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Dopamine induces autophagic cell death and α‐synuclein increase in human neuroblastoma SH‐SY5Y cells
Author(s) -
GómezSantos Cristina,
Ferrer Isidre,
Santidrián Antonio F.,
Barrachina Marta,
Gil Joan,
Ambrosio Santiago
Publication year - 2003
Publication title -
journal of neuroscience research
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.72
H-Index - 160
eISSN - 1097-4547
pISSN - 0360-4012
DOI - 10.1002/jnr.10663
Subject(s) - autophagy , sh sy5y , microbiology and biotechnology , p38 mitogen activated protein kinases , dopamine , programmed cell death , viability assay , dopaminergic , dopamine transporter , alpha synuclein , mapk/erk pathway , chemistry , oxidative stress , vacuole , biology , kinase , neuroblastoma , cell , cytoplasm , biochemistry , cell culture , endocrinology , medicine , parkinson's disease , apoptosis , genetics , disease
Abstract Free cytoplasmic dopamine may be involved in the genesis of neuronal degeneration in Parkinson's disease and other such diseases. We used SH‐SY5Y human neuroblastoma cells to study the effect of dopamine on cell death, activation of stress‐induced pathways, and expression of α‐synuclein, the characteristic protein accumulated in Lewy bodies. We show that 100 and 500 μM dopamine causes a 40% and 60% decrease of viability, respectively, and triggers autophagy after 24 hr of exposure, characterized by the presence of numerous cytoplasmic vacuoles with inclusions. Dopamine causes mitochondrial aggregation in adherent cells prior to the loss of functionality. Plasma membrane and nucleus also maintain their integrity. Cell viability is protected by the dopamine transporter blocker nomifensine and the antioxidants N‐acetylcysteine and ascorbic acid. Dopamine activates the stress‐response kinases, SAPK/JNK and p38, but not ERK/MAPK or MEK, and increases α‐synuclein expression. Both cell viability and the increase in α‐synuclein expression are prevented by antioxidants; by the specific inhibitors of p38 and SAPK/JNK, SB203580 and SP600125, respectively; and by the inhibitor of autophagy 3‐methyladenine. This indicates that oxidative stress, stress‐activated kinases, and factors involved in autophagy up‐regulate α‐synuclein content. The results show that nonapoptotic death pathways are triggered by dopamine, leading to autophagy. These findings should be taken into account in the search for strategies to protect dopaminergic neurons from degeneration. © 2003 Wiley‐Liss, Inc.

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