Your search keyword '"Morris, Patrick J."' showing total 17 results

1. Comparative Assessment and High-Throughput Drug-Combination Profiling of TEAD-Palmitoylation Inhibitors in Hippo Pathway Deficient Mesothelioma.

Author

Evsen, Lale, Morris, Patrick J., Thomas, Craig J., and Ceribelli, Michele

Subjects

*HIPPO signaling pathway, *MESOTHELIOMA, *YAP signaling proteins, *HIGH throughput screening (Drug development), *TRANSCRIPTION factors

Abstract

The hippo signaling pathway is a central tumor suppressor cascade frequently inactivated in selected human cancers, leading to the aberrant activation of TEAD transcription factors. Whereas several TEAD auto-palmitoylation inhibitors are currently in development, a comprehensive assessment of this novel drug-modality is missing. Here, we report a comparative analysis among six TEADi(s) using cell-based and biochemical assays in Hippo pathway deficient mesothelioma. Our analysis revealed varying potency and selectivity across TEADi, also highlighting their limited efficacy. To overcome this limitation, we performed an unbiased, quantitative high-throughput drug screening by combining the TEADi VT-103 with a library of approximately 3000 oncology-focused drugs. By exploiting this library's mechanistic redundancy, we identified several drug-classes robustly synergized with TEADi. These included glucocorticoid-receptor (GR) agonists, Mek1/2 inhibitors, mTOR inhibitors, and PI3K inhibitors, among others. Altogether, we report a coherent single-agent dataset informing on potency and selectivity of TEAD-palmitoylation inhibitors as single-agents. We also describe a rational pipeline enabling the systematic identification of TEAD druggable co-dependencies. This data should support the pre-clinical development of drug combination strategies for the treatment of Hippo-deficient mesothelioma, and more broadly, for other cancers dependent on the oncogenic activity of YAP/TEAD. [ABSTRACT FROM AUTHOR]

Published

2023

2. Mouse, rat, and dog bioavailability and mouse oral antidepressant efficacy of ( )-hydroxynorketamine.

Author

Highland, Jaclyn N., Morris, Patrick J., Zanos, Panos, Lovett, Jacqueline, Ghosh, Soumita, Wang, Amy Q., Zarate, Carlos A., Thomas, Craig J., Moaddel, Ruin, Gould, Todd D., and Zarate, Carlos A Jr

Subjects

*ANTIDEPRESSANTS, *KETAMINE, *MENTAL depression, *PHARMACOKINETICS, *ORAL medication

Abstract

Background: (R,S)-ketamine has gained attention for its rapid-acting antidepressant actions in patients with treatment-resistant depression. However, widespread use of ketamine is limited by its side effects, abuse potential, and poor oral bioavailability. The ketamine metabolite, (2R,6R)-hydroxynorketamine, exerts rapid antidepressant effects, without ketamine's adverse effects and abuse potential, in rodents.Methods: We evaluated the oral bioavailability of (2R,6R)-hydroxynorketamine in three species (mice, rats, and dogs) and also evaluated five candidate prodrug modifications for their capacity to enhance the oral bioavailability of (2R,6R)-hydroxynorketamine in mice. Oral administration of (2R,6R)-hydroxynorketamine was assessed for adverse behavioral effects and for antidepressant efficacy in the mouse forced-swim and learned helplessness tests.Results: (2R,6R)-hydroxynorketamine had absolute bioavailability between 46-52% in mice, 42% in rats, and 58% in dogs. Compared to intraperitoneal injection in mice, the relative oral bioavailability of (2R,6R)-hydroxynorketamine was 62%, which was not improved by any of the candidate prodrugs tested. Following oral administration, (2R,6R)-hydroxynorketamine readily penetrated the brain, with brain to plasma ratios between 0.67-1.2 in mice and rats. Oral administration of (2R,6R)-hydroxynorketamine to mice did not alter locomotor activity or precipitate behaviors associated with discomfort, sickness, or stereotypy up to a dose of 450 mg/kg. Oral (2R,6R)-hydroxynorketamine reduced forced-swim test immobility time (15-150 mg/kg) and reversed learned helplessness (50-150 mg/kg) in mice.Conclusions: These results demonstrate that (2R,6R)-hydroxynorketamine has favorable oral bioavailability in three species and exhibits antidepressant efficacy following oral administration in mice. [ABSTRACT FROM AUTHOR]

Published

2019

3. Synthesis and N-Methyl-D-aspartate (NMDA) Receptor Activity of Ketamine Metabolites.

Author

Morris, Patrick J., Moaddel, Ruin, Zanos, Panos, Moore, Curtis E., Gould, Todd, Zarate Jr., Carlos A., and Thomas, Craig J.

Subjects

*ASPARTIC acid, *ANESTHESIA adjuvants, *AMINES, *AMINATION, *ORGANIC compounds, *KETAMINE

Abstract

Ketamine is rapidly metabolized in the human body to a variety of metabolites, including the hydroxynorketamines. At least two hydroxynorketamines have significant antidepressant action in rodent models, with limited action against the N-methyl-D-aspartate (NMDA) receptor. The synthesis of 12 hydroxynorketamines and their binding affinity to the NMDA receptor is presented here. [ABSTRACT FROM AUTHOR]

Published

2017

4. Palladium-Catalyzed Diastereo- and Enantioselective Formal [3 + 2]-Cycloadditions of Substituted Vinylcyclopropanes.

Author

Trost, Barry M., Morris, Patrick J., and Sprague, Simon J.

Subjects

*PALLADIUM catalysts, *ENANTIOSELECTIVE catalysis, *RING formation (Chemistry), *VINYLCYCLOPROPANES, *ALKENES, *ALKYLIDENES, *ELECTRIC properties, *LIGANDS (Chemistry)

Abstract

We describe a palladium-catalyzed diastereo- and enantioselective formal [3 + 2]-cycloaddition between substituted vinylcyclopropanes and electron-deficient olefins in the form of azlactone- and Meldrum's acid alkylidenes to give highly substituted cyclopentane products. By modulation of the electronic properties of the vinylcyclopropane and the electron-deficient olefin, high levels of stereoselectivity were obtained. The remote stereoinduction afforded by the catalyst, distal from the chiral pocket generated by the ligand, is proposed to be the result of a new mechanism invoking the Curtin-Hammett principle. [ABSTRACT FROM AUTHOR]

Published

2012

5. A comparison of the pharmacokinetics and NMDAR antagonism-associated neurotoxicity of ketamine, (2R,6R)-hydroxynorketamine and MK-801.

Author

Morris, Patrick J., Burke, Richard D., Sharma, Alok K., Lynch, Daniel C., Lemke-Boutcher, Leslie E., Mathew, Shiny, Elayan, Ikram, Rao, Deepa B., Gould, Todd D., Zarate, Carlos A., Zanos, Panos, Moaddel, Ruin, and Thomas, Craig J.

Subjects

*KETAMINE, *LABORATORY rats, *PHARMACOKINETICS, *RATS, *EXPOSURE dose, *NEUROTOXICOLOGY, *METHYL aspartate receptors

Abstract

With the increasing use of ketamine as an off-label treatment for depression and the recent FDA approval of (S)-ketamine for treatment-resistant depression, there is an increased need to understand the long-term safety profile of chronic ketamine administration. Of particular concern is the neurotoxicity previously observed in rat models following acute exposure to high doses of ketamine, broadly referred to as 'Olney's lesions'. This type of toxicity presents as abnormal neuronal cellular vacuolization, followed by neuronal death and has been associated with ketamine's inhibition of the N -methyl- d -aspartate receptor (NMDAR). In this study, a pharmacological and neuropathological analysis of ketamine, the potent NMDAR antagonist MK-801, and the ketamine metabolite (2R,6R)-hydroxynorketamine [(2R,6R)-HNK)] in rats is described following both single dose and repeat dose drug exposures. Ketamine dosing was studied up to 20 mg/kg intravenously for the single-dose neuropathology study and up to 60 mg/kg intraperitoneally for the multiple-dose neuropathology study. MK-801 dosing was studied up to 0.8 mg/kg subcutaneously for both the single and multiple-dose neuropathology studies, while (2R,6R)-HNK dosing was studied up to 160 mg/kg intravenously in both studies. These studies confirm dose-dependent induction of 'Olney's lesions' following both single dose and repeat dosing of MK-801. Ketamine exposure, while showing common behavioral effects, did not induce wide-spread Olney's lesions. Treatment with (2R,6R)-HNK did not produce behavioral effects, toxicity or any evidence of Olney's lesion formation. Based on these results, future NMDAR-antagonist neurotoxicity studies should strongly consider taking pharmacokinetics more thoroughly into account. • MK-801 demonstrates a pronounced sex-based disparity in pharmacokinetics in rats. • MK-801 induces dose-dependent Olney's lesion formation in Han Wistar rats. • Intravenous ketamine does not produce Olney's lesions in Wistar rats up to 20 mg/kg. • (2 R ,6 R)-HNK does not demonstrate any neurotoxicology at doses up to 160 mg/kg. [ABSTRACT FROM AUTHOR]

Published

2021

6. 18F-labeled radiotracers for in vivo imaging of DREADD with positron emission tomography.

Author

Hu, Feng, Morris, Patrick J., Bonaventura, Jordi, Fan, Hong, Mathews, William B., Holt, Daniel P., Lam, Sherry, Boehm, Matthew, Dannals, Robert F., Pomper, Martin G., Michaelides, Michael, and Horti, Andrew G.

Subjects

*RADIOACTIVE tracers, *POSITRON emission tomography, *DESIGNER drugs, *TRANSGENIC mice

Abstract

Designer Receptors Exclusively Activated by Designer Drugs (DREADD) are a preclinical chemogenetic approach with clinical potential for various disorders. In vivo visualization of DREADDs has been achieved with positron emission tomography (PET) using 11C radiotracers. The objective of this study was to develop DREADD radiotracers labeled with 18F for a longer isotope half-life. A series of non-radioactive fluorinated analogs of clozapine with a wide range of in vitro binding affinities for the hM3Dq and hM4Di DREADD receptors has been synthesized for PET. Compound [18F] 7b was radiolabeled via a modified 18F-deoxyfluorination protocol with a commercial ruthenium reagent. [18F] 7b demonstrated encouraging PET imaging properties in a DREADD hM3Dq transgenic mouse model, whereas the radiotracer uptake in the wild type mouse brain was low. [18F] 7b is a promising long-lived alternative to the DREADD radiotracers [11C]clozapine ([11C]CLZ) and [11C]deschloroclozapine ([11C]DCZ). Image 1 • New ligands for Designer Receptors Exclusively Activated by Designer Drugs. • Compounds 7a-7i are suitable candidates for DREADD PET imaging. • [18F] 7b is radiolabeled via a modified 18F-deoxyfluorination protocol. • [18F] 7b specifically labels hM3Dq in PET study in a DREADD transgenic mouse model. [ABSTRACT FROM AUTHOR]

Published

2021

7. Correction to "Synthesis and N-Methyl-d-aspartate (NMDA) Receptor Activity of Ketamine Metabolites".

Author

Morris, Patrick J., Moaddel, Ruin, Zanos, Panos, Moore, Curtis E., Gould, Todd D., Zarate Jr., Carlos A., and Thomas, Craig J.

Subjects

*CHEMICAL synthesis, *METHYL aspartate receptors, *KETAMINE

Published

2017

8. ChemInform Abstract: Palladium-Catalyzed Diastereo- and Enantioselective Formal [3 + 2]-Cycloadditions of Substituted Vinylcyclopropanes.

Author

Trost, Barry M., Morris, Patrick J., and Sprague, Simon J.

Published

2013

9. (R)-Ketamine exerts antidepressant actions partly via conversion to (2R,6R)-hydroxynorketamine, while causing adverse effects at sub-anaesthetic doses.

Author

Zanos, Panos, Highland, Jaclyn N., Liu, Xin, Troppoli, Timothy A., Georgiou, Polymnia, Lovett, Jacqueline, Morris, Patrick J., Stewart, Brent W., Thomas, Craig J., Thompson, Scott M., Moaddel, Ruin, and Gould, Todd D.

Subjects

*ANTIDEPRESSANTS, *METHYL aspartate receptors, *CAUSATION (Philosophy)

Abstract

Background and Purpose: (R)-Ketamine (arketamine) may have utility as a rapidly acting antidepressant. While (R)-ketamine has lower potency than (R,S)-ketamine to inhibit NMDA receptors in vitro, the extent to which (R)-ketamine shares the NMDA receptor-mediated adverse effects of (R,S)-ketamine in vivo has not been fully characterised. Furthermore, (R)-ketamine is metabolised to (2R,6R)-hydroxynorketamine (HNK), which may contribute to its antidepressant-relevant actions.Experimental Approach: Using mice, we compared (R)-ketamine with a deuterated form of the drug (6,6-dideutero-(R)-ketamine, (R)-d2 -ketamine), which hinders its metabolism to (2R,6R)-HNK, in behavioural tests predicting antidepressant responses. We also examined the actions of intracerebroventricularly infused (2R,6R)-HNK. Further, we quantified putative NMDA receptor inhibition-mediated adverse effects of (R)-ketamine.Key Results: (R)-d2 -Ketamine was identical to (R)-ketamine in binding to and functionally inhibiting NMDA receptors but hindered (R)-ketamine's metabolism to (2R,6R)-HNK. (R)-Ketamine exerted greater potency than (R)-d2 -ketamine in several antidepressant-sensitive behavioural measures, consistent with a role of (2R,6R)-HNK in the actions of (R)-ketamine. There were dose-dependent sustained antidepressant-relevant actions of (2R,6R)-HNK following intracerebroventricular administration. (R)-Ketamine exerted NMDA receptor inhibition-mediated behaviours similar to (R,S)-ketamine, including locomotor stimulation, conditioned-place preference, prepulse inhibition deficits, and motor incoordination, with approximately half the potency of the racemic drug.Conclusions and Implications: Metabolism of (R)-ketamine to (2R,6R)-HNK increases the potency of (R)-ketamine to exert antidepressant-relevant actions in mice. Adverse effects of (R)-ketamine require higher doses than those necessary for antidepressant-sensitive behavioural changes in mice. However, our data revealing that (R)-ketamine's adverse effects are elicited at sub-anaesthetic doses indicate a potential risk for sensory dissociation and abuse liability. [ABSTRACT FROM AUTHOR]

Published

2019

10. (2R,6R)-hydroxynorketamine exerts mGlu2 receptor-dependent antidepressant actions.

Author

Zanos, Panos, Highland, Jaclyn N., Stewart, Brent W., Georgiou, Polymnia, Jenne, Carleigh E., Lovett, Jacqueline, Morris, Patrick J., Thomas, Craig J., Moaddel, Ruin, Zarate Jr., Carlos A., and Gould, Todd D.

Subjects

*ANTIDEPRESSANTS, *KETAMINE, *GLUTAMATE receptors, *DEPRESSED persons, *DRUG efficacy

Abstract

Currently approved antidepressant drugs often take months to take full effect, and ~30% of depressed patients remain treatment resistant. In contrast, ketamine, when administered as a single subanesthetic dose, exerts rapid and sustained antidepressant actions. Preclinical studies indicate that the ketamine metabolite (2R,6R)-hydroxynorketamine [(2R,6R)-HNK] is a rapid-acting antidepressant drug candidate with limited dissociation properties and abuse potential. We assessed the role of group II metabotropic glutamate receptor subtypes 2 (mGlu2) and 3 (mGlu3) in the antidepressant-relevant actions of (2R,6R)-HNK using behavioral, genetic, and pharmacological approaches as well as cortical quantitative EEG (qEEG) measurements in mice. Both ketamine and (2R,6R)-HNK prevented mGlu2/3 receptor agonist (LY379268)-induced body temperature increases in mice lacking the Grm3, but not Grm2, gene. This action was not replicated by NMDA receptor antagonists or a chemical variant of ketamine that limits metabolism to (2R,6R)-HNK. The antidepressant-relevant behavioral effects and 30- to 80-Hz qEEG oscillation (gamma-range) increases resultant from (2R,6R)-HNK administration were prevented by pretreatment with an mGlu2/3 receptor agonist and absent in mice lacking the Grm2, but not Grm3-/-, gene. Combined subeffective doses of the mGlu2/3 receptor antagonist LY341495 and (2R,6R)-HNK exerted synergistic increases on gamma oscillations and antidepressant-relevant behavioral actions. These findings highlight that (2R,6R)-HNK exerts antidepressant-relevant actions via a mechanism converging with mGlu2 receptor signaling and suggest enhanced cortical gamma oscillations as a marker of target engagement relevant to antidepressant efficacy. Moreover, these results support the use of (2R,6R)-HNK and inhibitors of mGlu2 receptor function in clinical trials for treatment-resistant depression either alone or in combination. [ABSTRACT FROM AUTHOR]

Published

2019

11. Antidepressant-relevant concentrations of the ketamine metabolite (2R,6R)-hydroxynorketamine do not block NMDA receptor function.

Author

Lumsden, Eric W., Troppoli, Timothy A., Myers, Scott J., Zanos, Panos, Aracava, Yasco, Kehr, Jan, Lovett, Jacqueline, Kim, Sukhan, Fu-Hua Wang, Schmidt, Staffan, Jenne, Carleigh E., Peixiong Yuan, Morris, Patrick J., Thomas, Craig J., Zarate Jr., Carlos A., Moaddel, Ruin, Traynelis, Stephen F., Pereira, Edna F. R., Thompson, Scott M., and Albuquerque, Edson X.

Subjects

*KETAMINE, *CHLOROBENZENE, *ANTIDEPRESSANTS, *PSYCHIATRIC drugs, *MENTAL depression, *AMINO acid receptors, *HIPPOCAMPUS (Brain)

Abstract

Preclinical studies indicate that (2R,6R)-hydroxynorketamine (HNK) is a putative fast-acting antidepressant candidate. Although inhibition of NMDA-type glutamate receptors (NMDARs) is one mechanism proposed to underlie ketamine's antidepressant and adverse effects, the potency of (2R,6R)-HNK to inhibit NMDARs has not been established. We used a multidisciplinary approach to determine the effects of (2R,6R)-HNK on NMDAR function. Antidepressant-relevant behavioral responses and (2R,6R)-HNK levels in the extracellular compartment of the hippocampus were measured following systemic (2R,6R)-HNK administration in mice. The effects of ketamine, (2R,6R)-HNK, and, in some cases, the (2S,6S)-HNK stereoisomer were evaluated on the following: (i) NMDA-induced lethality in mice, (ii) NMDAR-mediated field excitatory postsynaptic potentials (fEPSPs) in the CA1 field of mouse hippocampal slices, (iii) NMDARmediated miniature excitatory postsynaptic currents (mEPSCs) and NMDA-evoked currents in CA1 pyramidal neurons of rat hippocampal slices, and (iv) recombinant NMDARs expressed in Xenopus oocytes. While a single i.p. injection of 10 mg/kg (2R,6R)-HNK exerted antidepressant-related behavioral and cellular responses in mice, the ED50 of (2R,6R)-HNK to prevent NMDA-induced lethality was found to be 228 mg/kg, compared with 6.4 mg/kg for ketamine. The 10 mg/kg (2R,6R)-HNK dose generated maximal hippocampal extracellular concentrations of ~8 µM, which were well below concentrations required to inhibit synaptic and extrasynaptic NMDARs in vitro. (2S,6S)-HNK was more potent than (2R,6R)-HNK, but less potent than ketamine at inhibiting NMDARs. These data demonstrate the stereoselectivity of NMDAR inhibition by (2R,6R;2S,6S)- HNK and support the conclusion that direct NMDAR inhibition does not contribute to antidepressant-relevant effects of (2R,6R)-HNK. [ABSTRACT FROM AUTHOR]

Published

2019

12. Identification of Combinations of Approved Drugs With Synergistic Activity Against Ebola Virus in Cell Cultures.

Author

Dyall, Julie, Nelson, Elizabeth A, DeWald, Lisa Evans, Guha, Rajarshi, Hart, Brit J, Zhou, Huanying, Postnikova, Elena, Logue, James, Vargas, Walter M, Gross, Robin, Michelotti, Julia, Deiuliis, Nicole, Bennett, Richard S, Crozier, Ian, Holbrook, Michael R, Morris, Patrick J, Klumpp-Thomas, Carleen, McKnight, Crystal, Mierzwa, Tim, and Shinn, Paul

Subjects

*EBOLA virus, *CELL culture, *VIRAL transmission, *MARBURG virus, *HEMORRHAGIC fever, TREATMENT of Ebola virus diseases

Abstract

Background: A need to develop therapeutics to treat Ebola virus disease patients in remote and resource-challenged settings remains in the wake of the 2013-2016 epidemic in West Africa. Toward this goal, we screened drugs under consideration as treatment options and other drugs of interest, most being small molecules approved by the Food and Drug Administration. Drugs demonstrating in vitro antiviral activity were advanced for evaluation in combinations because of advantages often provided by drug cocktails.Methods: Drugs were screened for blockade of Ebola virus infection in cultured cells. Twelve drugs were tested in all (78 pair-wise) combinations, and 3 were tested in a subset of combinations.Results: Multiple synergistic drug pairs emerged, with the majority comprising 2 entry inhibitors. For the pairs of entry inhibitors studied, synergy was demonstrated at the level of virus entry into host cells. Highly synergistic pairs included aripiprazole/piperacetazine, sertraline/toremifene, sertraline/bepridil, and amodiaquine/clomiphene.Conclusions: Our study shows the feasibility of identifying pairs of approved drugs that synergistically block Ebola virus infection in cell cultures. We discuss our findings in terms of the theoretic ability of these or alternate combinations to reach therapeutic levels. Future research will assess selected combinations in small-animal models of Ebola virus disease. [ABSTRACT FROM AUTHOR]

Published

2018

13. Plasma metabolomic profiling of a ketamine and placebo crossover trial of major depressive disorder and healthy control subjects.

Author

Moaddel, Ruin, Shardell, Michelle, Khadeer, Mohammed, Lovett, Jacqueline, Kadriu, Bashkim, Ravichandran, Sarangan, Morris, Patrick J., Yuan, Peixiong, Thomas, Craig J., Gould, Todd D., Ferrucci, Luigi, and Zarate, Carlos A.

Subjects

*MENTAL depression, *KETAMINE, *METABOLOMICS, *KYNURENINE, *BIOAVAILABILITY

Abstract

(R,S)-Ketamine produces rapid, robust, and sustained antidepressant effects in major depressive disorder. Specifically, its pharmacological efficacy in treatment refractory depression is considered a major breakthrough in the field. However, the mechanism of action of ketamine’s rapid effect remains to be determined. In order to identify pathways that are responsible for ketamine’s effect, a targeted metabolomic approach was carried out using a double-blind, placebo-controlled crossover design, with infusion order randomized with medication-free patients with treatment-resistant major depressive disorder (29 subjects) and healthy controls (25 subjects). The metabolomic profile of these subjects was characterized at multiple time points, and a comprehensive analysis was investigated between the following: MDD and healthy controls, treatment and placebo in both groups and the corresponding response to ketamine treatment. Ketamine treatment resulted in a general increase in circulating sphingomyelins, levels which were not correlated with response. Ketamine response resulted in more pronounced effects in the kynurenine pathway and the arginine pathway at 4 h post-infusion, where a larger decrease in circulating kynurenine levels and a larger increase in the bioavailability of arginine were observed in responders to ketamine treatment, suggesting possible mechanisms for response to ketamine treatment. [ABSTRACT FROM AUTHOR]

Published

2018

14. Activation of the NRF2 antioxidant program generates an imbalance in central carbon metabolism in cancer.

Author

Sayin, Volkan I., LeBoeuf, Sarah E., Singh, Simranjit X., Davidson, Shawn M., Biancur, Douglas, Guzelhan, Betul S., Alvarez, Samantha W., Wu, Warren L., Karakousi, Triantafyllia R., Zavitsanou, Anastasia Maria, Ubriaco, Julian, Muir, Alexander, Karagiannis, Dimitris, Morris, Patrick J., Thomas, Craig J., Possemato, Richard, Vander Heiden, Matthew G., and Papagiannakopoulos, Thales

Subjects

*CARBON metabolism, *NEOPLASTIC cell transformation, *REACTIVE oxygen species, *HOMEOSTASIS, *CANCER cell growth, *GLUTAMIC acid, *GLUTATHIONE

Abstract

During tumorigenesis, the high metabolic demand of cancer cells results in increased production of reactive oxygen species. To maintain oxidative homeostasis, tumor cells increase their antioxidant production through hyperactivation of the NRF2 pathway, which promotes tumor cell growth. Despite the extensive characterization of NRF2-driven metabolic rewiring, little is known about the metabolic liabilities generated by this reprogramming. Here, we show that activation of NRF2, in either mouse or human cancer cells, leads to increased dependency on exogenous glutamine through increased consumption of glutamate for glutathione synthesis and glutamate secretion by xc- antiporter system. Together, this limits glutamate availability for the tricarboxylic acid cycle and other biosynthetic reactions creating a metabolic bottleneck. Cancers with genetic or pharmacological activation of the NRF2 antioxidant pathway have a metabolic imbalance between supporting increased antioxidant capacity over central carbon metabolism, which can be therapeutically exploited. [ABSTRACT FROM AUTHOR]

Published

2017

15. The phosphatidylinositol-3-phosphate 5-kinase inhibitor apilimod blocks filoviral entry and infection.

Author

Nelson, Elizabeth A., Dyall, Julie, Hoenen, Thomas, Barnes, Alyson B., Zhou, Huanying, Liang, Janie Y., Michelotti, Julia, Dewey, William H., DeWald, Lisa Evans, Bennett, Richard S., Morris, Patrick J., Guha, Rajarshi, Klumpp-Thomas, Carleen, McKnight, Crystal, Chen, Yu-Chi, Xu, Xin, Wang, Amy, Hughes, Emma, Martin, Scott, and Thomas, Craig

Subjects

*PHOSPHATIDYLINOSITOL 3-kinases, *EBOLA virus disease, *MARBURG virus, *FILOVIRIDAE, *IMMUNOLOGY, *CATHEPSIN B

Abstract

Phosphatidylinositol-3-phosphate 5-kinase (PIKfyve) is a lipid kinase involved in endosome maturation that emerged from a haploid genetic screen as being required for Ebola virus (EBOV) infection. Here we analyzed the effects of apilimod, a PIKfyve inhibitor that was reported to be well tolerated in humans in phase 2 clinical trials, for its effects on entry and infection of EBOV and Marburg virus (MARV). We first found that apilimod blocks infections by EBOV and MARV in Huh 7, Vero E6 and primary human macrophage cells, with notable potency in the macrophages (IC50, 10 nM). We next observed that similar doses of apilimod block EBOV-glycoprotein-virus like particle (VLP) entry and transcription-replication competent VLP infection, suggesting that the primary mode of action of apilimod is as an entry inhibitor, preventing release of the viral genome into the cytoplasm to initiate replication. After providing evidence that the anti-EBOV action of apilimod is via PIKfyve, we showed that it blocks trafficking of EBOV VLPs to endolysosomes containing Niemann-Pick C1 (NPC1), the intracellular receptor for EBOV. Concurrently apilimod caused VLPs to accumulate in early endosome antigen 1-positive endosomes. We did not detect any effects of apilimod on bulk endosome acidification, on the activity of cathepsins B and L, or on cholesterol export from endolysosomes. Hence by antagonizing PIKfyve, apilimod appears to block EBOV trafficking to its site of fusion and entry into the cytoplasm. Given the drug’s observed anti-filoviral activity, relatively unexplored mechanism of entry inhibition, and reported tolerability in humans, we propose that apilimod be further explored as part of a therapeutic regimen to treat filoviral infections. [ABSTRACT FROM AUTHOR]

Published

2017

16. Reply to: Antidepressant Actions of Ketamine Versus Hydroxynorketamine.

Author

Zanos, Panos, Moaddel, Ruin, Morris, Patrick J., Wainer, Irving W., Albuquerque, Edson X., Thompson, Scott M., Thomas, Craig J., Jr.Zarate, Carlos A., and Gould, Todd D.

Subjects

*METHYL aspartate receptors, *NEUROPLASTICITY, *EMOTIONAL conditioning, *ISOXAZOLES, *PROPIONIC acid

Published

2017

17. Metabolic Profiling Reveals PAFAH1B3 as a Critical Driver of Breast Cancer Pathogenicity.

Author

Mulvihill, Melinda M., Benjamin, Daniel I., Ji, Xiaodan, Le Scolan, Erwan, Louie, Sharon M., Shieh, Alice, Green, McKenna, Narasimhalu, Tara, Morris, Patrick J., Luo, Kunxin, and Nomura, Daniel K.

Subjects

*METABOLIC profile tests, *GENETIC transformation, *CANCER invasiveness, *PLATELET activating factor, *BREAST cancer prognosis, *TUMOR suppressor genes, *CELLULAR signal transduction

Abstract

Many studies have identified metabolic pathways that underlie cellular transformation, but the metabolic drivers of cancer progression remain less well understood. The Hippo transducer pathway has been shown to confer malignant traits on breast cancer cells. In this study, we used metabolic mapping platforms to identify biochemical drivers of cellular transformation and malignant progression driven through RAS and the Hippo pathway in breast cancer and identified platelet-activating factor acetylhydrolase 1B3 (PAFAH1B3) as a key metabolic driver of breast cancer pathogenicity that is upregulated in primary human breast tumors and correlated with poor prognosis. Metabolomic profiling suggests that PAFAH1B3 inactivation attenuates cancer pathogenicity through enhancing tumor-suppressing signaling lipids. Our studies provide a map of altered metabolism that underlies breast cancer progression and put forth PAFAH1B3 as a critical metabolic node in breast cancer. • We have performed a metabolic profiling study to identify drivers of breast cancer • Cancer metabolism is regulated by RAS and Hippo pathways • PAFAH1B3 is a driver of breast cancer • PAFAH1B3 is a metabolic target for breast cancer therapy Using metabolic mapping approaches, Mulvihill et al. identify PAFAH1B3 as a driver of cellular transformation and malignant progression in breast cancer. The enzyme taps into the RAS and Hippo pathways and regulates the landscape tumor-suppressing lipids. [ABSTRACT FROM AUTHOR]

Published

2014