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Market Research Report

Neurogenomics and Neurotherapeutic Strategies: New Directions in Platforms, Targets, and Therapeutic Approaches

Published by Insight Pharma Reports Contact us : +1-860-674-8796
Published 2005/03 Content info 296 pages
Product code 25781
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Description TOC

Table of Contents

Chapter 1. Introduction

  • 1.1 Alzheimers Disease
  • 1.2 Parkinsons Disease
  • 1.3 Amyotrophic Lateral Sclerosis
  • 1.4 Schizophrenia
  • 1.5 Depression
  • 1.6 Bipolar Disorder
  • 1.7 Conclusion
  • Part 1. Neurological Diseases

Chapter 2. Alzheimers Disease

  • 2.1 Epidemiology of Alzheimers Disease
  • 2.2 Types of Dementia
  • -Parkinsons Disease
  • -Diffuse Lewy Body Disease
  • -Vascular Dementia
  • -Multi-Infarct Dementia
  • -Subcortical Vascular Dementia
  • -Frontal Lobe Dementia and Picks Disease
  • -Huntingtons Disease
  • 2.3 Etiology and Pathophysiology: How the AD Brain Works
  • 2.4 The Genetics of AD
  • -Classification of AD Types Based on Genetic Inheritance
  • -Genes Involved in Early- and Late-Onset AD
  • --The Apolipoprotein E (APOE) Gene
  • --The GSTO1 Gene and Age of Onset of AD
  • 2.5 AD Therapeutics
  • -Cholinesterase Inhibitors: The Gold Standard for Mild-to-Moderate AD
  • -Treatment for Moderate to Severe AD: The Glutamate Pathway
  • -Investigative Therapies for AD
  • --Axonyxs Phenserine
  • --Cortex Pharmaceuticals CX516
  • --Ceregenes Nerve Growth Factor (NGF)
  • --Neurochems Alzhemed
  • --Targacepts NNRs
  • --Memory Pharmaceuticals Compounds
  • --Myriad Genetics Compounds
  • --Eunoes COGNIShunt: A Medical Device
  • --Prana Biotechnologys PTB-1 Compound
  • --Praecis Pharmaceuticals Apan
  • --ReGen Therapeutics Colostrinin
  • --Acumen Pharmaceuticals ADDL Mechanism
  • --Sanofi-Synthelabo
  • --GlaxoSmithKline
  • --Wyeth
  • --Bristol-Myers Squibb
  • --Forest Laboratories
  • --Boehringer-Ingelheim Pharmaceuticals
  • --Hoffmann-La Roche
  • -Alternative Treatments for Alzheimers Disease
  • --Coenzyme Q10 or Ubiquinone
  • --Ginkgo biloba
  • --Huperzine A
  • --Phosphatidylserine
  • --Vitamin E
  • --Other Naturopathic Treatments
  • 2.6 Early-Stage Tools and Approaches Used in Alzheimers R&D
  • -A Urine Test to Detect AD
  • -The Trojan Horse Strategy
  • -Notch-Protein Signaling Cascade
  • -Transthyretin Protein
  • -Samaritan Pharmaceuticals Neuroprotective Compound SP-33
  • -Biomarkers for AD
  • --CCR1 As a Biomarker
  • --The M266 Biomarker for Amyloid in the Blood
  • --A Biomarker Panel for AD Detection
  • -Vaccines for AD
  • --Elans AN-1792 Vaccine (Suspended)
  • --Oral Vaccine Developed
  • -Repurposing Other Drugs for AD
  • --Clioquinol: An Antibiotic
  • --Lithium Shows Promise in AD Mouse Model
  • --Lipitor and Other Statins
  • -Cell Therapy
  • -In Vitro Brain Slice Techniques
  • -The Role of Fyn in Synaptic Impairment
  • 2.6 R&D Platforms
  • -Molecular Imaging
  • --Positron Emission Tomography (PET)
  • --Pittsburgh Compound B
  • --FDDNP
  • --Applications of PET in Drug Efficacy Testing
  • -Selected Imaging Initiatives Focusing on AD
  • --The NIAs Neuroscience and Neuropsychology of Aging Program
  • --The Alzheimers Disease Neuroimaging Initiative
  • --The UCLA Neuroimaging Lab
  • --Li-Cor Biosciences Odyssey Infrared Imaging System for AD
  • -Animal Models of AD
  • --APP Models
  • --PS1 Models
  • --Transgenic Mice
  • --Transgenic Flies
  • -Companies and Organizations and Their AD Animal Models
  • --Tranzyme Pharmas TranzExpression Technology
  • --Neuromes Analysis of Elans Mouse Model of AD
  • --Baylor College of Medicines VGLUT1 Knockout Mice
  • --Harvard Medical Schools p25 and Cdk5 mouse model
  • --Johns Hopkins Universitys Mouse Model of BACE1 Inhibition
  • --University of California at Irvines Triple Transgenic Mice

Chapter 3. Parkinsons Disease

  • 3.1 Epidemiology of PD
  • 3.2 Etiology and Pathology of PD
  • 3.3 Symptoms of PD
  • -Tremor
  • -Rigidity
  • -Bradykinesia
  • -Postural Instability
  • 3.4 The Genetics of PD
  • -Genetic Risk Factors
  • -Mitochondrial Impairment
  • -Genes for Early-Onset PD
  • -Genes for Late-Onset PD
  • 3.5 Other Theories of Etiology
  • -Oxidative Neuronal Damage
  • -Smoking and Coffee
  • -Free-Radical Theory
  • -Endogenous and Exogenous Toxins
  • 3.6 Parkinsonism: Conditions That Mimic PD
  • -Postencephalitic Parkinsonism
  • -Drug-Induced Parkinsonism
  • -Striatonigral Degeneration
  • -Arteriosclerotic Parkinsonism
  • -Toxin-Induced Parkinsonism
  • -Parkinsonism-Dementia Complex of Guam
  • -Parkinsonism Accompanying Other Conditions
  • 3.7 Parkinsons Disease Therapeutics
  • -Levodopa-Carbidopa: The Gold-Standard Treatment
  • -Other Leading Therapeutic Classes
  • --Dopamine Agonists
  • --Selegiline
  • --Anticholinergic Drugs
  • --Amantadine
  • --COMT Inhibitors
  • -Improvements on Current Therapies
  • --Tolcapone Combination Therapy
  • --Parcopa Orally Disintegrating Tablets
  • -Investigational Treatments for Parkinsons Disease
  • --Newron Pharmaceuticals Safinamide
  • --Aderis Pharmaceuticals SPM-962 (Rotigotine)
  • --Avigens AV-201 Gene Therapy Approach
  • --Ceregenes GDNF Gene Delivery Approach
  • --Acadia Pharmaceuticals ACP-103
  • --Boston Life Sciences Altropane Imaging Agent
  • --Cephalons CEP-1347
  • --Neurologixs NLX-P101 Gene Therapy
  • --Schering-Ploughs Adenosine-2a Antagonist
  • --Teva Neuroscience/Eisais Agilect (Rasagiline mesylate)
  • --Titan Pharmaceuticals Speramine
  • --Guilford Pharmaceuticals Neuroimmunophilin Ligands
  • --GlaxoSmithKlines ReQuip
  • 3.8 Surgical Procedures to Treat Parkinsons Disease
  • -Lesioning Techniques
  • -Deep-Brain Stimulation
  • -Activa Tremor Control System
  • 3.9 Investigative Pathways and Techniques
  • -The Dopamine Degeneration Theory of PD
  • --MPTP As an Investigative Tool
  • --Dopamine Transporter Malfunction
  • --Novel Dopamine Receptors
  • --Dopamine Implants
  • --PET Scanning of Dopamine Receptors
  • --Controlled-Release Formulas and Implantable Pumps
  • -Cellular Implant Therapies
  • --Nerve Cell Implantation
  • --LEAPS: Encapsulated Cell Delivery of GDNF
  • --Stem-Cell Approaches
  • -The Inflammation Model of PD
  • -Sonic Hedgehog and Gli-1 Proteins
  • 3.10 Animal Models Platforms in PD
  • -Transgenic Mice and Other Nonprimate Models: Applications and Limitations
  • -Nonhuman Primate Models
  • -Toxin Models
  • --MPTP
  • --6-OHDA
  • --Rotenone
  • -Gene-Knockout and Transgenic Animals

Chapter 4. Amyotrophic Lateral Sclerosis

  • 4.1 Epidemiology of ALS
  • 4.2 Etiology, Pathophysiology, and Genetic Components of ALS
  • -SOD1: The First ALS Gene
  • -ALS2
  • -ALS4
  • -Linkage to Chromosome 16
  • -Other ALS Gene Mutations
  • -Neurofilament Gene Mutations in Sporadic ALS
  • 4.3 ALS Therapeutics
  • -Riluzole: The Gold-Standard Treatment for ALS
  • -Other Treatments for ALS
  • --Colchicine
  • --Fluorouracil (Pfizers Adrucil)
  • -Investigational Treatments for ALS
  • --CytRxs RNAi Gene-Silencing Technology
  • --Ceregene and Chirons IGF-1 Gene Therapy Programs
  • --Ceftriaxone, Promethazine, and Ebselen
  • -Compounds Under Investigation at the ALS Therapy Development Foundation
  • --Lantus
  • --Insulin ICV
  • --Long-Acting IGF-1
  • --Trehalose
  • --Nelfinavir
  • --Guanidine hydrochloride
  • --TNF-alpha
  • --Polyamines
  • --Counting Neurons
  • 4.4 Early-Stage Approaches in ALS R&D
  • -The Oxidative Stress Model
  • -The SOD1 Toxin Model
  • -Regenerating Axons via Nogo Inhibition
  • -SOD1 Mutations: Neuronal Aggregates and Abnormal Protein Folding
  • 4.5 Tools and Platforms for Discovery
  • -Biomarkers
  • -Stem Cells
  • --The Challenge to the Use of Stem Cells in ALS
  • --Olfactory Bulb Stem Cells
  • --Olfactory Neural Stem Cells in the Mouse Model for ALS
  • --Spinal Cord Stem Cells
  • -The Role of Astrocytes in Neuronal Degeneration
  • -Peripherin and the Role of Toxic Splice Variants in ALS
  • -Gene Therapy
  • -Trophic Factors
  • --IGF-1
  • --Autoimmunity and IgG
  • --VEGF
  • -Animal Models
  • --The SOD1 Transgenic Mouse Model of ALS
  • --The Wobbler Mouse
  • --Candida albicans
  • --Reintroduction of Stem-Cell-Generated Motor Neurons into an ALS Rat
  • --Model
  • --The SOD1 C. elegans Model
  • --Zebrafish Model

Part 2. Psychiatric Disorders

Chapter 5. Schizophrenia

  • 5.1 Epidemiology of Schizophrenia
  • 5.2 Types of Schizophrenia and Related Illnesses
  • -Paranoid Schizophrenia
  • -Disorganized (Hebephrenic) Schizophrenia
  • -Catatonic Schizophrenia
  • -Residual Schizophrenia.
  • -Schizoaffective Disorder
  • -Undifferentiated Schizophrenia.
  • -Differential Diagnosis: Bipolar Disorder (Manic Depression)
  • 5.3 Pathophysiology of Schizophrenia
  • 5.4 Manifestations and Symptoms
  • -Manifestations
  • -Symptomatology
  • --Distorted Perceptions of Reality
  • --Hallucinations and Illusions
  • --Delusions
  • --Disordered Thinking
  • --Emotional Expression
  • 5.5 Genetic Basis of Schizophrenia
  • -Genetic Predisposition
  • -Familial Linkage
  • -Genes Discovered
  • -Key Genes Involved
  • --Dysbindin-1
  • --Neuregulin-1 (NRG1)
  • --ERBB3
  • --G30, G72, and DAO
  • --RGS4
  • --COMT
  • --PRODH
  • Conclusion
  • 5.6 Schizophrenia Therapeutics
  • -Currently Marketed Antipsychotic Drugs
  • -Companies with Therapeutics Under Investigation
  • --GlaxoSmithKline
  • --Wyeth
  • --Targacept
  • --American Biogenetic Sciences
  • --NPS Pharmaceuticals
  • --Cortex Pharmaceuticals
  • --deCODE genetics
  • --Acadia Pharmaceuticals
  • --Potomac Pharma and the Stanley Medical Research Institute
  • 5.7 Mechanisms of Action and Pathways Under Investigation
  • -Glutamate and Dopamine Neurotransmitter Systems
  • -Glutamate Receptor: GRM
  • -Linkage Mapping Studies
  • -Research at the Mental Health Research Institute
  • --Brain Scans
  • --The Muscarinic Receptors
  • --Serotonin Receptors
  • --Benzodiazepine Binding Sites
  • --Role of Apolipoproteins
  • --Protein S100b
  • --High-Throughput Screening to Identify Genes Involved in
  • --Schizophrenia Pathology
  • --Brain Serotonin
  • --Abnormal Eye Movements
  • --Unraveling Endophenotypes
  • --New Dynamic Imaging Techniques for Studying Schizophrenia
  • --Brain Imaging
  • --The Endocannabinoid System
  • --PKC Overactivation
  • --Glycine Transporters
  • --Prenatal Evidence of Schizophrenia As a Developmental Disorder
  • --Early Biochemical Changes
  • 5.8 Animal Models
  • -Prepulse Inhibition in Mice and Rats
  • -Administration of Hallucinogens in Animal Models
  • -Blocking NMDA Receptors in Animal Models
  • -Mice Lacking the Brain Protein Calcineurin

Chapter 6. Major Depression

  • 6.1 Epidemiology
  • 6.2 Types of Depression
  • -Dysthymia
  • -Bipolar Depression
  • -Seasonal Affective Disorder
  • 6.3 Symptoms
  • 6.4 Causes of Major Depression
  • -The Monoamine Theory
  • 6.5 Therapeutic Classes for Depression
  • -Marketed Therapeutic Treatments
  • --Tricyclic Antidepressants
  • --Monoamine Oxidase Inhibitors
  • --Selective Serotonin Reuptake Inhibitors
  • --Serotonin and Norepinephrine Reuptake Inhibitors
  • --Bupropion
  • -Therapeutics Under Investigation
  • --Neurocrine Biosciences: Corticotropin-Releasing Factor
  • --Pherin Pharmaceuticals
  • --Targacept
  • --Wyeth
  • --GlaxoSmithKline
  • --Pfizer
  • --Sanofi-Synthelabo
  • --AstraZeneca
  • --Aventis Pharmaceuticals
  • --Eli Lilly
  • --Forest Laboratories
  • --Lexicon Genetics
  • --Somerset Pharmaceuticals
  • -Alternative Treatments
  • --Psychotherapy
  • --Cognitive-Behavioral Therapy
  • --Interpersonal Therapy
  • --Electroconvulsive Therapy
  • 6.6 New Genes Discovered
  • -TPH2 Isoform
  • -A New Gene Discovery: CHRM2
  • -NIMH Research Efforts
  • -University of Pittsburgh Research Efforts: Locating Chromosomal
  • -Regions
  • -CREB1 Gene
  • -Susceptibility Gene
  • 6.7 Mechanisms of Action and Pathways Under Investigation
  • -Fibroblast Growth Factors
  • -Blocking Neuron Formation
  • 6.8 Tools and Platforms Used to Study Depression
  • -Imaging Technologies
  • --Brain Imaging
  • --PET Technology
  • Animal Models
  • -Catecholamine Deficiency
  • -Learned Helplessness
  • -Behavioral Despair

Chapter 7. Bipolar Disorder

  • 7.1 Epidemiology
  • 7.2 Symptoms
  • -Hypomania
  • -Psychosis
  • 7.3 Types of Bipolar Disorder
  • 7.4 Causes of Bipolar Disorder
  • 7.5 Bipolar Disorder Treatments
  • -Currently Marketed Treatments
  • --Mood Stabilizers
  • --Antiseizure Medications
  • --Antidepressants
  • --Atypical Antipsychotics
  • --Psychotropics
  • -Psychosocial Interventions
  • -Alternative Treatments
  • --Electroconvulsive Therapy
  • --Herbal Remedies
  • 7.6 Genetic Elements and Investigational Methods and Approaches
  • -DARPP-32, PENK, and TAC1
  • -G-Protein Receptor Kinase 3
  • -Other GRK3 Gene Evidence
  • -GSK-3 Inhibition
  • -Brain-Imaging Studies
  • -Benzodiazepine Binding Sites
  • -Protein S100b
  • -LifeShirt System for Monitoring Cardiopulmonary Parameters
  • -Fine Mapping in Candidate Chromosomal Regions
  • -Scanning Genes for Variation

Part 3. Companies and Pipelines

Chapter 8. Therapeutics in Development

  • Introduction
  • 8.1 Company Profiles: Company Focus; Targets and Technology; In the Pipeline
  • -Ceregene
  • -NPS Pharmaceuticals
  • -Targacept
  • -Cortex Pharmaceuticals
  • -Neurocrine Biosciences
  • -Neurochem
  • -Lexicon Genetics
  • -Avigen
  • -Neurologix
  • -CytRx
  • -Cephalon
  • -Newron Pharmaceuticals
  • -deCODE genetics
  • -Acadia Pharmaceuticals
  • -Prana Biotechnology
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