Your search keyword '"Karen Apelskog-Torres"' showing total 2 results

1. Reversible inhibitors of monoamine oxidase-A (RIMAs): robust, reversible inhibition of human brain MAO-A by CX157

Author

Millard Jayne, Payton King, Elena Shumay, Barry Scott Brand, Daniel Burch, Wei Zhu, Karen Apelskog-Torres, Scott Carter, Robert M. Fielding, Youwen Xu, Michael J. Schueller, David Alexoff, Gene-Jack Wang, Colleen Shea, James Cecil Free, Amy K Poshusta, Pauline Carter, Joanna S. Fowler, Barbara Hubbard, Frank Telang, Jean Logan, Donald Warner, Mahnaz Asgharnejad, Lisa Muench, and Albert J. Azzaro

Subjects

Adult, Male, Clorgyline, Monoamine Oxidase Inhibitors, Monoamine oxidase, Nerve Tissue Proteins, Pharmacology, chemistry.chemical_compound, Young Adult, Dopamine, Heterocyclic Compounds, medicine, Humans, CX157, Monoamine Oxidase, biology, business.industry, Brain, Human brain, Middle Aged, Psychiatry and Mental health, Monoamine neurotransmitter, medicine.anatomical_structure, chemistry, Biochemistry, Positron-Emission Tomography, biology.protein, Original Article, Serotonin, Monoamine oxidase A, business, medicine.drug, Protein Binding

Abstract

Reversible inhibitors of monoamine oxidase-A (RIMA) inhibit the breakdown of three major neurotransmitters, serotonin, norepinephrine and dopamine, offering a multi-neurotransmitter strategy for the treatment of depression. CX157 (3-fluoro-7-(2,2,2-trifluoroethoxy)phenoxathiin-10,10-dioxide) is a RIMA, which is currently in development for the treatment of major depressive disorder. We examined the degree and reversibility of the inhibition of brain monoamine oxidase-A (MAO-A) and plasma CX157 levels at different times after oral dosing to establish a dosing paradigm for future clinical efficacy studies, and to determine whether plasma CX157 levels reflect the degree of brain MAO-A inhibition. Brain MAO-A levels were measured with positron emission tomography (PET) imaging and [(11)C]clorgyline in 15 normal men after oral dosing of CX157 (20-80 mg). PET imaging was conducted after single and repeated doses of CX157 over a 24-h time course. We found that 60 and 80 mg doses of CX157 produced a robust dose-related inhibition (47-72%) of [(11)C]clorgyline binding to brain MAO-A at 2 h after administration and that brain MAO-A recovered completely by 24 h post drug. Plasma CX157 concentration was highly correlated with the inhibition of brain MAO-A (EC(50): 19.3 ng/ml). Thus, CX157 is the first agent in the RIMA class with documented reversible inhibition of human brain MAO-A, supporting its classification as a RIMA, and the first RIMA with observed plasma levels that can serve as a biomarker for the degree of brain MAO-A inhibition. These data were used to establish the dosing regimen for a current clinical efficacy trial with CX157.

Published

2009

2. Effects of modafinil on dopamine and dopamine transporters in the male human brain: clinical implications

Author

Lisa Muench, Jacob M. Hooker, Christopher Wong, Payton King, Gene-Jack Wang, Karen Apelskog-Torres, Nora D. Volkow, Joanna S. Fowler, Millard Jayne, David Alexoff, Donald Warner, Youwen Xu, Frank Telang, Wei Zhu, Colleen Shea, Pauline Carter, Barbara Hubbard, and Jean Logan

Subjects

Adult, Male, Substance-Related Disorders, Dopamine Plasma Membrane Transport Proteins, Dopamine, Modafinil, Pilot Projects, Pharmacology, Nucleus Accumbens, Article, chemistry.chemical_compound, Young Adult, Cocaine, mental disorders, Medicine, Humans, Carbon Radioisotopes, Benzhydryl Compounds, Neurotransmitter, Dopamine transporter, Raclopride, biology, business.industry, Receptors, Dopamine D2, Armodafinil, Putamen, Receptors, Dopamine D3, Brain, General Medicine, Middle Aged, chemistry, Anesthesia, Positron-Emission Tomography, biology.protein, Catecholamine, Central Nervous System Stimulants, Caudate Nucleus, business, medicine.drug

Abstract

Modafinil, a wake-promoting drug used to treat narcolepsy, is increasingly being used as a cognitive enhancer. Although initially launched as distinct from stimulants that increase extracellular dopamine by targeting dopamine transporters, recent preclinical studies suggest otherwise.To measure the acute effects of modafinil at doses used therapeutically (200 mg and 400 mg given orally) on extracellular dopamine and on dopamine transporters in the male human brain.Positron emission tomography with [(11)C]raclopride (D(2)/D(3) radioligand sensitive to changes in endogenous dopamine) and [(11)C]cocaine (dopamine transporter radioligand) was used to measure the effects of modafinil on extracellular dopamine and on dopamine transporters in 10 healthy male participants. The study took place over an 8-month period (2007-2008) at Brookhaven National Laboratory.Primary outcomes were changes in dopamine D(2)/D(3) receptor and dopamine transporter availability (measured by changes in binding potential) after modafinil when compared with after placebo.Modafinil decreased mean (SD) [(11)C]raclopride binding potential in caudate (6.1% [6.5%]; 95% confidence interval [CI], 1.5% to 10.8%; P = .02), putamen (6.7% [4.9%]; 95% CI, 3.2% to 10.3%; P = .002), and nucleus accumbens (19.4% [20%]; 95% CI, 5% to 35%; P = .02), reflecting increases in extracellular dopamine. Modafinil also decreased [(11)C]cocaine binding potential in caudate (53.8% [13.8%]; 95% CI, 43.9% to 63.6%; P.001), putamen (47.2% [11.4%]; 95% CI, 39.1% to 55.4%; P.001), and nucleus accumbens (39.3% [10%]; 95% CI, 30% to 49%; P = .001), reflecting occupancy of dopamine transporters.In this pilot study, modafinil blocked dopamine transporters and increased dopamine in the human brain (including the nucleus accumbens). Because drugs that increase dopamine in the nucleus accumbens have the potential for abuse, and considering the increasing use of modafinil, these results highlight the need for heightened awareness for potential abuse of and dependence on modafinil in vulnerable populations.

Published

2009