Compounds from an Unbiased Chemical Screen Reverse Both Er-to-Golgi Trafficking Defects and Mitochondrial Dysfunction in Parkinson's Disease Models

Su, L. J.; Auluck, P. K.; Outeiro, T. F.; Yeger-Lotem, E.; Kritzer, J. A.; Tardiff, D. F.; Strathearn, K. E.; Liu, F.; Cao, S.; Hamamichi, S.; Hill, K. J.; Caldwell, K. A.; Bell, G. W.; Fraenkel, E.; Cooper, A. A.; Caldwell, G. A.; McCaffery, J. M.; Rochet, J.-C.; Lindquist, S.

Author(s)

Su, Linhui Julie; Auluck, Pavan K.; Outeiro, Tiago Fleming; Yeger-Lotem, Esti; Kritzer, Joshua A.; ... Show more

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Abstract

α-Synuclein (α-syn) is a small lipid-binding protein involved in vesicle trafficking whose function is poorly characterized. It is of great interest to human biology and medicine because α-syn dysfunction is associated with several neurodegenerative disorders, including Parkinson’s disease (PD). We previously created a yeast model of α-syn pathobiology, which established vesicle trafficking as a process that is particularly sensitive to α-syn expression. We also uncovered a core group of proteins with diverse activities related to α-syn toxicity that is conserved from yeast to mammalian neurons. Here, we report that a yeast strain expressing a somewhat higher level of α-syn also exhibits strong defects in mitochondrial function. Unlike our previous strain, genetic suppression of endoplasmic reticulum (ER)-to-Golgi trafficking alone does not suppress α-syn toxicity in this strain. In an effort to identify individual compounds that could simultaneously rescue these apparently disparate pathological effects of α-syn, we screened a library of 115,000 compounds. We identified a class of small molecules that reduced α-syn toxicity at micromolar concentrations in this higher toxicity strain. These compounds reduced the formation of α-syn foci, re-established ER-to-Golgi trafficking and ameliorated α-syn-mediated damage to mitochondria. They also corrected the toxicity of α-syn in nematode neurons and in primary rat neuronal midbrain cultures. Remarkably, the compounds also protected neurons against rotenone-induced toxicity, which has been used to model the mitochondrial defects associated with PD in humans. That single compounds are capable of rescuing the diverse toxicities of α-syn in yeast and neurons suggests that they are acting on deeply rooted biological processes that connect these toxicities and have been conserved for a billion years of eukaryotic evolution. Thus, it seems possible to develop novel therapeutic strategies to simultaneously target the multiple pathological features of PD.

Date issued

2010-01

URI

http://hdl.handle.net/1721.1/66913

Department

Massachusetts Institute of Technology. Department of Biological Engineering; Massachusetts Institute of Technology. Department of Biology; Whitehead Institute for Biomedical Research

Journal

Disease Models and Mechanisms

Publisher

Company of Biologists Limited

Citation

Su, L. J. et al. “Compounds from an unbiased chemical screen reverse both ER-to-Golgi trafficking defects and mitochondrial dysfunction in Parkinson’s disease models.” Disease Models & Mechanisms 3 (2009): 194-208. Web. 3 Nov. 2011. © 2010 Company of Biologists Limited

Version: Author's final manuscript

ISSN

1754-8403

1754-8411

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