Your search keyword '"Benzodiazepinones chemistry"' showing total 231 results

1. Stereochemical properties of quazepam and its affinity for the GABA A receptor.

Author

Takano R, Tanaka R, Nakamura K, Tabata H, Oshitari T, Natsugari H, and Takahashi H

Subjects

Stereoisomerism, Structure-Activity Relationship, Molecular Structure, Humans, Benzodiazepinones chemistry, Benzodiazepinones pharmacology, Benzodiazepinones chemical synthesis, Density Functional Theory, Receptors, GABA-A metabolism, Receptors, GABA-A chemistry

Abstract

C9-methylated quazepam 1 was prepared, and its physicochemical properties were investigated. The atropisomers of 1 were isolated as (a 1 R, a 2 S) and (a 1 S, a 2 R) isomers. Their absolute configurations were determined based on ECD spectra in comparison with those calculated using the time-dependent density functional theory. Preliminary examination of affinity for the GABA A receptor revealed that the (a 1 R, a 2 S) isomer of 1 possessed higher activity than its antipode (a 1 S, a 2 R) isomer. The active configuration of C9-methylated quazepam 1 is the same as that of 1,4-benzodiazepin-2-ones., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Author(s). Published by Elsevier Ltd.. All rights reserved.)

Published

2024

2. μ-Oxo-Hypervalent-Iodine-Catalyzed Oxidative C-H Amination for Synthesis of Benzolactam Derivatives.

Author

Sasa H, Mori K, Kikushima K, Kita Y, and Dohi T

Subjects

Amination, Benzodiazepinones chemical synthesis, Catalysis, Cyclization, Oxidation-Reduction, Benzodiazepinones chemistry, Carbon chemistry, Hydrogen chemistry, Iodine chemistry

Abstract

Benzolactams have unique biological activity and high utility in the synthesis of valuable compounds with direct applicability to oxindole alkaloids and antibacterial agents. Despite recent advances in organic chemistry and the growing number of reported methods for synthesizing benzolactams, their preparation still requires a multistep process. C-H amination reactions can convert aromatic C(sp 2 )-H bonds directly to C(sp 2 )-N bonds, and this direct approach to C-N bond formation offers effective access to benzolactams. Hypervalent iodine reagents are promising tools for achieving oxidative C-H amination. Motivated by our ongoing research efforts toward the development of useful hypervalent-iodine-mediated oxidative transformations, we herein describe an effective intramolecular oxidative C-H amination reaction based on μ-oxo hypervalent iodine catalysis for the synthesis of benzolactams bearing various functional groups.

Published

2022

3. Structural Basis of the Negative Allosteric Modulation of 5-BDBD at Human P2X4 Receptors.

Author

Bidula S, Nadzirin IB, Cominetti M, Hickey H, Cullum SA, Searcey M, Schmid R, and Fountain SJ

Subjects

Allosteric Regulation drug effects, Allosteric Regulation physiology, Benzodiazepinones pharmacology, HEK293 Cells, Humans, Molecular Dynamics Simulation, Protein Structure, Secondary, Protein Structure, Tertiary, Purinergic P2X Receptor Antagonists pharmacology, Benzodiazepinones chemistry, Benzodiazepinones metabolism, Purinergic P2X Receptor Antagonists chemistry, Purinergic P2X Receptor Antagonists metabolism, Receptors, Purinergic P2X4 chemistry, Receptors, Purinergic P2X4 metabolism

Abstract

The P2X4 receptor is a ligand-gated ion channel activated by extracellular ATP. P2X4 activity is associated with neuropathic pain, vasodilation, and pulmonary secretion and is therefore of therapeutic interest. The structure-activity relationship of P2X4 antagonists is poorly understood. Here we elucidate the structure-activity of 5-(3-bromophenyl)-1,3-dihydro-2H-benzofuro[3,2- e ]-1,4-diazepin-2-one (5-BDBD) at human P2X4 by combining pharmacology, electrophysiology, molecular modeling, and medicinal chemistry. 5-BDBD antagonized P2X4 in a noncompetitive manner but lacked effect at human P2X2. Molecular modeling and site-directed mutagenesis suggested an allosteric binding site for 5-BDBD located between two subunits in the body region of P2X4, with M109, F178, Y300, and I312 on one subunit and R301 on the neighboring subunit as key residues involved in antagonist binding. The bromine group of 5-BDBD was redundant for the antagonist activity of 5-BDBD, although an interaction between the carbonyl group of 5-BDBD and R301 in P2X4 was associated with 5-BDBD activity. 5-BDBD could inhibit the closed channel but poorly inhibited the channel in the open/desensitizing state. We hypothesize that this is due to constriction of the allosteric site after transition from closed to open channel state. We propose that M109, F178, Y300, R301, and I312 are key residues for 5-BDBD binding; provide a structural explanation of how they contribute to 5-BDBD antagonism; and highlight that the limited action of 5-BDBD on open versus closed channels is due to a conformational change in the allosteric site. SIGNIFICANCE STATEMENT: Activity of P2X4 receptor is associated with neuropathic pain, inflammation, and vasodilatation. Molecular information regarding small-molecule interaction with P2X4 is very limited. Here, this study provides a structural explanation for the action of the small-molecule antagonist 5-BDBD at the human P2X4 receptor., (Copyright © 2021 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2022

4. New Insights into the Structure-Activity Relationship and Neuroprotective Profile of Benzodiazepinone Derivatives of Neurounina-1 as Modulators of the Na + /Ca 2+ Exchanger Isoforms.

Author

Magli E, Fattorusso C, Persico M, Corvino A, Esposito G, Fiorino F, Luciano P, Perissutti E, Santagada V, Severino B, Tedeschi V, Pannaccione A, Pignataro G, Caliendo G, Annunziato L, Secondo A, and Frecentese F

Subjects

Animals, Benzodiazepinones chemistry, Drug Design, Protein Isoforms metabolism, Sodium-Calcium Exchanger metabolism, Structure-Activity Relationship, Benzodiazepinones pharmacology, Neuroprotective Agents pharmacology, Protein Isoforms antagonists & inhibitors, Pyrrolidines chemistry, Sodium-Calcium Exchanger antagonists & inhibitors

Abstract

Due to the neuroprotective role of the Na + /Ca 2+ exchanger (NCX) isoforms NCX1 and NCX3, we synthesized novel benzodiazepinone derivatives of the unique NCX activator Neurounina-1 , named compounds 1-19 . The derivatives are characterized by a benzodiazepinonic nucleus linked to five- or six-membered cyclic amines via a methylene, ethylene, or acetyl spacer. The compounds have been screened on NCX1/NCX3 isoform activities by a high-throughput screening approach, and the most promising were characterized by patch-clamp electrophysiology and Fura-2AM video imaging. We identified two novel modulators of NCX: compound 4 , inhibiting NCX1 reverse mode, and compound 14 , enhancing NCX1 and NCX3 activity. Compound 1 displayed neuroprotection in two preclinical models of brain ischemia. The analysis of the conformational and steric features led to the identification of the molecular volume required for selective NCX1 activation for mixed NCX1/NCX3 activation or for NCX1 inhibition, providing the first prototypal model for the design of optimized isoform modulators.

Published

2021

5. Ligand recognition and G-protein coupling selectivity of cholecystokinin A receptor.

Author

Liu Q, Yang D, Zhuang Y, Croll TI, Cai X, Dai A, He X, Duan J, Yin W, Ye C, Zhou F, Wu B, Zhao Q, Xu HE, Wang MW, and Jiang Y

Subjects

Amino Acid Sequence, Benzodiazepinones chemistry, Cryoelectron Microscopy, Humans, Ligands, Models, Molecular, Protein Binding, Protein Conformation, Protein Multimerization, Sincalide chemistry, Triazoles chemistry, Cholecystokinin chemistry, Receptor, Cholecystokinin A chemistry, Receptors, G-Protein-Coupled chemistry, Sincalide analogs & derivatives

Abstract

Cholecystokinin A receptor (CCK A R) belongs to family A G-protein-coupled receptors and regulates nutrient homeostasis upon stimulation by cholecystokinin (CCK). It is an attractive drug target for gastrointestinal and metabolic diseases. One distinguishing feature of CCK A R is its ability to interact with a sulfated ligand and to couple with divergent G-protein subtypes, including G s , G i and G q . However, the basis for G-protein coupling promiscuity and ligand recognition by CCK A R remains unknown. Here, we present three cryo-electron microscopy structures of sulfated CCK-8-activated CCK A R in complex with G s , G i and G q heterotrimers, respectively. CCK A R presents a similar conformation in the three structures, whereas conformational differences in the 'wavy hook' of the Gα subunits and ICL3 of the receptor serve as determinants in G-protein coupling selectivity. Our findings provide a framework for understanding G-protein coupling promiscuity by CCK A R and uncover the mechanism of receptor recognition by sulfated CCK-8., (© 2021. The Author(s).)

Published

2021

6. Bioguided Isolation of Cyclopenin Analogues as Potential SARS-CoV-2 M pro Inhibitors from Penicillium citrinum TDPEF34.

Author

Thissera B, Sayed AM, Hassan MHA, Abdelwahab SF, Amaeze N, Semler VT, Alenezi FN, Yaseen M, Alhadrami HA, Belbahri L, and Rateb ME

Subjects

Benzodiazepinones chemistry, Benzodiazepinones isolation & purification, Coronavirus 3C Proteases antagonists & inhibitors, Coronavirus 3C Proteases chemistry, Cysteine Proteinase Inhibitors chemistry, Cysteine Proteinase Inhibitors isolation & purification, Molecular Docking Simulation, Molecular Dynamics Simulation, Penicillium chemistry, SARS-CoV-2 enzymology

Abstract

SARS-CoV-2 virus mutations might increase its virulence, and thus the severity and duration of the ongoing pandemic. Global drug discovery campaigns have successfully developed several vaccines to reduce the number of infections by the virus. However, finding a small molecule pharmaceutical that is effective in inhibiting SARS-CoV-2 remains a challenge. Natural products are the origin of many currently used pharmaceuticals and, for this reason, a library of in-house fungal extracts were screened to assess their potential to inhibit the main viral protease M pro in vitro. The extract of Penicillium citrinum , TDPEF34, showed potential inhibition and was further analysed to identify potential M pro inhibitors. Following bio-guided isolation, a series of benzodiazepine alkaloids cyclopenins with good-to-moderate activity against SARS-CoV-2 M pro were identified. The mode of enzyme inhibition of these compounds was predicted by docking and molecular dynamic simulation. Compounds 1 (isolated as two conformers of S- and R-isomers), 2 , and 4 were found to have promising in vitro inhibitory activity towards M pro , with an IC 50 values range of 0.36-0.89 µM comparable to the positive control GC376. The in silico investigation revealed compounds to achieve stable binding with the enzyme active site through multiple H-bonding and hydrophobic interactions. Additionally, the isolated compounds showed very good drug-likeness and ADMET properties. Our findings could be utilized in further in vitro and in vivo investigations to produce anti-SARS-CoV-2 drug candidates. These findings also provide critical structural information that could be used in the future for designing potent M pro inhibitors., Competing Interests: The authors declare no conflict of interest.

Published

2021

7. Novel pyrrolo[2,1-c][1,4]benzodiazepine-3,11-dione (PBD) derivatives as selective HDAC6 inhibitors to suppress tumor metastasis and invasion in vitro and in vivo.

Author

Li Y, Quan J, Song H, Li D, Ma E, Wang Y, and Ma C

Subjects

Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Benzodiazepinones chemical synthesis, Benzodiazepinones chemistry, Cell Proliferation drug effects, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Histone Deacetylase 6 metabolism, Histone Deacetylase Inhibitors chemical synthesis, Histone Deacetylase Inhibitors chemistry, Humans, Molecular Structure, Structure-Activity Relationship, Tumor Cells, Cultured, Antineoplastic Agents pharmacology, Benzodiazepinones pharmacology, Histone Deacetylase 6 antagonists & inhibitors, Histone Deacetylase Inhibitors pharmacology

Abstract

Selective inhibition of histone deacetylase 6 (HDAC6) has been emerged as a promising approach to cancer treatment. As a pivotal strategy for drug discovery,molecular hybridization was introduced in this study and a series of pyrrolo[2,1-c][1,4] benzodiazepine-3,11-diones (PBDs) based hydroxamic acids was rationally designed and synthesizedas novel selective HDAC6 inhibitors. Preliminary in vitro enzyme inhibition assay and structure-activity relationship (SAR) discussion confirmed our design strategy and met the expectation. Several of the compounds showed high potent against HDAC6 enzyme in vitro, and compound A7 with a long aliphatic linker was revealed to have the similar activity as the positive control tubastatin A. Further in vitro characterization of A7 demonstrates the metastasis inhibitory potency in MDA-MB-231 cell line and western blotting showed that A7 could induce the upregulation of Ac-α-tubulin, but not induce the excessive acetylation of histone H3, which indicated that the compound had HDAC6 targeting effect in MDA-MB-231 cells. In vivo study revealed that compound A7 has satisfactory inhibitory effects onliver and lung metastasis of breast cancer in mice. Molecular docking released that A7 could fit well with the receptor and interact with some key residues, which lays a foundation for further structural modifications to elucidate the interaction mode between compounds and target protein. This pharmacological investigation workflow provided a reasonable and reference methodto examine the pharmacological effects of inhibiting HDAC6 with a single molecule, either in vitro or in vivo. All of these results suggested that A7 is a promising lead compound that could lead to the further development of novel selective HDAC6 inhibitors for the treatment of tumor metastasis., (Copyright © 2021. Published by Elsevier Inc.)

Published

2021

8. Controlling Intramolecular Interactions in the Design of Selective, High-Affinity Ligands for the CREBBP Bromodomain.

Author

Brand M, Clayton J, Moroglu M, Schiedel M, Picaud S, Bluck JP, Skwarska A, Bolland H, Chan AKN, Laurin CMC, Scorah AR, See L, Rooney TPC, Andrews KH, Fedorov O, Perell G, Kalra P, Vinh KB, Cortopassi WA, Heitel P, Christensen KE, Cooper RI, Paton RS, Pomerantz WCK, Biggin PC, Hammond EM, Filippakopoulos P, and Conway SJ

Subjects

Benzodiazepinones chemical synthesis, Benzodiazepinones chemistry, CREB-Binding Protein metabolism, Dose-Response Relationship, Drug, E1A-Associated p300 Protein metabolism, HCT116 Cells, Humans, Ligands, Molecular Structure, Small Molecule Libraries chemical synthesis, Small Molecule Libraries chemistry, Structure-Activity Relationship, Benzodiazepinones pharmacology, CREB-Binding Protein antagonists & inhibitors, Drug Design, E1A-Associated p300 Protein antagonists & inhibitors, Small Molecule Libraries pharmacology

Abstract

CREBBP (CBP/KAT3A) and its paralogue EP300 (KAT3B) are lysine acetyltransferases (KATs) that are essential for human development. They each comprise 10 domains through which they interact with >400 proteins, making them important transcriptional co-activators and key nodes in the human protein-protein interactome. The bromodomains of CREBBP and EP300 enable the binding of acetylated lysine residues from histones and a number of other important proteins, including p53, p73, E2F, and GATA1. Here, we report a work to develop a high-affinity, small-molecule ligand for the CREBBP and EP300 bromodomains [(-)-OXFBD05] that shows >100-fold selectivity over a representative member of the BET bromodomains, BRD4(1). Cellular studies using this ligand demonstrate that the inhibition of the CREBBP/EP300 bromodomain in HCT116 colon cancer cells results in lowered levels of c-Myc and a reduction in H3K18 and H3K27 acetylation. In hypoxia (<0.1% O 2 ), the inhibition of the CREBBP/EP300 bromodomain results in the enhanced stabilization of HIF-1α.

Published

2021

9. Dibenzodiazepinone-type muscarinic receptor antagonists conjugated to basic peptides: Impact of the linker moiety and unnatural amino acids on M 2 R selectivity.

Author

Weinhart CG, Wifling D, Schmidt MF, Neu E, Höring C, Clark T, Gmeiner P, and Keller M

Subjects

Amino Acids metabolism, Animals, Benzodiazepinones chemical synthesis, Benzodiazepinones chemistry, Cells, Cultured, Dose-Response Relationship, Drug, Humans, Molecular Docking Simulation, Molecular Structure, Muscarinic Antagonists chemical synthesis, Muscarinic Antagonists chemistry, Peptides chemistry, Receptor, Muscarinic M2 metabolism, Structure-Activity Relationship, Amino Acids antagonists & inhibitors, Benzodiazepinones pharmacology, Muscarinic Antagonists pharmacology, Peptides pharmacology, Receptor, Muscarinic M2 antagonists & inhibitors

Abstract

The family of human muscarinic acetylcholine receptors (MRs) is characterized by a high sequence homology among the five subtypes (M 1 R-M 5 R), being the reason for a lack of subtype selective MR ligands. In continuation of our work on dualsteric dibenzodiazepinone-type M 2 R antagonists, a series of M 2 R ligands containing a dibenzodiazepinone pharmacophore linked to small basic peptides was synthesized (64 compounds). The linker moiety was varied with respect to length, number of basic nitrogens (0-2) and flexibility. Besides proteinogenic basic amino acids (Lys, Arg), shorter homologues of Lys and Arg, containing three and two methylene groups, respectively, as well as D-configured amino acids were incorporated. The type of linker had a marked impact on M 2 R affinity and also effected M 2 R selectivity. In contrast, the structure of the basic peptide rather determined M 2 R selectivity than M 2 R affinity. For example, the most M 2 R selective compound (UR-CG188, 89) with picomolar M 2 R affinity (pK i 9.60), exhibited a higher M 2 R selectivity (ratio of K i M 1 R/M 2 R/M 3 R/M 4 R/M 5 R: 110:1:5200:55:2300) compared to the vast majority of reported M 2 R preferring MR ligands. For selected ligands, M 2 R antagonism was confirmed in a M 2 R miniG protein recruitment assay., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2021 Elsevier Masson SAS. All rights reserved.)

Published

2021

10. Selective Fragments for the CREBBP Bromodomain Identified from an Encoded Self-assembly Chemical Library.

Author

Catalano M, Moroglu M, Balbi P, Mazzieri F, Clayton J, Andrews KH, Bigatti M, Scheuermann J, Conway SJ, and Neri D

Subjects

Benzodiazepinones chemical synthesis, Benzodiazepinones chemistry, CREB-Binding Protein metabolism, Cell Cycle Proteins metabolism, Enzyme-Linked Immunosorbent Assay, Humans, Models, Molecular, Molecular Structure, Small Molecule Libraries chemical synthesis, Small Molecule Libraries chemistry, Transcription Factors metabolism, Benzodiazepinones pharmacology, CREB-Binding Protein antagonists & inhibitors, Cell Cycle Proteins antagonists & inhibitors, Small Molecule Libraries pharmacology, Transcription Factors antagonists & inhibitors

Abstract

DNA-encoded chemical libraries (DECLs) are collections of chemical moieties individually coupled to distinctive DNA barcodes. Compounds can be displayed either at the end of a single DNA strand (i. e., single-pharmacophore libraries) or at the extremities of two complementary DNA strands (i. e., dual-pharmacophore libraries). In this work, we describe the use of a dual-pharmacophore encoded self-assembly chemical (ESAC) library for the affinity maturation of a known 4,5-dihydrobenzodiazepinone ring (THBD) acetyl-lysine (KAc) mimic for the cyclic-AMP response element binding protein (CREB) binding protein (CREBBP or CBP) bromodomain. The new pair of fragments discovered from library selection showed a sub-micromolar affinity for the CREBBP bromodomain in fluorescence polarization and ELISA assays, and selectivity against BRD4(1)., (© 2020 Wiley-VCH GmbH.)

Published

2020

11. Structure-Activity Relationship Studies of Retro-1 Analogues against Shiga Toxin.

Author

Abdelkafi H, Michau A, Pons V, Ngadjeua F, Clerget A, Ait Ouarab L, Buisson DA, Montoir D, Caramelle L, Gillet D, Barbier J, and Cintrat JC

Subjects

Golgi Apparatus drug effects, Golgi Apparatus metabolism, HeLa Cells, Humans, Protein Transport drug effects, Protein Transport physiology, Shiga Toxins metabolism, Structure-Activity Relationship, Benzodiazepinones chemistry, Benzodiazepinones pharmacology, Shiga Toxins antagonists & inhibitors

Abstract

High-throughput screening has shown that Retro-1 inhibits ricin and Shiga toxins by diminishing their intracellular trafficking via the retrograde route, from early endosomes to the Golgi apparatus. To improve the activity of Retro-1, a structure-activity relationship (SAR) study was undertaken and yielded an analogue with a roughly 70-fold better half-maximal effective concentration (EC 50 ) against Shiga toxin cytotoxicity measured in a cell protein synthesis assay.

Published

2020

12. CCK 2 R antagonists: from SAR to clinical trials.

Author

Novak D, Anderluh M, and Kolenc Peitl P

Subjects

Animals, Benzodiazepinones chemistry, Benzodiazepinones therapeutic use, Clinical Trials as Topic, Furans chemistry, Furans therapeutic use, Humans, Lactams chemistry, Lactams therapeutic use, Receptor, Cholecystokinin B metabolism, Structure-Activity Relationship, Sulfonamides chemistry, Sulfonamides therapeutic use, Tetragastrin chemistry, Tetragastrin therapeutic use, Receptor, Cholecystokinin B antagonists & inhibitors

Abstract

The widespread involvement of the cholecystokinin-2/gastrin receptor (CCK 2 R) in multiple (patho)physiological processes has propelled extensive searches for nonpeptide small-molecule CCK 2 R antagonists. For the past three decades, considerable research has yielded numerous chemically heterogeneous compounds. None of these entered into the clinic, mainly because of inadequate biological effects. However, it appears that the ultimate goal of a clinically useful CCK 2 R antagonist is now just around the corner, with the most promising compounds, netazepide and nastorazepide, now in Phase II clinical trials. Here, we illustrate the structure-activity relationships (SARs) of stablished CCK 2 R antagonists of various structural classes, and the most recent proof-of-concept studies where new applicabilities of CCK 2 R antagonists as visualizing agents are presented., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

13. New pyrazolyl-dibenzo[b,e][1,4]diazepinones: room temperature one-pot synthesis and biological evaluation.

Author

Brahmbhatt GC, Sutariya TR, Atara HD, Parmar NJ, Gupta VK, Lagunes I, Padrón JM, Murumkar PR, and Yadav MR

Subjects

Cell Line, Tumor, Cell Proliferation drug effects, Humans, Microbial Sensitivity Tests, Molecular Docking Simulation, Mycobacterium tuberculosis drug effects, Structure-Activity Relationship, Temperature, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Antioxidants chemistry, Antioxidants pharmacology, Antitubercular Agents chemistry, Antitubercular Agents pharmacology, Benzodiazepinones chemistry, Benzodiazepinones pharmacology, Pyrazoles chemistry, Pyrazoles pharmacology

Abstract

Several new (5-aryloxy-pyrazolyl)- and (5-aryl/olefin-sulfanyl-pyrazolyl)-dibenzo[b,e] [1,4] diazepinone scaffolds have been synthesized, by assembling 5-substituted 3-methyl-1-phenyl-pyrazole-4-carbaldehydes of varied nature with different cyclic diketones and aromatic diamines successfully in the presence of indium chloride in acetonitrile, at room temperature. Desired products are excellent in the purity and isolated without chromatography. All new structures are confirmed, on the basis of single-crystal X-ray diffraction data of representative 29e. Compounds reported in the present work revealed good antioxidant, antimicrobial and antiproliferative activities with promising FRAP (ferric reducing antioxidant power), bacterial resistance and human solid tumor cell growth inhibitory values, respectively. Compounds 25c and 29e, overall, registered good to moderate activity against A549 (lung), HeLa (cervix), SW1573 (lung) T-47D (breast) and WiDr (colon) cell lines, with GI 50 values in the 2.6-5.1 μM and 1.8-7.5 μM ranges, respectively. Molecular docking was carried out to elucidate the binding modes of the compounds (25c, 29e) to topoisomerase I and II.

Published

2020

14. Discovery of novel PTHR1 antagonists: Design, synthesis, and structure activity relationships.

Author

Arai Y, Kiyotsuka Y, Shimada K, Oyama K, and Izumi M

Subjects

Benzodiazepinones chemical synthesis, Benzodiazepinones chemistry, Dose-Response Relationship, Drug, Humans, Molecular Structure, Receptor, Parathyroid Hormone, Type 1 metabolism, Structure-Activity Relationship, Benzodiazepinones pharmacology, Drug Discovery, Receptor, Parathyroid Hormone, Type 1 antagonists & inhibitors

Abstract

The discovery and optimization of a novel series of PTHR1 antagonists are described. Starting from known PTHR1 antagonists, we identified more potent 1,4-benzodiazepin-2-one derivatives by means of a scaffold-hopping approach. The representative compound 23 (DS08210767) exhibited nanomolar-level PTHR1 antagonist activity and potential oral bioavailability in a pharmacokinetic study., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

15. Rovalpituzumab Tesirine: A Novel DLL3-Targeting Antibody-Drug Conjugate.

Author

Lashari BH, Vallatharasu Y, Kolandra L, Hamid M, and Uprety D

Subjects

Antibodies, Monoclonal, Humanized adverse effects, Antibodies, Monoclonal, Humanized chemistry, Antineoplastic Agents adverse effects, Antineoplastic Agents chemistry, Apoptosis drug effects, Benzodiazepinones adverse effects, Benzodiazepinones chemistry, Cell Proliferation drug effects, Clinical Trials, Phase I as Topic, Humans, Immunoconjugates adverse effects, Immunoconjugates chemistry, Intracellular Signaling Peptides and Proteins metabolism, Lung Neoplasms metabolism, Lung Neoplasms pathology, Membrane Proteins metabolism, Small Cell Lung Carcinoma metabolism, Small Cell Lung Carcinoma pathology, Antibodies, Monoclonal, Humanized pharmacology, Antineoplastic Agents pharmacology, Benzodiazepinones pharmacology, Immunoconjugates pharmacology, Intracellular Signaling Peptides and Proteins antagonists & inhibitors, Lung Neoplasms drug therapy, Membrane Proteins antagonists & inhibitors, Small Cell Lung Carcinoma drug therapy

Abstract

Small cell lung cancer (SCLC) comprises about 15% of all cases of lung cancer. In recent years, owing to a change in the epidemiology of smoking habits, the incidence of the tumor has decreased; however, it remains a significant challenge to global health. While the tumor has a favorable initial response to chemoradiation, relapse is invariable, and second-line regimens may be intolerable given the severity of side effects. For patients with tumors resistant to second-line regimens, no current standard regimens exist. Rovalpituzumab tesirine is a novel antibody-drug conjugate, targeting delta-like protein 3, fundamental in the downstream cellular signaling for proliferation and apoptosis. This drug is reported to have shown promise in pre-clinical and phase I trials. It appears effective in decreasing tumor burden and is reported to be well tolerated, albeit with a significant adverse effect profile. Currently, it is being studied as part of initial and subsequent line chemotherapeutic regimens; it remains to be seen if this is a viable option in the treatment of SCLC. This may add to the agents that can be used against SCLC, and help improve outcomes.

Published

2018

16. Auranthine, a Benzodiazepinone from Penicillium aurantiogriseum: Refined Structure, Absolute Configuration, and Cytotoxicity.

Author

Kalinina SA, Kalinin DV, Hövelmann Y, Daniliuc CG, Mück-Lichtenfeld C, Cramer B, and Humpf HU

Subjects

Antibiotics, Antineoplastic chemistry, Benzodiazepines chemistry, Benzodiazepinones chemistry, Benzodiazepinones pharmacology, Cell Line, Tumor, Circular Dichroism, Humans, Magnetic Resonance Spectroscopy, Molecular Structure, X-Ray Diffraction, Antibiotics, Antineoplastic pharmacology, Benzodiazepines pharmacology, Penicillium chemistry

Abstract

The structure of the known Penicillium aurantiogriseum-derived secondary metabolite auranthine was refined using a combination of synthetic, spectroscopic, and X-ray diffractometric approaches. Thus, auranthine was shown to be a fused quinazolino benzodiazepinedione (2) bearing an acyclic aliphatic nitrile moiety, thereby significantly differing from the originally proposed structure 1 published in 1986. Its absolute configuration was confirmed by CD spectroscopy and DFT calculations. The cultivation of P. aurantiogriseum was optimized, allowing high production of auranthine. The cytotoxicity profile of auranthine and its semisynthetic analogues is reported. The refined structure of auranthine provides a valid target for the total synthesis of this underexplored natural product and its derivatives.

Published

2018

17. Synthesis and biological evaluation of benzo[b]furo[3,4-e][1,4]diazepin-1-one derivatives as anti-cancer agents.

Author

Malayeri SO, Tayarani-Najaran Z, Behbahani FS, Rashidi R, Delpazir S, and Ghodsi R

Subjects

Antineoplastic Agents chemical synthesis, Apoptosis drug effects, Benzodiazepinones chemical synthesis, Cell Line, Tumor, Drug Screening Assays, Antitumor, Humans, Neoplasms metabolism, Podophyllotoxin chemical synthesis, Podophyllotoxin chemistry, Podophyllotoxin pharmacology, Structure-Activity Relationship, Tubulin metabolism, Tubulin Modulators chemical synthesis, Tubulin Modulators chemistry, Tubulin Modulators pharmacology, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Benzodiazepinones chemistry, Benzodiazepinones pharmacology, Neoplasms drug therapy

Abstract

A new series of novel Podophyllotoxin-like benzo[b]furo[3,4-e][1,4]diazepin-1-ones possessing structural elements of 4-aza-2,3-didehydropodophyllotoxins with central diazepine ring was designed and synthesized as anti-cancer agents. In initial assessment, the cytotoxic activity of the synthesized compounds was evaluated against three cancer cell lines including MCF-7, PC3 and B16-F10 employing the MTT assay. Some of compounds (12h, 13a, 13c and 14b) showed significant cytotoxic activity. So, we investigated the cytotoxicity of compounds 12h, 13a, 13c and 14b, along with podophyllotoxin as the reference drug in different cancer cell lines including A549, A2780, DU145, HeLa, and normal Huvec cell line. Among these four compounds, 13c showed promising antiproliferative activity against all cancer cells stronger than the other compounds and comparable to reference drug podophyllotoxin in some cancer cells. All these four compounds did not show significant cytotoxicity on normal Huvec cell line. The flow cytometry analysis of the MCF-7, PC3 and A2780 human cancer cell lines treated with 13c showed that 13c, induced apoptosis in the MCF-7, PC3 and A2780 human cancer cell lines, which is in good agreement to its cytotoxic activity as well. Compound 13c did not show significant influence on tubulin assembly and exert its cytotoxic effects via induction of apoptosis and has potent and selective cytotoxic effects in cancer cells., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

18. Structure-specific endonuclease activity of SNM1A enables processing of a DNA interstrand crosslink.

Author

Buzon B, Grainger R, Huang S, Rzadki C, and Junop MS

Subjects

Base Pairing, Base Sequence, Benzodiazepinones chemistry, Benzodiazepinones pharmacology, Cell Cycle Proteins, Cloning, Molecular, Cross-Linking Reagents chemistry, Cross-Linking Reagents pharmacology, DNA Damage, DNA Replication drug effects, DNA, Single-Stranded genetics, DNA, Single-Stranded metabolism, Escherichia coli genetics, Escherichia coli metabolism, Exodeoxyribonucleases metabolism, Gene Expression, Humans, Nucleic Acid Conformation drug effects, Oligonucleotides metabolism, Plasmids chemistry, Plasmids metabolism, Pyrroles chemistry, Pyrroles pharmacology, Recombinant Proteins genetics, Recombinant Proteins metabolism, Saccharomyces cerevisiae genetics, Saccharomyces cerevisiae metabolism, DNA Repair, DNA, Single-Stranded chemistry, Exodeoxyribonucleases genetics, Oligonucleotides chemistry

Abstract

DNA interstrand crosslinks (ICLs) covalently join opposing strands, blocking both replication and transcription, therefore making ICL-inducing compounds highly toxic and ideal anti-cancer agents. While incisions surrounding the ICL are required to remove damaged DNA, it is currently unclear which endonucleases are needed for this key event. SNM1A has been shown to play an important function in human ICL repair, however its suggested role has been limited to exonuclease activity and not strand incision. Here we show that SNM1A has endonuclease activity, having the ability to cleave DNA structures that arise during the initiation of ICL repair. In particular, this endonuclease activity cleaves single-stranded DNA. Given that unpaired DNA regions occur 5' to an ICL, these findings suggest SNM1A may act as either an endonuclease and/or exonuclease during ICL repair. This finding is significant as it expands the potential role of SNM1A in ICL repair.

Published

2018

19. Structural and Atropisomeric Factors Governing the Selectivity of Pyrimido-benzodiazipinones as Inhibitors of Kinases and Bromodomains.

Author

Wang J, Erazo T, Ferguson FM, Buckley DL, Gomez N, Muñoz-Guardiola P, Diéguez-Martínez N, Deng X, Hao M, Massefski W, Fedorov O, Offei-Addo NK, Park PM, Dai L, DiBona A, Becht K, Kim ND, McKeown MR, Roberts JM, Zhang J, Sim T, Alessi DR, Bradner JE, Lizcano JM, Blacklow SC, Qi J, Xu X, and Gray NS

Subjects

Benzodiazepinones chemistry, Benzodiazepinones pharmacology, Cell Cycle Proteins, Crystallography, X-Ray, HeLa Cells, Humans, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2 antagonists & inhibitors, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2 chemistry, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2 metabolism, Mitogen-Activated Protein Kinase 7 antagonists & inhibitors, Mitogen-Activated Protein Kinase 7 chemistry, Mitogen-Activated Protein Kinase 7 metabolism, Models, Molecular, Nuclear Proteins chemistry, Nuclear Proteins metabolism, Polypharmacology, Structure-Activity Relationship, Transcription Factors chemistry, Transcription Factors metabolism, Nuclear Proteins antagonists & inhibitors, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors pharmacology, Pyrimidines chemistry, Pyrimidines pharmacology, Transcription Factors antagonists & inhibitors

Abstract

Bromodomains have been pursued intensively over the past several years as emerging targets for the development of anticancer and anti-inflammatory agents. It has recently been shown that some kinase inhibitors are able to potently inhibit the bromodomains of BRD4. The clinical activities of PLK inhibitor BI-2536 and JAK2-FLT3 inhibitor TG101348 have been attributed to this unexpected polypharmacology, indicating that dual-kinase/bromodomain activity may be advantageous in a therapeutic context. However, for target validation and biological investigation, a more selective target profile is desired. Here, we report that benzo[e]pyrimido-[5,4- b]diazepine-6(11H)-ones, versatile ATP-site directed kinase pharmacophores utilized in the development of inhibitors of multiple kinases, including several previously reported kinase chemical probes, are also capable of exhibiting potent BRD4-dependent pharmacology. Using a dual kinase-bromodomain inhibitor of the kinase domains of ERK5 and LRRK2, and the bromodomain of BRD4 as a case study, we define the structure-activity relationships required to achieve dual kinase/BRD4 activity, as well as how to direct selectivity toward inhibition of either ERK5 or BRD4. This effort resulted in identification of one of the first reported kinase-selective chemical probes for ERK5 (JWG-071), a BET selective inhibitor with 1 μM BRD4 IC 50 (JWG-115), and additional inhibitors with rationally designed polypharmacology (JWG-047, JWG-069). Co-crystallography of seven representative inhibitors with the first bromodomain of BRD4 demonstrate that distinct atropisomeric conformers recognize the kinase ATP-site and the BRD4 acetyl lysine binding site, conformational preferences supported by rigid docking studies.

Published

2018

20. Natural products from thioester reductase containing biosynthetic pathways.

Author

Mullowney MW, McClure RA, Robey MT, Kelleher NL, and Thomson RJ

Subjects

Alkaloids biosynthesis, Alkaloids chemistry, Azabicyclo Compounds chemistry, Azabicyclo Compounds metabolism, Benzodiazepinones chemistry, Benzodiazepinones metabolism, Biological Products chemistry, Biological Products pharmacology, Biosynthetic Pathways genetics, Cyclization, Depsipeptides chemistry, Depsipeptides metabolism, Dipeptides chemistry, Dipeptides metabolism, Indoles chemistry, Indoles metabolism, Lactams chemistry, Lactams metabolism, Leupeptins chemistry, Leupeptins metabolism, Lysine analogs & derivatives, Lysine chemistry, Lysine metabolism, Multigene Family, Peptide Synthases genetics, Polyketide Synthases genetics, Protein Domains, Biological Products metabolism, Peptide Synthases metabolism, Polyketide Synthases metabolism

Abstract

Covering: up to 2018 Thioester reductase domains catalyze two- and four-electron reductions to release natural products following assembly on nonribosomal peptide synthetases, polyketide synthases, and their hybrid biosynthetic complexes. This reductive off-loading of a natural product yields an aldehyde or alcohol, can initiate the formation of a macrocyclic imine, and contributes to important intermediates in a variety of biosyntheses, including those for polyketide alkaloids and pyrrolobenzodiazepines. Compounds that arise from reductase-terminated biosynthetic gene clusters are often reactive and exhibit biological activity. Biomedically important examples include the cancer therapeutic Yondelis (ecteinascidin 743), peptide aldehydes that inspired the first therapeutic proteasome inhibitor bortezomib, and numerous synthetic derivatives and antibody drug conjugates of the pyrrolobenzodiazepines. Recent advances in microbial genomics, metabolomics, bioinformatics, and reactivity-based labeling have facilitated the detection of these compounds for targeted isolation. Herein, we summarize known natural products arising from this important category, highlighting their occurrence in Nature, biosyntheses, biological activities, and the technologies used for their detection and identification. Additionally, we review publicly available genomic data to highlight the remaining potential for novel reductively tailored compounds and drug leads from microorganisms. This thorough retrospective highlights various molecular families with especially privileged bioactivity while illuminating challenges and prospects toward accelerating the discovery of new, high value natural products.

Published

2018

21. Quantitative surface field analysis: learning causal models to predict ligand binding affinity and pose.

Author

Cleves AE and Jain AN

Subjects

Benzodiazepinones chemistry, Binding Sites, Dihydrotestosterone chemistry, Estradiol chemistry, Ligands, Machine Learning, Physical Phenomena, Protein Binding, Protein Conformation, Quantitative Structure-Activity Relationship, Quantum Theory, Thermodynamics, Models, Molecular, Sex Hormone-Binding Globulin chemistry

Abstract

We introduce the QuanSA method for inducing physically meaningful field-based models of ligand binding pockets based on structure-activity data alone. The method is closely related to the QMOD approach, substituting a learned scoring field for a pocket constructed of molecular fragments. The problem of mutual ligand alignment is addressed in a general way, and optimal model parameters and ligand poses are identified through multiple-instance machine learning. We provide algorithmic details along with performance results on sixteen structure-activity data sets covering many pharmaceutically relevant targets. In particular, we show how models initially induced from small data sets can extrapolatively identify potent new ligands with novel underlying scaffolds with very high specificity. Further, we show that combining predictions from QuanSA models with those from physics-based simulation approaches is synergistic. QuanSA predictions yield binding affinities, explicit estimates of ligand strain, associated ligand pose families, and estimates of structural novelty and confidence. The method is applicable for fine-grained lead optimization as well as potent new lead identification.

Published

2018

22. The benzodiazepine-like natural product tilivalline is produced by the entomopathogenic bacterium Xenorhabdus eapokensis.

Author

Wolff H and Bode HB

Subjects

Benzodiazepinones chemistry, Biological Products chemistry, Chromatography, High Pressure Liquid, Escherichia coli genetics, Escherichia coli metabolism, Gene Expression, Genes, Bacterial, Molecular Structure, Multigene Family, Tandem Mass Spectrometry, Benzodiazepinones metabolism, Biological Products metabolism, Enterobacteriaceae metabolism

Abstract

The pyrrolobenzodiazepine tilivalline (1) was originally identified in the human gut pathobiont Klebsiella oxytoca, the causative agent of antibiotic-associated hemorrhagic colitis. Here we show the identification of tilivalline and analogs thereof in the entomopathogenic bacterium Xenorhabdus eapokensis as well as the identification of its biosynthesis gene cluster encoding a bimodular non-ribosomal peptide synthetase. Heterologous expression of both genes in E. coli resulted in the production of 1 and from mutasynthesis and precursor directed biosynthesis 11 new tilivalline analogs were identified in X. eapokensis. These results allowed the prediction of the tilivalline biosynthesis being similar to that in K. oxytoca.

Published

2018

23. Biosynthesis of the Klebsiella oxytoca Pathogenicity Factor Tilivalline: Heterologous Expression, in Vitro Biosynthesis, and Inhibitor Development.

Author

von Tesmar A, Hoffmann M, Abou Fayad A, Hüttel S, Schmitt V, Herrmann J, and Müller R

Subjects

Benzodiazepinones chemical synthesis, Benzodiazepinones chemistry, Cytotoxins chemical synthesis, Enterocolitis, Pseudomembranous etiology, Indoles metabolism, Klebsiella oxytoca chemistry, Klebsiella oxytoca metabolism, Multigene Family, Virulence Factors genetics, Virulence Factors metabolism, ortho-Aminobenzoates metabolism, Benzodiazepinones metabolism, Enterocolitis, Pseudomembranous drug therapy, Klebsiella oxytoca pathogenicity

Abstract

Tilvalline is a pyrrolo[4,2]benzodiazepine derivative produced by the pathobiont Klebsiella oxytoca and is the causative toxin in antibiotic associated hemorrhagic colitis (AAHC). Heterologous expression of the tilivalline biosynthetic gene cluster along with in vitro reconstitution of the respective NRPS (NpsA, ThdA, NpsB) was employed to reveal a nonenzymatic indole incorporation via a spontaneous Friedel-Crafts-like alkylation reaction. Furthermore, the heterologous system was used to generate novel tilivalline derivatives by supplementation of respective anthranilate and indole precursors. Finally, it could be shown that salicylic and acetylsalicylic acid inhibit the biosynthesis of tilivalline in K. oxytoca liquid culture, presumably by blocking the peptidyl carrier protein ThdA, pointing toward a potential application in combination therapy to prevent or alleviate the symptoms of AAHC.

Published

2018

24. Novel (S)-1,3,4,12a-tetrahydropyrazino[2,1-c][1,4]benzodiazepine-6,12(2H,11H)-dione derivatives: Selective inhibition of MV-4-11 biphenotypic B myelomonocytic leukemia cells' growth is accompanied by reactive oxygen species overproduction and apoptosis.

Author

Mieczkowski A, Psurski M, Bagiński M, Bieszczad B, Mroczkowska M, Wilczek M, Czajkowska J, Trzybiński D, Woźniak K, and Wietrzyk J

Subjects

Animals, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Antineoplastic Agents toxicity, Benzodiazepinones chemical synthesis, Benzodiazepinones chemistry, Benzodiazepinones toxicity, Cell Line, Tumor, Cell Proliferation drug effects, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, G1 Phase Cell Cycle Checkpoints drug effects, Humans, Leukemia drug therapy, Mice, Pyrazines chemical synthesis, Pyrazines chemistry, Pyrazines toxicity, S Phase Cell Cycle Checkpoints drug effects, Stereoisomerism, Structure-Activity Relationship, Antineoplastic Agents pharmacology, Apoptosis drug effects, Benzodiazepinones pharmacology, Pyrazines pharmacology, Reactive Oxygen Species metabolism

Abstract

A series of optically pure (R)- and (S)-1,3,4,12a-tetrahydropyrazino[2,1-c][1,4]benzodiazepine-6,12(2H,11H)-dione derivatives was designed and synthesized as novel anthramycin analogues in a three-step, one-pot procedure, and tested for their antiproliferative activity on nine following cell lines: MV-4-11, UMUC-3, MDA-MB-231, MCF7, LoVo, HT-29, A-549, A2780 and BALB/3T3. The key structural features responsible for exhibition of cytotoxic effect were determined: the (S)-configuration of chiral center and the presence of hydrophobic 4-biphenyl substituent in the side chain. Introduction of bromine atom into the 8 position (8g) or substitution of dilactam ring with benzyl group (8m) further improved the activity and selectivity of investigated compounds. Among others, compound 8g exhibited selective cytotoxic effect against MV-4-11 (IC 50  = 8.7 μM) and HT-29 (IC 50  = 17.8 μM) cell lines, while 8m showed noticeable anticancer activity against MV-4-11 (IC 50  = 10.8 μM) and LoVo (IC 50  = 11.0 μM) cell lines. The cell cycle arrest in G 1 /S checkpoint and apoptosis associated with overproduction of reactive oxygen species was also observed for 8e and 8m., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

25. Synthesis and In Vitro and In Vivo Evaluation of [ 3 H]LRRK2-IN-1 as a Novel Radioligand for LRRK2.

Author

Malik N, Gifford AN, Sandell J, Tuchman D, and Ding YS

Subjects

Animals, Autoradiography, Benzodiazepinones chemistry, Corpus Striatum metabolism, Humans, Kidney metabolism, Ligands, Male, Pyrimidines chemistry, Radiopharmaceuticals chemistry, Rats, Sprague-Dawley, Tissue Distribution, Benzodiazepinones chemical synthesis, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2 metabolism, Pyrimidines chemical synthesis, Radiopharmaceuticals chemical synthesis, Tritium chemistry

Abstract

Purpose: LRRK2 (leucine-rich repeat kinase 2) has recently been proven to be a promising drug target for Parkinson's disease (PD) due to an apparent enhanced activity caused by mutations associated with familial PD. To date, there have been no reports in which a LRRK2 inhibitor has been radiolabeled and used for in in vitro or in vivo studies of LRRK2. In the present study, we radiolabeled the LRRK2 ligand, LRRK-IN-1, for the purposes of performing in vitro (IC 50 , K d , B max , autoradiography) and in vivo (biodistribution, and blocking experiments) evaluations in rodents and human striatum tissues., Procedures: [ 3 H]LRRK2-IN-1 was prepared with high radiochemical purity (>99 %) and a specific activity of 41 Ci/mmol via tritium/hydrogen (T/H) exchange using Crabtree's catalyst. For IC 50 , K d , and B max determination, LRRK2-IN-1 was used as a competing drug for nonspecific binding assessment. The specific binding of the tracer was further evaluated via an in vivo blocking study in mice with a potent LRRK2 inhibitor, Pf-06447475., Results: In vitro binding studies demonstrated a saturable binding site for [ 3 H]LRRK2-IN-1 in rat kidney, rat brain striatum and human brain striatum with K d of 26 ± 3 and 43 ± 8, 48 ± 2 nM, respectively. In rat, the density of LRRK2 binding sites (B max ) was higher in kidney (6.4 ± 0.04 pmol/mg) than in brain (2.5 ± 0.03 pmol/mg), however, in human brain striatum, the B max was 0.73 ± 0.01 pmol/mg protein. Autoradiography imaging in striatum of rat and human brain tissues gave results consistent with binding studies. In in vivo biodistribution and blocking studies in mice, co-administration with Pf-06447475 (10 mg/kg) reduced the uptake of [ 3 H]LRRK2-IN-1 (%ID/g) by 50-60% in the kidney or brain., Conclusion: The high LRRK2 brain density observed in our study suggests the feasibility for positron emission tomography imaging of LRRK2 (a potential target) with radioligands of higher affinity and specificity.

Published

2017

26. Total Biosynthesis of the Pyrrolo[4,2]benzodiazepine Scaffold Tomaymycin on an In Vitro Reconstituted NRPS System.

Author

von Tesmar A, Hoffmann M, Pippel J, Fayad AA, Dausend-Werner S, Bauer A, Blankenfeldt W, and Müller R

Subjects

Benzodiazepinones chemistry, Benzodiazepinones metabolism, Models, Molecular, Peptide Synthases chemistry, Protein Domains, Substrate Specificity, Benzodiazepines chemistry, Peptide Synthases metabolism, Pyrroles chemistry

Abstract

In vitro reconstitution and biochemical analysis of natural product biosynthetic pathways remains a challenging endeavor, especially if megaenzymes of the nonribosomal peptide synthetase (NRPS) type are involved. In theory, all biosynthetic steps may be deciphered using mass spectrometry (MS)-based analyses of both the carrier protein-coupled intermediates and the free intermediates. We here report the "total biosynthesis" of the pyrrolo[4,2]benzodiazepine scaffold tomaymycin using an in vitro reconstituted NRPS system. Proteoforms were analyzed by liquid chromatography (LC)-MS to decipher every step of the biosynthesis on its respective megasynthetase with up to 170 kDa in size. To the best of our knowledge, this is the first report of a comprehensive analysis of virtually all chemical steps involved in the biosynthesis of nonribosomally synthesized natural products. The study includes experiments to determine substrate specificities of the corresponding A-domains in competition assays by analyzing the adenylation step as well as the transfer to the respective carrier protein domain., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

27. New psychoactive substances: Studies on the metabolism of XLR-11, AB-PINACA, FUB-PB-22, 4-methoxy-α-PVP, 25-I-NBOMe, and meclonazepam using human liver preparations in comparison to primary human hepatocytes, and human urine.

Author

Richter LHJ, Maurer HH, and Meyer MR

Subjects

Benzodiazepinones chemistry, Benzodiazepinones metabolism, Butyrophenones chemistry, Butyrophenones metabolism, Cannabinoids chemistry, Cannabinoids metabolism, Hepatocytes metabolism, Humans, Indazoles chemistry, Indazoles metabolism, Indoles chemistry, Indoles metabolism, Liver enzymology, Liver metabolism, Microsomes, Liver metabolism, Molecular Structure, Phenethylamines chemistry, Phenethylamines metabolism, Psychotropic Drugs chemistry, Pyrrolidines chemistry, Pyrrolidines metabolism, Quinolines chemistry, Quinolines metabolism, Valine analogs & derivatives, Valine chemistry, Valine metabolism, Psychotropic Drugs metabolism

Abstract

New psychoactive substances (NPS) are an increasing problem in clinical and forensic toxicology. The knowledge of their metabolism is important for toxicological risk assessment and for developing toxicological urine screenings. Considering the huge numbers of NPS annually appearing on the market, metabolism studies should be realized in a fast, simple, cost efficient, and reliable way. Primary human hepatocytes (PHH) were recommended to be the gold standard for in vitro metabolism studies as they are expected to contain natural enzyme clusters, co-substrates, and drug transporters. In addition, they were already successfully used for metabolism studies of NPS. However, they also have disadvantages such as high costs and limited applicability without special equipment. The aims of the present study were therefore first to investigate exemplarily the phase I and phase II metabolism of six NPS (XLR-11, AB-PINACA, FUB-PB-22, 4-methoxy-α-PVP, 25-I-NBOMe, and meclonazepam) from different drug classes using pooled human S9 fraction (pS9) or pooled human liver microsomes combined with cytosol (pHLM/pHLC) after addition of the co-substrates for the main metabolic phase I and II reactions. Second to compare results to published data generated using primary human hepatocytes and human urine samples. Results of the incubations with pS9 or pHLM/pHLC were comparable in number and abundance of metabolites. Formation of metabolites, particularly after multi-step reactions needed a longer incubation time. However, incubations using human liver preparations resulted in a lower number of total detected metabolites compared to PHH, but they were still able to allow the identification of the main human urinary excretion products. Human liver preparations and particularly the pooled S9 fraction could be shown to be a sufficient and more cost-efficient alternative in context of metabolism studies also for developing toxicological urine screenings. It might be recommended to use the slightly cheaper pS9 fraction instead of a pHLM/pHLC combination. As formation of some metabolites needed a long incubation time, two sampling points at 60 and 360min should be recommended., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

28. Diversity of Alkylproline Moieties in Pyrrolobenzodiazepines Arises from Postcondensation Modifications of a Unified Building Block.

Author

Kamenik Z, Kadlcik S, Gazak R, Vobruba S, Palanova L, Kuzma M, and Janata J

Subjects

Antineoplastic Agents metabolism, Benzodiazepines classification, Benzodiazepinones chemistry, Biological Products chemistry, Biological Products metabolism, Chemistry, Pharmaceutical, Molecular Structure, Pyrroles classification, Antineoplastic Agents chemistry, Benzodiazepines chemistry, Pyrroles chemistry

Abstract

Anticancer pyrrolobenzodiazepines (PBDs) are one of several groups of natural products that contain unusual 4-alkyl-l-proline derivatives (APDs) in their structure. APD moieties of PBDs are characterized by high structural diversity achieved through unknown biosynthetic machinery. Based on LC-MS analysis of culture broths, feeding experiments, and protein assays, we show that APDs are not incorporated into PBDs in their final form as was previously hypothesized. Instead, a uniform building block, 4-propylidene-l-proline or 4-ethylidene-l-proline, enters the condensation reaction. The subsequent postcondensation steps are initiated by the introduction of an additional double bond catalyzed by a FAD-dependent oxidoreductase, which we demonstrated with Orf7 from anthramycin biosynthesis. The resulting double bond arrangement presumably represents a prerequisite for further modifications of the APD moieties. Our study gives general insight into the diversification of APD moieties of natural PBDs and provides proof-of-principle for precursor directed and combinatorial biosynthesis of new PBD-based antitumor compounds.

Published

2017

29. Metal-free oxidative ring contraction of benzodiazepinones: an entry to quinoxalinones.

Author

Mtiraoui H, Renault K, Sanselme M, Msaddek M, Renard PY, and Sabot C

Subjects

Dimethyl Sulfoxide chemistry, Oxidation-Reduction, Benzodiazepinones chemistry, Quinoxalines chemistry

Abstract

A novel and practical synthesis of 3-benzoylquinoxalin-2(1H)-ones from benzodiazepin-2-ones in two steps from commercially available starting materials is reported. The reaction was achieved in the presence of N-bromosuccinimide in DMSO which served both as a solvent and an oxidant. Significantly, the yet unknown ketone to alcohol fluorescence turn-on of benzoylquinoxalinones was unveiled through the preparation of a fluorescently labelled cholesterol conjugate.

Published

2017

30. New compounds from a hydrothermal vent crab-associated fungus Aspergillus versicolor XZ-4.

Author

Pan C, Shi Y, Chen X, Chen CA, Tao X, and Wu B

Subjects

Anti-Bacterial Agents chemistry, Anti-Bacterial Agents isolation & purification, Benzodiazepinones chemistry, Benzodiazepinones isolation & purification, Benzodiazepinones pharmacology, Biological Products chemistry, Biological Products isolation & purification, Dose-Response Relationship, Drug, Microbial Sensitivity Tests, Molecular Structure, Oxepins chemistry, Oxepins isolation & purification, Quinazolines chemistry, Quinazolines isolation & purification, Structure-Activity Relationship, Anti-Bacterial Agents pharmacology, Aspergillus chemistry, Biological Products pharmacology, Escherichia coli drug effects, Oxepins pharmacology, Quinazolines pharmacology

Abstract

Three new quinazoline derivatives (1-3), one new oxepin-containing natural product (4) and four new cyclopenin derivatives (5-7 and 9) have been isolated from an EtOAc extract of the Taiwan Kueishantao hydrothermal vent crab-associated fungus Aspergillus versicolor XZ-4. Their planar structures were established by HRMS, 1D and 2D NMR spectroscopic data analyses. The absolute configurations for compounds 1 and 4 were determined by chiral phase HPLC analysis of their hydrolysis products. The absolute configurations of 2, 3 and 7 were defined mainly by comparison of the quantum chemical TDDFT calculated and the experimental ECD spectra, and the absolute configuration of 5 was deduced from comparison of the optical rotation values reported in the literature. The presence of two atropisomers of 5 was established by NOE analyses. The Ile & Val units in compounds 1-3 allowed the assignment of a new quinazoline skeleton and it's the first time the configuration of isoleucine in the quinazoline skeleton was defined. A series of 7-methoxy cyclopenin derivatives were reported for the first time in this study. The bioevaluation of compounds 5, 7, 8 and 9 revealed inhibitory activities against E. coli at MIC values around 32 μg mL -1 .

Published

2017

31. ITH14001, a CGP37157-Nimodipine Hybrid Designed to Regulate Calcium Homeostasis and Oxidative Stress, Exerts Neuroprotection in Cerebral Ischemia.

Author

Buendia I, Tenti G, Michalska P, Méndez-López I, Luengo E, Satriani M, Padín-Nogueira F, López MG, Ramos MT, García AG, Menéndez JC, and León R

Subjects

Animals, Animals, Newborn, Benzodiazepinones chemistry, Benzodiazepinones pharmacology, Benzodiazepinones therapeutic use, Brain Ischemia pathology, Cattle, Cell Hypoxia drug effects, Cell Line, Tumor, Cells, Cultured, Chromaffin Cells, Disease Models, Animal, Embryo, Mammalian, Hippocampus drug effects, Hippocampus pathology, Male, Neuroblastoma pathology, Neuroprotective Agents pharmacology, Neuroprotective Agents therapeutic use, Nimodipine analogs & derivatives, Nimodipine chemistry, Rats, Rats, Sprague-Dawley, Thiazepines chemistry, Thiazepines pharmacology, Brain Ischemia drug therapy, Calcium metabolism, Nimodipine pharmacology, Nimodipine therapeutic use, Oxidative Stress drug effects, Thiazepines therapeutic use

Abstract

During brain ischemia, oxygen and glucose deprivation induces calcium overload, extensive oxidative stress, neuroinflammation, and, finally, massive neuronal loss. In the search of a neuroprotective compound to mitigate this neuronal loss, we have designed and synthesized a new multitarget hybrid (ITH14001) directed at the reduction of calcium overload by acting on two regulators of calcium homeostasis; the mitochondrial Na + /Ca 2+ exchanger (mNCX) and L-type voltage dependent calcium channels (VDCCs). This compound is a hybrid of CGP37157 (mNCX inhibitor) and nimodipine (L-type VDCCs blocker), and its pharmacological evaluation revealed a moderate ability to selectively inhibit both targets. These activities conferred concentration-dependent neuroprotection in two models of Ca 2+ overload, such as toxicity induced by high K + in the SH-SY5Y cell line (60% protection at 30 μM) and veratridine in hippocampal slices (26% protection at 10 μM). It also showed neuroprotective effect against oxidative stress, an activity related to its nitrogen radical scavenger effect and moderate induction of the Nrf2-ARE pathway. Its Nrf2 induction capability was confirmed by the increase of the expression of the antioxidant and anti-inflammatory enzyme heme-oxygenase I (3-fold increase). In addition, the multitarget profile of ITH14001 led to anti-inflammatory properties, shown by the reduction of nitrites production induced by lipopolysaccharide in glial cultures. Finally, it showed protective effect in two acute models of cerebral ischemia in hippocampal slices, excitotoxicity induced by glutamate (31% protection at 10 μM) and oxygen and glucose deprivation (76% protection at 10 μM), reducing oxidative stress and iNOS deleterious induction. In conclusion, our hybrid derivative showed improved neuroprotective properties when compared to its parent compounds CGP37157 and nimodipine.

Published

2017

32. Retro-1 Analogues Differentially Affect Oligonucleotide Delivery and Toxin Trafficking.

Author

Yang B, Ming X, Abdelkafi H, Pons V, Michau A, Gillet D, Cintrat JC, Barbier J, and Juliano R

Subjects

Cell Survival drug effects, Dose-Response Relationship, Drug, Drug Carriers chemistry, HeLa Cells, Humans, Molecular Structure, Shiga Toxin chemistry, Structure-Activity Relationship, Benzodiazepinones chemistry, Drug Delivery Systems, Oligonucleotides chemistry, Shiga Toxin pharmacology, Small Molecule Libraries chemistry

Abstract

Retro-1 is a small molecule that displays two important biological activities: First, it blocks the actions of certain toxins by altering their intracellular trafficking. Second, it enhances the activity of oligonucleotides by releasing them from entrapment in endosomes. This raises the question of whether the two actions involve the same cellular target. Herein we report the effects of several Retro-1 analogues on both toxins and oligonucleotides. We found analogues that affect toxins but not oligonucleotides and vice-versa, while Retro-1 is the only compound that affects both. This indicates that the molecular target(s) involved in the two processes are distinct., (© 2016 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2016

33. Development of 4,5-dihydro-benzodiazepinone derivatives as a new chemical series of BRD4 inhibitors.

Author

Li J, Wang P, Zhou B, Shi J, Liu J, Li X, Fan L, Zheng Y, and Ouyang L

Subjects

Benzodiazepinones metabolism, Cell Cycle Proteins, Cell Line, Tumor, Drug Evaluation, Preclinical, Humans, Molecular Docking Simulation, Nuclear Proteins chemistry, Nuclear Proteins metabolism, Protein Conformation, Transcription Factors chemistry, Transcription Factors metabolism, Benzodiazepinones chemistry, Benzodiazepinones pharmacology, Drug Design, Nuclear Proteins antagonists & inhibitors, Transcription Factors antagonists & inhibitors

Abstract

Bromodomains (BRDs) are protein interaction modules that selectively recognize ε -N-lysine residues, serving as key epigenetic readers and play a key role in epigenetic regulation of gene transcription. Bromodomain-containing protein 4 (BRD4), a protein containing two BRDs termed BD1 and BD2, has emerged as an attractive candidate for the development of inhibitors targeting gene transcription in several types of cancers. In this study, we made structural modifications of previously reported BRD4 inhibitors, to develop new chemical scaffold 3,4-dihydroquinoxalin-2(1H)-one. Four series of compounds (compounds 7-10) were synthesized, and the BRD4-inhibitory activity and anti-proliferative effect of these compounds were evaluated. We found compound 10d has remarkable anti-proliferative activities toward leukemia cells and could induce apoptosis by mitochondrial pathways. Notably, the analysis of molecular docking suggested that hydrophobic interaction was essential for compound 10d to bind to BD1. In conclusion, these results demonstrate the potential of compound 10d to be utilized as a BRD4 inhibitor with apoptosis inducing effect in future leukemia therapy., (Copyright © 2016 Elsevier Masson SAS. All rights reserved.)

Published

2016

34. Biochemical and Structural Insights into Doublecortin-like Kinase Domain 1.

Author

Patel O, Dai W, Mentzel M, Griffin MD, Serindoux J, Gay Y, Fischer S, Sterle S, Kropp A, Burns CJ, Ernst M, Buchert M, and Lucet IS

Subjects

Adenosine Triphosphate metabolism, Amino Acid Motifs, Animals, Antineoplastic Agents chemistry, Benzodiazepinones chemistry, Benzodiazepinones pharmacology, Binding Sites, Crystallography, X-Ray, Doublecortin-Like Kinases, Gene Expression, HEK293 Cells, Humans, Intracellular Signaling Peptides and Proteins chemistry, Intracellular Signaling Peptides and Proteins genetics, Intracellular Signaling Peptides and Proteins metabolism, Mice, Mice, Inbred C57BL, Mice, Transgenic, Microtubules drug effects, Microtubules metabolism, Microtubules ultrastructure, Models, Molecular, Protein Binding, Protein Domains, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors pharmacology, Protein Serine-Threonine Kinases chemistry, Protein Serine-Threonine Kinases genetics, Protein Serine-Threonine Kinases metabolism, Protein Structure, Secondary, Pyrimidines chemistry, Pyrimidines pharmacology, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Stomach Neoplasms enzymology, Stomach Neoplasms genetics, Stomach Neoplasms pathology, Substrate Specificity, Tubulin Modulators chemistry, Tubulin Modulators pharmacology, Xenograft Model Antitumor Assays, Adenosine Triphosphate chemistry, Antineoplastic Agents pharmacology, Intracellular Signaling Peptides and Proteins antagonists & inhibitors, Mutation, Protein Serine-Threonine Kinases antagonists & inhibitors, Stomach Neoplasms drug therapy

Abstract

Doublecortin-like kinase 1 (DCLK1) is a serine/threonine kinase that belongs to the family of microtubule-associated proteins. Originally identified for its role in neurogenesis, DCLK1 has recently been shown to regulate biological processes outside of the CNS. DCLK1 is among the 15 most common putative driver genes for gastric cancers and is highly mutated across various other human cancers. However, our present understanding of how DCLK1 dysfunction leads to tumorigenesis is limited. Here, we provide evidence that DCLK1 kinase activity negatively regulates microtubule polymerization. We present the crystal structure of the DCLK1 kinase domain at 1.7 Å resolution, providing detailed insight into the ATP-binding site that will serve as a framework for future drug design. This structure also allowed for the mapping of cancer-causing mutations within the kinase domain, suggesting that a loss of kinase function may contribute to tumorigenesis., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

35. Mechanistic Investigation of a Non-Heme Iron Enzyme Catalyzed Epoxidation in (-)-4'-Methoxycyclopenin Biosynthesis.

Author

Chang WC, Li J, Lee JL, Cronican AA, and Guo Y

Subjects

Alkenes chemistry, Aspergillus nidulans enzymology, Benzodiazepinones chemistry, Benzodiazepinones metabolism, Kinetics, Oxygen chemistry, Biocatalysis, Enzymes metabolism, Epoxy Compounds chemistry, Iron

Abstract

Mechanisms have been proposed for α-KG-dependent non-heme iron enzyme catalyzed oxygen atom insertion into an olefinic moiety in various natural products, but they have not been examined in detail. Using a combination of methods including transient kinetics, Mössbauer spectroscopy, and mass spectrometry, we demonstrate that AsqJ-catalyzed (-)-4'-methoxycyclopenin formation uses a high-spin Fe(IV)-oxo intermediate to carry out epoxidation. Furthermore, product analysis on (16)O/(18)O isotope incorporation from the reactions using the native substrate, 4'-methoxydehydrocyclopeptin, and a mechanistic probe, dehydrocyclopeptin, reveals evidence supporting oxo↔hydroxo tautomerism of the Fe(IV)-oxo species in the non-heme iron enzyme catalysis.

Published

2016

36. Fluorination of an antiepileptic drug: A self supporting transporter by oxygen enrichment mechanism.

Author

Natchimuthu V, Amoros J, and Ravi S

Subjects

Anticonvulsants chemical synthesis, Anticonvulsants metabolism, Anticonvulsants toxicity, Benzodiazepinones chemical synthesis, Benzodiazepinones toxicity, Carbamazepine toxicity, Fructose analogs & derivatives, Fructose toxicity, Halogenation, Humans, MCF-7 Cells, Molecular Weight, Pyrroles chemical synthesis, Pyrroles toxicity, Solubility, Stereoisomerism, Toluene chemical synthesis, Toluene chemistry, Toluene toxicity, Topiramate, Transition Temperature, Anticonvulsants chemistry, Benzodiazepinones chemistry, Pyrroles chemistry, Toluene analogs & derivatives

Abstract

Drug therapy of seizures involves producing high levels of antiepileptic drugs in the blood. Drug must enter the brain by crossing from the blood into the brain tissue, called a transvascular route (TVR). Even before the drug can reach the brain tissue, factors such as systemic toxicity, macrophage phagocytises and reduction in oxygen content limit the success of this TVR. Encapsulating the drug within a nano scale delivering system, synthesising drugs with low molecular weight are the best mechanisms to deliver the drug to the brain. But through this article, we have explored a possibility of attaching a molecule 4-(trifluoromethyl) benzoic acid (TFMBA), that possess more number of fluorine atom, to benzodiazepine (BDZ) resulting in an ionic salt (S)-(+)-2,3-dihydro-1H-pyrrolo[2,1-c][1,4]benzodiazepine5,11(10H,11aH)-dione with 4-(trifluoromethyl)benzoic acid. By this way, reducing the toxicity of BDZ than the conventional anti-epileptic drugs (AEDs), increasing the solubility, reducing the melting point, enriching the TVR with excess oxygen content with the support of fluorine. With all these important prerequisites fulfilled, the drug along with the attached molecule is expected to travel more comfortably through the TVR without any external support than any other conventional AEDs. FTIR, (1)H NMR, (13)C NMR, HRMS spectroscopy, HRTEM and In vitro cytotoxicity analysis supports this study., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2016

37. Molecular Mechanism of Action of Triazolobenzodiazepinone Agonists of the Type 1 Cholecystokinin Receptor. Possible Cooperativity across the Receptor Homodimeric Complex.

Author

Desai AJ, Lam PC, Orry A, Abagyan R, Christopoulos A, Sexton PM, and Miller LJ

Subjects

Allosteric Site, Amino Acid Sequence, Animals, Benzodiazepines pharmacology, Benzodiazepinones pharmacology, CHO Cells, Cricetulus, Humans, Molecular Docking Simulation, Molecular Sequence Data, Mutation, Protein Multimerization, Radioligand Assay, Rats, Receptor, Cholecystokinin A genetics, Receptor, Cholecystokinin A metabolism, Receptor, Cholecystokinin B genetics, Receptor, Cholecystokinin B metabolism, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Sequence Alignment, Structure-Activity Relationship, Triazoles pharmacology, Benzodiazepines chemistry, Benzodiazepinones chemistry, Receptor, Cholecystokinin A agonists, Triazoles chemistry

Abstract

The type 1 cholecystokinin receptor (CCK1R) has multiple physiologic roles relating to nutrient homeostasis, including mediation of postcibal satiety. This effect has been central in efforts to develop agonists of this receptor as part of a program to manage and/or prevent obesity. While a number of small molecule CCK1R agonists have been developed, none have yet been approved for clinical use, based on inadequate efficacy, side effects, or the potential for toxicity. Understanding the molecular details of docking and mechanism of action of these ligands can be helpful in the rational refinement and enhancement of small molecule drug candidates. In the current work, we have defined the mechanism of binding and activity of two triazolobenzodiazepinones, CE-326597 and PF-04756956, which are reported to be full agonist ligands. To achieve this, we utilized receptor binding with a series of allosteric and orthosteric radioligands at structurally related CCK1R and CCK2R, as well as chimeric CCK1R/CCK2R constructs exchanging residues in the allosteric pocket, and assessment of biological activity. These triazolobenzodiazepinones docked within the intramembranous small molecule allosteric ligand pocket, with higher affinity binding to CCK2R than CCK1R, yet with biological activity exclusive to or greatly enhanced at CCK1R. These ligands exhibited cooperativity with benzodiazepine binding across the CCK1R homodimeric complex, resulting in their ability to inhibit only a fraction of the saturable binding of a benzodiazepine radioligand, unlike other small molecule antagonists and agonists of this receptor. This may contribute to the understanding of the unique short duration and reversible gallbladder contraction observed in vivo upon administration of these drugs.

Published

2015

38. Chemoselective Alkylation for Diversity-Oriented Synthesis of 1,3,4-Benzotriazepin-2-ones and Pyrrolo[1,2][1,3,4]benzotriazepin-6-ones, Potential Turn Surrogates.

Author

Douchez A and Lubell WD

Subjects

Alkylation, Azepines chemistry, Benzodiazepinones chemistry, Crystallography, X-Ray, Molecular Conformation, Molecular Structure, Benzodiazepinones chemical synthesis

Abstract

1,3,4-Benzotriazepin-2-ones garner interest for medicinal applications, in part due to their relationship with benzodiazepinones. Ten 1,3,4-benzotriazepin-2-ones 6 and 19 and six pyrrolo[1,2][1,3,4]benzotriazepin-6-ones 7 and 23 were prepared in four to seven steps and 4-60% overall yields by a divergent strategy from methyl anthranilate employing chemoselective alkylations of common linear and cyclic precursors to diversify three triazepinone ring positions (N1, N3, and C5). X-ray crystallography demonstrated that benzotriazepinone 19g may serve as a γ-turn mimic.

Published

2015

39. Structural analysis of quazepam metabolites in bile by ion trap time-of-flight mass spectrometry.

Author

Yamaguchi K, Goda T, Yamaki S, and Ohno Y

Subjects

Benzodiazepines analysis, Benzodiazepinones chemistry, Bile chemistry, Forensic Toxicology, Humans, Hypnotics and Sedatives analysis, Male, Mass Spectrometry methods, Middle Aged, Molecular Structure, Benzodiazepines chemistry, Hypnotics and Sedatives chemistry

Abstract

Quazepam (QZP) is a long-acting benzodiazepine-type hypnotic. We searched for novel QZP metabolites in bile and determined their structures by liquid chromatography-ion trap time-of-flight mass spectrometry (LC-IT-TOF MS). The metabolites were extracted with ethyl acetate after β-glucuronidase treatment. First, a single MS spectrum was acquired. Second, MS(n) spectra were acquired for peaks that consisted of ions with the isotope pattern corresponding to molecules bearing one chlorine atom. The novel QZP metabolites found in this study were hydroxyquazepam, hydroxy-methoxyquazepam, hydroxy-oxoquazepam, and hydroxy-methoxy-oxoquazepam, which have the hydroxy and methoxy groups on the fluorophenyl group, and dihydroxy-oxoquazepam and dihydroxy-methoxy-oxoquazepam, which have one hydroxy group at the 3-position of the seven-membered ring and the other hydroxy group and the methoxy group on the fluorophenyl group. We demonstrated that LC-IT-TOF MS was a useful tool for determining the structure of the metabolites. However, the exact locations of the hydroxy and methoxy groups on the fluorophenyl group could not be identified., (Copyright © 2015 Elsevier Ireland Ltd. All rights reserved.)

Published

2015

40. A novel synthetic compound exerts effective anti-tumour activity in vivo via the inhibition of tubulin polymerisation in A549 cells.

Author

Yan J, Pang Y, Sheng J, Wang Y, Chen J, Hu J, Huang L, and Li X

Subjects

Animals, Antineoplastic Agents adverse effects, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Apoptosis drug effects, Benzodiazepinones adverse effects, Benzodiazepinones chemistry, Benzodiazepinones pharmacology, Carcinoma, Non-Small-Cell Lung metabolism, Cell Line, Tumor, Cell Proliferation drug effects, Cells, Cultured, Drug Resistance, Neoplasm, Drugs, Investigational adverse effects, Drugs, Investigational chemistry, Drugs, Investigational pharmacology, Human Umbilical Vein Endothelial Cells cytology, Human Umbilical Vein Endothelial Cells drug effects, Human Umbilical Vein Endothelial Cells metabolism, Humans, Lung Neoplasms metabolism, Male, Mice, Inbred BALB C, Mice, Nude, Microtubules metabolism, Molecular Docking Simulation, Organophosphates adverse effects, Organophosphates chemistry, Organophosphates pharmacology, Random Allocation, Stilbenes chemistry, Tubulin metabolism, Tubulin Modulators adverse effects, Tubulin Modulators chemistry, Tubulin Modulators pharmacology, Xenograft Model Antitumor Assays, Antineoplastic Agents therapeutic use, Benzodiazepinones therapeutic use, Carcinoma, Non-Small-Cell Lung drug therapy, Drugs, Investigational therapeutic use, Lung Neoplasms drug therapy, Microtubules drug effects, Organophosphates therapeutic use, Tubulin chemistry, Tubulin Modulators therapeutic use

Abstract

Microtubules are critical elements that are involved in a wide range of cellular processes, and thus, they have become an attractive target for many anticancer drugs. A novel synthesised compound, 12P, was identified as new microtubule inhibitor. This compound inhibits tubulin polymerisation through binding to the colchicine-binding site of tubulin. 12P exhibits excellent anti-proliferative activities against a panel of human cancer cell lines, with IC₅₀ values range from 9 to 55nM. Interestingly, compound 12P also displayed equally potent cytotoxicity against several drug-resistant cell lines, and it showed high selectivity for active human umbilical vein endothelial cells (HUVECs). Further flow cytometric analysis showed that 12P induces G₂/M phase arrest and apoptosis in A549 cells. Cellular studies have revealed that the induction of apoptosis by 12P was associated with a collapse of mitochondrial membrane potential (MMP), accumulation of reactive oxygen species (ROS), alterations in the expression of some cell cycle-related proteins (e.g. Cyclin B1, Cdc25c, Cdc2) and some apoptosis-related proteins (e.g. Bax, Bad, Bcl-2, Bcl-xl). Importantly, 12P significantly reduced the growth of xenograft tumours of A549 cells in vivo (tumour inhibitory rate of 12P: 84.2%), without any loss of body weight. Taken together, these in vitro and in vivo results suggested that 12P may become a promising lead compound for the development of new anticancer drugs., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published

2015

41. γ-Turn Mimicry with Benzodiazepinones and Pyrrolobenzodiazepinones Synthesized from a Common Amino Ketone Intermediate.

Author

Dörr AA and Lubell WD

Subjects

Benzodiazepines chemistry, Benzodiazepinones chemistry, Biomimetics, Molecular Structure, Oxidation-Reduction, Amino Acids chemistry, Aniline Compounds chemistry, Benzodiazepines chemical synthesis, Benzodiazepinones chemical synthesis, Ketones chemistry, Pentanones chemistry

Abstract

To investigate diazepinone analogues as γ-turn mimics, seven 1,4-benzodiazepin-2-ones 6 and fourteen pyrrolo[1,2-d][1,4]benzodiazepin-6-ones 4 and 5 were synthesized from 1-(2-aminophenyl)pent-4-en-1-one (7). Acylation of aniline 7 with N-Boc-amino acids, olefin oxidation, Boc removal, and intramolecular Paal-Knorr condensation gave 4 and 5. Alternatively, Boc removal prior to oxidation gave benzodiazepinones 6, which were converted to 4 by ozonolysis and cyclization. Comparison of dihedral angle values for the amino acid component from X-ray analyses of 4g, 5f, and 6f and related diazepinones has catalogued the manner by which ring substituents affect the component's ability to mimic the central residues of γ-turns.

Published

2015

42. M2 Subtype preferring dibenzodiazepinone-type muscarinic receptor ligands: Effect of chemical homo-dimerization on orthosteric (and allosteric?) binding.

Author

Keller M, Tränkle C, She X, Pegoli A, Bernhardt G, Buschauer A, and Read RW

Subjects

Allosteric Site, Animals, Benzodiazepinones chemical synthesis, Benzodiazepinones metabolism, CHO Cells drug effects, Chemistry Techniques, Synthetic, Cricetulus, Dimerization, Dose-Response Relationship, Drug, Humans, Inhibitory Concentration 50, Ligands, N-Methylscopolamine metabolism, Piperidines chemistry, Radioligand Assay, Receptor, Muscarinic M2 genetics, Benzodiazepinones chemistry, Receptor, Muscarinic M2 metabolism, Structure-Activity Relationship

Abstract

A series of new dibenzodiazepinone-type muscarinic receptor ligands, including two homo-dimeric compounds, was prepared. Sixteen representative compounds were characterized in equilibrium binding studies with [(3)H]N-methylscopolamine ([(3)H]NMS) at the muscarinic receptor subtype M2, and seven selected compounds were additionally investigated at M1, M3, M4 and M5 with respect to receptor subtype selectivity. The side chain of the known M2 preferring muscarinic receptor antagonist DIBA was widely varied with respect to chain length and type of the basic group (amine, imidazole, guanidine and piperazine). Most of the structural changes were well tolerated with respect to muscarinic receptor binding, determined by displacement of [(3)H]NMS. Compounds investigated at all subtypes shared a similar selectivity profile, which can be summarized as M2>M1≈M4>M3≈M5 (46, 50, 57, 62-64) and M2>M1≈M4>M3>M5 (1, 58). The homo-dimeric dibenzodiazepinone derivatives UNSW-MK250 (63) and UNSW-MK262 (64) exhibited the highest M2 receptor affinities (pIC50=9.0 and 9.2, respectively). At the M2 receptor a steep curve slope of -2 was found for the dimeric ligand 63, which cannot be described according to the law of mass action, suggesting a more complex mechanism of binding. In addition to equilibrium binding studies, for selected ligands, we determined pEC50,diss, an estimate of affinity to the allosteric site of M2 receptors occupied with [(3)H]NMS. Compounds 58 and 62-64 were capable of retarding [(3)H]NMS dissociation by a factor >10 (Emax,diss >92%), with highest potency (pEC50,diss=5.56) residing in the dimeric compound 64. As the monomeric counterpart of 64 was 100 times less potent (62: pEC50,diss=3.59), these data suggest that chemical dimerization of dibenzodiazepinone-type M receptor ligands can enhance allosteric binding., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

43. Synthesis, Chiral Separation, Absolute Configuration Assignment, and Biological Activity of Enantiomers of Retro-1 as Potent Inhibitors of Shiga Toxin.

Author

Abdelkafi H, Michau A, Clerget A, Buisson DA, Johannes L, Gillet D, Barbier J, and Cintrat JC

Subjects

Benzodiazepinones chemistry, Benzodiazepinones isolation & purification, Crystallography, X-Ray, Dose-Response Relationship, Drug, Escherichia coli chemistry, Models, Molecular, Molecular Structure, Shiga Toxin metabolism, Shigella dysenteriae chemistry, Stereoisomerism, Structure-Activity Relationship, Benzodiazepinones chemical synthesis, Benzodiazepinones pharmacology, Shiga Toxin antagonists & inhibitors

Abstract

The Shiga toxin (Stx) family is composed of related protein toxins produced by the bacteria Shigella dysenteriae and certain pathogenic strains of E. coli. No effective therapies for Stx intoxication have been developed yet. However, inhibitors that act on the intracellular trafficking of these toxins may provide new options for the development of therapeutic strategies. This study reports the synthesis, chromatographic separation, and pharmacological evaluation of the two enantiomers of Retro-1, a compound active against Stx and other such protein toxins. Retro-1 works by inhibiting retrograde transport of these toxins inside cells. In vitro experiments proved that the configuration of the stereocenter at position 5 is not crucial for the activity of this compound. X-ray diffraction data revealed (S)-Retro-1 to be slightly more active than (R)-Retro-1., (© 2015 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2015

44. Differential Inhibition of Signal Peptide Peptidase Family Members by Established γ-Secretase Inhibitors.

Author

Ran Y, Ladd GZ, Ceballos-Diaz C, Jung JI, Greenbaum D, Felsenstein KM, and Golde TE

Subjects

Alanine analogs & derivatives, Alanine chemistry, Alanine metabolism, Amino Acid Sequence, Amyloid Precursor Protein Secretases metabolism, Amyloid beta-Peptides genetics, Amyloid beta-Peptides metabolism, Animals, Aspartic Acid Endopeptidases genetics, Aspartic Acid Endopeptidases metabolism, Azepines chemistry, Azepines metabolism, Benzodiazepinones chemistry, Benzodiazepinones metabolism, Cell Line, Enzyme-Linked Immunosorbent Assay, HEK293 Cells, Humans, Immunoprecipitation, Membrane Proteins chemistry, Membrane Proteins genetics, Membrane Proteins metabolism, Mice, Molecular Sequence Data, Protease Inhibitors metabolism, Recombinant Fusion Proteins biosynthesis, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins genetics, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Substrate Specificity, Amyloid Precursor Protein Secretases antagonists & inhibitors, Aspartic Acid Endopeptidases antagonists & inhibitors, Protease Inhibitors chemistry

Abstract

The signal peptide peptidases (SPPs) are biomedically important proteases implicated as therapeutic targets for hepatitis C (human SPP, (hSPP)), plasmodium (Plasmodium SPP (pSPP)), and B-cell immunomodulation and neoplasia (signal peptide peptidase like 2a, (SPPL2a)). To date, no drug-like, selective inhibitors have been reported. We use a recombinant substrate based on the amino-terminus of BRI2 fused to amyloid β 1-25 (Aβ1-25) (FBA) to develop facile, cost-effective SPP/SPPL protease assays. Co-transfection of expression plasmids expressing the FBA substrate with SPP/SPPLs were conducted to evaluate cleavage, which was monitored by ELISA, Western Blot and immunoprecipitation/MALDI-TOF Mass spectrometry (IP/MS). No cleavage is detected in the absence of SPP/SPPL overexpression. Multiple γ-secretase inhibitors (GSIs) and (Z-LL)2 ketone differentially inhibited SPP/SPPL activity; for example, IC50 of LY-411,575 varied from 51±79 nM (on SPPL2a) to 5499±122 nM (on SPPL2b), while Compound E showed inhibition only on hSPP with IC50 of 1465±93 nM. Data generated were predictive of effects observed for endogenous SPPL2a cleavage of CD74 in a murine B-Cell line. Thus, it is possible to differentially inhibit SPP family members. These SPP/SPPL cleavage assays will expedite the search for selective inhibitors. The data also reinforce similarities between SPP family member cleavage and cleavage catalyzed by γ-secretase.

Published

2015

45. Optimisation of LRRK2 inhibitors and assessment of functional efficacy in cell-based models of neuroinflammation.

Author

Munoz L, Kavanagh ME, Phoa AF, Heng B, Dzamko N, Chen EJ, Doddareddy MR, Guillemin GJ, and Kassiou M

Subjects

Anti-Inflammatory Agents chemistry, Benzodiazepinones chemistry, Cells, Cultured, Glioma enzymology, Glioma pathology, Humans, Inflammation enzymology, Inflammation pathology, Interleukin-1beta pharmacology, Interleukin-6 metabolism, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2, Microglia cytology, Microglia enzymology, Models, Biological, Pyrimidines chemistry, Anti-Inflammatory Agents pharmacology, Benzodiazepinones pharmacology, Glioma drug therapy, Inflammation drug therapy, Microglia drug effects, Protein Kinase Inhibitors pharmacology, Protein Serine-Threonine Kinases antagonists & inhibitors, Pyrimidines pharmacology

Abstract

LRRK2IN1 is a highly potent inhibitor of leucine-rich repeat kinase 2 (LRRK2, IC50 = 7.9 nM), an established target for treatment of Parkinson's disease. Two LRRK2IN1 analogues 1 and 2 were synthesised which retained LRRK2 inhibitory activity (1: IC50 = 72 nM; 2: IC50 = 51 nM), were predicted to have improved bioavailability and were efficacious in cell-based models of neuroinflammation. Analogue 1 inhibited IL-6 secretion from LPS-stimulated primary human microglia with EC50 = 4.26 μM. In order to further optimize the molecular properties of LRRK2IN1, a library of truncated analogues was designed based on docking studies. Despite lacking LRRK2 inhibitory activity, these compounds show anti-neuroinflammatory efficacy at micromolar concentration. The compounds developed were valuable tools in establishing a cell-based assay for assessing anti-neuroinflammatory efficacy of LRRK2 inhibitors. Herein, we present data that IL-1β stimulated U87 glioma cell line is a reliable model for neuroinflammation, as data obtained in this model were consistent with results obtained using primary human microglia and astrocytes., (Copyright © 2015 Elsevier Masson SAS. All rights reserved.)

Published

2015

46. BMS-871: a novel orally active pan-Notch inhibitor as an anticancer agent.

Author

Shan W, Balog A, Quesnelle C, Gill P, Han WC, Norris D, Mandal S, Thiruvenkadam R, Gona KB, Thiyagarajan K, Kandula S, McGlinchey K, Menard K, Wen ML, Rose A, White R, Guarino V, Shen DR, Cvijic ME, Ranasinghe A, Dai J, Zhang Y, Wu DR, Mathur A, Rampulla R, Trainor G, Hunt JT, Vite GD, Westhouse R, Lee FY, and Gavai AV

Subjects

Administration, Oral, Animals, Antineoplastic Agents chemistry, Benzodiazepinones chemistry, Cell Line, Tumor, Cell Proliferation drug effects, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Humans, Mice, Microsomes, Liver drug effects, Microsomes, Liver metabolism, Molecular Structure, Neoplasms, Experimental drug therapy, Neoplasms, Experimental metabolism, Neoplasms, Experimental pathology, Receptors, Notch metabolism, Structure-Activity Relationship, Antineoplastic Agents administration & dosage, Antineoplastic Agents pharmacology, Benzodiazepinones administration & dosage, Benzodiazepinones pharmacology, Receptors, Notch antagonists & inhibitors

Abstract

This Letter describes synthesis, SAR, and biological activity of (2-oxo-1,4-benzodiazepin-3-yl)-succinamides as inhibitors of γ-secretase mediated signaling of Notch receptors. Optimization of this series led to the identification of BMS-871 (compound 30) which displayed robust in vivo efficacy in Notch-dependent leukemia and solid tumor xenograft models., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

47. Benzodiazepinone derivatives protect against endoplasmic reticulum stress-mediated cell death in human neuronal cell lines.

Author

Zou H, Limpert AS, Zou J, Dembo A, Lee PS, Grant D, Ardecky R, Pinkerton AB, Magnuson GK, Goldman ME, Rong J, Teriete P, Sheffler DJ, Reed JC, and Cosford ND

Subjects

Animals, Calcium metabolism, Cell Death drug effects, Cell Line, Dose-Response Relationship, Drug, Enzyme Inhibitors toxicity, Homeostasis drug effects, Humans, Imidazoles pharmacology, Ionomycin pharmacology, Leupeptins pharmacology, MAP Kinase Signaling System drug effects, Oleanolic Acid analogs & derivatives, Oleanolic Acid pharmacology, Rats, Structure-Activity Relationship, Thapsigargin chemistry, Thapsigargin toxicity, Benzodiazepinones chemistry, Benzodiazepinones pharmacology, Endoplasmic Reticulum Stress drug effects, Neurons drug effects

Abstract

Endoplasmic reticulum (ER) stress causes neuronal dysfunction followed by cell death and is recognized as a feature of many neurodegenerative diseases. Using a phenotypic screen, we recently identified benzodiazepinone derivatives that reduce ER stress-mediated apoptosis in a rat neuronal progenitor cell line (CSM14.1). Herein we describe how structure-activity relationship (SAR) studies around these screening hits led to compounds that display robust cytoprotective activity against thapsigargin-induced ER stress in SH-SY5Y and H4 human neuronal cell lines. We demonstrate that the most potent of these derivatives, compound 4hh, inhibits the activation of p38 MAP kinase (p38) and c-Jun N-terminal kinase (JNK), protein kinases that are downstream signal effectors of the unfolded protein response (UPR). Compound 4hh specifically protects against thapsigargin-induced cell death and displays no protection against other insults known to induce cellular stress or activate p38. However, compound 4hh provides moderate inhibition of p38 activity stimulated by compounds that disrupt calcium homeostasis. Our data indicate that probe compound 4hh is a valuable small molecule tool that can be used to investigate the effects of ER stress on human neurons. This approach may provide the basis for the future development of therapeutics for the treatment of neurodegenerative diseases.

Published

2015

48. Development of certain novel N-(2-(2-(2-oxoindolin-3-ylidene)hydrazinecarbonyl)phenyl)-benzamides and 3-(2-oxoindolin-3-ylideneamino)-2-substituted quinazolin-4(3H)-ones as CFM-1 analogs: design, synthesis, QSAR analysis and anticancer activity.

Author

Alafeefy AM, Ashour AE, Prasad O, Sinha L, Pathak S, Alasmari FA, Rishi AK, and Abdel-Aziz HA

Subjects

Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Benzamides chemical synthesis, Benzamides chemistry, Benzodiazepinones chemical synthesis, Benzodiazepinones chemistry, Cell Line, Tumor, Cell Proliferation drug effects, Dose-Response Relationship, Drug, HeLa Cells, Humans, Indoles chemical synthesis, Indoles chemistry, Molecular Structure, Quinazolinones chemical synthesis, Quinazolinones chemistry, Structure-Activity Relationship, Antineoplastic Agents pharmacology, Benzamides pharmacology, Benzodiazepinones pharmacology, Drug Design, Indoles pharmacology, Quantitative Structure-Activity Relationship, Quinazolinones pharmacology

Abstract

The reaction of N-(2-(hydrazinecarbonyl)aryl)benzamides 2a, b with indoline-2,3-diones 4ae in acidified ethanolic solution furnished the corresponding N-(2-(2-(2-oxoindolin-3-ylidene)hydrazinecarbonyl)phenyl)benzamides 5aj, respectively. Furthermore, 3-(2-oxoindolin-3-ylideneamino)-2-substituted quinazolin-4(3H)-ones 6aj were prepared by the reaction of 3-amino-2-arylquinazolin-4(3H)-one 3a, b with 4ae. Six derivatives of the twenty newly synthesized compounds showed remarkable antitumor activity against most of the tested cell lines, Daoy, UW228-2, Huh-7, Hela and MDA-MB231. Although these six compounds were more potent than the standard drug (CFM-1), indeed compounds 5b, 5d and 6b were the best candidates with IC50 values in the range 1.866.87, 4.4210.89 and 1.468.60 μg/ml and percentage inhibition in the range 77.188.7, 59.4184.8 and 75.488.0%, respectively. QSAR analyses on the current series of derivatives also have been performed for all five cancer cell lines and thus 10 statistically significant models were developed and internally cross validated., (Copyright © 2014 Elsevier Masson SAS. All rights reserved.)

Published

2015

49. Design, synthesis, and biological evaluation of combretabenzodiazepines: a novel class of anti-tubulin agents.

Author

Galli U, Travelli C, Aprile S, Arrigoni E, Torretta S, Grosa G, Massarotti A, Sorba G, Canonico PL, Genazzani AA, and Tron GC

Subjects

Antineoplastic Agents chemistry, Benzodiazepinones chemical synthesis, Benzodiazepinones chemistry, Cell Proliferation drug effects, Crystallography, X-Ray, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Humans, Models, Molecular, Molecular Structure, Structure-Activity Relationship, Tubulin Modulators chemistry, Tumor Cells, Cultured, Antineoplastic Agents chemical synthesis, Antineoplastic Agents pharmacology, Benzodiazepinones pharmacology, Drug Design, Tubulin metabolism, Tubulin Modulators chemical synthesis, Tubulin Modulators pharmacology

Abstract

In the present manuscript, starting from the 1,4-benzodiazepin-2-one nucleus, a privileged structure in medicinal chemistry, we have synthesized a novel class of cis-locked combretastatins named combreatabenzodiazepines. They show similar cytotoxic and antitubulin activity compared to combretastatin A-4 in neuroblastoma cells, showing a better pharmacokinetic profile. This class of compounds has therefore the potential for further development as antitubulin agents.

Published

2015

50. Integrated Ugi-based assembly of functionally, skeletally, and stereochemically diverse 1,4-benzodiazepin-2-ones.

Author

Azuaje J, Pérez-Rubio JM, Yaziji V, El Maatougui A, González-Gomez JC, Sánchez-Pedregal VM, Navarro-Vázquez A, Masaguer CF, Teijeira M, and Sotelo E

Subjects

Combinatorial Chemistry Techniques, Molecular Structure, Organic Chemistry Phenomena, Stereoisomerism, Benzodiazepinones chemistry

Abstract

A practical, integrated and versatile U-4CR-based assembly of 1,4-benzodiazepin-2-ones exhibiting functionally, skeletally, and stereochemically diverse substitution patterns is described. By virtue of its convergence, atom economy, and bond-forming efficiency, the methodology documented herein exemplifies the reconciliation of structural complexity and experimental simplicity in the context of medicinal chemistry projects.

Published

2015