Chronic, low-dose rotenone reproduces Lewy neurites found in early stages of Parkinson's disease, reduces mitochondrial movement and slowly kills differentiated SH-SY5Y neural cells

doi:10.1186/1750-1326-3-21

Molecular Neurodegeneration

Volume 3

Viewing options:

Abstract
Full text
PDF (2.9MB)

Associated material:

Related literature:

Articles citing this article
on BioMed Central
on Google Scholar
on ISI Web of Science
on PubMed Central
Other articles by authors
on Google Scholar

Borland MK
Trimmer PA
Rubinstein JD
Keeney PM
Mohanakumar KP
Liu L
Bennett JP

on PubMed

Borland MK
Trimmer PA
Rubinstein JD
Keeney PM
Mohanakumar KP
Liu L
Bennett JP
Related articles/pages
on Google

on Google Scholar

on PubMed

Tools:

Post to:

Research article

Chronic, low-dose rotenone reproduces Lewy neurites found in early stages of Parkinson's disease, reduces mitochondrial movement and slowly kills differentiated SH-SY5Y neural cells

M Kathleen Borland¹^* , Patricia A Trimmer¹^* , Jeremy D Rubinstein¹ , Paula M Keeney¹ , KP Mohanakumar² , Lei Liu³ and James P Bennett Jr¹

¹Center for the Study of Neurodegenerative Diseases and Morris K. Udall Parkinson's Disease Research Center of Excellence, University of Virginia, Charlottesville, Virginia, USA

²Division of Cell Biology & Physiology, Laboratory of Experimental & Clinical Neuroscience, Indian Institute of Chemical Biology, Calcutta, India

³Department of Statistics, Virginia Polytechnic Institute and State University, Blacksburg, Virginia, USA

author email corresponding author email* Contributed equally

Molecular Neurodegeneration 2008, 3:21doi:10.1186/1750-1326-3-21


Published:	29 December 2008

Abstract

Background

Parkinson's disease, the most common adult neurodegenerative movement disorder, demonstrates a brain-wide pathology that begins pre-clinically with alpha-synuclein aggregates ("Lewy neurites") in processes of gut enteric and vagal motor neurons. Rostral progression into substantia nigra with death of dopamine neurons produces the motor impairment phenotype that yields a clinical diagnosis. The vast majority of Parkinson's disease occurs sporadically, and current models of sporadic Parkinson's disease (sPD) can utilize directly infused or systemic neurotoxins.

Results

We developed a differentiation protocol for human SH-SY5Y neuroblastoma that yielded non-dividing dopaminergic neural cells with long processes that we then exposed to 50 nM rotenone, a complex I inhibitor used in Parkinson's disease models. After 21 days of rotenone, ~60% of cells died. Their processes retracted and accumulated ASYN-(+) and UB-(+) aggregates that blocked organelle transport. Mitochondrial movement velocities were reduced by 8 days of rotenone and continued to decline over time. No cytoplasmic inclusions resembling Lewy bodies were observed. Gene microarray analyses showed that the majority of genes were under-expressed. qPCR analyses of 11 mtDNA-encoded and 10 nDNA-encoded mitochondrial electron transport chain RNAs' relative expressions revealed small increases in mtDNA-encoded genes and lesser regulation of nDNA-encoded ETC genes.

Conclusion

Subacute rotenone treatment of differentiated SH-SY5Y neuroblastoma cells causes process retraction and partial death over several weeks, slowed mitochondrial movement in processes and appears to reproduce the Lewy neuritic changes of early Parkinson's disease pathology but does not cause Lewy body inclusions. The overall pattern of transcriptional regulation is gene under-expression with minimal regulation of ETC genes in spite of rotenone's being a complex I toxin. This rotenone-SH-SY5Y model in a differentiated human neural cell mimics changes of early Parkinson's disease and may be useful for screening therapeutics for neuroprotection in that disease stage.