Your search keyword '"Shen, Jingkang"' showing total 12 results

1. Discovery of 1 H -Imidazo[4,5- b ]pyridine Derivatives as Potent and Selective BET Inhibitors for the Management of Neuropathic Pain.

Author

Chen X, Cao D, Liu C, Meng F, Zhang Z, Xu R, Tong Y, Xin Y, Zhang W, Kang W, Bao Q, Shen J, Xiong B, You Q, and Jiang Z

Subjects

Mice, Animals, Protein Domains, Cytokines, Pyridines pharmacology, Pyridines therapeutic use, Drug Discovery methods, Neuralgia drug therapy

Abstract

Neuropathic pain (NP) is an intolerable pain syndrome that arises from continuous inflammation and excitability after nerve injury. Only a few NP therapeutics are currently available, and all of them do not provide adequate pain relief. Herein, we report the discovery of a selective and potent inhibitor of the bromodomain and extra-terminal (BET) proteins for reducing neuroinflammation and excitability to treat NP. Starting with the screening hit 1 from an in-house compound library, iterative optimization resulted in the potent BET inhibitor DDO-8926 with a unique binding mode and a novel chemical structure. DDO-8926 exhibits excellent BET selectivity and favorable drug-like properties. In mice with spared nerve injury, DDO-8926 significantly alleviated mechanical hypersensitivity by inhibiting pro-inflammatory cytokine expression and reducing excitability. Collectively, these results implicate that DDO-8926 is a promising agent for the treatment of NP.

Published

2023

2. The discovery of a novel series of potential ERRα inverse agonists based on p-nitrobenzenesulfonamide template for triple-negative breast cancer in vivo .

Author

Gao Z, Wang T, Li R, Du Y, Lv H, Zhang L, Chen H, Shi X, Li Q, and Shen J

Subjects

Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Cell Line, Tumor, Cell Proliferation drug effects, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Female, Humans, Molecular Docking Simulation, Molecular Structure, Nitrobenzenes chemical synthesis, Nitrobenzenes chemistry, Structure-Activity Relationship, Sulfonamides chemical synthesis, Sulfonamides chemistry, Triple Negative Breast Neoplasms metabolism, Triple Negative Breast Neoplasms pathology, ERRalpha Estrogen-Related Receptor, Antineoplastic Agents pharmacology, Drug Discovery, Nitrobenzenes pharmacology, Receptors, Estrogen metabolism, Sulfonamides pharmacology, Triple Negative Breast Neoplasms drug therapy

Abstract

Oestrogen related receptor α participated in the regulation of oxidative metabolism and mitochondrial biogenesis, and was overexpressed in many cancers including triple-negative breast cancer. A set of new ERRα inverse agonists based on p-nitrobenzenesulfonamide template were discovered and compound 11 with high potent activity (IC 50 = 0.80 μM) could significantly inhibit the transcription of ERRα-regulated target genes. By regulating the downstream signalling pathway, compound 11 could suppress the migration and invasion of the ER-negative MDA-MB-231 cell line. Furthermore, compound 11 demonstrated a significant growth suppression of breast cancer xenograft tumours in vivo (inhibition rate 23.58%). The docking results showed that compound 11 could form hydrogen bonds with Glu331 and Arg372 in addition to its hydrophobic interaction with ligand-binding domain. Our data implied that compound 11 represented a novel and effective ERRα inverse agonist, which had broad application prospects in the treatment of triple-negative breast cancer.

Published

2022

3. Phage-Display Based Discovery and Characterization of Peptide Ligands against WDR5.

Author

Cao J, Fan T, Li Y, Du Z, Chen L, Wang Y, Wang X, Shen J, Huang X, Xiong B, and Cao D

Subjects

Humans, Intracellular Signaling Peptides and Proteins metabolism, Ligands, Peptides, Cyclic chemical synthesis, Peptides, Cyclic chemistry, Protein Binding, Drug Discovery, Intracellular Signaling Peptides and Proteins antagonists & inhibitors, Peptide Library, Peptides, Cyclic pharmacology

Abstract

WD40 is a ubiquitous domain presented in at least 361 human proteins and acts as scaffold to form protein complexes. Among them, WDR5 protein is an important mediator in several protein complexes to exert its functions in histone modification and chromatin remodeling. Therefore, it was considered as a promising epigenetic target involving in anti-cancer drug development. In view of the protein-protein interaction nature of WDR5, we initialized a campaign to discover new peptide-mimic inhibitors of WDR5. In current study, we utilized the phage display technique and screened with a disulfide-based cyclic peptide phage library. Five rounds of biopanning were performed and isolated clones were sequenced. By analyzing the sequences, total five peptides were synthesized for binding assay. The four peptides are shown to have the moderate binding affinity. Finally, the detailed binding interactions were revealed by solving a WDR5-peptide cocrystal structure.

Published

2021

4. Discovery and optimization of a series of 3-substituted indazole derivatives as multi-target kinase inhibitors for the treatment of lung squamous cell carcinoma.

Author

Wang Q, Dai Y, Ji Y, Shi H, Guo Z, Chen D, Chen Y, Peng X, Gao Y, Wang X, Chen L, Jiang Y, Geng M, Shen J, Ai J, and Xiong B

Subjects

Animals, Carcinoma, Squamous Cell enzymology, Discoidin Domain Receptor 2 antagonists & inhibitors, Heterografts, Humans, Indazoles chemistry, Indazoles pharmacology, Lung Neoplasms enzymology, Mice, Protein Kinase Inhibitors therapeutic use, Receptor, Fibroblast Growth Factor, Type 1 antagonists & inhibitors, Structure-Activity Relationship, Antineoplastic Agents chemical synthesis, Carcinoma, Squamous Cell drug therapy, Drug Discovery, Indazoles chemical synthesis, Lung Neoplasms drug therapy, Protein Kinase Inhibitors chemistry

Abstract

Although lung adenocarcinoma patients have benefited from the development of targeted therapy, patients with lung squamous cell carcinoma (SqCC) have no effective treatment due to the complexity and heterogeneity of the disease. Therefore, basing on the genetic analysis of mutations in lung squamous cell carcinoma to design multi-target inhibitors represents a potential strategy for the medical treatment. In this study, through screening an in-house focused library, we identified an interesting indazole scaffold. And following with binding analysis, we elaborated the structure-activity relationship of this hit compound by optimizing four parts guided by the DDR2 enzymatic assay, which resulted in a potent lead compound 10a. We conducted further optimization of dual enzymatic inhibitions towards FGFR1 and DDR2, two important kinases in lung squamous cell carcinoma. Finally, from the cellular antiproliferative activity tests and in vivo pharmacokinetic test, 3-substituted indazole derivative 11k was found to be a promising candidate and subjected to in vivo pharmacology study with the mouse xenograft models, demonstrating profound anti-tumor efficacy. Additional in vitro druglike assessment reinforced that compound 11k could be valuable for SqCC drug development., (Copyright © 2018 Elsevier Masson SAS. All rights reserved.)

Published

2019

5. Fragment-based drug discovery of triazole inhibitors to block PDEδ-RAS protein-protein interaction.

Author

Chen D, Chen Y, Lian F, Chen L, Li Y, Cao D, Wang X, Chen L, Li J, Meng T, Huang M, Geng M, Shen J, Zhang N, and Xiong B

Subjects

Cell Line, Tumor, Cell Membrane metabolism, Humans, Neoplasms drug therapy, Signal Transduction drug effects, Triazoles pharmacology, Drug Discovery, Phosphodiesterase Inhibitors pharmacology, Phosphoric Diester Hydrolases metabolism, Protein Binding drug effects, Triazoles therapeutic use, ras Proteins metabolism

Abstract

Although mutated Ras protein is well recognized as an important drug target, direct targeting Ras has proven to be a daunting task. Recent studies demonstrated that Ras protein needs PDEδ to relocate to plasma membrane to execute its signaling transduction function, which provides a new avenue for modulating the Ras protein. To find small molecules antagonizing the interactions between PDEδ and Ras, here we presented a successful application of fragment-based drug discovery of PDEδ inhibitors. Under the guidance of crystal structures, we are able to quickly optimize the initial fragment into highly potent inhibitors, with more than 2000-fold improvement in binding activity, which further adds to the arsenal towards the inhibition of Ras signaling in cancer therapy., (Copyright © 2018 Elsevier Masson SAS. All rights reserved.)

Published

2019

6. Structure-Based Discovery of a Series of 5H-Pyrrolo[2,3-b]pyrazine FGFR Kinase Inhibitors.

Author

Jiang A, Liu Q, Wang R, Wei P, Dai Y, Wang X, Xu Y, Ma Y, Ai J, Shen J, Ding J, and Xiong B

Subjects

Cell Proliferation drug effects, Crystallography, X-Ray, Humans, Inhibitory Concentration 50, Molecular Docking Simulation, Receptors, Fibroblast Growth Factor metabolism, Structure-Activity Relationship, Drug Discovery, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors pharmacology, Receptors, Fibroblast Growth Factor antagonists & inhibitors

Abstract

Fibroblast growth factor receptors (FGFRs), a subfamily of receptor tyrosine kinases, are aberrant in various cancer types, and considered to be promising targets for cancer therapy. We started with a weak-active compound that was identified from our internal hepatocyte growth factor receptor (also called c-Met) inhibitor project, and optimized it with the guidance of a co-crystal structure of compound 8 with FGFR1. Through rational design, synthesis, and the biological evaluation of a series of 5 H -pyrrolo[2,3- b ]pyrazine derivatives, we discovered several potent FGFR kinase inhibitors. Among them, compound 13 displayed high selectivity and favorable metabolic properties, demonstrating a promising lead for further development., Competing Interests: The authors declare no conflict of interest.

Published

2018

7. Discovery of novel high potent and cellular active ADC type PTP1B inhibitors with selectivity over TC-PTP via modification interacting with C site.

Author

Du Y, Zhang Y, Ling H, Li Q, and Shen J

Subjects

Dose-Response Relationship, Drug, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Humans, Molecular Docking Simulation, Molecular Structure, Protein Tyrosine Phosphatase, Non-Receptor Type 1 metabolism, Protein Tyrosine Phosphatase, Non-Receptor Type 2 metabolism, Structure-Activity Relationship, Drug Discovery, Enzyme Inhibitors pharmacology, Protein Tyrosine Phosphatase, Non-Receptor Type 1 antagonists & inhibitors, Protein Tyrosine Phosphatase, Non-Receptor Type 2 antagonists & inhibitors

Abstract

PTP1B serving as a key negative regulator of insulin signaling is a novel target for type 2 diabetes and obesity. Modification at ring B of N-{4-[(3-Phenyl-ureido)-methyl]-phenyl}-methane-sulfonamide template to interact with residues Arg47 and Lys41 in the C site of PTP1B by molecular docking aided design resulted in the discovery of a series of novel high potent and selective inhibitors of PTP1B. The structure activity relationship interacting with the C site of PTP1B was well illustrated. Compounds 8 and 18 were shown to be the high potent and most promising PTP1B inhibitors with cellular activity and great selectivity over the highly homologous TCPTP and other PTPs., (Copyright © 2017 Elsevier Masson SAS. All rights reserved.)

Published

2018

8. Discovery of a series of dihydroquinoxalin-2(1H)-ones as selective BET inhibitors from a dual PLK1-BRD4 inhibitor.

Author

Hu J, Wang Y, Li Y, Xu L, Cao D, Song S, Damaneh MS, Wang X, Meng T, Chen YL, Shen J, Miao Z, and Xiong B

Subjects

Animals, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Cell Cycle Proteins metabolism, Cell Line, Tumor, Cell Proliferation drug effects, Dose-Response Relationship, Drug, Female, Humans, Mice, Mice, Inbred BALB C, Mice, Nude, Molecular Structure, Neoplasms, Experimental drug therapy, Neoplasms, Experimental pathology, Nuclear Proteins metabolism, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors chemistry, Protein Serine-Threonine Kinases metabolism, Proto-Oncogene Proteins metabolism, Quinoxalines chemical synthesis, Quinoxalines chemistry, Structure-Activity Relationship, Transcription Factors metabolism, Xenograft Model Antitumor Assays, Polo-Like Kinase 1, Antineoplastic Agents pharmacology, Cell Cycle Proteins antagonists & inhibitors, Drug Discovery, Nuclear Proteins antagonists & inhibitors, Protein Kinase Inhibitors pharmacology, Protein Serine-Threonine Kinases antagonists & inhibitors, Proto-Oncogene Proteins antagonists & inhibitors, Quinoxalines pharmacology, Transcription Factors antagonists & inhibitors

Abstract

Recent years have seen much effort to discover new chemotypes of BRD4 inhibitors. Interestingly, some kinase inhibitors have been demonstrated to be potent bromodomain inhibitors, especially the PLK1 inhibitor BI-2536 and the JAK2 inhibitor TG101209, which can bind to BRD4 with IC 50 values of 0.025 μM and 0.13 μM, respectively. Although the concept of dual inhibition is intriguing, selective BRD4 inhibitors are preferred as they may diminish off-target effects and provide more flexibility in anticancer drug combination therapy. Inspired by BI-2536, we designed and prepared a series of dihydroquinoxalin-2(1H)-one derivatives as selective bromodomain inhibitors. We found compound 54 had slightly higher activity than (+)-JQ1 in the fluorescence anisotropy assay and potent antiproliferative cellular activity in the MM.1S cell line. We have successfully solved the cocrystal structure of 52 in complex with BRD4-BD1, providing a solid structural basis for the binding mode of compounds of this series. Compound 54 exhibited high selectivity over most non-BET subfamily members and did not show bioactivity towards the PLK1 kinase at 10 or 1 μM. From in vivo studies, compound 54 demonstrated a good PK profile, and the results from in vivo pharmacological studies clearly showed the efficacy of 54 in the mouse MM.1S xenograft model., (Copyright © 2017 Elsevier Masson SAS. All rights reserved.)

Published

2017

9. Fragment-based drug discovery of 2-thiazolidinones as BRD4 inhibitors: 2. Structure-based optimization.

Author

Zhao L, Wang Y, Cao D, Chen T, Wang Q, Li Y, Xu Y, Zhang N, Wang X, Chen D, Chen L, Chen YL, Xia G, Shi Z, Liu YC, Lin Y, Miao Z, Shen J, and Xiong B

Subjects

Antineoplastic Agents chemical synthesis, Cell Cycle Proteins, Cell Proliferation drug effects, Crystallography, X-Ray, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, HT29 Cells, Humans, Models, Molecular, Molecular Structure, Structure-Activity Relationship, Thiazolidines chemical synthesis, Thiazolidines chemistry, Tumor Cells, Cultured, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Drug Discovery, Nuclear Proteins antagonists & inhibitors, Thiazolidines pharmacology, Transcription Factors antagonists & inhibitors

Abstract

The signal transduction of acetylated histone can be processed through a recognition module, bromodomain. Several inhibitors targeting BRD4, one of the bromodomain members, are in clinical trials as anticancer drugs. Hereby, we report our efforts on discovery and optimization of a new series of 2-thiazolidinones as BRD4 inhibitors along our previous study. In this work, guided by crystal structure analysis, we reversed the sulfonamide group and identified a new binding mode. A structure-activity relationship study on this new series led to several potent BRD4 inhibitors with IC50 of about 0.05-0.1 μM in FP binding assay and GI50 of 0.1-0.3 μM in cell based assays. To complete the lead-like assessment of this series, we further checked its effects on BRD4 downstream protein c-Myc, investigated its selectivity among five different bromodomain proteins, as well as the metabolic stability test, and reinforced the utility of 2-thiazolidinone scaffold as BET bromodomain inhibitors in novel anticancer drug development.

Published

2015

10. Discovery of pyrazole as C-terminus of selective BACE1 inhibitors.

Author

Zou Y, Xu L, Chen W, Zhu Y, Chen T, Fu Y, Li L, Ma L, Xiong B, Wang X, Li J, He J, Zhang H, Xu Y, Li J, and Shen J

Subjects

Animals, Cells, Cultured, Crystallography, X-Ray, Enzyme Activation drug effects, Humans, Inhibitory Concentration 50, Mice, Mice, Transgenic, Protease Inhibitors chemical synthesis, Protease Inhibitors chemistry, Protease Inhibitors pharmacology, Pyrazoles chemistry, Structure-Activity Relationship, Amyloid Precursor Protein Secretases antagonists & inhibitors, Aspartic Acid Endopeptidases antagonists & inhibitors, Drug Discovery, Pyrazoles chemical synthesis, Pyrazoles pharmacology

Abstract

We recently discovered and reported dual inhibitor 5 of AChE and BACE1 with N-benzylpiperidine ethyl as C-terminus. Compound 5 showed potent inhibitory activities for BACE1, and could reduce endogenous Aβ1-40 production in APP transgenic mice. In present work, we rapidly identified substituted triazole as the C-terminus of compound 5 by replacing the benzylpiperidine ethyl group with click chemistry and tested these synthesized compounds by in situ screening assay. As revealed by the crystal structures of BACE1 in complex with our triazole compound 12, we found that Pro70 and Thr72 located in the flap region were the critical components for binding with these inhibitors. With the aid of the crystal structure, a new series of five-membered heterocyclic compounds was prepared in order to explore the structure-activity relationship (SAR) of this class of molecules. From these efforts, pyrazole was discovered as a novel C-terminus of BACE1 inhibitors. After further modification of pyrazole with variable substituents, compound 37 exhibited good potency in enzyme inhibition assay (IC50=0.025 μM) and compound 33 showed moderate inhibition effects on Aβ production of APP transfected HEK293 cells. Moreover, these pyrazole derivatives demonstrated good selectivity versus cathepsin D. Our results indicated that the vicinity of Pro70 and Thr72 might be utilized as a subsite, and the discovered pyrazole derivatives might provide useful hints for developing novel BACE1 inhibitors as anti-AD drugs., (Copyright © 2013 Elsevier Masson SAS. All rights reserved.)

Published

2013

11. Virtual screening and structure-based discovery of indole acylguanidines as potent β-secretase (BACE1) inhibitors.

Author

Zou Y, Li L, Chen W, Chen T, Ma L, Wang X, Xiong B, Xu Y, and Shen J

Subjects

Amyloid Precursor Protein Secretases chemistry, Amyloid Precursor Protein Secretases metabolism, Aspartic Acid Endopeptidases chemistry, Aspartic Acid Endopeptidases metabolism, Binding Sites, Humans, Structure-Activity Relationship, Amyloid Precursor Protein Secretases antagonists & inhibitors, Aspartic Acid Endopeptidases antagonists & inhibitors, Drug Discovery, Guanidines chemical synthesis, Guanidines chemistry, Guanidines pharmacology, Indoles chemical synthesis, Indoles chemistry, Indoles pharmacology, Molecular Docking Simulation, Protease Inhibitors chemical synthesis, Protease Inhibitors chemistry, Protease Inhibitors pharmacology

Abstract

Proteolytic cleavage of amyloid precursor protein by β-secretase (BACE1) is a key step in generating the N-terminal of β-amyloid (Aβ), which further forms into amyloid plaques that are considered as the hallmark of Alzheimer's disease. Inhibitors of BACE1 can reduce the levels of Aβ and thus have a therapeutic potential for treating the disease. We report here the identification of a series of small molecules bearing an indole acylguanidine core structure as potent BACE1 inhibitors. The initial weak fragment was discovered by virtual screening, and followed with a hit-to-lead optimization. With the aid of co-crystal structures of two discovered inhibitors (compounds 19 and 25) with BACE1, we explored the SAR around the indole and aryl groups, and obtained several BACE1 inhibitors about 1,000-fold more potent than the initial fragment hit. Accompanying the lead optimization, a previously under-explored sub-site opposite the flap loop was redefined as a potential binding site for later BACE1 inhibitor design.

Published

2013

12. Potent and novel 11β-HSD1 inhibitors identified from shape and docking based virtual screening.

Author

Xia G, Xue M, Liu L, Yu J, Liu H, Li P, Wang J, Li Y, Xiong B, and Shen J

Subjects

11-beta-Hydroxysteroid Dehydrogenase Type 1 genetics, 11-beta-Hydroxysteroid Dehydrogenase Type 1 metabolism, 11-beta-Hydroxysteroid Dehydrogenase Type 2 antagonists & inhibitors, 11-beta-Hydroxysteroid Dehydrogenase Type 2 genetics, 11-beta-Hydroxysteroid Dehydrogenase Type 2 metabolism, Animals, Computer Simulation, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 CYP3A Inhibitors, Databases, Factual, Drug Evaluation, Preclinical, Enzyme Inhibitors pharmacokinetics, Enzyme Inhibitors pharmacology, HEK293 Cells, High-Throughput Screening Assays, Humans, Inhibitory Concentration 50, Metabolic Syndrome drug therapy, Metabolic Syndrome pathology, Mice, Models, Molecular, Structure-Activity Relationship, 11-beta-Hydroxysteroid Dehydrogenase Type 1 antagonists & inhibitors, Drug Design, Drug Discovery methods, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Metabolic Syndrome prevention & control

Abstract

Several potent and novel 11β-hydroxysteroid dehydrogenase 1 (11β-HSD1) inhibitors were discovered from in silico screening the commercially available Maybridge database. Among them, seven hit compounds showed good affinity, with IC(50) values lower than 100 nM and the best one 3.7 nM. To select the lead for further optimization, computational ADME/T prediction, the CYP3A4 inhibition and 11β-HSD1 over 11β-HSD2 selectivity test were also performed. Taking all of the above factors into consideration, two promising compounds were selected as lead structures for further development. The employed hierarchical virtual screening protocol not only demonstrates its efficiency, but also provides novel and selective compounds for developing 11β-HSD1 inhibitors to protect against metabolic syndrome., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011