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1. Top Priorities for Cerebroprotective Studies—A Paradigm Shift: Report From STAIR XI

Author

Patrick Lyden, Alastair Buchan, Johannes Boltze, Marc Fisher, Saeed Ansari, Joseph P Broderick, Bruce CV Campbell, Napasri Chaisinanunkul, Christopher Chen, James C Grotta, Walid Haddad, Randa Hareedy, Michael D Hill, Gary Houser, Ashutosh P Jadhav, Pooja Khatri, W Taylor Kimberly, James I Koenig, William S Korinek, Jaren W Landen, Maarten G Lansberg, Lawrence L Latour, David S Liebeskind, Theodore E Liston, John Lynch, John McGonigle, Eva A Mistry, J Mocco, Kent E Pryor, Jeffrey L Saver, Sean I Savitz, Kevin N Sheth, Yoram Solberg, Achala Vagal, Chitra Venkatasubramanian, and Nikolaos K Ziogas

Subjects
0301 basic medicine, Advanced and Specialized Nursing, medicine.medical_specialty, business.industry, Clinical study design, Gold standard, medicine.disease, Neuroprotection, Entire brain, Clinical trial, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Physical medicine and rehabilitation, Paradigm shift, Ischemic stroke, Medicine, Neurology (clinical), Cardiology and Cardiovascular Medicine, business, Stroke, 030217 neurology & neurosurgery
Abstract

Despite years of basic research and pioneering clinical work, ischemic stroke remains a major public health concern. Prior STAIR (Stroke Treatment Academic Industry Roundtable) conferences identified both failures of clinical trial design and failures in preclinical assessment in developing putative ischemic stroke treatments. At STAIR XI, participants in workshop no. 1 Top Priorities for Neuroprotection sought to redefine the neuroprotection paradigm and given the paucity of evidence underlying preclinical assessment, offer consensus-based recommendations. STAIR proposes the term brain cytoprotection or cerebroprotection to replace the term neuroprotection when the intention of an investigation is to demonstrate that a new, candidate treatment benefits the entire brain. Although “time is still brain,” tissue imaging techniques have been developed to identify patients with both predicted core injury and penumbral, salvageable brain tissue, regardless of time after stroke symptom onset. STAIR XI workshop participants called this imaging approach a tissue window to select patients for recanalization. Elements of the neurovascular unit show differential vulnerability evolving over differing time scales in different brain regions. STAIR proposes the term target window to suggest therapies that target the different elements of the neurovascular unit at different times. Based on contemporary principles of rigor and transparency, the workshop updated, revised, and enhanced the STAIR preclinical recommendations for developing new treatments in 2 phases: an exploratory qualification phase and a definitive validation phase. For new, putative treatments, investigators should carefully characterize the mechanism of action, the pharmacokinetics/pharmacodynamics, demonstrate target engagement, and confirm penetration through the blood-brain barrier. Before clinical trials, testing of candidate molecules in stroke models could proceed in a comprehensive manner using animals of both sexes and to include significant variables such as age and comorbid conditions. Comprehensive preclinical assessment might include multicenter, collaborative testing, for example, network trials. In the absence of a proven cerebroprotective agent to use as a gold standard, however, it remains speculative whether such comprehensive preclinical assessment can effectively predict clinical outcome.

Published
2021

2. Ponezumab in mild-to-moderate Alzheimer's disease: Randomized phase II PET-PIB study

Author

Jaren W. Landen, Niels Andreasen, Carol Cronenberger, Henrik Östlund, Martin M. Bednar, Anne Börjesson-Hanson, Pamela F. Schwartz, Catherine Sattler, and Brendon Binneman

Subjects
0301 basic medicine, medicine.medical_specialty, Amyloid, Neurology, Pharmacology, Placebo, Loading dose, 03 medical and health sciences, 0302 clinical medicine, Cerebrospinal fluid, Ponezumab, Pharmacokinetics, Anti-drug antibodies, Medicine, Antibody, business.industry, PIB, Featured Article, Alzheimer's disease, Tolerability, Psychiatry and Mental health, 030104 developmental biology, Pharmacodynamics, Neurology (clinical), Safety, business, 030217 neurology & neurosurgery
Abstract

Introduction The safety, pharmacokinetics, and effect on peripheral and central amyloid β (Aβ) of multiple doses of ponezumab, an anti-Aβ monoclonal antibody, were characterized in subjects with mild-to-moderate Alzheimer's disease treated for 1 year. Methods Subjects were aged ≥50 years with Mini–Mental State Examination scores 16 to 26. Cohort Q was randomized to ponezumab 10 mg/kg ( n = 12) or placebo ( n = 6) quarterly. Cohort M was randomized to a loading dose of ponezumab 10 mg/kg or placebo, followed by monthly ponezumab 7.5 mg/kg ( n = 12) or placebo ( n = 6), respectively. Results Ponezumab was generally well tolerated. Plasma concentrations increased dose dependently, but cerebrospinal fluid (CSF) penetration was low. Plasma Aβ increased dose dependently with ponezumab, but CSF biomarkers, brain amyloid burden, cognition, and function were not affected. Conclusions Both ponezumab dosing schedules were generally safe and well tolerated but did not alter CSF biomarkers, brain amyloid burden, or clinical outcomes.

Published
2017

3. Effect of Baseline Characteristics on the Pain Response to Pregabalin in Fibromyalgia Patients with Comorbid Depression

Author

Stuart L. Silverman, Miroslav Backonja, Richard Vissing, Pritha Bhadra Brown, Lynne Pauer, Andrew Clair, Jaren W. Landen, and Joseph M. Scavone

Subjects
Adult, Male, medicine.medical_specialty, Fibromyalgia, Adolescent, Pregabalin, Comorbidity, Placebo, law.invention, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Double-Blind Method, Randomized controlled trial, law, Internal medicine, Post-hoc analysis, Humans, Medicine, Psychiatry, Irritable bowel syndrome, Depression (differential diagnoses), Aged, 030203 arthritis & rheumatology, Analgesics, Cross-Over Studies, Depression, business.industry, General Medicine, Middle Aged, medicine.disease, Crossover study, Antidepressive Agents, Anesthesiology and Pain Medicine, Female, Neurology (clinical), business, 030217 neurology & neurosurgery, medicine.drug
Abstract

Objective To evaluate the effect of baseline characteristics on the treatment response to pregabalin in fibromyalgia (FM) patients with depression. Design Post hoc analysis from a randomized, double-blind, placebo-controlled, two-way crossover study of pregabalin (300 or 450 mg/day, twice daily). Subjects A total of 193 FM patients taking an antidepressant for comorbid depression. Methods The effect of patient baseline characteristics on the treatment response to pregabalin vs placebo was assessed for the primary efficacy end point (mean pain score on an 11-point numeric rating scale). Variables were analyzed using a linear mixed effects model with sequence, period, and treatment as fixed factors, and subject within sequence and within subject error as random factors. Results Pregabalin significantly improved mean pain scores vs placebo irrespective of age, duration of FM, number of prior FM medications, depression diagnosis, shorter-term depression (

Published
2017

4. Multiple-dose ponezumab for mild-to-moderate Alzheimer's disease: Safety and efficacy

Author

Sharon Cohen, Qinying Zhao, Carol Cronenberger, Aaron H. Burstein, Pamela F. Schwartz, William T. Duggan, Martin M. Bednar, Kejal Kantarci, Clifford R. Jack, Brendon Binneman, Scot Styren, Jae-Hong Lee, Jaren W. Landen, Clare B. Billing, Ken J. Sprenger, and Catherine Sattler

Subjects
Monoclonal antibody, 0301 basic medicine, medicine.medical_specialty, Phases of clinical research, Placebo, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Cerebrospinal fluid, Ponezumab, Pharmacokinetics, Internal medicine, Medicine, Adverse effect, business.industry, Amyloid β, Featured Article, Alzheimer's disease, Phase-II study, 3. Good health, Psychiatry and Mental health, 030104 developmental biology, Pharmacodynamics, Anesthesia, Cerebrospinal fluid penetration, Immunotherapy, Neurology (clinical), business, Biomarkers, 030217 neurology & neurosurgery
Abstract

Introduction Multiple intravenous doses of ponezumab, an anti-amyloid antibody, were evaluated in subjects with mild-to-moderate Alzheimer's disease (AD). Methods In part A, 77 subjects were randomized to ponezumab 0.1, 0.5, or 1 mg/kg (75 treated) and 26 to placebo (24 treated). In part B, 63 subjects were randomized and treated with ponezumab 3 or 8.5 mg/kg and 32 with placebo. Subjects received 10 infusions over 18 months and were followed for 6 months thereafter. Results Ponezumab was generally safe and well tolerated. Most common adverse events were fall (16.7% ponezumab, 21.4% placebo), headache (13.8%, 21.4%), and cerebral microhemorrhage (13.8%, 19.6%). Plasma ponezumab increased dose-dependently with limited accumulation. Cerebrospinal fluid penetration was low. Plasma Aβ 1–x and Aβ 1–40 showed robust increases, but cerebrospinal fluid biomarkers showed no dose response. Ponezumab had no effects on cognitive/functional outcomes or brain volume. Conclusions Multiple-dose ponezumab was generally safe, but not efficacious, in mild-to-moderate AD.

Published
2017

5. A randomized, double-blind, placebo-controlled trial and open-label extension study to evaluate the efficacy and safety of pregabalin in the treatment of neuropathic pain associated with human immunodeficiency virus neuropathy

Author

David M. Simpson, Jaren W. Landen, Jonathan Sporn, David Semel, Birol Emir, Andrew S.C. Rice, and Marci L. Chew

Subjects
Adult, Male, Population, Pregabalin, Placebo-controlled study, HIV Infections, Placebo, law.invention, Polyneuropathies, Young Adult, Double-Blind Method, Randomized controlled trial, law, medicine, Humans, Single-Blind Method, education, Adverse effect, Aged, Pain Measurement, Analgesics, education.field_of_study, business.industry, Middle Aged, Interim analysis, Treatment Outcome, Anesthesiology and Pain Medicine, Neurology, Anesthesia, Neuropathic pain, Neuralgia, Female, Neurology (clinical), business, medicine.drug
Abstract

The objective of these studies was to assess the efficacy and safety of pregabalin in the treatment of human immunodeficiency virus (HIV)-associated neuropathic pain. Patients with HIV-associated distal sensory polyneuropathy (DSP) were randomized to treatment with flexible-dose pregabalin (150-600 mg/day) or placebo for 17 weeks in a single-blind, placebo lead-in, randomized, double-blind, parallel-group, placebo-controlled multinational trial. The primary efficacy outcome was the change in mean pain score on an 11-point numeric rating scale (NRS) from baseline to study endpoint. Participants who completed this trial were invited to participate in a 6-month open-label extension study with pregabalin. Of the 377 patients enrolled in the randomized controlled trial (pregabalin, n=183; placebo, n=194), 68.4% completed treatment. In the open-label extension, 217 patients were treated and 59.4% completed treatment. Both studies were terminated by the sponsor after a preplanned interim analysis indicated trial futility. At endpoint, the change from baseline in least-squares mean NRS pain scores in the intent-to-treat population was -2.04 for pregabalin versus -2.11 for placebo (P=.709). There were no significant differences between the pregabalin and placebo groups in the secondary efficacy measures. Incidence of adverse events was lower than seen in previous pregabalin studies. Overall, this trial did not show pregabalin to be more efficacious than placebo in treating HIV-associated DSP. Studies such as these, which fail to support their primary hypotheses, may be important in informing the methodology of future trials, especially when novel approaches to limit variability in the control group are included. ClinicalTrials.gov identifiers: NCT01049217 and NCT01145417.

Published
2014

6. Safety and Pharmacology of a Single Intravenous Dose of Ponezumab in Subjects With Mild-to-Moderate Alzheimer Disease

Author

Michael Borrie, James Kupiec, Kelly R. Bales, Clare B. Billing, Michael Woodward, Qinying Zhao, Jerry Yang, Jaren W. Landen, Sharon Cohen, Martin M. Bednar, Christine Alvey, and Fred McCush

Subjects
Male, Pharmacology, Antibodies, Monoclonal, Humanized, Placebo, Lesion, Ponezumab, Cerebrospinal fluid, Double-Blind Method, Pharmacokinetics, Alzheimer Disease, Humans, Medicine, Pharmacology (medical), Infusions, Intravenous, Adverse effect, Aged, Aged, 80 and over, Amyloid beta-Peptides, Dose-Response Relationship, Drug, business.industry, Middle Aged, Dose–response relationship, Pharmacodynamics, Female, Neurology (clinical), medicine.symptom, business, Follow-Up Studies
Abstract

Objectives Ponezumab is a humanized antiamyloid beta (Aβ) monoclonal antibody designed to treat Alzheimer disease (AD). Methods This randomized, double-blind, single-dose-escalation study evaluated the safety, pharmacokinetics, and pharmacodynamics of 0.1, 0.3, 1, 3, and 10 mg/kg ponezumab (n = 4, 4, 4, 6, and 8, respectively) versus placebo (n = 11) after a 2-hour intravenous infusion in subjects with mild-to-moderate AD. Cerebrospinal fluid (CSF) samples were obtained from the 1- and 10-mg/kg groups at baseline and at day 29. The subjects were followed for 1 year. Results All subjects completed the trial. Ponezumab was well tolerated with no drug-attributed serious adverse events. The most common adverse events were upper respiratory tract infection, headache, and back pain, all mild to moderate. One subject (10 mg/kg) experienced a mild hypersensitivity reaction. Another subject (0.1 mg/kg) demonstrated slight enlargement of a preexisting midbrain lesion. Electrocardiography and laboratory values (including CSF) were unremarkable. No evidence of new microhemorrhage, vasogenic edema, or meningoencephalitis was noted. Plasma maximum observed concentration increased approximately dose proportionally, and the area under the plasma concentration-time profile from time zero extrapolated to infinite time (AUC(inf)) increased slightly more than dose proportionally. Mean terminal half-life was approximately 6 weeks. Two subjects (10 mg/kg) had measurable CSF ponezumab concentrations (~0.5% of plasma values) at day 29. Plasma Aβ(1-x) and Aβ(1-40) increased dose dependently, and mean CSF Aβ(1-x) increased 38% from baseline with 10 mg/kg (P = 0.002 vs placebo). Conclusions A 2-hour infusion of 0.1 to 10 mg/kg ponezumab was well tolerated in subjects with mild-to-moderate AD. Plasma pharmacokinetic profile was approximately linear. Plasma Aβ increased with dose, and CSF Aβ increased at the highest dose, suggesting that intravenous ponezumab alters central Aβ levels.

Published
2013

7. Evaluation of structural models to describe the effect of placebo upon the time course of major depressive disorder

Author

Michael Krams, Jaren W. Landen, Nicholas G. Denman, Megan A. Gibbs, Tanya Russell, Diane R. Mould, and Elizabeth Y. Shang

Subjects
Adult, Male, medicine.medical_specialty, Placebo, Models, Biological, Statistics, Nonparametric, Placebos, Young Adult, Double-Blind Method, Rating scale, Hamd, medicine, Humans, Computer Simulation, Psychiatry, Depression (differential diagnoses), Aged, Randomized Controlled Trials as Topic, Psychiatric Status Rating Scales, Pharmacology, Depressive Disorder, Major, business.industry, Middle Aged, Placebo Effect, medicine.disease, NONMEM, Clinical trial, Treatment Outcome, Epidemiologic Research Design, Time course, Disease Progression, Major depressive disorder, Female, business, Algorithms, Clinical psychology
Abstract

Major depressive disorder (MDD) is the leading cause of disability in many countries. Designing and evaluating clinical trials of antidepressants is difficult due to the pronounced and variable placebo response which is poorly defined and may be affected by trial design. Approximately half of recent clinical trials of commonly used antidepressants failed to show statistical superiority for the drug over placebo, which is partly attributable to a marked placebo response. These failures suggest the need for new tools to evaluate placebo response and drug effect in depression, as well as to help design more informative clinical trials. Disease progression modeling is a tool that has been employed for such evaluations and several models have been proposed to describe MDD. Placebo data from three clinical depression trials were used to evaluate three published models: the inverse Bateman (IBM), indirect response (IDR) and transit (TM) models. Each model was used to describe Hamilton Rating Scale for major depression (HAMD) data and results were evaluated. The IBM model had several deficiencies, making it unsuitable. The IDR and TM models performed well on most evaluations and appear suitable. Comparing the IDR and TM models showed less clear distinctions, although overall the TM was found to be somewhat better than the IDR model. Model based evaluation can provide a useful tool for evaluating the time course of MDD and detecting drug effect. However, the models used should be robust, with well estimated parameters.

Published
2009

8. Effects of a NR2B selective NMDA glutamate antagonist, CP-101,606, on dyskinesia and parkinsonism

Author

Michael Krams, Jaren W. Landen, Steven A. Gunzler, Trish Kirchhoff, Penelope Hogarth, Jerry Weaver, Brenda D. Jamerson, Frank S. Menniti, and John G. Nutt

Subjects
Levodopa, Parkinson's disease, Dopamine Agents, Amnesia, Pharmacology, Severity of Illness Index, Article, Double-Blind Method, Parkinsonian Disorders, Piperidines, medicine, Humans, Aged, Cross-Over Studies, Dyskinesias, business.industry, Parkinsonism, Glutamate receptor, Antagonist, Middle Aged, medicine.disease, nervous system diseases, Neurology, Dyskinesia, NMDA receptor, Neurology (clinical), medicine.symptom, business, Excitatory Amino Acid Antagonists, Neuroscience, medicine.drug
Abstract

Glutamate antagonists decrease dyskinesia and augment the antiparkinsonian effects of levodopa in animal models of Parkinson’s disease (PD). In a randomized, double-blind, placebo-controlled clinical trial we investigated the acute effects of placebo and two doses of a NR2B subunit selective NMDA glutamate antagonist, CP-101,606, on the response to two-hour levodopa infusions in 12 PD subjects with motor fluctuations and dyskinesia. Both doses of CP-101,606 reduced the maximum severity of levodopa-induced dyskinesia approximately 30% but neither dose improved parkinsonism. CP-101,606 was associated with a dose-related dissociation and amnesia. These results support the hypothesis that glutamate antagonists may be useful antidyskinetic agents. However, future studies will have to determine if the benefits of dyskinesia suppression can be achieved without adverse cognitive effects.

Published
2008

9. Burden of illness in fibromyalgia patients with comorbid depression

Author

Lucinda, Bateman, Piercarlo, Sarzi-Puttini, Claire L, Burbridge, Jaren W, Landen, Elizabeth T, Masters, Pritha, Bhadra Brown, Joseph M, Scavone, Birol, Emir, Richard S, Vissing, Andrew G, Clair, and Lynne R, Pauer

Subjects
Adult, Male, Psychiatric Status Rating Scales, Depressive Disorder, Fibromyalgia, Comorbidity, Middle Aged, Severity of Illness Index, Antidepressive Agents, Diagnostic Self Evaluation, Cost of Illness, Activities of Daily Living, Outcome Assessment, Health Care, Quality of Life, Humans, Female, Health Expenditures, Pain Measurement
Abstract

To assess the burden of fibromyalgia (FM) in patients with FM taking antidepressant medication for comorbid depression.Symptom burden, impact on work and activity, and healthcare resource utilisation (HCRU) was examined at randomisation in patients enrolled in a clinical trial. Symptom burden was estimated based on self-reported health status measures. The Work Productivity and Activity Impairment: Specific Health Problem scale adapted to FM and a separate HCRU questionnaire were completed. The relationship between FM severity and burden was evaluated.The total population analysed comprised 193 patients; 71 (36.8%) had moderate FM and 119 (61.7%) severe FM. Patients had moderate pain, severe impairment in functioning due to FM, sleep disruption, mild anxiety, and mild depression. In the 7 days preceding randomisation, an average of 58.0% overall work impairment was reported, with 15.2% of working hours missed and 54.0% productivity while at work. In the 3 months preceding randomisation, on average, 5.0 visits per patient were made to healthcare professionals. Physical treatments were used by 34.7% and supplements by 31.6% of patients. Prescription and non-prescription medications, as well as professional services providing help with activities of daily living (ADL) that are impacted by FM, were used by75% of patients. In addition, 50.4 hours of unpaid help was provided for ADL assistance. Total out-of-pocket expenditures were US$307.1, €410.4, or C$211.3, depending on location. FM burden worsened with increasing FM severity.This study demonstrates the significant burden of FM in patients with comorbid depression treated with an antidepressant.

Published
2015

10. Efficacy and Safety of Pregabalin in Patients with Fibromyalgia and Comorbid Depression Taking Concurrent Antidepressant Medication: A Randomized, Placebo-controlled Study

Author

Joseph Driscoll, Andrew Clair, Lynne Pauer, Tahira Khan, Jaren W. Landen, Piercarlo Sarzi-Puttini, Joseph M. Scavone, Lesley M. Arnold, Pritha Bhadra Brown, and Pierre Arsenault

Subjects
Adult, Male, Fibromyalgia, medicine.drug_class, Serotonin reuptake inhibitor, Immunology, Pregabalin, Placebo-controlled study, Placebo, Rheumatology, Norepinephrine reuptake inhibitor, Double-Blind Method, medicine, Immunology and Allergy, Humans, Drug Interactions, Serotonin–norepinephrine reuptake inhibitor, Analgesics, Depressive Disorder, Cross-Over Studies, Dose-Response Relationship, Drug, business.industry, Middle Aged, medicine.disease, Crossover study, Antidepressive Agents, Treatment Outcome, Anesthesia, Female, business, medicine.drug
Abstract

Objective.To assess pregabalin efficacy and safety in patients with fibromyalgia (FM) with comorbid depression taking concurrent antidepressant medication.Methods.This randomized, placebo-controlled, double-blind, 2-period, 2-way crossover study was composed of two 6-week treatment periods separated by a 2-week taper/washout phase. Patients with FM (aged ≥ 18 yrs) taking a stable dose of a selective serotonin reuptake inhibitor (SSRI) or a serotonin/norepinephrine reuptake inhibitor (SNRI) for depression were randomized 1:1 to receive pregabalin/placebo or placebo/pregabalin (optimized to 300 or 450 mg/day). Antidepressant medication was continued throughout the study. The primary efficacy outcome was the mean pain score on an 11-point numerical rating scale. Secondary efficacy outcomes included measures of anxiety, depression, patient function, and sleep.Results.Of 197 patients randomized to treatment, 181 and 177 received ≥ 1 dose of pregabalin and placebo, respectively. At baseline, 52.3% of patients were taking an SSRI and 47.7% an SNRI, and mean pain score was 6.7. Mean pain scores at endpoint were statistically significantly reduced with pregabalin (least squares mean difference from placebo −0.61, 95% CI −0.91 – −0.31, p = 0.0001). Pregabalin significantly improved Hospital Anxiety and Depression Scale-Anxiety (difference −0.95, p < 0.0001) and -Depression (difference −0.88, p = 0.0005) scores, Fibromyalgia Impact Questionnaire total score (difference −6.60, p < 0.0001), and sleep quality (difference 0.57, p < 0.0001), but not EuroQol 5-Dimensions score (difference 0.02, p = 0.3854). Pregabalin safety was consistent with previous studies and current product labeling.Conclusion.Compared with placebo, pregabalin statistically significantly improved FM pain and other symptoms in patients taking antidepressant medication for comorbid depression. ClinicalTrials.gov identifier: NCT01432236.

Published
2015

11. Noscapine Crosses the Blood-Brain Barrier and Inhibits Glioblastoma Growth

Author

David R. Archer, Mingshen Wang, Vincent S. Hau, Brian J. Ciliax, Harish C. Joshi, Erwin G. Van Meir, Bruce H. Wainer, Jaren W. Landen, Thomas P. Davis, and Johnathan D. Glass

Subjects
Noscapine, Cancer Research, Time Factors, Cell Count, Mice, SCID, Pharmacology, Microtubules, S Phase, Mice, Tubulin, Image Processing, Computer-Assisted, Coloring Agents, Chromatography, High Pressure Liquid, Brain Neoplasms, Brain, Anatomy, Flow Cytometry, medicine.anatomical_structure, Oncology, Blood-Brain Barrier, Toxicity, Neuroglia, Female, medicine.drug, Neurite, Central nervous system, Mice, Nude, Mitosis, Antineoplastic Agents, Biology, Blood–brain barrier, Models, Biological, Inhibitory Concentration 50, In vivo, Cell Line, Tumor, medicine, Animals, Humans, Cell Proliferation, Dose-Response Relationship, Drug, Cell growth, Microcirculation, DNA, Rats, Antitussive Agents, Bromodeoxyuridine, Cattle, Endothelium, Vascular, Glioblastoma, Neoplasm Transplantation
Abstract

The opium alkaloid noscapine is a commonly used antitussive agent available in Europe, Asia, and South America. Although the mechanism by which it suppresses coughing is currently unknown, it is presumed to involve the central nervous system. In addition to its antitussive action, noscapine also binds to tubulin and alters microtubule dynamics in vitro and in vivo. In this study, we show that noscapine inhibits the proliferation of rat C6 glioma cells in vitro (IC50 = 100 μm) and effectively crosses the blood-brain barrier at rates similar to the ones found for agents such as morphine and [Met]enkephalin that have potent central nervous system activity (P ≤ 0.05). Daily oral noscapine treatment (300 mg/kg) administered to immunodeficient mice having stereotactically implanted rat C6 glioblasoma into the striatum revealed a significant reduction of tumor volume (P ≤ 0.05). This was achieved with no identifiable toxicity to the duodenum, spleen, liver, or hematopoietic cells as determined by pathological microscopic examination of these tissues and flow cytometry. Furthermore, noscapine treatment resulted in little evidence of toxicity to dorsal root ganglia cultures as measured by inhibition of neurite outgrowth and yielded no evidence of peripheral neuropathy in animals. However, evidence of vasodilation was observed in noscapine-treated brain tissue. These unique properties of noscapine, including its ability to cross the blood-brain barrier, interfere with microtubule dynamics, arrest tumor cell division, reduce tumor growth, and minimally affect other dividing tissues and peripheral nerves, warrant additional investigation of its therapeutic potential.

Published
2004

12. Minor Alteration of Microtubule Dynamics Causes Loss of Tension across Kinetochore Pairs and Activates the Spindle Checkpoint

Author

Jaren W. Landen, Dulal Panda, Jun Zhou, Leslie Wilson, and Harish C. Joshi

Subjects
Noscapine, Time Factors, Mad2, Blotting, Western, Cell Cycle Proteins, Spindle Apparatus, Microtubules, Biochemistry, Spindle pole body, Microtubule polymerization, Fungal Proteins, Tubulin, Microtubule, Animals, Humans, Kinetochores, Molecular Biology, Microtubule nucleation, biology, Kinetochore, Calcium-Binding Proteins, Nuclear Proteins, DNA, Cell Biology, Flow Cytometry, Cell biology, Spindle checkpoint, Microscopy, Fluorescence, biology.protein, Cattle, Carrier Proteins, HeLa Cells
Abstract

We have previously identified the opium alkaloid noscapine as a microtubule interacting agent that binds stoichiometrically to tubulin and alters its conformation. Here we show that, unlike many other microtubule inhibitors, noscapine does not significantly promote or inhibit microtubule polymerization. Instead, it alters the steady-state dynamics of microtubule assembly, primarily by increasing the amount of time that the microtubules spend in an attenuated (pause) state. Further studies reveal that even at high concentrations, noscapine does not alter the tubulin polymer/monomer ratio in HeLa cells. Cells treated with noscapine arrest at mitosis with nearly normal bipolar spindles. Strikingly, although most of the chromosomes in these cells are aligned at the metaphase plate, the rest remain near the spindle poles, both of which exhibit loss of tension across kinetochore pairs. Furthermore, levels of the spindle checkpoint proteins Mad2, Bub1, and BubR1 decrease by 138-, 3.7-, and 3.9-fold, respectively, at the kinetochore region upon chromosome alignment. Our results thus suggest that an exquisite control of microtubule dynamics is required for kinetochore tension generation and chromosome alignment during mitosis. Our data also support the idea that Mad2 and Bub1/BubR1 respond to kinetochore-microtubule attachment and/or tension to different degrees.

Published
2002

13. Sustained Activation of p34 Is Required for Noscapine-induced Apoptosis

Author

Harish C. Joshi, Keqiang Ye, Jaren W. Landen, Jun Zhou, and E. Morton Bradbury

Subjects
Cyclin-dependent kinase 1, Kinase, Mutant, Cell Biology, Transfection, Biology, Biochemistry, Noscapine, Cell biology, Apoptosis, medicine, Signal transduction, Molecular Biology, Mitosis, medicine.drug
Abstract

Mitotic arrest and subsequent apoptosis has been observed in many types of cells treated with anti-microtubule agents. However, the molecular mechanisms underlying the two events as well as their relationship are not well understood; on the contrary, there has been increasing evidence indicating that anti-microtubule agents might induce apoptosis via signaling pathways independent of mitosis. In this study, we found that apoptosis induced by noscapine, an anti-microtubule drug previously shown to cause both mitotic arrest and apoptotic cell death, was blocked by inhibiting p34 cdc2 activity with olomoucine in FM3A murine mammary carcinoma cells or by reducing the level and activity of p34 cdc2 in a mutant cell line FT210 derived from FM3A. Furthermore, transfection of the mutant FT210 cells with wild-type p34cdc2 restored their ability to undergo mitotic arrest and then apoptosis in response to noscapine. Thus, we conclude that sustained activation of the p34 cdc2 kinase during mitotic arrest is required for subsequent apoptosis induced by noscapine, establishing a link between the two events.

Published
2001

14. Safety and pharmacology of ponezumab (PF-04360365) after a single 10-minute intravenous infusion in subjects with mild to moderate Alzheimer disease

Author

Joel Ross, Qinying Zhao, James Kupiec, Martin M. Bednar, Fred McCush, Jaren W. Landen, Scot Styren, Wendy Ma, Aaron H. Burstein, and Christine Alvey

Subjects
Male, Time Factors, Pharmacology, Antibodies, Monoclonal, Humanized, law.invention, Lethargy, Cerebrospinal fluid, Ponezumab, Pharmacokinetics, Randomized controlled trial, Double-Blind Method, law, Alzheimer Disease, Medicine, Humans, Pharmacology (medical), Adverse effect, Infusions, Intravenous, Aged, Volume of distribution, Aged, 80 and over, business.industry, Middle Aged, Pharmacodynamics, Anesthesia, Female, Neurology (clinical), business, Follow-Up Studies
Abstract

Objective Ponezumab (PF-04360365) is a humanized anti-amyloid beta (Aβ) monoclonal antibody designed for treatment of Alzheimer disease (AD). A single 2-hour intravenous infusion of 0.1 to 10 mg/kg was previously shown to be safe and well tolerated in subjects with mild to moderate AD, with measurable effects on plasma and cerebrospinal fluid Aβ. This phase I, dose-escalation, open-label study evaluated the safety, pharmacokinetics, and pharmacodynamics of a single 10-minute intravenous infusion. Methods Subjects with mild to moderate AD received ponezumab 1 mg/kg (n = 3), 3 mg/kg (n = 3), 5 mg/kg (n = 4), or 10 mg/kg (n = 5). They were followed up as outpatients for 6 months. Results All subjects completed the trial. Ponezumab was safe and well tolerated with no deaths, withdrawals, or drug-related moderate, severe, or serious adverse events. Mild drug-related adverse events included headache (3 patients) and lethargy and hypoesthesia (both in 1 patient). No infusion reactions, clinically meaningful laboratory abnormalities, vital sign changes, electrocardiographic changes, or antidrug antibodies were detected. There was no evidence of brain microhemorrhage, vasogenic edema, encephalitis, or other imaging abnormality. Cognitive function showed no treatment-related trends. Ponezumab displayed approximately dose-proportional increases in plasma exposure. Steady-state volume of distribution was 113 to 172 mL/kg, clearance was 2.7 to 3.0 mL/d/kg, and terminal half-life was 35 to 52 days. Plasma maximum observed concentration and the area under the plasma concentration-time profile from time 0 extrapolated to infinite time of Aβ(1-x) and Aβ(1-40) increased dose-dependently. Conclusions Administration of ponezumab as a 10-minute infusion was safe and well tolerated and produced effects on plasma Aβ species comparable with a 2-hour infusion. Shorter infusions may provide more flexibility, comfort, and convenience for patients and caregivers.

Published
2013

15. P1‐012: Effect of ponezumab on CSF biomarkers: Pooled analysis of phase IIa studies in subjects with mild‐to‐moderate Alzheimer's disease

Author

Kelly R. Bales, Kaj Blennow, Jaren W. Landen, Brendon Binneman, Kathryn Wright, Carol Cronenberger, Pam Schwartz, Henrik Zetterberg, Nathan Chen, and Scot Styren

Subjects
medicine.medical_specialty, Epidemiology, business.industry, Health Policy, Disease, Gastroenterology, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Pooled analysis, Ponezumab, Developmental Neuroscience, Internal medicine, Csf biomarkers, medicine, Neurology (clinical), Geriatrics and Gerontology, business
Published
2012

16. P4‐208: Safety, efficacy, pharmacokinetics and pharmacodynamics of multiple doses of Ponezumab in subjects with mild‐to‐moderate Alzheimer's disease

Author

Catherine Sattler, Aaron H. Burstein, Scot Styren, Clare B. Billing, Carol Cronenberger, Martin M. Bednar, Sharon Cohen, Jae-Hong Lee, Jaren W. Landen, and Clifford R. Jack

Subjects
Epidemiology, business.industry, Health Policy, Disease, Pharmacology, Multiple dosing, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Ponezumab, Developmental Neuroscience, Pharmacokinetics, Medicine, Neurology (clinical), Geriatrics and Gerontology, business
Published
2012

17. P4‐209: Safety, tolerability, pharmacokinetics and pharmacodynamics of monthly and quarterly doses of Ponezumab (PF‐04360365) in subjects with mild‐to‐moderate Alzheimer's disease

Author

Brendon Binneman, Pam Schwartz, Niels Andreasen, Carol Cronenberger, Catherine Sattler, Martin M. Bednar, James Kupiec, Henrik Östlund, Anne Börjesson-Hanson, and Jaren W. Landen

Subjects
Epidemiology, business.industry, Health Policy, Safety tolerability, Disease, Pharmacology, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Ponezumab, Developmental Neuroscience, Pharmacokinetics, Medicine, Neurology (clinical), Geriatrics and Gerontology, business
Published
2012

18. P2‐372: The prevalence of brain microhemorrhages and infarcts in a cohort of patients with mild‐to‐moderate Alzheimer's disease

Author

JClifford R. Jack, Denise A. Reyes, Jaren W. Landen, Catherine Sattler, Matt A. Bernstein, James T. Kupiec, Kajal Kantarci, Martin M. Bednar, Brett J. Borowski, and Aaron H. Burstein

Subjects
Pediatrics, medicine.medical_specialty, Epidemiology, business.industry, Health Policy, Disease, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Cohort, medicine, Neurology (clinical), Geriatrics and Gerontology, business
Published
2010

19. P4‐118: Safety and Pharmacokinetics Following a Single Infusion of the Anti‐amyloid Monoclonal Antibody Ponezumab (pf‐04360365) in Patients With Mild‐to‐moderate Alzheimer's Disease: Final Results

Author

James Kupiec, Qinying Zhao, Michael Borrie, Martin M. Bednar, Jaren W. Landen, Clare B. Billing, Christine Alvey, Sharon Cohen, and Michael Woodward

Subjects
Amyloid, Epidemiology, business.industry, medicine.drug_class, Health Policy, Disease, Pharmacology, Monoclonal antibody, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Ponezumab, Developmental Neuroscience, Pharmacokinetics, Medicine, In patient, Neurology (clinical), Geriatrics and Gerontology, business
Published
2010

20. O3‐07‐05: Pharmacokinetics and pharmacodynamics of ponezumab (PF‐04360365) following a single‐dose intravenous infusion in patients with mild to moderate Alzheimer's disease

Author

Frederick McCush, Aaron H. Burstein, Clare B. Billing, Christine Alvey, Jaren W. Landen, Qinying Zhao, Martin M. Bednar, James Kupiec, and Wendy Ma

Subjects
Epidemiology, business.industry, Health Policy, Disease, Pharmacology, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Ponezumab, Developmental Neuroscience, Pharmacokinetics, Medicine, In patient, Neurology (clinical), Geriatrics and Gerontology, business
Published
2010

21. P3‐451: Enhancing global reliability of the ADAS‐cog and MMSE: part 1‐the harmonization/standardization project of word lists and phrases

Author

SangYun Kim, William R. Lenderking, Elias Schwam, Daniella Mulder, Rob Goldman, Rebecca Evans, and Jaren W. Landen

Subjects
Standardization, Epidemiology, business.industry, Computer science, Health Policy, Harmonization, computer.software_genre, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Adas cog, Neurology (clinical), Artificial intelligence, Geriatrics and Gerontology, business, computer, Word (computer architecture), Reliability (statistics), Natural language processing
Published
2010

22. P1‐459: IP/MS analysis of human CSF Aβ following a single dose of the C‐terminal anti‐Aβ antibody ponezumab (PF‐04360365) to Alzheimer patients

Author

Kieran F. Geoghegan, Kelly R. Bales, James J. Conboy, Kathleen M. Wood, Robert A. Durham, Martin M. Bednar, Frederick McCush, Jaren W. Landen, and Barbara Tate

Subjects
biology, Epidemiology, business.industry, Health Policy, Ms analysis, Pharmacology, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Ponezumab, Developmental Neuroscience, biology.protein, Medicine, Neurology (clinical), Geriatrics and Gerontology, Antibody, business
Published
2010

24. P3‐450: Safety and pharmacokinetics following a single 10‐minute intravenous infusion of the anti‐amyloid mAb ponezumab (PF‐04360365) in patients with mild to moderate Alzheimer's disease

Author

Joel Ross, Wendy M. Ma, Frederick McCush, Aaron H. Burstein, Martin M. Bednar, James T. Kupiec, Christine Alvey, Qinying Zhao, Scot Styren, and Jaren W. Landen

Subjects
Amyloid, Epidemiology, medicine.drug_class, business.industry, Health Policy, Disease, Pharmacology, Monoclonal antibody, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Ponezumab, Developmental Neuroscience, Pharmacokinetics, medicine, In patient, Neurology (clinical), Geriatrics and Gerontology, business
Published
2010

25. O4‐04‐03: Safety and pharmacokinetics of the anti‐amyloid monoclonal antibody PF‐04360365 following a single infusion in patients with mild‐to‐moderate Alzheimer's disease: Preliminary results

Author

Kevin Rohrbacher, Qinying Zhao, Clare B. Billing, Martin M. Bednar, James Kupiec, and Jaren W. Landen

Subjects
Amyloid, Epidemiology, business.industry, medicine.drug_class, Health Policy, Disease, Pharmacology, Monoclonal antibody, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Pharmacokinetics, Medicine, In patient, Neurology (clinical), Geriatrics and Gerontology, business
Published
2009

26. P1‐262: Preliminary population pharmacokinetic modeling of PF‐04360365, a humanized anti‐amyloid monoclonal antibody, in patients with mild‐to‐moderate Alzheimer's disease

Author

Qinying Zhao, Martin M. Bednar, Rene Laurencot, Timothy Nicholas, Clare B. Billing, William Knebel, Jaren W. Landen, James Kupiec, Brian Corrigan, and Marc R. Gastonguay

Subjects
education.field_of_study, Amyloid, Epidemiology, medicine.drug_class, business.industry, Health Policy, Population, Pharmacokinetic modeling, Disease, Monoclonal antibody, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Immunology, medicine, In patient, Neurology (clinical), Geriatrics and Gerontology, education, business
Published
2009

27. Pregabalin bei HIV-Infektion

Author

Birol Emir, M L Chew, Andrew S.C. Rice, Jaren W. Landen, David Semel, J Sporn, and David M. Simpson

Subjects
Gynecology, Double blind, medicine.medical_specialty, business.industry, medicine, virus diseases, business
Abstract

Bei Patienten mit einer HIV-Infektion kommt es haufig zu einer peripheren, symmetrischen, distal beginnenden sensorischen Neuropathie, resultierend aus einer Nervenschadigung durch das Virus selbst oder durch die antiretrovirale Therapie. Pregabalin hat sich bei einigen Neuropathien als wirksam erwiesen, doch wirkt es auch bei der HIV-Neuropathie?

Published
2015

28. Noscapine alters microtubule dynamics in living cells and inhibits the progression of melanoma

Author

Jaren W, Landen, Roland, Lang, Steve J, McMahon, Nasser M, Rusan, Anne-Marie, Yvon, Ashley W, Adams, Mia D, Sorcinelli, Ross, Campbell, Paola, Bonaccorsi, John C, Ansel, David R, Archer, Patricia, Wadsworth, Cheryl A, Armstrong, and Harish C, Joshi

Subjects
Mice, Inbred C57BL, Noscapine, Mice, Disease Progression, Melanoma, Experimental, Administration, Oral, Animals, Antineoplastic Agents, Female, Microtubules, Cell Division
Abstract

Cellular microtubules, polymers of tubulin, alternate relentlessly between phases of growth and shortening. We now show that noscapine, a tubulin-binding agent, increases the time that cellular microtubules spend idle in a paused state. As a result, most mammalian cell types observed arrest in mitosis in the presence of noscapine. We demonstrate that noscapine-treated murine melanoma B16LS9 cells do not arrest in mitosis but rather become polyploid followed by cell death, whereas primary melanocytes reversibly arrest in mitosis and resume a normal cell cycle after noscapine removal. Furthermore, in a syngeneic murine model of established s.c. melanoma, noscapine treatment resulted in an 85% inhibition of tumor volume on day 17 when delivered by gavage compared with untreated animals (Por= 0.01), without evidence of toxicity to the spleen, liver, duodenum, bone marrow, or peripheral blood. This inhibition was greater than that seen in vivo by paclitaxel (Taxol) alone and similar to the inhibition of tumor volume observed when noscapine was combined with paclitaxel. Importantly, noscapine also demonstrated the ability to significantly inhibit melanoma progression by 83% on day 18 when delivered in drinking water (Por= 0.01) and conferred a significant survival advantage (Por= 0.01). Our results demonstrate that p.o.-administered noscapine significantly inhibits the progression of melanoma cells through alterations in microtubule dynamics, with no detected toxicity to the host. Consequently, noscapine could be a valuable chemotherapeutic agent, alone or in combination, for the treatment of advanced melanoma.

Published
2002

29. THU0321 A Randomized Controlled Study of Pregabalin in Patients with Fibromyalgia and Comorbid Depression Taking Concurrent Antidepressant Medication

Author

Joseph Driscoll, Lynne Pauer, Lesley M. Arnold, Joseph M. Scavone, P. Bhadra Brown, Jaren W. Landen, Piercarlo Sarzi-Puttini, Andrew Clair, Tahira Khan, and Pierre Arsenault

Subjects
medicine.medical_specialty, business.industry, Immunology, Pregabalin, Citalopram, medicine.disease, Placebo, Hospital Anxiety and Depression Scale, General Biochemistry, Genetics and Molecular Biology, law.invention, chemistry.chemical_compound, Rheumatology, Randomized controlled trial, chemistry, law, Anesthesia, Fibromyalgia, Internal medicine, medicine, Immunology and Allergy, Major depressive disorder, Duloxetine, business, medicine.drug
Abstract

Background Depression is often comorbid with fibromyalgia (FM) and many FM patients (pts) take antidepressants for their depression. Managing FM pain in these pts is important. Objectives To determine the efficacy and safety of pregabalin (PGB) for FM pain in FM pts taking a serotonin specific reuptake inhibitor (SSRI) or a serotonin/norepinephrine reuptake inhibitor (SNRI) for comorbid depression. Methods This was a randomized, 2-way crossover, double-blind, placebo (PBO)-controlled study comprising two 6-week treatment periods separated by a 2-week, single-blind taper/washout phase. Pts were randomized 1:1 to PGB/PBO or PBO/PGB. PGB starting dose was 150mg/d, optimized to 300 or 450mg/d (twice-daily allocation). Stable SSRI or SNRI medication was taken throughout. The primary efficacy endpoint was mean pain score (0–10 numeric rating scale) based on the mean of the last 7 daily pain scores. Secondary endpoints included: number of 30% and 50% pain responders; Hospital Anxiety and Depression Scale – Anxiety and Depression (HADS-A and HADS-D); Fibromyalgia Impact Questionnaire (FIQ); Subjective Sleep Questionnaire (SSQ); Patient Global Impression of Change (PGIC); and EuroQoL 5-Dimension (EQ-5D). Results 197 pts were randomized; 181 received ≥1 dose of PGB and 177 PBO. At baseline, 84 (43.5%) pts had major depressive disorder, 101 (52.3%) depression not otherwise specified and 8 (4.2%) dysthymia; the mean ± SD HADS-D score was 8.0±3.6, indicating mild depression. 101 (52.3%) pts were taking an SSRI and 92 (47.7%) an SNRI; the commonest were duloxetine (31.6%) and citalopram (16.6%). The mean ± SD pain score was 6.7±1.2. At endpoint, the least squares mean ± SE pain score was significantly lower with PGB (4.84±0.15) vs. PBO (5.45±0.16; difference -0.61; 95% confidence interval [CI] -0.91,-0.31; p=0.0001). Mean pain scores were significantly lower with PGB in pts taking an SSRI (difference -0.48; 95% CI -0.89,-0.07; p=0.0211) or an SNRI (difference -0.76; 95% CI -1.21,-0.31; p=0.0012). Significantly more PGB- vs. PBO-treated pts were 30% (45.3% vs. 27.7%; p=0.0007) and 50% (26.0% vs. 15.8%; p=0.0205) pain responders. PGB also significantly improved HADS-D (difference -0.88; 95% CI -1.37,-0.39; p=0.0005), HADS-A (difference -0.95; 95% CI -1.40,-0.50; p Conclusions In pts with FM taking an SSRI or SNRI for comorbid depression, PGB significantly improved FM pain vs. PBO. The safety profile of PGB in these pts was consistent with previous studies and current product labelling. Acknowledgements This study was funded by Pfizer Inc. Medical writing support was provided by David Cope PhD, of Engage Scientific Solutions, and funded by Pfizer Inc. Disclosure of Interest : P. Sarzi-Puttini Consultant for: Abbvie, Bristol-Myers Squibb, Merck Sharp & Dohme, Pfizer Inc, Roche, L. Arnold Consultant for: Pfizer Inc, Eli Lilly and Company, Takeda, AstraZeneca, Forest Laboratories, Theravance, Dainippon Sumitomo Pharma, Daiichi Sankyo, Purdue Pharma L.P., Shire and Tonix Pharmaceuticals, P. Arsenault Consultant for: Pfizer Canada, Speakers bureau: Pfizer Inc, Purdue Pharma, Valeant Pharmaceuticals, Eli Lilly and Company and Janssen (Canada), T. Khan Shareholder of: Pfizer Inc, Employee of: Pfizer Inc, P. Bhadra Brown Shareholder of: Pfizer Inc, Employee of: Pfizer Inc, A. Clair Shareholder of: Pfizer Inc, Employee of: Pfizer Inc, J. Scavone Shareholder of: Pfizer Inc, Employee of: Pfizer Inc, J. Driscoll Consultant for: Pfizer Inc, J. Landen Shareholder of: Pfizer Inc, Employee of: Pfizer Inc, L. Pauer Shareholder of: Pfizer Inc, Employee of: Pfizer Inc DOI 10.1136/annrheumdis-2014-eular.4084

Published
2014

30. (395) Pregabalin improves fibromyalgia symptoms in patients with fibromyalgia and comorbid depression receiving antidepressant medication: results from a randomized, 2-way crossover, double-blind, placebo-controlled study

Author

Pierre Arsenault, Piercarlo Sarzi-Puttini, Tahira Khan, Lynne Pauer, Andrew Clair, Lesley M. Arnold, P. Bhadra Brown, Jaren W. Landen, and Joseph Driscoll

Subjects
medicine.medical_specialty, business.industry, Pregabalin, Placebo-controlled study, medicine.disease, Double blind, Antidepressant medication, Anesthesiology and Pain Medicine, Neurology, Fibromyalgia, medicine, Physical therapy, In patient, Neurology (clinical), business, Psychiatry, Depression (differential diagnoses), medicine.drug
Published
2014

31. Reply to Comments by Dr Hashimoto

Author

Sheldon H. Preskorn, Sheela Kolluri, Michael Krams, Bryan Baker, Frank S. Menniti, and Jaren W. Landen

Subjects
Psychiatry and Mental health, Pharmacology (medical)
Published
2009

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