Your search keyword '"Brain penetration"' showing total 218 results

1. Adagrasib in the Treatment of KRAS p.G12C Positive Advanced NSCLC: Design, Development and Place in Therapy

Author

Warnecke B and Nagasaka M

Subjects

kristen rat sarcoma viral oncogene homolog, sotorasib, amg510, mrtx849, krystal, codebreak, brain penetration, Therapeutics. Pharmacology, RM1-950

Abstract

Brian Warnecke,1 Misako Nagasaka1,2 1Department of Medicine, University of California Irvine School of Medicine, Chao Family Comprehensive Cancer Center, Orange, CA, USA; 2Department of Medicine, St. Marianna University School of Medicine, Kawasaki, JapanCorrespondence: Misako Nagasaka, Department of Medicine, University of California Irvine School of Medicine, Chao Family Comprehensive Cancer Center, Orange, CA, 92868, USA, Email nagasakm@hs.uci.eduAbstract: One of the most common mutations seen in lung cancers are mutations in Kristen Rat Sarcoma Viral Oncogene Homolog (KRAS), observed in 25– 30% of patients with NSCLC. Mutations in KRAS result in oncogenesis via persistent activation of the MAPK/ERK pathways. Although once thought to be “undruggable”, KRAS p.G12C inhibitors such as sotorasib and adagrasib have been developed. This paper focuses on adagrasib, the second KRAS p.G12C inhibitor to obtain regulatory approval by the FDA and describes the details on its study design, development and current place in therapy.Keywords: Kristen Rat Sarcoma Viral Oncogene Homolog, sotorasib, AMG510, MRTX849, KRYSTAL, CodeBreaK, brain penetration

Published

2024

2. Solubility-Permeability Interplay in Facilitating the Prediction of Drug Disposition Routes, Extent of Absorption, Food Effects, Brain Penetration and Drug Induced Liver Injury Potential

Author

Benet, Leslie Z

Subjects

Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Orphan Drug, Rare Diseases, Humans, Solubility, Permeability, Biopharmaceutics, Chemical and Drug Induced Liver Injury, Brain, Pharmaceutical Preparations, Permeability rate, BDDCS, ECCS, BCS, Food effects, Brain penetration, DILI, Pharmacology & Pharmacy, Pharmacology and pharmaceutical sciences

Abstract

Here I detail the use of measures of permeability rate and solubility in predicting drug disposition characteristics through the utilization of the Biopharmaceutics Drug Disposition Classification System (BDDCS) and the Extended Clearance Classification System (ECCS) as well as the accuracy of the systems in predicting the major route of elimination and the extent of oral absorption of a new small molecule therapeutics. I compare the BDDCS and ECCS with the FDA Biopharmaceutics Classification System (BCS). I also detail the use of the BCS in predicting food effects and the BDDCS in predicting brain disposition of small molecule therapeutics and in validating DILI predictive metrics. This review provides an update of the current status of these classification systems and their uses in the drug development process.

Published

2023

3. Identification and preliminary structure–activity relationship of brain‐penetrant quinoxaline‐based compounds with in vitro anti‐glioblastoma activity.

Author

Ahn, Seohyeon, Kim, Eun Hye, Lee, Chaemi, Nam, Yoon Chae, Lee, Joo‐Youn, Song, Jin Sook, Kim, Seong Hwan, and Jeon, Moon‐Kook

Subjects

*STRUCTURE-activity relationships, *ANAPLASTIC lymphoma kinase, *CENTRAL nervous system, *CELL permeability, *PROTEIN-tyrosine kinases

Abstract

A central nervous system (CNS)‐oriented compound collection was screened to find hit compounds for human glioblastoma T98G cell growth inhibition. A series of quinoxaline‐based derivatives were identified as hit compounds having one‐ to two‐digit micromolar GI50 values. Anti‐glioblastoma activity was improved in structure–activity relationship studies varying the substituents on the quinoxaline ring system, resulting in the discovery of four compounds exhibiting sub‐micromolar GI50 values. The potentials of the four compounds to induce apoptosis were confirmed by annexin V staining assay. The development potential of the four compounds as CNS drug leads was evaluated by in vitro MDR‐MDCK cell permeability and in vivo brain disposition in mice. The mouse pharmacokinetic and kinome profiling studies for compound 10g, which showed high brain‐penetrating ability, revealed that the compound is orally bioavailable and inhibits the kinase activities of anaplastic lymphoma kinase (ALK) and Erb‐B2 receptor tyrosine kinase (ERBB3). [ABSTRACT FROM AUTHOR]

Published

2023

4. Targeting the Brain with Single-Domain Antibodies: Greater Potential Than Stated So Far?

Author

Tsitokana, Mireille Elodie, Lafon, Pierre-André, Prézeau, Laurent, Pin, Jean-Philippe, and Rondard, Philippe

Subjects

*MONOCLONAL antibodies, *IMMUNOGLOBULINS, *CENTRAL nervous system diseases, *BLOOD-brain barrier, *BRAIN diseases

Abstract

Treatments for central nervous system diseases with therapeutic antibodies have been increasingly investigated over the last decades, leading to some approved monoclonal antibodies for brain disease therapies. The detection of biomarkers for diagnosis purposes with non-invasive antibody-based imaging approaches has also been explored in brain cancers. However, antibodies generally display a low capability of reaching the brain, as they do not efficiently cross the blood−brain barrier. As an alternative, recent studies have focused on single-domain antibodies (sdAbs) that correspond to the antigen-binding fragment. While some reports indicate that the brain uptake of these small antibodies is still low, the number of studies reporting brain-penetrating sdAbs is increasing. In this review, we provide an overview of methods used to assess or evaluate brain penetration of sdAbs and discuss the pros and cons that could affect the identification of brain-penetrating sdAbs of therapeutic or diagnostic interest. [ABSTRACT FROM AUTHOR]

Published

2023

5. TAS2940, a novel brain‐penetrable pan‐ERBB inhibitor, for tumors with HER2 and EGFR aberrations.

Author

Oguchi, Kei, Araki, Hikari, Tsuji, Shingo, Nakamura, Masayuki, Miura, Akihiro, Funabashi, Kaoru, Osada, Akiko, Tanaka, Sakiho, Suzuki, Takamasa, Kobayashi, Susumu S., and Mizuarai, Shinji

Abstract

Genetic alterations in human epidermal growth factor receptor type 2 (HER2)/epidermal growth factor receptor (EGFR) are commonly associated with breast and lung cancers and glioblastomas. Cancers with avian erythroblastosis oncogene B (ERBB) deregulation are highly metastatic and can cause primary brain tumors. Currently, no pan‐ERBB inhibitor with remarkable brain penetration is available. Here, TAS2940, a novel irreversible pan‐ERBB inhibitor with improved brain penetrability, was evaluated for its efficacy against several ERBB aberrant cancer models. The selectivity of TAS2940 was evaluated by enzymatic kinase assays. The inhibitory effects of TAS2940 against ERBB genetic alterations were examined using MCF10A cells expressing various HER2 or EGFR mutations and other generic cell lines harboring deregulated ERBB expression. In vivo efficacy of TAS2940 was examined following oral treatment in subcutaneous or intracranial xenograft cancer models. TAS2940 was highly potent against cells harboring HER2/EGFR alterations. TAS2940 could selectively inhibit phosphorylation of targets and the growth of cancer cells with ERBB aberrations in vitro. TAS2940 also inhibited tumor growth in xenograft mouse models with ERBB aberrations: HER2 amplification, HER2/EGFR exon 20 insertions, and EGFR vIII mutation. TAS2940 was effective in the intracranial xenograft models of HER2/EGFR cancers and improved the survival of these mice. TAS2940 has promising therapeutic effects in preclinical study against cancers harboring HER2/EGFR mutations, especially metastatic and primary brain tumors. Our results highlight potential novel strategies against lung cancers with brain metastases harboring HER2/EGFR exon 20 insertions and glioblastomas with EGFR aberrations. [ABSTRACT FROM AUTHOR]

Published

2023

6. TRUST-II: a global phase II study of taletrectinib in ROS1-positive non-small-cell lung cancer and other solid tumors.

Author

Nagasaka, Misako, Ohe, Yuichiro, Zhou, Caicun, Choi, Chang-min, Yang, Nong, Liu, Geoffrey, Felip, Enriqueta, Pérol, Maurice, Besse, Benjamin, Nieva, Jorge, Raez, Luis, Pennell, Nathan A, Dimou, Anastasios, Marinis, Filippo de, Ciardiello, Fortunato, Seto, Takashi, Hu, Zheyi, Pan, Max, Wang, Weiqing, and Li, Shuanglian

Abstract

Crizotinib and entrectinib have been approved to treat ROS1 fusion-positive (ROS1+) non-small-cell lung cancer. However, unmet needs remain, including treatment of patients with resistance mutations, efficacy in brain metastasis and avoidance of neurological side effects. Taletrectinib was designed to: improve efficacy; overcome resistance to first-generation ROS1 inhibitors; and address brain metastasis while conferring fewer neurological adverse events. All of these features are demonstrated and supported by the interim data from the regional phase II TRUST-I clinical study. Here we describe the rationale and design of TRUST-II, a global phase II study of taletrectinib in patients with locally advanced/metastatic ROS1+ non-small-cell lung cancer and other ROS1+ solid tumors. The primary end point is confirmed objective response rate. Secondary end points include duration of response, progression-free survival, overall survival and safety. This trial is enrolling patients in North America, Europe and Asia. The targeted therapies crizotinib and entrectinib are the first options available to treat a type of lung cancer called ROS1 fusion-positive non-small-cell lung cancer (ROS1+ NSCLC). However, not all patients with ROS1+ NSCLC respond to these drugs. In addition, most patients who take these drugs find their cancer eventually develops resistance and begins to grow again. Patients with disease that has spread (metastasized) to the brain have worse outcomes. Taletrectinib is a new type of targeted therapy that is being developed to treat people who have metastatic ROS1+ NSCLC. Data from a regional phase II clinical trial showed that taletrectinib is well tolerated, effective for patients who have never taken a ROS1 targeted therapy and inhibits ROS1+ NSCLC for patients whose cancer has developed some types of resistance to these drugs. It has also been shown to treat ROS1+ NSCLC tumors that have spread to the brain. This article discusses the rationale and design of a new trial called TRUST-II, which is a global phase II clinical trial looking at how well taletrectinib works and how safe it is. TRUST-II is actively enrolling patients in North America, Europe and Asia. Clinical Trial Registration:NCT04919811 (ClinicalTrials.gov) [ABSTRACT FROM AUTHOR]

Published

2023

7. Unraveling the drug distribution in brain enabled by MALDI MS imaging with laser-assisted chemical transfer

Author

Shuai Guo, Kening Li, Yanwen Chen, and Bin Li

Subjects

Pharmaceutical analysis, Laser-assisted chemical transfer, Mass spectrometry imaging, Drug distribution, Brain penetration, Therapeutics. Pharmacology, RM1-950

Abstract

Accurate localization of central nervous system (CNS) drug distribution in the brain is quite challenging to matrix-assisted laser desorption/ionization (MALDI) mass spectrometry imaging (MSI), owing to the ionization competition/suppression of highly abundant endogenous biomolecules and MALDI matrix. Herein, we developed a highly efficient sample preparation technique, laser-assisted chemical transfer (LACT), to enhance the detection sensitivity of CNS drugs in brain tissues. A focused diode laser source transilluminated the tissue slide coated with α-cyano-4-hydroxycinnamic acid, an optimal matrix to highly absorb the laser radiation at 405 nm, and a very thin-layer chemical film mainly containing drug molecule was transferred to the acceptor glass slide. Subsequently, MALDI MSI was performed on the chemical film without additional sample treatment. One major advantage of LACT is to minimize ionization competition/suppression from the tissue itself by removing abundant endogenous lipid and protein components. The superior performance of LACT led to the successful visualization of regional distribution patterns of 16 CNS drugs in the mouse brain. Furthermore, the dynamic spatial changes of risperidone and its metabolite were visualized over a 24-h period. Also, the brain-to-plasma (B/P) ratio could be obtained according to MALDI MSI results, providing an alternative means to assess brain penetration in drug discovery.

Published

2022

8. D-DOPA Is a Potent, Orally Bioavailable, Allosteric Inhibitor of Glutamate Carboxypeptidase II.

Author

Gori, Sadakatali S., Thomas, Ajit G., Pal, Arindom, Wiseman, Robyn, Ferraris, Dana V., Gao, Run-duo, Wu, Ying, Alt, Jesse, Tsukamoto, Takashi, Slusher, Barbara S., and Rais, Rana

Subjects

*GLUTAMIC acid, *CAFFEIC acid, *SODIUM benzoate, *DOPA, *NEUROLOGICAL disorders, *CATECHOL-O-methyltransferase, *PHARMACOKINETICS

Abstract

Glutamate carboxypeptidase-II (GCPII) is a zinc-dependent metalloenzyme implicated in numerous neurological disorders. The pharmacophoric requirements of active-site GCPII inhibitors makes them highly charged, manifesting poor pharmacokinetic (PK) properties. Herein, we describe the discovery and characterization of catechol-based inhibitors including L-DOPA, D-DOPA, and caffeic acid, with sub-micromolar potencies. Of these, D-DOPA emerged as the most promising compound, with good metabolic stability, and excellent PK properties. Orally administered D-DOPA yielded high plasma exposures (AUCplasma = 72.7 nmol·h/mL) and an absolute oral bioavailability of 47.7%. Unfortunately, D-DOPA brain exposures were low with AUCbrain = 2.42 nmol/g and AUCbrain/plasma ratio of 0.03. Given reports of isomeric inversion of D-DOPA to L-DOPA via D-amino acid oxidase (DAAO), we evaluated D-DOPA PK in combination with the DAAO inhibitor sodium benzoate and observed a >200% enhancement in both plasma and brain exposures (AUCplasma = 185 nmol·h/mL; AUCbrain = 5.48 nmol·h/g). Further, we demonstrated GCPII target engagement; orally administered D-DOPA with or without sodium benzoate caused significant inhibition of GCPII activity. Lastly, mode of inhibition studies revealed D-DOPA to be a noncompetitive, allosteric inhibitor of GCPII. To our knowledge, this is the first report of D-DOPA as a distinct scaffold for GCPII inhibition, laying the groundwork for future optimization to obtain clinically viable candidates. [ABSTRACT FROM AUTHOR]

Published

2022

9. Unraveling the drug distribution in brain enabled by MALDI MS imaging with laser-assisted chemical transfer.

Author

Guo, Shuai, Li, Kening, Chen, Yanwen, and Li, Bin

Subjects

LASER beams, SEMICONDUCTOR lasers, CENTRAL nervous system, MASS spectrometry, DRUG coatings

Abstract

Accurate localization of central nervous system (CNS) drug distribution in the brain is quite challenging to matrix-assisted laser desorption/ionization (MALDI) mass spectrometry imaging (MSI), owing to the ionization competition/suppression of highly abundant endogenous biomolecules and MALDI matrix. Herein, we developed a highly efficient sample preparation technique, laser-assisted chemical transfer (LACT), to enhance the detection sensitivity of CNS drugs in brain tissues. A focused diode laser source transilluminated the tissue slide coated with α -cyano-4-hydroxycinnamic acid, an optimal matrix to highly absorb the laser radiation at 405 nm, and a very thin-layer chemical film mainly containing drug molecule was transferred to the acceptor glass slide. Subsequently, MALDI MSI was performed on the chemical film without additional sample treatment. One major advantage of LACT is to minimize ionization competition/suppression from the tissue itself by removing abundant endogenous lipid and protein components. The superior performance of LACT led to the successful visualization of regional distribution patterns of 16 CNS drugs in the mouse brain. Furthermore, the dynamic spatial changes of risperidone and its metabolite were visualized over a 24-h period. Also, the brain-to-plasma (B/P) ratio could be obtained according to MALDI MSI results, providing an alternative means to assess brain penetration in drug discovery. A laser-assisted chemical transfer (LACT) technique has been developed for MALDI MS imaging of CNS drug distribution in brain tissue. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2022

10. Drug Transporters ABCB1 (P-gp) and OATP, but not Drug-Metabolizing Enzyme CYP3A4, Affect the Pharmacokinetics of the Psychoactive Alkaloid Ibogaine and its Metabolites.

Author

F. Martins, Margarida L., Heydari, Paniz, Li, Wenlong, Martínez-Chávez, Alejandra, Venekamp, Nikkie, Lebre, Maria C., Lucas, Luc, Beijnen, Jos H., and Schinkel, Alfred H.

Subjects

CYTOCHROME P-450 CYP3A, METABOLITES, P-glycoprotein, PHARMACOKINETICS, ALKALOIDS

Abstract

The psychedelic alkaloid ibogaine is increasingly used as an oral treatment for substance use disorders, despite being unlicensed in most countries and having reported adverse events. Using wild-type and genetically modified mice, we investigated the impact of mouse (m)Abcb1a/1b and Abcg2 drug efflux transporters, human and mouse OATP drug uptake transporters, and the CYP3A drug-metabolizing complex on the pharmacokinetics of ibogaine and its main metabolites. Following oral ibogaine administration (10 mg/kg) to mice, we observed a rapid and extensive conversion of ibogaine to noribogaine (active metabolite) and noribogaine glucuronide. Mouse Abcb1a/1b, in combination with mAbcg2, modestly restricted the systemic exposure (plasma AUC) and peak plasma concentration (Cmax) of ibogaine. Accordingly, we found a ∼2-fold decrease in the relative recovery of ibogaine in the small intestine with fecal content in the absence of both transporters compared to the wild-type situation. Ibogaine presented good intrinsic brain penetration even in wild-type mice (brain-to-plasma ratio of 3.4). However, this was further increased by 1.5-fold in Abcb1a/1b;Abcg2 −/− mice, but not in Abcg2 −/− mice, revealing a stronger effect of mAbcb1a/1b in restricting ibogaine brain penetration. The studied human OATP transporters showed no major impact on ibogaine plasma and tissue disposition, but the mOatp1a/1b proteins modestly affected the plasma exposure of ibogaine metabolites and the tissue disposition of noribogaine glucuronide. No considerable role of mouse Cyp3a knockout or transgenic human CYP3A4 overexpression was observed in the pharmacokinetics of ibogaine and its metabolites. In summary, ABCB1, in combination with ABCG2, limits the oral availability of ibogaine, possibly by mediating its hepatobiliary and/or direct intestinal excretion. Moreover, ABCB1 restricts ibogaine brain penetration. Variation in ABCB1/ABCG2 activity due to genetic variation and/or pharmacologic inhibition might therefore affect ibogaine exposure in patients, but only to a limited extent. The insignificant impact of human CYP3A4 and OATP1B1/1B3 transporters may be clinically advantageous for ibogaine and noribogaine use, as it decreases the risks of undesirable drug interactions or interindividual variation related to CYP3A4 and/or OATP activity. [ABSTRACT FROM AUTHOR]

Published

2022

11. Pamiparib is a potent and selective PARP inhibitor with unique potential for the treatment of brain tumor

Author

Yao Xiong, Yin Guo, Ye Liu, Hexiang Wang, Wenfeng Gong, Yong Liu, Xing Wang, Yajuan Gao, Fenglong Yu, Dan Su, Fan Wang, Yutong Zhu, Yuan Zhao, Yiyuan Wu, Zhen Qin, Xuebing Sun, Bo Ren, Bin Jiang, Wei Jin, Zhirong Shen, Zhiyu Tang, Xiaomin Song, Lai Wang, Xuesong Liu, Changyou Zhou, and Beibei Jiang

Subjects

Pamiparib, PARP, TMZ, Brain penetration, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Pamiparib, an investigational Poly (ADP-ribose) polymerase (PARP) inhibitor in clinical development, demonstrates excellent selectivity for both PARP1 and PARP2, and superb anti-proliferation activities in tumor cell lines with BRCA1/2 mutations or HR pathway deficiency (HRD). Pamiparib has good bioavailability and is 16-fold more potent than olaparib in an efficacy study using BRCA1 mutated MDA-MB-436 breast cancer xenograft model. Pamiparib also shows strong anti-tumor synergy with temozolomide (TMZ), a DNA alkylating agent used to treat brain tumors. Compared to other PARP inhibitors, pamiparib demonstrated improved penetration across the blood brain barrier (BBB) in mice. Oral administration of pamiparib at a dose as low as 3 mg/kg is sufficient to abrogate PARylation in brain tumor tissues. In SCLC-derived, TMZ-resistant H209 intracranial xenograft model, combination of pamiparib with TMZ overcomes its resistance and shows significant tumor inhibitory effects and prolonged life span. Our data suggests that combination of pamiparib with TMZ has unique potential for treatment of brain tumors. Currently, the combination therapy of pamiparib with TMZ is evaluated in clinical trial [NCT03150862].

Published

2020

12. Lasmiditan mechanism of action – review of a selective 5-HT1F agonist

Author

David B. Clemow, Kirk W. Johnson, Helen M. Hochstetler, Michael H. Ossipov, Ann M. Hake, and Andrew M. Blumenfeld

Subjects

Migraine, Lasmiditan, Lipophilicity, Brain penetration, 5-HT1F, CGRP, Medicine

Abstract

Abstract Migraine is a leading cause of disability worldwide, but it is still underdiagnosed and undertreated. Research on the pathophysiology of this neurological disease led to the discovery that calcitonin gene-related peptide (CGRP) is a key neuropeptide involved in pain signaling during a migraine attack. CGRP-mediated neuronal sensitization and glutamate-based second- and third-order neuronal signaling may be an important component involved in migraine pain. The activation of several serotonergic receptor subtypes can block the release of CGRP, other neuropeptides, and neurotransmitters, and can relieve the symptoms of migraine. Triptans were the first therapeutics developed for the treatment of migraine, working through serotonin 5-HT1B/1D receptors. The discovery that the serotonin 1F (5-HT1F) receptor was expressed in the human trigeminal ganglion suggested that this receptor subtype may have a role in the treatment of migraine. The 5-HT1F receptor is found on terminals and cell bodies of trigeminal ganglion neurons and can modulate the release of CGRP from these nerves. Unlike 5-HT1B receptors, the activation of 5-HT1F receptors does not cause vasoconstriction. The potency of different serotonergic agonists towards 5-HT1F was correlated in an animal model of migraine (dural plasma protein extravasation model) leading to the development of lasmiditan. Lasmiditan is a newly approved acute treatment for migraine in the United States and is a lipophilic, highly selective 5-HT1F agonist that can cross the blood-brain barrier and act at peripheral nervous system (PNS) and central nervous system (CNS) sites. Lasmiditan activation of CNS-located 5-HT1F receptors (e.g., in the trigeminal nucleus caudalis) could potentially block the release of CGRP and the neurotransmitter glutamate, thus preventing and possibly reversing the development of central sensitization. Activation of 5-HT1F receptors in the thalamus can block secondary central sensitization of this region, which is associated with progression of migraine and extracephalic cutaneous allodynia. The 5-HT1F receptors are also elements of descending pain modulation, presenting another site where lasmiditan may alleviate migraine. There is emerging evidence that mitochondrial dysfunction might be implicated in the pathophysiology of migraine, and that 5-HT1F receptors can promote mitochondrial biogenesis. While the exact mechanism is unknown, evidence suggests that lasmiditan can alleviate migraine through 5-HT1F agonist activity that leads to inhibition of neuropeptide and neurotransmitter release and inhibition of PNS trigeminovascular and CNS pain signaling pathways.

Published

2020

13. Panobinostat penetrates the blood–brain barrier and achieves effective brain concentrations in a murine model.

Author

Homan, Morgan J., Franson, Andrea, Ravi, Karthik, Roberts, Holly, Pai, Manjunath P., Liu, Cai, He, Miao, Matvekas, Aleksas, Koschmann, Carl, and Marini, Bernard L.

Subjects

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

Abstract

Purpose: Panobinostat, an orally bioavailable pan-HDAC inhibitor, has demonstrated potent activity in multiple malignancies, including pediatric brain tumors such as DIPG, with increased activity against H3K27M mutant cell lines. Given limited evidence regarding the CNS penetration of panobinostat, we sought to characterize its BBB penetration in a murine model. Methods: Panobinostat 15 mg/kg was administered IV to 12 CD-1 female mice. At specified time points, mice were euthanized, blood samples were collected, and brains were removed. LC–MS was performed to quantify panobinostat concentrations. Cmax and AUC were estimated and correlated with previously published pharmacokinetic analyses and reports of IC-50 values in DIPG cell lines. Results: Mean panobinostat plasma concentrations (ng/mL) were 27.3 ± 2.5 at 1 h, 7.56 ± 1.8 at 2 h, 1.48 ± 0.56 at 4 h, and 2.33 ± 1.18 at 7 h. Mean panobinostat brain concentrations (ng/g) were 60.5 ± 6.1 at 1 h, 42.9 ± 5.4 at 2 h, 33.2 ± 6.1 at 4 h, and 28.1 ± 4.3 at 7 h. Brain-to-plasma ratio at 1 h was 2.22 and the brain to plasma AUC ratio was 2.63. Based on the published human pharmacokinetic data, the anticipated Cmax in humans is expected to be significantly higher than the IC-50 identified in DIPG models. Conclusion: It is expected that panobinostat would be effective in CNS tumors where the IC-50 is in the low nanomolar range. Thus, our data demonstrate panobinostat crosses the BBB and achieves concentrations above the IC-50 for DIPG and other brain tumors and should be explored further for clinical efficacy. [ABSTRACT FROM AUTHOR]

Published

2021

14. An improved, scalable synthesis of Notum inhibitor LP-922056 using 1-chloro-1,2-benziodoxol-3-one as a superior electrophilic chlorinating agent

Author

Nicky J. Willis, Elliott D. Bayle, George Papageorgiou, David Steadman, Benjamin N. Atkinson, William Mahy, and Paul V. Fish

Subjects

brain penetration, 1-chloro-1,2-benziodoxol-3-one, electrophilic chlorination, lp-922056, notum inhibitor, Science, Organic chemistry, QD241-441

Abstract

Background: The carboxylesterase Notum has been shown to act as a key negative regulator of the Wnt signalling pathway by mediating the depalmitoleoylation of Wnt proteins. LP-922056 (1) is an orally active inhibitor of Notum. We are investigating the role of Notum in modulating Wnt signalling in the central nervous system and wished to establish if 1 would serve as a peripherally restricted control. An accessible and improved synthetic route would allow 1 to become more readily available as a chemical tool to explore the fundamental biology of Notum and build target validation to underpin new drug discovery programs.Results: An improved, scalable synthesis of 1 is reported. Key modifications include: (1) the introduction of the C7-cyclopropyl group was most effectively achieved with a Suzuki–Miyaura cross-coupling reaction with MIDA-boronate 11 (5 → 6), and (2) C6 chlorination was performed with 1-chloro-1,2-benziodoxol-3-one (12) (6 → 7) as a mild and selective electrophilic chlorination agent. This 7-step route from 16 has been reliably performed on large scale to produce multigram quantities of 1 in good efficiency and high purity. Pharmacokinetic studies in mouse showed CNS penetration of 1 is very low with a brain/plasma concentration ratio of just 0.01. A small library of amides 17 were prepared from acid 1 to explore if 1 could be modified to deliver a CNS penetrant tool by capping off the acid as an amide. Although significant Notum inhibition activity could be achieved, none of these amides demonstrated the required combination of metabolic stability along with cell permeability without evidence of P-gp mediated efflux.Conclusion: Mouse pharmacokinetic studies demonstrate that 1 is unsuitable for use in models of disease where brain penetration is an essential requirement of the compound but would be an ideal peripherally restricted control. These data will contribute to the understanding of drug levels of 1 to overlay with appropriate in vivo efficacy endpoints, i.e., the PK-PD relationship. The identification of a suitable analogue of 1 (or 17) which combines Notum inhibition with CNS penetration would be a valuable chemical probe for investigating the role of Notum in disease models.

Published

2019

15. D-DOPA Is a Potent, Orally Bioavailable, Allosteric Inhibitor of Glutamate Carboxypeptidase II

Author

Sadakatali S. Gori, Ajit G. Thomas, Arindom Pal, Robyn Wiseman, Dana V. Ferraris, Run-duo Gao, Ying Wu, Jesse Alt, Takashi Tsukamoto, Barbara S. Slusher, and Rana Rais

Subjects

catechol, glutamate carboxypeptidase II, CNS, D-DOPA, pharmacokinetics, brain penetration, Pharmacy and materia medica, RS1-441

Abstract

Glutamate carboxypeptidase-II (GCPII) is a zinc-dependent metalloenzyme implicated in numerous neurological disorders. The pharmacophoric requirements of active-site GCPII inhibitors makes them highly charged, manifesting poor pharmacokinetic (PK) properties. Herein, we describe the discovery and characterization of catechol-based inhibitors including L-DOPA, D-DOPA, and caffeic acid, with sub-micromolar potencies. Of these, D-DOPA emerged as the most promising compound, with good metabolic stability, and excellent PK properties. Orally administered D-DOPA yielded high plasma exposures (AUCplasma = 72.7 nmol·h/mL) and an absolute oral bioavailability of 47.7%. Unfortunately, D-DOPA brain exposures were low with AUCbrain = 2.42 nmol/g and AUCbrain/plasma ratio of 0.03. Given reports of isomeric inversion of D-DOPA to L-DOPA via D-amino acid oxidase (DAAO), we evaluated D-DOPA PK in combination with the DAAO inhibitor sodium benzoate and observed a >200% enhancement in both plasma and brain exposures (AUCplasma = 185 nmol·h/mL; AUCbrain = 5.48 nmol·h/g). Further, we demonstrated GCPII target engagement; orally administered D-DOPA with or without sodium benzoate caused significant inhibition of GCPII activity. Lastly, mode of inhibition studies revealed D-DOPA to be a noncompetitive, allosteric inhibitor of GCPII. To our knowledge, this is the first report of D-DOPA as a distinct scaffold for GCPII inhibition, laying the groundwork for future optimization to obtain clinically viable candidates.

Published

2022

16. Integrated Lead Optimization: Translational Models as We Advance Toward the Clinic

Author

Liederer, Bianca M., Liu, Xingrong, Wong, Simon, Mudra, Daniel R., Crommelin, Daan J. A., Editor-in-chief, Lipper, Robert A., Editor-in-chief, Bhattachar, Shobha N., editor, Morrison, John S., editor, Mudra, Daniel R., editor, and Bender, David M., editor

Published

2017

17. Diosgenin content is a novel criterion to assess memory enhancement effect of yam extracts.

Author

Yang, Ximeng, Nomoto, Kaori, and Tohda, Chihiro

Abstract

Several studies have suggested that some kind of Dioscorea species (yam) or yam-contained herbal medicines have cognitive enhancement effect. However, it has been unknown what is a crucial factor for cognitive enhancement in each Dioscorea species. In this study, we aimed to investigate whether one of the main and brain-penetrating components in yams, diosgenin, can be a novel criterion to assess memory enhancement effect of yam extracts. Although our previous studies showed that administration of diosgenin or diosgenin-rich yam extract enhanced cognitive function in normal mice and healthy humans, we have never evaluated whether the effect depends on diosgenin content or not. Therefore, we compared memory enhancement effects of low diosgenin-contained general yam water extract with diosgenin-rich yam extract on cognitive function in normal mice. We found that unlike diosgenin-rich yam, administration of general yam water extract did not enhance object recognition memory in normal mice. LC–MS/MS analyses revealed that after administration of general yam, diosgenin concentration in the brain did not reach to the effective dose because of the low diosgenin content in the original yam extract. On the other hand, when diosgenin was artificially added into general yam, the extract showed memory enhancement in normal mice and promoted neurite outgrowth in neurons. Our study suggests that diosgenin is actually an active compound in yams for memory enhancement, and diosgenin content can be a criterion for predicting cognitive enhancement effect of yam extracts. [ABSTRACT FROM AUTHOR]

Published

2021

18. Novel centrally active oxime reactivators of acetylcholinesterase inhibited by surrogates of sarin and VX

Author

Janice E. Chambers and Edward C. Meek

Subjects

Neuroprotection, Oxime, Nitrophenyl isopropyl methylphosphonate (NIMP), Brain penetration, Seizure-like behavior cessation, Neuropathology protection, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

A novel oxime platform, the substituted phenoxyalkyl pyridinium oximes (US patent 9,227,937), was invented at Mississippi State University with an objective of discovering a brain-penetrating antidote to highly potent organophosphate anticholinesterases, such as the nerve agents. The goal was reactivation of inhibited brain acetylcholinesterase to attenuate the organophosphate-induced hypercholinergic activity that results in glutamate-mediated excitotoxicity and neuropathology. The currently approved oxime antidote in the US, 2-PAM, cannot do this. Using highly relevant surrogates of sarin and VX that leave acetylcholinesterase phosphylated with the same chemical moiety as their respective nerve agents, in vitro screens and in vivo tests in rats were conducted to identify the most efficacious members of this platform. The most promising novel oximes provided 24-h survival of lethal level surrogate exposure better than 2-PAM in almost all cases, and two of the oximes shortened the time to cessation of seizure-like behavior while 2-PAM did not. The most promising novel oximes attenuated neuropathology as indicated by immunohistochemical stains for both glia and neurons, while 2-PAM did not protect either glia or neurons. These results strongly suggest that these novel oximes can function within the brain to protect it, and therefore show great promise as potential future nerve agent antidotes.

Published

2020

19. Characterization and Validation of Canine P-Glycoprotein-Deficient MDCK II Cell Lines for Efflux Substrate Screening.

Author

Ye, Dong, Harder, Anna, Fang, Zhizhou, Weinheimer, Manuel, Laplanche, Loic, and Mezler, Mario

Subjects

*CELL lines, *PARTITION coefficient (Chemistry), *ZINC-finger proteins, *DRUG abuse, *PERMEABILITY

Abstract

Purpose: We characterized three canine P-gp (cP-gp) deficient MDCKII cell lines. Their relevance for identifying efflux transporter substrates and predicting limitation of brain penetration were evaluated. In addition, we discuss how compound selection can be done in drug discovery by using these cell systems. Method: hMDR1, hBCRP-transfected, and non-transfected MDCKII ZFN cells (all with knock-down of endogenous cP-gp) were used for measuring permeability and efflux ratios for substrates. The compounds were also tested in MDR1_Caco-2 and BCRP_Caco-2, each with a double knock-out of BCRP/MRP2 or MDR1/MRP2 transporters respectively. Efflux results were compared between the MDCK and Caco-2 models. Furthermore, in vitro MDR1_ZFN efflux data were correlated with in vivo unbound drug brain-to-plasma partition coefficient (Kp,uu). Results: MDR1 and BCRP substrates are correctly classified and robust transporter affinities with control substrates are shown. Cell passage mildly influenced mRNA levels of transfected transporters, but the transporter activity was proven stable for several years. The MDCK and Caco-2 models were in high consensus classifying same efflux substrates. Approx. 80% of enlisted substances were correctly predicted with the MDR1_ZFN model for brain penetration. Conclusion: cP-gp deficient MDCKII ZFN models are reliable tools to identify MDR1 and BCRP substrates and useful for predicting efflux liability for brain penetration. [ABSTRACT FROM AUTHOR]

Published

2020

20. Pamiparib is a potent and selective PARP inhibitor with unique potential for the treatment of brain tumor.

Author

Xiong, Yao, Guo, Yin, Liu, Ye, Wang, Hexiang, Gong, Wenfeng, Liu, Yong, Wang, Xing, Gao, Yajuan, Yu, Fenglong, Su, Dan, Wang, Fan, Zhu, Yutong, Zhao, Yuan, Wu, Yiyuan, Qin, Zhen, Sun, Xuebing, Ren, Bo, Jiang, Bin, Jin, Wei, and Shen, Zhirong

Subjects

*BRAIN tumors, *POLY(ADP-ribose) polymerase, *TUMOR treatment, *ALKYLATING agents, *BRCA genes, *POLY ADP ribose, *METHYLGUANINE

Abstract

Pamiparib, an investigational Poly (ADP-ribose) polymerase (PARP) inhibitor in clinical development, demonstrates excellent selectivity for both PARP1 and PARP2, and superb anti-proliferation activities in tumor cell lines with BRCA1/2 mutations or HR pathway deficiency (HRD). Pamiparib has good bioavailability and is 16-fold more potent than olaparib in an efficacy study using BRCA1 mutated MDA-MB-436 breast cancer xenograft model. Pamiparib also shows strong anti-tumor synergy with temozolomide (TMZ), a DNA alkylating agent used to treat brain tumors. Compared to other PARP inhibitors, pamiparib demonstrated improved penetration across the blood brain barrier (BBB) in mice. Oral administration of pamiparib at a dose as low as 3 mg/kg is sufficient to abrogate PARylation in brain tumor tissues. In SCLC-derived, TMZ-resistant H209 intracranial xenograft model, combination of pamiparib with TMZ overcomes its resistance and shows significant tumor inhibitory effects and prolonged life span. Our data suggests that combination of pamiparib with TMZ has unique potential for treatment of brain tumors. Currently, the combination therapy of pamiparib with TMZ is evaluated in clinical trial [NCT03150862]. [ABSTRACT FROM AUTHOR]

Published

2020

21. Organic anion transporting polypeptide 2B1 (OATP2B1), an expanded substrate profile, does it align with OATP2B1's hypothesized function?

Author

Bednarczyk, Dallas and Sanghvi, Menaka V.

Subjects

*ION transport (Biology), *ERLOTINIB, *DRUG approval, *ANGIOTENSIN II, *ANGIOTENSIN receptors, *INTESTINAL absorption

Abstract

An expanded view of the substrate landscape of organic anion transporting polypeptide (OATP) 2B1 was pursued with the goal of understanding if the identification of novel in vitro substrates could shed additional light on the impact of OATP2B1 on intestinal absorption and brain penetration. To examine this hypothesis, a series of experiments measured the cellular accumulation of a diverse array of compounds. Representative angiotensin II receptor blockers (ARBs) and other compounds of interest were subsequently investigated for inhibition, time dependence, and kinetics. The study identified ARBs as a class of OATP2B1 substrates and found balsalazide, olsalzine, and gavestinel to be novel substrates of OATP2B1 too. Some compounds previously reported to be OATP2B1 substrates in the literature, aliskiren, erlotinib, montelukast, fexofenadine, and taurocholate could not be confirmed as substrates. Literature describing in vivo outcomes for OATP2B1 substrates, coproporphyrin III, ARBs, balsalazide, olsalzine, and gavestinel highlight the absence of a substantial impact of OATP2B1 on the oral absorption and/or brain penetration of OATP2B1 substrates. Suggestions of including OATP2B1 assessment as part of the drug approval process are likely premature and further mechanistic work with more robust OATP2B1 substrates, which may include some of those described here, is desirable. [ABSTRACT FROM AUTHOR]

Published

2020

22. Withanolide a penetrates brain via intra-nasal administration and exerts neuroprotection in cerebral ischemia reperfusion injury in mice.

Author

Mukherjee, Sumedha, Kumar, Gaurav, and Patnaik, Ranjana

Subjects

*CEREBRAL ischemia, *BLOOD-brain barrier, *REPERFUSION injury, *CEREBRAL edema, *MYOCARDIAL reperfusion, *PARKINSON'S disease, *ALZHEIMER'S disease

Abstract

1. Withanolide A (WA), a major constituent phytochemical of the Ayurvedic herb Withania somnifera reportedly combats neurodegeneration in Alzheimer's disease and Parkinson's disease. But no study has yet reported the ability of WA in crossing the blood–brain barrier (BBB). The present study analyses the brain penetration ability of WA after intra-nasal administration and assesses its neuroprotective ability in cerebral ischemia-reperfusion injury in adult mice model. 2. Brain penetration of WA after intranasal administration in cortex and cerebellum was assessed using HPLC-UV. Three different doses (1 mg/kg, 5 mg/kg and 10 mg/kg) of the phytochemical were used to study the neuroprotective ability of WA by evaluating the brain damage, changes in cerebral neurotransmitter levels and brain tissue morphology. 3. Intranasal administration of the phytochemical facilitates its penetration in the cortex and cerebellum. Post-treatment with WA significantly reduced cerebral infarction, restored BBB disruption and cerebral oedema. The WA post-treatment also lowered the ischemia-induced elevated neurotransmitter and biochemical levels in brain compartments. The highest dose (10 mg/kg) of WA also markedly reduced the morphological damages, apoptotic and necrotic cell death in brain tissue occurring due to cerebral ischemia pathophysiology. 4. Intra-nasal administration enables brain penetration of WA and allows the phytochemical to exert neuroprotective ability in the global cerebral ischemia model. [ABSTRACT FROM AUTHOR]

Published

2020

23. Lasmiditan mechanism of action – review of a selective 5-HT1F agonist.

Author

Clemow, David B., Johnson, Kirk W., Hochstetler, Helen M., Ossipov, Michael H., Hake, Ann M., and Blumenfeld, Andrew M.

Subjects

*BLOOD-brain barrier, *CALCITONIN, *CENTRAL nervous system, *MIGRAINE, *PERIPHERAL nervous system, *NEUROPEPTIDES, *SEROTONIN agonists, *PAIN threshold, *PHARMACODYNAMICS

Abstract

Migraine is a leading cause of disability worldwide, but it is still underdiagnosed and undertreated. Research on the pathophysiology of this neurological disease led to the discovery that calcitonin gene-related peptide (CGRP) is a key neuropeptide involved in pain signaling during a migraine attack. CGRP-mediated neuronal sensitization and glutamate-based second- and third-order neuronal signaling may be an important component involved in migraine pain. The activation of several serotonergic receptor subtypes can block the release of CGRP, other neuropeptides, and neurotransmitters, and can relieve the symptoms of migraine. Triptans were the first therapeutics developed for the treatment of migraine, working through serotonin 5-HT1B/1D receptors. The discovery that the serotonin 1F (5-HT1F) receptor was expressed in the human trigeminal ganglion suggested that this receptor subtype may have a role in the treatment of migraine. The 5-HT1F receptor is found on terminals and cell bodies of trigeminal ganglion neurons and can modulate the release of CGRP from these nerves. Unlike 5-HT1B receptors, the activation of 5-HT1F receptors does not cause vasoconstriction. The potency of different serotonergic agonists towards 5-HT1F was correlated in an animal model of migraine (dural plasma protein extravasation model) leading to the development of lasmiditan. Lasmiditan is a newly approved acute treatment for migraine in the United States and is a lipophilic, highly selective 5-HT1F agonist that can cross the blood-brain barrier and act at peripheral nervous system (PNS) and central nervous system (CNS) sites. Lasmiditan activation of CNS-located 5-HT1F receptors (e.g., in the trigeminal nucleus caudalis) could potentially block the release of CGRP and the neurotransmitter glutamate, thus preventing and possibly reversing the development of central sensitization. Activation of 5-HT1F receptors in the thalamus can block secondary central sensitization of this region, which is associated with progression of migraine and extracephalic cutaneous allodynia. The 5-HT1F receptors are also elements of descending pain modulation, presenting another site where lasmiditan may alleviate migraine. There is emerging evidence that mitochondrial dysfunction might be implicated in the pathophysiology of migraine, and that 5-HT1F receptors can promote mitochondrial biogenesis. While the exact mechanism is unknown, evidence suggests that lasmiditan can alleviate migraine through 5-HT1F agonist activity that leads to inhibition of neuropeptide and neurotransmitter release and inhibition of PNS trigeminovascular and CNS pain signaling pathways. [ABSTRACT FROM AUTHOR]

Published

2020

24. 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

25. Synthesis, SAR study, and biological evaluation of novel 2,3-dihydro-1H-imidazo[1,2-a]benzimidazole derivatives as phosphodiesterase 10A inhibitors.

Author

Chino, Ayaka, Honda, Shugo, Morita, Masataka, Yonezawa, Koichi, Hamaguchi, Wataru, Amano, Yasushi, Moriguchi, Hiroyuki, Yamazaki, Mayako, Aota, Masaki, Tomishima, Masaki, and Masuda, Naoyuki

Subjects

*BENZIMIDAZOLES, *IMIDAZOPYRIDINES, *BENZIMIDAZOLE derivatives, *PHOSPHODIESTERASE inhibitors, *STRUCTURE-activity relationships, *SHORT-term memory, *P-glycoprotein

Abstract

Phosphodiesterase 10A (PDE10A) inhibitors were designed and synthesized based on the dihydro-imidazobenzimidazole scaffold. Compound 5a showed moderate inhibitory activity and good permeability, but unfavorable high P-glycoprotein (P-gp) liability for brain penetration. We performed an optimization study to improve both the P-gp efflux ratio and PDE10A inhibitory activity. As a result, 6d was identified with improved P-gp liability and high PDE10A inhibitory activity. Compound 6d also showed satisfactory brain penetration, suppressed phencyclidine-induced hyperlocomotion and improved MK-801-induced working memory deficit. [ABSTRACT FROM AUTHOR]

Published

2019

26. Validation of Human MDR1-MDCK and BCRP-MDCK Cell Lines to Improve the Prediction of Brain Penetration.

Author

Feng, Bo, West, Mark, Patel, Nandini C., Wager, Travis, Hou, Xinjun, Johnson, Jillian, Tremaine, Larry, and Liras, Jennifer

Subjects

*CELL lines, *BLOOD-brain barrier, *CARRIER proteins, *MULTIDRUG resistance, *BRAIN, *PROTEIN expression, *BREAST cancer

Abstract

It is of great challenge to predict human brain penetration for substrates of multidrug resistance protein 1 (MDR1) and breast cancer resistance protein (BCRP), 2 major efflux transporters at blood-brain barrier. Thus, a physiologically based pharmacokinetic (PBPK) model with the incorporation of in vitro MDR1 and BCRP transporter function data and transporter protein expression levels has been developed. As such, it is crucial to generate MDR1 and BCRP substrate data with a high fidelity. In this study, 2 widely used human MDR1 cell lines from Borst and National Institutes of Health laboratories were evaluated using rodent brain penetration data, and the study suggested that the MDR1 expressed in Madin-Darby canine kidney (MDCK) cell line from National Institutes of Health laboratory predicted brain penetration better, particularly for compounds with a high passive permeability. In addition, human BCRP-MDCK cell line with 1 μM PSC833, a specific MDR1 inhibitor, demonstrated the ability to identify BCRP substrates without the confounding of endogenous canine Mdr1. Comparison of human BCRP and mouse Bcrp transporter functions revealed that the functional differences of BCRP between the 2 species is minimal. The incorporation of both the validated MDR1 and BCRP assays into our brain PBPK model has significantly improved the prediction for the brain penetration of MDR1 and BCRP substrates across species. [ABSTRACT FROM AUTHOR]

Published

2019

27. Pharmacokinetics and brain penetration study of chlorogenic acid in rats.

Author

Kumar, Gaurav, Paliwal, Pankaj, Mukherjee, Sumedha, Patnaik, Nishant, Krishnamurthy, Sairam, and Patnaik, Ranjana

Subjects

*PHARMACOKINETICS, *CHLOROGENIC acid, *CEREBROSPINAL fluid, *LABORATORY rats, *NEURODEGENERATION

Abstract

1. The present study is designed to investigate the brain distribution and plasma pharmacokinetics profiles of chlorogenic acid (CGA) after intranasal administration in Charles-Foster rats to evaluate whether the CGA molecules are transported directly via the nose-to-brain path. 2. The CGA is administered intravenously (IV) and intranasally (IN) at the dose of 10 mg/kg. Further, its concentration in the plasma, cerebrospinal fluid (CSF) and the whole brain is analyzed by HPLC-UV method. 3. The study observes that CGA is rapidly absorbed in plasma with tmax of 1 min similar to IV route after IN administration. The peak plasma concentration and AUC0-24 are higher by 3.5 and 4.0 times respectively in IV administration, compared to IN delivery that represents the significant less systemic exposure of CGA in IN route. 4. However, the concentration of CGA in the brain is 4, 6.5, 5.3, 5.2 and 4.5 times higher at 30, 60, 120, 240 and 360 min, respectively in IN administration compared to IV administration. The exposure of CGA in the brain after IN administration (AUCbrain, IN) was significantly greater (4 times) as compared to the exposure of CGA in the brain (AUCbrain, IV) after IV administration reflecting significant brain uptake of CGA through nasal route. Therefore, IN delivery of CGA can be a promising approach for the treatment of stroke and neurodegenerative disorders. [ABSTRACT FROM AUTHOR]

Published

2019

28. 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

29. P-glycoprotein (MDR1/ABCB1) and Breast Cancer Resistance Protein (BCRP/ABCG2) limit brain accumulation of the FLT3 inhibitor quizartinib in mice.

Author

Wang, Jing, Gan, Changpei, Retmana, Irene A., Sparidans, Rolf W., Li, Wenlong, Lebre, Maria C., Beijnen, Jos H., and Schinkel, Alfred H.

Subjects

*BREAST cancer, *GLYCOPROTEINS, *EFFLUX (Microbiology), *PHARMACOKINETICS, *BIOAVAILABILITY

Abstract

Graphical abstract Abstract Quizartinib, a second-generation FLT3 inhibitor, is in clinical development for the treatment of acute myeloid leukemia. We studied its pharmacokinetic interactions with the multidrug efflux transporters ABCB1 and ABCG2 and the multidrug metabolizing enzyme CYP3A, using in vitro transport assays and knockout and transgenic mouse models. Quizartinib was transported by human ABCB1 in vitro , and by mouse (m)Abcb1 and mAbcg2 in vivo. Upon oral administration, the brain accumulation of quizartinib was 6-fold decreased by mAbcb1 and 2-fold by mAbcg2 (together: 12-fold). Unexpectedly, the absence of mAbcb1 resulted in a ∼2-fold lower plasma exposure in Abcb1a/1b −/− and Abcb1a/1b;Abcg2 −/− mice, suggesting that loss of mAbcb1 causes compensatory alterations in alternative quizartinib elimination or uptake systems. mAbcb1 and mAbcg2 themselves did not appear to restrict quizartinib oral availability. Oral and intravenous pharmacokinetics of quizartinib were not substantially altered between wild-type, Cyp3a knockout and CYP3A4-humanized mice. All three strains showed relatively high (33–51%) oral bioavailability. If this also applies in humans, this would suggest a limited risk of CYP3A-related inter-individual variation in exposure for this drug. Our results provide a possible rationale for using pharmacological ABCB1/ABCG2 inhibitors together with quizartinib when treating malignant lesions situated in part or in whole behind the blood-brain barrier. [ABSTRACT FROM AUTHOR]

Published

2019

30. Assessing extent of brain penetration in vivo (Kp,uu,brain) in Göttingen minipig using a diverse set of reference drugs.

Author

Langthaler, Kristine, Jones, Christopher R., Brodin, Birger, and Bundgaard, Christoffer

Subjects

*MEDICATION safety, *DRUGS, *P-glycoprotein, *MONKEYS, *BLOOD-brain barrier

Abstract

• Successful determination of minipig K p,uu,brain was achieved by cassette dosing, employing a pseudo steady-state approach. • Brain penetration data are presented for the first time in Göttingen minipig for a large set of reference compounds. • Results support use of Göttingen minipig as a non-rodent drug safety model for CNS drug candidates. • Transporter substrates gave the most pronounced difference in K p,uu,brain comparing across minipig, dog, monkey and human. The application of Göttingen minipigs for non-rodent pharmacokinetics (PK) and drug safety testing has seen a dramatic increase in recent years. The aim of this study was to determine the total and unbound brain-to-plasma ratios (K p,brain and K p,uu,brain) for a diverse set of reference compounds in female Göttingen minipigs and compare these with K p,uu,brain values from other species to assess the suitability of Göttingen minipigs as a model for CNS drug safety testing and brain PK in clinical translation. The reference set consisted of 17 compounds with varying physico-chemical properties and included known human P-glycoprotein (P-gp) substrates. The results of the study showed, that minipig K p,brain and K p,uu,brain values for the tested compounds were in the range 0.03–86 and 0.02–2.4 (n = 3–4) respectively. The K p,uu,brain values were comparable between minipig and rat for a large proportion of the compounds (71% within 2-fold, n = 17). Comparisons of brain penetration across several species for a subset of reference compounds revealed that minipig values were quite similar to those of rat, dog, monkey and human. The study highlighted that the largest K p,uu,brain species differences were observed for compounds classified as transporter substrates (e.g. cimetidine, risperidone, Way-100635 and altanserin). In conclusion these brain penetration data add substantially to the available literature on PK and drug disposition for minipigs and support use of Göttingen minipig as a non-rodent drug safety model for CNS drug candidates and as a brain PK model for clinical translation. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

31. P-glycoprotein (MDR1/ABCB1) and Breast Cancer Resistance Protein (BCRP/ABCG2) affect brain accumulation and intestinal disposition of encorafenib in mice.

Author

Wang, Jing, Gan, Changpei, Sparidans, Rolf W., Wagenaar, Els, Van Hoppe, Stéphanie, Beijnen, Jos H., and Schinkel, Alfred H.

Subjects

*P-glycoprotein, *ATP-binding cassette transporters, *TARGETED drug delivery, *LABORATORY mice, ANTINEOPLASTIC agent development

Abstract

Encorafenib (LGX818) is a promising BRAF V600E inhibitor that has efficacy against metastatic melanoma. To better understand its pharmacokinetics, we studied its interactions with the multidrug efflux transporters ABCB1 and ABCG2 and the multidrug metabolizing enzyme CYP3A. In polarized MDCK-II cells, encorafenib was efficiently transported by canine and human ABCB1 and ABCG2 and by mouse Abcg2. Upon oral administration to wild-type, Abcb1a/1b −/− , Abcg2 −/− , and Abcb1a/1b;Abcg2 −/− mice, encorafenib was absorbed very quickly and to very high plasma levels, but without clear changes in oral availability between the strains. Upon oral or intravenous administration, encorafenib brain accumulation was markedly increased in Abcb1a/1b;Abcg2 −/− mice and to a lesser extent in Abcb1a/1b −/− mice. However, absolute brain concentrations and brain-to-plasma ratios remained very low in all strains, indicating intrinsically poor brain penetration of encorafenib. Upon intravenous administration, Abcb1a/1b;Abcg2 −/− mice showed somewhat reduced plasma elimination of encorafenib compared to wild-type mice, and lower accumulation of the drug in the intestinal tract, suggesting a limited role for these transporters in intestinal elimination of the drug. In Cyp3a −/− mice plasma levels of encorafenib were not markedly increased, suggesting a limited impact of Cyp3a on encorafenib oral availability. The low brain penetration of encorafenib might limit its efficacy against malignancies positioned behind a functional blood-brain barrier, but its oral bioavailability and distribution to other tested organs (liver, kidney, spleen, testis) was high. [ABSTRACT FROM AUTHOR]

Published

2018

32. The pharmacokinetics of targeted anticancer drugs and food toxins: Roles of ABC efflux and OATP uptake transporters

Author

Wang, Jing and Wang, Jing

Abstract

Membrane transporters can play important roles in pharmacokinetic pathways (drug absorption, distribution, metabolism, and excretion). In this thesis we investigated the pharmacological functions of ABC efflux transporters in vitro, by using transwell transport assays and in vivo, by using the single and combination knockout mouse models of ABCB1 and ABCG2. We further used CYP3A knockout and humanized transgenic mouse models to assess the in vivo impact of this multispecific drug-metabolizing complex on the study drugs. We also studied OATP uptake transporters in vivo using several knockout and humanized transgenic mouse strains with liver-specific expression of human OATP1B1 or OATP1B3. Firstly, we have demonstrated the usefulness of single and combination transporter knockout mouse models to study the impact of ABCB1 and ABCG2 on oral availability and brain accumulation of drugs, including several TKIs in vivo. We have shown that dual deficiency of ABCB1 and ABCG2 most effectively increases the brain penetration of the studied tyrosine kinase inhibitors (TKIs). The findings in this thesis suggest that tumors expressing ABCB1 and/or ABCG2 may demonstrate resistance to tivozanib-, quizartinib- and EAI045-based cancer therapy. Inhibiting both these ABC transporters during therapy might therefore be beneficial for the response of these tumors. However, for the BRAFV600E inhibitor encorafenib, it is suggested that it may not be the optimal choice for the treatment of melanoma brain metastases when the blood-brain barrier (BBB) is intact. The oral availability of encorafenib, tivozanib, quizartinib and EAI045, however, does not seem to be noticeably affected by the activity of ABCB1 or ABCG2, at least in mice. On the other hand, the high intrinsic oral availability of encorafenib, if replicated in humans, would present a relatively favorable situation for the clinical application of this anticancer drug. Secondly, characterization of pharmacological functions of human O

Published

2022

33. Correlation of pharmacokinetics and brain penetration data of adult zebrafish with higher mammals including humans.

Author

Kulkarni, Pushkar, Medishetti, Raghavender, Nune, Nagaraju, Yellanki, Swapna, Sripuram, Vijaykumar, Rao, Pallavi, Sriram, Dharmarajan, Saxena, Uday, Oruganti, Srinivas, and Yogeeswari, Perumal

Subjects

*PHARMACOKINETICS, *ZEBRA danio, *IRINOTECAN, *BLOOD-brain barrier, *PHARMACODYNAMICS, *PHYSIOLOGY

Abstract

Introduction Adult zebrafish pharmacology is evolving rapidly for creating efficacy and safety models for drug discovery. However, there is very limited research in understanding pharmacokinetics (PK) in adult zebrafish. Methods for understanding PK will help in conducting pharmacokinetic – pharmacodynamic (PK-PD) correlations and improving the quality and applicability of data obtained using zebrafish. Methods We conducted adult zebrafish PK and brain penetration studies on two known compounds (irinotecan and lorcaserin) with distinct PK and brain penetration properties using validated LCMS/MS method. Irinotecan was studied at a dose of 100 mg/kg i.p. and levels of the parent drug and active metabolite SN-38 were measured. Loracserin was studies at a dose of 10 mg/kg by two routes i.p. and p.o. Results Zebrafish PK and brain penetration profiles for both compounds were very similar to that of higher mammals including humans. Irinotecan was metabolised to SN-38 in ratios similar to ratios seen in other species and the compound had long half life with very low brain penetration in our studies. Loracasin was highly permeable in brain as compared to the exposure in blood, with long half life and high relative bioavailability, similar to other mammalian species including humans. Discussion Adult zebrafish PK studies are relatively an unexplored area of zebrafish research. The zebrafish data for key parameters of irinotecan and loracserin shows a high correlation to the data from higher species, including human. This report explores and discusses the use of adult zebrafish as a predictive PK tool for higher animal studies. [ABSTRACT FROM AUTHOR]

Published

2017

34. Noninvasive nanoparticle strategies for brain tumor targeting.

Author

Sun, Chunmeng, Ding, Yang, Zhou, Li, Shi, Di, Sun, Linlin, Webster, Thomas J., and Shen, Yan

Subjects

NANOMEDICINE, BRAIN tumor treatment, NONINVASIVE diagnostic tests, DRUG administration, BLOOD-brain barrier, TARGETED drug delivery

Abstract

The blood–brain barrier (BBB) maintains the integrity and homeostasis of the central nervous system (CNS) yet represents an intimidating hurdle for efficient drug delivery to brain tumors. This up-to-date review summarizes strategies that have been employed to cross the BBB with a focus on non-invasive nanoparticles that could pass the BBB after systemic administration. Recent advances in liposomes, polymeric nanoparticles, micelles, and inorganic nanoparticles are scrutinized mechanistically with an emphasis on design principles. As highlighted in this review, effective drug delivery to brain tumors may be achieved by rationally engineering nanoparticles to possess appropriate sizes, surface properties, and ligands. [ABSTRACT FROM AUTHOR]

Published

2017

35. Pharmaceutical development of an amorphous solid dispersion formulation of elacridar hydrochloride for proof-of-concept clinical studies.

Author

Sawicki, E., Schellens, J. H. M., Beijnen, J. H., and Nuijen, B.

Subjects

DRUG development, AMORPHOUS substances, DISPERSION (Chemistry), EXCIPIENTS, DRUG solubility

Abstract

Objective:A novel tablet formulation containing an amorphous solid dispersion (ASD) of elacridar hydrochloride was developed with the purpose to resolve the drug’s low solubility in water and to conduct proof-of-concept clinical studies. Significance:Elacridar is highly demanded for proof-of-concept clinical trials that study the drug’s suitability to boost brain penetration and bioavailability of numerous anticancer agents. Previously, clinical trials with elacridar were performed with a tablet containing elacridar hydrochloride. However, this tablet formulation resulted in poor and unpredictable absorption which was caused by the low aqueous solubility of elacridar hydrochloride. Methods:Twenty four different ASDs were produced and dissolution was compared to crystalline elacridar hydrochloride and a crystalline physical mixture. The formulation with highest dissolution was characterized for amorphicity. Subsequently, a tablet was developed and monitored for chemical/physical stability for 12 months at +15–25 °C, +2–8 °C and −20 °C. Results:The ASD powder was composed of freeze dried elacridar hydrochloride–povidone K30–sodium dodecyl sulfate (1:6:1, w/w/w), appeared fully amorphous and resulted in complete dissolution whereas crystalline elacridar hydrochloride resulted in only 1% dissolution. The ASD tablets contained 25 mg elacridar hydrochloride and were stable for at least 12 months at –20 °C. Conclusions:The ASD tablet was considered feasible for proof-of-concept clinical studies and is now used as such. [ABSTRACT FROM AUTHOR]

Published

2017

36. Generation-6 hydroxyl PAMAM dendrimers improve CNS penetration from intravenous administration in a large animal brain injury model.

Author

Zhang, Fan, Trent Magruder, J., Lin, Yi-An, Crawford, Todd C., Grimm, Joshua C., Sciortino, Christopher M., Wilson, Mary Ann, Blue, Mary E., Kannan, Sujatha, Johnston, Michael V., Baumgartner, William A., and Kannan, Rangaramanujam M.

Subjects

*INTRAVENOUS therapy, *POLYAMIDOAMINE dendrimers, *INTRAVENOUS catheterization, *BRAIN injuries, *MICROGLIA

Abstract

Hypothermic circulatory arrest (HCA) provides neuroprotection during cardiac surgery but entails an ischemic period that can lead to excitotoxicity, neuroinflammation, and subsequent neurologic injury. Hydroxyl polyamidoamine (PAMAM) dendrimers target activated microglia and damaged neurons in the injured brain, and deliver therapeutics in small and large animal models. We investigated the effect of dendrimer size on brain uptake and explored the pharmacokinetics in a clinically-relevant canine model of HCA-induced brain injury. Generation 6 (G6, ~ 6.7 nm) dendrimers showed extended blood circulation times and increased accumulation in the injured brain compared to generation 4 dendrimers (G4, ~ 4.3 nm), which were undetectable in the brain by 48 h after final administration. High levels of G6 dendrimers were found in cerebrospinal fluid (CSF) of injured animals with a CSF/serum ratio of ~ 20% at peak, a ratio higher than that of many neurologic pharmacotherapies already in clinical use. Brain penetration (measured by drug CSF/serum level) of G6 dendrimers correlated with the severity of neuroinflammation observed. G6 dendrimers also showed decreased renal clearance rate, slightly increased liver and spleen uptake compared to G4 dendrimers. These results, in a large animal model, may offer insights into the potential clinical translation of dendrimers. [ABSTRACT FROM AUTHOR]

Published

2017

37. Quantitative projection of human brain penetration of the H 3 antagonist PF-03654746 by integrating rat-derived brain partitioning and PET receptor occupancy.

Author

Sawant-Basak, Aarti, Chen, Laigao, Shaffer, Christopher L., Palumbo, Donna, Schmidt, Anne, Tseng, Elaine, Spracklin, Douglas K., Gallezot, Jean-Dominique, Labaree, David, Nabulsi, Nabeel, Huang, Yiyun, Carson, Richard E., and McCarthy, Timothy

Subjects

*POLYETHYLENE terephthalate, *PARALLEL algorithms, *BLOOD-brain barrier, *CYCLOBUTANE, *CARBOXAMIDES

Abstract

1. Unbound brain drug concentration (Cb,u), a valid surrogate of interstitial fluid drug concentration (CISF), cannot be directly determined in humans, which limits accurately defining the humanCb,u:Cp,uof investigational molecules. 2. For the H3R antagonist (1R,3R)-N-ethyl-3-fluoro-3-[3-fluoro-4-(pyrrolidin-1-lmethyl)phenyl]cyclobutane-1-carboxamide (PF-03654746), we interrogatedCb,u:Cp,uin humans and nonhuman primate (NHP). 3. In rat,PF-03654746achieved net blood–brain barrier (BBB) equilibrium (Cb,u:Cp,uof 2.11). 4. In NHP and humans, the PET receptor occupancy-basedCp,uIC50ofPF-03654746was 0.99 nM and 0.31 nM, respectively, which were 2.1- and 7.4-fold lower than itsin vitrohuman H3Ki(2.3 nM). 5. In an attempt to understand this higher-than-expected potency in humans and NHP, rat-derivedCb,u:Cp,uofPF-03654746was integrated withCp,uIC50to identify unbound (neuro) potency ofPF-03654746,nIC50. 6. ThenIC50ofPF-03654746was 2.1 nM in NHP and 0.66 nM in human which better correlated (1.1- and 3.49-fold lower) within vitrohuman H3Ki(2.3 nM). 7. This correlation of thenIC50andin vitro hH3Kisuggested the translation of net BBB equilibrium ofPF-03654746from rat to NHP and humans, and confirmed the use ofCp,uas a reliable surrogate ofCb,u. 8. Thus,nIC50quantitatively informed the humanCb,u:Cp,uofPF-03654746. [ABSTRACT FROM PUBLISHER]

Published

2017

38. Placement of Subthalamic DBS Electrodes in a Radiology Suite Using Interventional MRI

Author

Starr, P. A., Martin, A. J., Talke, P., Ostrem, J., Sootsman, W. K., Levesque, N., Meyers, J., Larson, P. S., van Hilten, Bob, editor, and Nuttin, Bart, editor

Published

2007

39. The pharmacokinetics of targeted anticancer drugs and food toxins: Roles of ABC efflux and OATP uptake transporters

Subjects

ABC efflux transporters, OATP uptake transporters, Cytochrome P450 enzymes, brain penetration, blood-brain-barrier, encorafenib, quizartinib, tivozanib, EAI045, Ochratoxin A

Abstract

Membrane transporters can play important roles in pharmacokinetic pathways (drug absorption, distribution, metabolism, and excretion). In this thesis we investigated the pharmacological functions of ABC efflux transporters in vitro, by using transwell transport assays and in vivo, by using the single and combination knockout mouse models of ABCB1 and ABCG2. We further used CYP3A knockout and humanized transgenic mouse models to assess the in vivo impact of this multispecific drug-metabolizing complex on the study drugs. We also studied OATP uptake transporters in vivo using several knockout and humanized transgenic mouse strains with liver-specific expression of human OATP1B1 or OATP1B3. Firstly, we have demonstrated the usefulness of single and combination transporter knockout mouse models to study the impact of ABCB1 and ABCG2 on oral availability and brain accumulation of drugs, including several TKIs in vivo. We have shown that dual deficiency of ABCB1 and ABCG2 most effectively increases the brain penetration of the studied tyrosine kinase inhibitors (TKIs). The findings in this thesis suggest that tumors expressing ABCB1 and/or ABCG2 may demonstrate resistance to tivozanib-, quizartinib- and EAI045-based cancer therapy. Inhibiting both these ABC transporters during therapy might therefore be beneficial for the response of these tumors. However, for the BRAFV600E inhibitor encorafenib, it is suggested that it may not be the optimal choice for the treatment of melanoma brain metastases when the blood-brain barrier (BBB) is intact. The oral availability of encorafenib, tivozanib, quizartinib and EAI045, however, does not seem to be noticeably affected by the activity of ABCB1 or ABCG2, at least in mice. On the other hand, the high intrinsic oral availability of encorafenib, if replicated in humans, would present a relatively favorable situation for the clinical application of this anticancer drug. Secondly, characterization of pharmacological functions of human OATPs by using mouse models suggest that mouse Oatp1a/1b has at best a very modest uptake function for tivozanib and EAI045 into liver, without affecting overall plasma kinetics. Lastly, we use different mouse models to study the possible effects on oral availability and tissue distribution of Ochratoxin A (OTA), a dietary mycotoxin that can cause nephrotoxicity, hepatotoxicity, and neurotoxicity and may be carcinogenic. We found that in mice OTA is transported by the drug transporters mouse (m)Abcb1 and/or mAbcg2, mOatp1a/1b, and human (h)OATP1B3. The complete deletion of mAbcb1 and mAbcg2 resulted in ~2-fold higher OTA liver and kidney accumulation upon intravenous injection. Upon oral administration, absence of mOatp1a/1b led to a substantial (>3-fold) decrease in hepatic and small intestinal exposure of OTA. Furthermore, in humanized mouse strains, hepatic expression of transgenic hOATP1B3, but not hOATP1B1, partly reversed the reduced liver concentration of OTA in Oatp1a/1b knockout mice. These data indicate that transgenic hOATP1B3 can significantly transport OTA into the liver, and can at least partly compensate for the loss of the mOatp1a/1b transporters. This study shows that some ABC and OATP transporters can substantially affect the pharmacokinetics of OTA, which might have implications for its toxicity behavior.

Published

2022

40. CI-1015 : An Orally Active CCK-B Receptor Antagonist with an Improved Pharmacokinetic Profile

Author

Trivedi, Bharat K., Hinton, Joanna P., Borchardt, Ronald T., editor, Freidinger, Roger M., editor, Sawyer, Tomi K., editor, and Smith, Philip L., editor

Published

1998

41. Brain Penetration of SDZ PSC 833 in Rats : A Comparison with Cyclosporin A

Author

Desrayaud, Sandrine, Lemaire, Michel, Couraud, Pierre-Olivier, editor, and Scherman, Daniel, editor

Published

1996

42. Functional Expression of Multidrug Resistance P-Glycoprotein in Cellular Models of Physiological Barriers

Author

Lechardeur, Delphine, Wils, Pierre, Schwartz, Bertrand, Scherman, Daniel, Couraud, Pierre-Olivier, editor, and Scherman, Daniel, editor

Published

1996

43. Comparative biodistribution and safety profiling of olmesartan medoxomil oil-in-water oral nanoemulsion.

Author

Gorain, Bapi, Choudhury, Hira, Tekade, Rakesh Kumar, Karan, Saumen, Jaisankar, P., and Pal, Tapan Kumar

Subjects

*COMPARATIVE studies, *EMULSIONS, *OIL-water interfaces, *ANGIOTENSIN II, *AQUEOUS solutions, *SOLUBILITY, *ESTERIFICATION, *BIOAVAILABILITY

Abstract

Poor aqueous solubility and unfavourable de-esterification of olmesartan medoxomil (a selective angiotensin II receptor blocker), results in low oral bioavailability of less than 26%. Improvement of oral bioavailability with prolonged pharmacodynamics activity of olmesartan in Wistar rats had been approached by nanoemulsification strategy in our previous article [ Colloid Surface B, 115, 2014: 286 ]. In continuation to that work, we herewith report the biodistribution behaviour and 28-day repeated dose sub-chronic toxicity of olmesartan medoxomil nanoemulsion in Wistar rats following oral administration. The levels of olmesartan in collected biological samples were estimated using our validated LC-MS/MS technique. Our biodistribution study showed significantly higher brain concentrations of olmesartan (0.290 ± 0.089 μg/mL, 0.333 ± 0.071 μg/mL and 0.217 ± 0.062 μg/mL at 0.5, 2.0 and 8.0 h post dosing, respectively) when administered orally as nanoemulsion formulation as compared to the aqueous suspension. In addition, the olmesartan nanoemulsion was found to be safe and non-toxic, as it neither produced any lethality nor remarkable haematological, biochemical and structural adverse effects as observed during the 28-days sub-chronic toxicity studies in experimental Wistar rats. It is herewith envisaged that the developed nanoemulsion formulation approach for the delivery of olmesartan medoxomil via oral route can further be explored in memory dysfunction and brain ischemia, for better brain penetration and improved clinical application in stroke patients. [ABSTRACT FROM AUTHOR]

Published

2016

44. 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

45. 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

46. Physicochemical property profile for brain permeability: comparative study by different approaches.

Author

Raevsky, Oleg A., Grigorev, Veniamin Y., Polianczyk, Daniel E., Sandakov, German I., Solodova, Svetlana L., Yarkov, Alexander V., Bachurin, Sergey O., and Dearden, John C.

Subjects

*BLOOD-brain barrier, *BRAIN chemistry, *PHYSICAL biochemistry, *TARGETED drug delivery, *SYNTHETIC aperture radar, *LOGISTIC regression analysis, *SUPPORT vector machines, *CENTRAL nervous system diseases, *THERAPEUTICS, *PHYSIOLOGY

Abstract

A comparative study of classification models of brain penetration by different approaches was carried out on a training set of 1000 chemicals and drugs, and an external test set of 100 drugs. Ten approaches were applied in this work: seven medicinal chemistry approaches (including “rule of 5” and multiparameter optimization) and also three SAR techniques: logistic regression (LR), random forest (RF) and support vector machine (SVM). Forty-one different medicinal chemistry descriptors representing diverse physicochemical properties were used in this work. Medicinal chemistry approaches based on the intuitive estimation of preference zones of CNS or non-CNS chemicals, with different rules and scoring functions, yield unbalanced models with poor classification accuracy. RF and SVM methods yielded 82% and 84% classification accuracy respectively for the external test set. LR was also successful in CNS/non-CNS (denoted in this study as CNS+/CNS−) classification and yielded an overall accuracy equivalent to that of SVM and RF. At the same time, LR is especially valuable for medicinal chemists because of its simplicity and the possibility of clear mechanistic interpretation. [ABSTRACT FROM PUBLISHER]

Published

2016

47. Pharmacokinetics and brain penetration of carbapenems in mice.

Author

Matsumoto, Kazuaki, Kurihara, Yuji, Kuroda, Yuko, Hori, Seiji, and Kizu, Junko

Subjects

*CARBAPENEMS, *DRUG side effects, *CENTRAL nervous system, *PHARMACOKINETICS, *LABORATORY mice, *THERAPEUTICS

Abstract

An adverse effect associated with the administration of carbapenems is central nervous system (CNS) toxicity, with higher brain concentrations of carbapenems being linked to an increased risk of seizures. However, the pharmacokinetics and brain penetration of carbapenems have not yet been examined. Thus, the aim of this in vivo investigation was to determine the pharmacokinetics and brain penetration of carbapenems in mice. Blood samples and brain tissue samples were obtained 10, 20, 30, 60, and 120 min after the subcutaneous administration of carbapenems (91 mg/kg). We obtained the following values for the pharmacokinetic parameters of carbapenems in mice: 1.20–1.71 L/h/kg for CL total /F, 1.41–2.03 h −1 for K e , 0.34–0.51 h for T 1/2 , 0.66–0.95 L/kg for V ss /F, 0.49–0.73 h for MRT, 83.46–110.58 μg/mL for C max, plasma , and 0.28–0.83 μg/g for C max, brain tissue . The AUC 0−∞ of the carbapenems tested in plasma were in the following order: doripenem > meropenem > biapenem > imipenem, and in brain tissue were: imipenem > doripenem > meropenem > biapenem. The degrees of brain tissue penetration, defined as the AUC 0−∞, brain tissue / f AUC 0−∞, plasma ratio, were 0.016 for imipenem, 0.004 for meropenem, 0.002 for biapenem, and 0.008 for doripenem. The results of the present study demonstrated that, of the carbapenems examined, imipenem penetrated brain tissue to the greatest extent. [ABSTRACT FROM AUTHOR]

Published

2016

48. In vivo real time non invasive monitoring of brain penetration of chemicals with near-infrared spectroscopy: Concomitant PK/PD analysis.

Author

Crespi, Francesco, Cattini, Stefano, Donini, Maurizio, Bandera, Andrea, and Rovati, Luigi

Subjects

*NEAR infrared spectroscopy, *OXYGENATION (Chemistry), *HEMOGLOBINS, *LABORATORY rats, *BRAIN physiology

Abstract

Background Near-infrared spectroscopy (NIRS) is a non-invasive technique that monitors changes in oxygenation of haemoglobin. The absorption spectra of near-infrared light differ for the oxygenation–deoxygenation states of haemoglobin (oxygenate (HbO 2 ) and deoxygenate (Hb), respectively) so that these two states can be directly monitored. Comparison with existing method(s) Different methodologies report different basal values of HbO 2 and Hb absolute concentrations in brain. Here, we attempt to calculate basal HbO 2 levels in rat CNS via evaluation of the influence of exogenous oxygen or exogenous carbon dioxide on the NIRS parameters measured in vivo. New method Furthermore the possibility that changes of haemoglobin oxygenation in rat brain as measured by NIRS might be a useful index of brain penetration of chemical entities has been investigated. Different compounds from different chemical classes were selected on the basis of parallel ex vivo and in vivo pharmacokinetic (PK/PD) studies of brain penetration and overall pharmacokinetic profile. Results It appeared that NIRS might contribute to assess brain penetration of chemical entities, i.e. significant changes in NIRS signals could be related to brain exposure, conversely the lack of significant changes in relevant NIRS parameters could be indicative of low brain exposure. Conclusions This work is proposing a further innovation on NIRS preclinical applications i.e. a “chemical” NIRS [chNIRS] approach for determining penetration of drugs in animal brain. Therefore, chNIRS could became a non invasive methodology for studies on neurobiological processes and psychiatric diseases in preclinical but also a translational strategy from preclinical to clinical investigations. [ABSTRACT FROM AUTHOR]

Published

2016

49. Improved controlled release and brain penetration of the small molecule S14 using PLGA nanoparticles

Author

Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Ministerio de Educación, Cultura y Deporte (España), European Commission, Nozal, Vanesa [0000-0001-5260-5683], Rojas-Prats, Elisa [0000-0002-5747-8764], Maestro, Inés [0000-0002-5026-5803], Gil, Carmen [0000-0002-3882-6081], Pérez, Daniel I. [0000-0003-1774-4471], Martínez, Ana [0000-0002-2707-8110], Nozal, Vanesa, Rojas-Prats, Elisa, Maestro, Inés, Gil, Carmen, Pérez, Daniel I., Martínez Gil, Ana, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Ministerio de Educación, Cultura y Deporte (España), European Commission, Nozal, Vanesa [0000-0001-5260-5683], Rojas-Prats, Elisa [0000-0002-5747-8764], Maestro, Inés [0000-0002-5026-5803], Gil, Carmen [0000-0002-3882-6081], Pérez, Daniel I. [0000-0003-1774-4471], Martínez, Ana [0000-0002-2707-8110], Nozal, Vanesa, Rojas-Prats, Elisa, Maestro, Inés, Gil, Carmen, Pérez, Daniel I., and Martínez Gil, Ana

Abstract

Phosphodiesterase 7 (PDE7) is an enzyme responsible for the degradation of cyclic adenosine monophosphate (cAMP), an important cellular messenger. PDE7’s role in neurotransmission, expression profile in the brain and the druggability of other phosphodiesterases have motivated the search for potent inhibitors to treat neurodegenerative and inflammatory diseases. Different heterocyclic compounds have been described over the years; among them, phenyl-2-thioxo-(1H)-quinazolin-4-one, called S14, has shown very promising results in different in vitro and in vivo studies. Recently, polymeric nanoparticles have been used as new formulations to target specific organs and produce controlled release of certain drugs. In this work, we describe poly(lactic-co-glycolic acid) (PLGA)-based polymeric nanoparticles loaded with S14. Their preparation, optimization, characterization and in vivo drug release profile are here presented as an effort to improve pharmacokinetic properties of this interesting PDE7 inhibitor.

Published

2021

50. Application of an in Vitro Blood–Brain Barrier Model in the Selection of Experimental Drug Candidates for the Treatment of Huntington’s Disease

Author

Mark Rose, Odalys Gonzalez Paz, Giulio Auciello, Annalise Di Marco, Todd Herbst, Ignacio Muñoz-Sanjuán, Domenico Vignone, Edith Monteagudo, Vinod Khetarpal, Matteo Zini, Maria Rosaria Battista, Laura Orsatti, Vincenzo Summa, Celia Dominguez, Leticia M Toledo-Sherman, Ivan Fini, Antonella Cellucci, Di Marco, A., Gonzalez Paz, O., Fini, I., Vignone, D., Cellucci, A., Battista, M. R., Auciello, G., Orsatti, L., Zini, M., Monteagudo, E., Khetarpal, V., Rose, M., Dominguez, C., Herbst, T., Toledo-Sherman, L., Summa, V., and Munoz-Sanjuan, I.

Subjects

Swine, Pharmaceutical Science, 02 engineering and technology, Pharmacology, efflux transporter, 030226 pharmacology & pharmacy, brain penetration, Rats, Sprague-Dawley, 0302 clinical medicine, Drug Discovery, Electric Impedance, Coculture Technique, Cells, Cultured, Cerebral Cortex, Endothelial Cell, Tight junction, Tight Junction, Drug discovery, Chemistry, Huntington's disease, Biological activity, 021001 nanoscience & nanotechnology, Huntington Disease, medicine.anatomical_structure, Blood-Brain Barrier, Molecular Medicine, Central Nervous System Agent, CNS, Astrocyte, 0210 nano-technology, ATP-Binding Cassette Transporter, Central nervous system, Blood–brain barrier, Models, Biological, Permeability, Tight Junctions, Capillary Permeability, 03 medical and health sciences, In vivo, Huntingtin Protein, medicine, Animals, Solute Carrier Protein, Solute Carrier Proteins, Animal, Endothelial Cells, medicine.disease, Coculture Techniques, Rats, Astrocytes, transport, Rat, ATP-Binding Cassette Transporters, Central Nervous System Agents

Abstract

Huntington's disease (HD) is a neurodegenerative disease caused by polyglutamine expansion in the huntingtin protein. For drug candidates targeting HD, the ability to cross the blood-brain barrier (BBB) and reach the site of action in the central nervous system (CNS) is crucial for achieving pharmacological activity. To assess the permeability of selected compounds across the BBB, we utilized a two-dimensional model composed of primary porcine brain endothelial cells and rat astrocytes. Our objective was to use this in vitro model to rank and prioritize compounds for in vivo pharmacokinetic and brain penetration studies. The model was first characterized using a set of validation markers chosen based on their functional importance at the BBB. It was shown to fulfill the major BBB characteristics, including functional tight junctions, high transendothelial electrical resistance, expression, and activity of influx and efflux transporters. The in vitro permeability of 54 structurally diverse known compounds was determined and shown to have a good correlation with the in situ brain perfusion data in rodents. We used this model to investigate the BBB permeability of a series of new HD compounds from different chemical classes, and we found a good correlation with in vivo brain permeation, demonstrating the usefulness of the in vitro model for optimizing CNS drug properties and for guiding the selection of lead compounds in a drug discovery setting. ©

Published

2019