Journal
/
Médecine
/
Gene-environment Interaction Models to Unmask Susceptibility Mechanisms in Parkinson’s Disease
Journal JoVE
Médecine
Un abonnement à JoVE est nécessaire pour voir ce contenu.  Connectez-vous ou commencez votre essai gratuit.
Journal JoVE Médecine
Gene-environment Interaction Models to Unmask Susceptibility Mechanisms in Parkinson’s Disease

Gene-environment Interaction Models to Unmask Susceptibility Mechanisms in Parkinson’s Disease

DOI:
10.3791/50960-v

08:09 min

January 07, 2014

, , ,
1Center for Health Sciences,SRI International, 2Department of Chemistry and Biochemistry,University of California-Santa Cruz

Chapitres

  • 00:05Titre
  • 01:25MPTP (1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine) Preparation
  • 03:50MPTP Administration
  • 05:59Results: 5-LOX and 12/15-LOX Differentially Impact the Nigrostriatal Dopaminergic Vulnerability
  • 07:40Conclusion

Summary

Traduction automatique

Traduction automatique

Lipoxygenase (LOX) isozymes can generate products that may increase or decrease neuroinflammation and neurodegeneration. A gene-environment interaction study could identify LOX isozyme-specific effects. Using the 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) model of nigrostriatal damage in two LOX isozyme-deficient transgenic lines allows for comparison of the contribution of LOX isozymes on dopaminergic integrity and inflammation.

Tags

Gene-environment InteractionLipoxygenaseParkinson’s DiseaseMPTPNeurodegenerative DisordersNigrostriatal DegenerationDopamineTyrosine HydroxylaseInflammationGFAPIba-1

Article

Embed

AJOUTER À LA PLAYLIST

Usage Statistics

Vidéos Connexes

Experimental Generation of Carcinoma-Associated Fibroblasts (CAFs) from Human Mammary Fibroblasts

Development of a Unilaterally-lesioned 6-OHDA Mouse Model of Parkinson’s Disease

MALDI Imaging Mass Spectrometry of Neuropeptides in Parkinson’s Disease

Skin Punch Biopsy Explant Culture for Derivation of Primary Human Fibroblasts

The Use of Primary Human Fibroblasts for Monitoring Mitochondrial Phenotypes in the Field of Parkinson’s Disease

Controlling Parkinson’s Disease With Adaptive Deep Brain Stimulation

Adapting Human Videofluoroscopic Swallow Study Methods to Detect and Characterize Dysphagia in Murine Disease Models

Ex Vivo Intestinal Sacs to Assess Mucosal Permeability in Models of Gastrointestinal Disease

Quantitative 3D In Silico Modeling (q3DISM) of Cerebral Amyloid-beta Phagocytosis in Rodent Models of Alzheimer’s Disease

Repeated Measurement of Respiratory Muscle Activity and Ventilation in Mouse Models of Neuromuscular Disease

Read Article