Your search keyword '"Brain penetration"' showing total 11 results

1. Design of a brain-penetrant CDK4/6 inhibitor for glioblastoma.

Author

Bronner, Sarah M., Merrick, Karl A., Murray, Jeremy, Salphati, Laurent, Moffat, John G., Pang, Jodie, Sneeringer, Christopher J., Dompe, Nicholas, Cyr, Patrick, Purkey, Hans, Boenig, Gladys de Leon, Li, Jun, Kolesnikov, Aleksandr, Larouche-Gauthier, Robin, Lai, Kwong Wah, Shen, Xiaoli, Aubert-Nicol, Samuel, Chen, Yi-Chen, Cheong, Jonathan, and Crawford, James J.

Subjects

*BLOOD-brain barrier, *CELL lines, *BRAIN tumors

Abstract

CDK4 and CDK6 are kinases with similar sequences that regulate cell cycle progression and are validated targets in the treatment of cancer. Glioblastoma is characterized by a high frequency of CDKN2A/CCND2/CDK4/CDK6 pathway dysregulation, making dual inhibition of CDK4 and CDK6 an attractive therapeutic approach for this disease. Abemaciclib, ribociclib, and palbociclib are approved CDK4/6 inhibitors for the treatment of HR+/HER2− breast cancer, but these drugs are not expected to show strong activity in brain tumors due to poor blood brain barrier penetration. Herein, we report the identification of a brain-penetrant CDK4/6 inhibitor derived from a literature molecule with low molecular weight and topological polar surface area (MW = 285 and TPSA = 66 Å2), but lacking the CDK2/1 selectivity profile due to the absence of a basic amine. Removal of a hydrogen bond donor via cyclization of the pyrazole allowed for the introduction of basic and semi-basic amines, while maintaining in many cases efflux ratios reasonable for a CNS program. Ultimately, a basic spiroazetidine (cp K a = 8.8) was identified that afforded acceptable selectivity over anti-target CDK1 while maintaining brain-penetration in vivo (mouse K p,uu = 0.20–0.59). To probe the potency and selectivity, our lead compound was evaluated in a panel of glioblastoma cell lines. Potency comparable to abemaciclib was observed in Rb-wild type lines U87MG, DBTRG-05MG, A172, and T98G, while Rb-deficient cell lines SF539 and M059J exhibited a lack of sensitivity. [ABSTRACT FROM AUTHOR]

Published

2019

2. Discovery of potent azaindazole leucine-rich repeat kinase 2 (LRRK2) inhibitors possessing a key intramolecular hydrogen bond – Part 2.

Author

Shore, Daniel G.M., Sweeney, Zachary K., Beresford, Alan, Chan, Bryan K., Chen, Huifen, Drummond, Jason, Gill, Andrew, Kleinheinz, Tracy, Liu, Xingrong, Medhurst, Andrew D., McIver, Edward G., Moffat, John G., Zhu, Haitao, and Estrada, Anthony A.

Subjects

*DARDARIN, *KINASE inhibitors, *HYDROGEN bonding, *INTRAMOLECULAR forces, *PARKINSON'S disease, *NEURODEGENERATION

Abstract

Graphical abstract Highlights • A series of potent azaindazole inhibitors of LRRK2 was discovered. • A putative intramolecular hydrogen bond was crucial for LRRK2 potency. • Optimization led to potent, metabolically stable, and brain-permeable molecules. • Compound 18 showed excellent LRRK2 potency and properties. Abstract The discovery of disease-modifying therapies for Parkinson's Disease (PD) represents a critical need in neurodegenerative medicine. Genetic mutations in LRRK2 are risk factors for the development of PD, and some of these mutations have been linked to increased LRRK2 kinase activity and neuronal toxicity in cellular and animal models. As such, research towards brain-permeable kinase inhibitors of LRRK2 has received much attention. In the course of a program to identify structurally diverse inhibitors of LRRK2 kinase activity, a 5-azaindazole series was optimized for potency, metabolic stability and brain penetration. A key design element involved the incorporation of an intramolecular hydrogen bond to increase permeability and potency against LRRK2. This communication will outline the structure-activity relationships of this matched pair series including the challenge of obtaining a desirable balance between metabolic stability and brain penetration. [ABSTRACT FROM AUTHOR]

Published

2019

3. Discovery of novel potent imidazo[1,2-b]pyridazine PDE10a inhibitors.

Author

Meegalla, Sanath K., Huang, Hui, Illig, Carl R., Parks, Daniel J., Chen, Jinsheng, Lee, Yu-Kai, Wilson, Kenneth J., Patel, Sharmila K., Cheung, Wing S., Lu, Tianbao, Kirchner, Thomas, Askari, Hossein B., Geisler, John, Patch, Raymond J., Gibbs, Alan C., Rady, Brian, Connelly, Margery, and Player, Mark R.

Subjects

*DRUG design, *PYRIDAZINES, *IMIDAZOLES, *PHARMACOKINETICS, *GHRELIN receptors, *IN vitro studies

Abstract

Design and optimization of a novel series of imidazo[1,2-b]pyridazine PDE10a inhibitors are described. Compound 31 displays excellent pharmacokinetic properties and was also evaluated as an insulin secretagogue in vitro and in vivo. [ABSTRACT FROM AUTHOR]

Published

2016

4. Synthesis and biological evaluation of novel imidazol-1-ylacetic acid derivatives as non-brain penetrant bombesin receptor subtype-3 (BRS-3) agonists.

Author

Kiyotsuka, Yohei, Shimada, Kousei, Kobayashi, Shozo, Suzuki, Masanori, Akiu, Mayuko, Asano, Masayoshi, Sogawa, Yoshitaka, Hara, Takashi, Konishi, Masahiro, Abe-Ohya, Rie, Izumi, Masanori, Nagai, Yoko, Yoshida, Kazuhiro, Abe, Yasuyuki, Takamori, Hideo, and Takahashi, Hisashi

Subjects

*IMIDAZOLES, *BOMBESIN receptors, *CHEMICAL synthesis, *CARBOXYLIC acids, *LABORATORY mice

Abstract

Novel compounds based on 1a were synthesized with the focus of obtaining agonists acting upon peripheral BRS-3. To identify potent anti-obesity compounds without adverse effects on the central nervous system (CNS), a carboxylic acid moiety and a labile carboxylic ester with an antedrug functionality were introduced. Through the extensive synthetic exploration and the pharmacokinetic studies of intravenous administration in mice, the ester 2b was selected owing to its most suitable pharmacological profile. In the evaluation of food intake suppression in C57BL/6N mice, 2b showed significant in vivo efficacy and no clear adverse effects on blood pressure change in dogs administered the compound by intravenous infusion. [ABSTRACT FROM AUTHOR]

Published

2016

5. Discovery of novel chiral diazepines as bombesin receptor subtype-3 (BRS-3) agonists with low brain penetration.

Author

Matsufuji, Tetsuyoshi, Shimada, Kousei, Kobayashi, Shozo, Kawamura, Asuka, Fujimoto, Teppei, Arita, Tsuyoshi, Hara, Takashi, Konishi, Masahiro, Abe-Ohya, Rie, Izumi, Masanori, Sogawa, Yoshitaka, Nagai, Youko, Yoshida, Kazuhiro, and Takahashi, Hisashi

Subjects

*DIAZEPINES, *CHIRALITY, *BOMBESIN receptors, *BRAIN physiology, *CENTRAL nervous system, *LABORATORY mice

Abstract

Abstract: The discovery and optimization of a novel series of BRS-3 agonists are described. We explored a potent BRS-3 agonist with low brain penetration to avoid an adverse effect derived from central nervous system exposure. Through the derivatization process, chiral diazepines 9f and 9g were identified as possessing low brain penetration as well as potent in vitro activity against human and mouse BRS-3s. [Copyright &y& Elsevier]

Published

2014

6. Indolyl and dihydroindolyl N-glycinamides as potent and in vivo active NPY5 antagonists

Author

Wu, Lingyun, Lu, Kai, Packiarajan, Mathivanan, Jubian, Vrej, Chandrasena, Gamini, Wolinsky, Toni C., and Walker, Mary W.

Subjects

*INDOLE compounds, *GLYCINAMIDE, *STRUCTURE-activity relationship in pharmacology, *NEUROPEPTIDE Y receptors, *DRUG dosage, *DRUG monitoring, *PHARMACOKINETICS

Abstract

Abstract: A novel series of indolyl and dihydroindolyl glycinamides were identified as potent NPY5 antagonists with in vivo activity from screen hit 1. The dihydroindolyl glycinamide 10a significantly inhibits NPY5 agonist induced feeding at a dose of 0.1mg/kg. The indolyl glycinamide 12c also inhibits NPY5 agonist induced feeding at a dose of 1mg/kg. Both compounds 10a and 12c represent potential tools for further investigation into the biology of the NPY5 receptor. [Copyright &y& Elsevier]

Published

2012

7. N-Heteroaryl glycinamides and glycinamines as potent NPY5 antagonists

Author

Wu, Lingyun, Lu, Kai, Desai, Mahesh, Packiarajan, Mathivanan, Joshi, Amita, Marzabadi, Mohammad R., Jubian, Vrej, Andersen, Kim, Chandrasena, Gamini, Boyle, Noel J., and Walker, Mary W.

Subjects

*AMIDES, *AMINES, *LIGANDS (Biochemistry), *MICROSOMES, *NEUROPEPTIDE Y, *HYDROGEN bonding

Abstract

Abstract: Subtype specific ligands are needed to evaluate the therapeutic potential of modulating the brain’s neuropeptide Y system. The benzothiazepine glycinamide 1a was identified as an NPY5 antagonist lead. While having acceptable solubility, the compound was found to suffer from high clearance and poor exposure. Optimization efforts are described targeting improvements in potency, microsomal stability, and PK properties. The low microsomal stability and poor PK properties were addressed through the optimization of the sulfonyl urea and replacement of the benzothiazepinone with other N-heteroaryl glycinamides. For example, the analogous benzoxazine glycinamide 2e has improvements in both affinity (human Y5 K i 4nM vs 1a 27nM) and microsomal stability (human CLint 2.5L/min vs 1a 35L/min). However the brain penetration (B/P 43/430nM at 10mg/kg PO) remained an unresolved issue. Further optimization by decreasing the hydrogen bond donating properties and PSA provided potent and brain penetrant NPY5 antagonists such as 5f (human Y5 K i 9nM, B/P 520/840nM 10mg/kg PO). [Copyright &y& Elsevier]

Published

2011

8. Discovery of 3,9-diazabicyclo[4.2.1]nonanes as potent dual orexin receptor antagonists with sleep-promoting activity in the rat

Author

Coleman, Paul J., Schreier, John D., Roecker, Anthony J., Mercer, Swati P., McGaughey, Georgia B., Cox, Christopher D., Hartman, George D., Harrell, C. Meacham, Reiss, Duane R., Doran, Scott M., Garson, Susan L., Anderson, Wayne B., Tang, Cuyue, Prueksaritanont, Thomayant, Winrow, Christopher J., and Renger, John J.

Subjects

*DRUG development, *DRUG synergism, *OREXINS, *HORMONE receptors, *CHEMICAL inhibitors, *LABORATORY rats, *NEUROPEPTIDES, *SLEEP-wake cycle

Abstract

Abstract: Orexins are excitatory neuropeptides that regulate arousal and sleep. Orexin receptor antagonists promote sleep and offer potential as a new therapy for the treatment of insomnia. In this Letter, we describe the synthesis of constrained diazepanes having a 3,9 diazabicyclo[4.2.1]nonane bicyclic core with good oral bioavailability and sleep-promoting activity in a rat EEG model. [Copyright &y& Elsevier]

Published

2010

9. N-Glycine-sulfonamides as potent dual orexin 1/orexin 2 receptor antagonists

Author

Aissaoui, Hamed, Koberstein, Ralf, Zumbrunn, Cornelia, Gatfield, John, Brisbare-Roch, Catherine, Jenck, Francois, Treiber, Alexander, and Boss, Christoph

Subjects

*GLYCINE, *SULFONAMIDES, *OREXINS, *ACETIC acid

Abstract

Abstract: A series of dual OX1R/OX2R orexin antagonists was prepared based on a N-glycine-sulfonamide core. SAR studies of a screening hit led to compounds with low nanomolar affinity for both receptors and good oral bioavailability. One of these compounds, 47, has demonstrated in vivo activity in rats following oral administration. [Copyright &y& Elsevier]

Published

2008

10. Discovery of brain penetrant, soluble, pyrazole amide EP1 receptor antagonists

Author

Hall, Adrian, Billinton, Andy, Bristow, Alan K., Brown, Susan H., Chowdhury, Anita, Cutler, Leanne, Giblin, Gerard M.P., Goldsmith, Paul, Hayhow, Thomas G., Kilford, Ian R., Naylor, Alan, Passingham, Barry, and Rawlings, D. Anthony

Subjects

*CARBOXYLIC acids, *PYRAZOLES, *AZOLES, *ORGANIC acids

Abstract

Abstract: We describe the discovery of a series of pyrazole amide EP1 receptor antagonists with good aqueous solubility and CNS penetration. In order to achieve solubility we investigated the incorporation of a basic group in the region of the molecule previously occupied by a carboxylic acid, which was known to be a key element of the pharmacophore. This study led to the identification of compounds such as 4h, 4j and 10b which demonstrated brain-to-blood ratios of 0.8:1–2.0:1 in addition to good solubility and metabolic stability. [Copyright &y& Elsevier]

Published

2008

11. 3,4-Dihydro-2H-benzo[1,4]oxazine derivatives as 5-HT6 receptor antagonists

Author

Zhao, Shu-Hai, Berger, Jacob, Clark, Robin D., Sethofer, Steven G., Krauss, Nancy E., Brothers, Julie M., Martin, Renee S., Misner, Dinah L., Schwab, Dietmar, and Alexandrova, Ludmila

Subjects

*CHEMICAL inhibitors, *ORGANIC compounds, *CARBON compounds, *BENZENE

Abstract

Abstract: A series of novel 3,4-dihydro-2H-benzo[1,4]oxazine derivatives has been designed and synthesized as 5-HT6 receptor antagonists. Many of the compounds displayed subnanomolar affinities for the 5-HT6 receptor and good brain penetration in rats. The relationship of structure and lipophilicity to hERG inhibition of this series of compounds is discussed. [Copyright &y& Elsevier]

Published

2007