inhibitors;
• Central nervous system;
• Fasudil

Abbreviations

• ACS, acute coronary syndrome;
• AP-1, activator protein-1;
• AT1, angiotensin II type 1 receptor;
• CNS, central nervous system;
• CPI-17, PKC-potentiated inhibitory protein 17;
• CPK, creatine phosphokinase;
• CRD, C-terminal cysteine-rich domain;
• CRMP-2, collapsin response mediator protein 2;
• DMPK, myotonic dystrophy kinase;
• ERK, extracellular signal-regulated kinase;
• ERM, ezrin/radixin/moesin family;
• ET-1, endothelin-1;
• GAPs, GTPase-activating proteins;
• GDIs, GDP dissociation inhibitors;
• GEFs, guanine nucleotide exchange factors;
• HCC, hepatocellular carcinoma;
• 5-HT, 5-hydroxytryptamine;
• IP3, inositol 1,4,5-trisphosphate;
• LDH, lactate dehydrogenase;
• MCP-1, monocyte chemoattractant protein-1;
• MEK, mitogen-activated protein kinase;
• MES, maximal electroconvulsive shock;
• MLC, myosin light chain;
• MRCK, myotonic dystrophy kinase-related CDC42-binding kinase;
• MYPT-1, myosin phosphatase target subunit 1;
• NLSs, nuclear localization signals;
• OpN, optic nerve;
• PAH, pulmonary arterial hypertension;
• PAI-1, plasminogen activator inhibitor-1;
• PH, pleckstrin homology;
• PTEN, phosphatase and tensin homolog deleted on chromosome 10;
• PTZ, pentylenetetrazole;
• RBD, Rho-binding domain;
• ROCK, Rho-kinase;
• UPS, ubiquitin–proteasome system;
• VA, vasospastic angina;
• VCAM-1, vascular cell adhesion molecule-1;
• VSMC, vascular smooth muscle cell

High RhoA Inhibition Activities with IC50 values of 1.24 to 3.00 μM

A series of first-in-class small molecular RhoA inhibitors:

Abstract

 

 

 

RhoA is a member of Rho GTPases, a subgroup of the Ras superfamily of small GTP-binding proteins.

 

 

RhoA, as an important regulator of diverse cellular signaling pathways, plays significant roles in cytoskeletal organization, transcription, and cell-cycle progression.

 

 

The RhoA/ROCK inhibitors have emerged as a new promising treatment for cardiovascular diseases.

 

 

However, to date, RhoA inhibitors are macromolecules, and to our knowledge, small molecular-based inhibitors have not been reported. In this study, a series of first-in-class small molecular RhoA inhibitors have been discovered by using structure-based virtual screening in conjunction with chemical synthesis and bioassay. Virtual screening of ∼200,000 compounds, followed by SPR-based binding affinity assays resulted in three compounds with binding affinities to RhoA at the micromolar level (compounds 1–3).

 

 

Compound 1 was selected for further structure modifications in considering binding activity and synthesis ease. Fourty-one new compounds (1, 12a–v, 13a–h, and 14a–j) were designed and synthesized accordingly. It was found that eight (12a, 12j, 14a, 14b, 14d, 14e, 14 g, and 14h) showed high RhoA inhibition activities with IC50 values of 1.24 to 3.00 μM. A pharmacological assay indicated that two compounds (14g and 14 h) demonstrated noticeable vasorelaxation effects against PE-induced contraction in thoracic aorta artery rings and served as good leads for developing more potent cardiovascular agents.

 

 

 

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• 

  Discovery of Novel Inhibitors Targeting the Macrophage Migration Inhibitory Factor via Structure-Based Virtual Screening and Bioassays

  Lei Xu, Yu Zhang, Longtai Zheng, Chunhua Qiao, Youyong Li, Dan Li, Xuechu Zhen, and Tingjun Hou
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  • Discovery of Novel Inhibitors Targeting the Macrophage Migration Inhibitory Factor via Structure-Based Virtual Screening and Bioassays

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    Journal of Medicinal Chemistry2014 57 (9), 3737-3745
    Macrophage migration inhibitory factor (MIF) is involved in regulation of both the innate and the adaptive immune responses and is regarded as an attractive anti-inflammatory pharmacological target. In this study, molecular docking-based virtual screening ...
    
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• 

  Hit Identification and Optimization in Virtual Screening: Practical Recommendations Based on a Critical Literature Analysis

  Tian Zhu, Shuyi Cao, Pin-Chih Su, Ram Patel, Darshan Shah, Heta B. Chokshi, Richard Szukala, Michael E. Johnson, and Kirk E. Hevener
  Journal of Medicinal Chemistry2013 56 (17), 6560-6572

Orally Bioavailable Dihydropyrimidine Inhibitors of Rho Kinase (ROCK1)

 Orally Bioavailable Dihydropyrimidine Inhibitors of Rho Kinase (ROCK1)

Abstract

Recent studies using known Rho-associated kinase isoform 1 (ROCK1) inhibitors along with cellular and molecular biology data have revealed a pivotal role of this enzyme in many aspects of cardiovascular function. Here we report a series of ROCK1 inhibitors which were originally derived from a dihydropyrimidinone core 1. Our efforts focused on the optimization of dihydropyrimidine 2, which resulted in the identification of a series of dihydropyrimidines with improved pharmacokinetics and P450 properties.

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This article has been cited by 8 ACS Journal articles (5 most recent appear below).

• 

  Molecular Basis for Small Molecule Inhibition of G Protein-Coupled Receptor Kinases

  Kristoff T. Homan and John J. G. Tesmer
  ACS Chemical Biology2014 Article ASAP

  • Molecular Basis for Small Molecule Inhibition of G Protein-Coupled Receptor Kinases

    Kristoff T.Homan and John J. G.Tesmer
    ACS Chemical Biology2014 Article ASAP
    Small molecules that inhibit the protein kinase A, G, and C (AGC) family of serine/threonine kinases can exert profound effects on cell homeostasis and thereby regulate fundamental processes such as heart rate, blood pressure, and metabolism, but there is ...
    
    Abstract | Full Text HTML | PDF | PDF w/ Links
• 

  Chemistry and Biology Of Multicomponent Reactions

  Alexander Dömling, Wei Wang, and Kan Wang
  Chemical Reviews2012 112 (6), 3083-3135

  • Chemistry and Biology Of Multicomponent Reactions

    AlexanderDömling, WeiWang, and KanWang
    Chemical Reviews2012 112 (6), 3083-3135
    Abstract | Full Text HTML | PDF | PDF w/ Links
• 

  Fragment-Based and Structure-Guided Discovery and Optimization of Rho Kinase Inhibitors

  Rongshi Li, Mathew P. Martin, Yan Liu, Binglin Wang, Ronil A. Patel, Jin-Yi Zhu, Nan Sun, Roberta Pireddu, Nicholas J. Lawrence, Jiannong Li, Eric B. Haura, Shen-Shu Sung, Wayne C. Guida, Ernst Schonbrunn, and Said M. Sebti
  Journal of Medicinal Chemistry2012 55 (5), 2474-2478

  • Fragment-Based and Structure-Guided Discovery and Optimization of Rho Kinase Inhibitors

    RongshiLi, Mathew P.Martin, YanLiu, BinglinWang, Ronil A.Patel, Jin-YiZhu, NanSun, RobertaPireddu, Nicholas J.Lawrence, JiannongLi, Eric B.Haura, Shen-ShuSung, Wayne C.Guida, ErnstSchonbrunn, and Said M.Sebti
    Journal of Medicinal Chemistry2012 55 (5), 2474-2478
    Using high concentration biochemical assays and fragment-based screening assisted by structure-guided design, we discovered a novel class of Rho-kinase inhibitors. Compound 18 was equipotent for ROCK1 (IC50 = 650 nM) and ROCK2 (IC50 = 670 nM), whereas ...
    
    Abstract | Full Text HTML | PDF | PDF w/ Links
• 

  Design and Synthesis of Small Molecule RhoA Inhibitors: A New Promising Therapy for Cardiovascular Diseases?

  Jing Deng, Enguang Feng, Sheng Ma, Yan Zhang, Xiaofeng Liu, Honglin Li, Huang Huang, Jin Zhu, Weiliang Zhu, Xu Shen, Liyan Miao, Hong Liu, Hualiang Jiang, and Jian Li
  Journal of Medicinal Chemistry2011 54 (13), 4508-4522

  • Design and Synthesis of Small Molecule RhoA Inhibitors: A New Promising Therapy for Cardiovascular Diseases?

    JingDeng, EnguangFeng, ShengMa, YanZhang, XiaofengLiu, HonglinLi, HuangHuang, JinZhu, WeiliangZhu, XuShen, LiyanMiao, HongLiu, HualiangJiang, and JianLi
    Journal of Medicinal Chemistry2011 54 (13), 4508-4522
    RhoA is a member of Rho GTPases, a subgroup of the Ras superfamily of small GTP-binding proteins. RhoA, as an important regulator of diverse cellular signaling pathways, plays significant roles in cytoskeletal organization, transcription, and cell-cycle ...
    
    Abstract | Full Text HTML | PDF | PDF w/ Links
• 

  Synopsis of Some Recent Tactical Application of Bioisosteres in Drug Design

  Nicholas A. Meanwell
  Journal of Medicinal Chemistry2011 54 (8), 2529-2591

  • Synopsis of Some Recent Tactical Application of Bioisosteres in Drug Design

    Nicholas A.Meanwell
    Journal of Medicinal Chemistry2011 54 (8), 2529-2591
    Abstract | Full Text HTML | PDF | PDF w/ Links

                 

GSK3 Inhibitors for the Treatment of Human African Trypanosomiasis

Abstract

 

 

 

Glycogen synthase kinase 3 (GSK3) is a genetically validated drug target for human African trypanosomiasis (HAT), also called African sleeping sickness.

 

 

We report the synthesis and biological evaluation of aminopyrazole derivatives as Trypanosoma brucei GSK3 short inhibitors. Low nanomolar inhibitors, which had high selectivity over the off-target human CDK2 and good selectivity over human GSK3β enzyme, have been prepared.

 

 

These potent kinase inhibitors with small molecular structure  demonstrated low micromolar levels of inhibition of the Trypanosoma brucei brucei parasite grown in culture.

 

 

Rhodanine (2-thioxothiazolidin-4-one) as reductase inhibitors

Rhodanine (2-thioxothiazolidin-4-one) class of compounds as inhibitors By Tyr-OH Hydrogen Bonding Activation;

Abstract

 

 

 

Enoyl acyl carrier protein (ACP) reductase,

one of the enzymes of the type II fatty acid biosynthesis pathway,

has been established as a promising target for the development of new drugs for malaria.

 

 

Here we present the discovery of a rhodanine (2-thioxothiazolidin-4-one) class of compounds as inhibitors of this enzyme using a combined approach of rational selection of compounds for screening, analogue search, docking studies, and lead optimization.

 

 

The most potent inhibitor exhibits an IC50 of 35.6 nM against Plasmodium falciparum enoyl ACP reductase (PfENR) and inhibits growth of the parasite in red blood cell cultures at an IC50 value of 750 nM.

 

 

Many more compounds of this class were found to inhibit PfENR at low nanomolar to low micromolar concentrations, expanding the scope for developing new antimalarial drugs. The structure−activity relationship of these rhodanine compounds is discussed.

 

 

 

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  Inhibitors of HCV NS5A: From Iminothiazolidinones to Symmetrical Stilbenes

  Jeffrey L. Romine, Denis R. St. Laurent, John E. Leet, Scott W. Martin, Michael H. Serrano-Wu, Fukang Yang, Min Gao, Donald R O’Boyle, II, Julie A. Lemm, Jin-Hua Sun, Peter T. Nower, Xiaohua (Stella) Huang, Milind S. Deshpande, Nicholas A. Meanwell, and Lawrence B. Snyder
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  • Inhibitors of HCV NS5A: From Iminothiazolidinones to Symmetrical Stilbenes

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  New Substructure Filters for Removal of Pan Assay Interference Compounds (PAINS) from Screening Libraries and for Their Exclusion in Bioassays

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  Journal of Medicinal Chemistry2010 53 (7), 2719-2740

  • New Substructure Filters for Removal of Pan Assay Interference Compounds (PAINS) from Screening Libraries and for Their Exclusion in Bioassays

    Jonathan B.Baell and Georgina A.Holloway
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    This report describes a number of substructural features which can help to identify compounds that appear as frequent hitters (promiscuous compounds) in many biochemical high throughput screens. The compounds identified by such substructural features are ...
    
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  Synthesis and Antimicrobial Properties of Novel Silver/Polyrhodanine Nanofibers

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  Biomacromolecules2008 9 (10), 2677-2681 

10A Tracer in Brain

A novel phosphodiesterase 10A (PDE10A) tracer candidate

Abstract

 

 

 

A radiolabeled tracer for imaging therapeutic targets in the brain is a valuable tool for lead optimization in CNS drug discovery and for dose selection in clinical development.

 

 

We report the rapid identification of a novel phosphodiesterase 10A (PDE10A) tracer candidate using a LC–MS/MS technology. This structurally distinct PDE10A tracer, AMG-7980 (5), has been shown to have good uptake in the striatum (1.2% ID/g tissue), high specificity (striatum/thalamus ratio of 10), and saturable binding in vivo. The PDE10A affinity (K_D) and PDE10A target density (B_max) were determined to be 0.94 nM and 2.3 pmol/mg protein, respectively, using [³H]5 on rat striatum homogenate. Autoradiography on rat brain sections indicated that the tracer signal was consistent with known PDE10A expression pattern. The specific binding of [³H]5 to rat brain was blocked by another structurally distinct, published PDE10A inhibitor, MP-10. Lastly, our tracer was used to measure in vivo PDE10A target occupancy of a PDE10A inhibitor in rats using LC–MS/MS technology.

 

 

 

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  Discovery of Clinical Candidate 1-(4-(3-(4-(1H-Benzo[d]imidazole-2-carbonyl)phenoxy)pyrazin-2-yl)piperidin-1-yl)ethanone (AMG 579), A Potent, Selective, and Efficacious Inhibitor of Phosphodiesterase 10A (PDE10A)

  Essa Hu, Ning Chen, Matthew P. Bourbeau, Paul E. Harrington, Kaustav Biswas, Roxanne K. Kunz, Kristin L. Andrews, Samer Chmait, Xiaoning Zhao, Carl Davis, Ji Ma, Jianxia Shi, Dianna Lester-Zeiner, Jean Danao, Jessica Able, Madelyn Cueva, Santosh Talreja, Thomas Kornecook, Hang Chen, Amy Porter, Randall Hungate, James Treanor, and Jennifer R. Allen
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  • Discovery of Clinical Candidate 1-(4-(3-(4-(1H-Benzo[d]imidazole-2-carbonyl)phenoxy)pyrazin-2-yl)piperidin-1-yl)ethanone (AMG 579), A Potent, Selective, and Efficacious Inhibitor of Phosphodiesterase 10A (PDE10A)

    EssaHu, NingChen, Matthew P.Bourbeau, Paul E.Harrington, KaustavBiswas, Roxanne K.Kunz, Kristin L.Andrews, SamerChmait, XiaoningZhao, CarlDavis, JiMa, JianxiaShi, DiannaLester-Zeiner, JeanDanao, JessicaAble, MadelynCueva, SantoshTalreja, ThomasKornecook, HangChen, AmyPorter, RandallHungate, JamesTreanor, and Jennifer R.Allen
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    We report the identification of a PDE10A clinical candidate by optimizing potency and in vivo efficacy of promising keto-benzimidazole leads 1 and 2. Significant increase in biochemical potency was observed when the saturated rings on morpholine 1 and N-...
    
    Abstract | Full Text HTML | PDF | PDF w/ Links
• 

  Discovery of Novel Imidazo[4,5-b]pyridines as Potent and Selective Inhibitors of Phosphodiesterase 10A (PDE10A)

  Essa Hu, Kristin Andrews, Samer Chmait, Xiaoning Zhao, Carl Davis, Silke Miller, Geraldine Hill Della Puppa, Mary Dovlatyan, Hang Chen, Dianna Lester-Zeiner, Jessica Able, Christopher Biorn, Ji Ma, Jianxia Shi, James Treanor, and Jennifer R. Allen
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  • Discovery of Novel Imidazo[4,5-b]pyridines as Potent and Selective Inhibitors of Phosphodiesterase 10A (PDE10A)

    EssaHu, KristinAndrews, SamerChmait, XiaoningZhao, CarlDavis, SilkeMiller, GeraldineHill Della Puppa, MaryDovlatyan, HangChen, DiannaLester-Zeiner, JessicaAble, ChristopherBiorn, JiMa, JianxiaShi, JamesTreanor, and Jennifer R.Allen
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    We report the discovery of novel imidazo[4,5-b]pyridines as potent and selective inhibitors of PDE10A. The investigation began with our recently disclosed ketobenzimidazole 1, which exhibited single digit nanomolar PDE10A activity but poor oral ...
    
    Abstract | Full Text HTML | PDF | PDF w/ Links
• 

  Design, Optimization, and Biological Evaluation of Novel Keto-Benzimidazoles as Potent and Selective Inhibitors of Phosphodiesterase 10A (PDE10A)

  Essa Hu, Roxanne K. Kunz, Ning Chen, Shannon Rumfelt, Aaron Siegmund, Kristin Andrews, Samer Chmait, Sharon Zhao, Carl Davis, Hang Chen, Dianna Lester-Zeiner, Ji Ma, Christopher Biorn, Jianxia Shi, Amy Porter, James Treanor, and Jennifer R. Allen
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