Polyglutamine protein aggregation and toxicity are linked to the cellular stress response

doi:10.1093/hmg/ddg151

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Human Molecular Genetics, 2003, Vol. 12, No. 12 1377-1391
DOI: 10.1093/hmg/ddg151
© 2003 Oxford University Press

Polyglutamine protein aggregation and toxicity are linked to the cellular stress response

K.J. Cowan¹, M.I. Diamond² and W.J. Welch¹^,*

¹Department of Surgery, University of California, San Francisco, Bldg 1, Room 210, San Francisco General Hospital, 1001 Potrero Ave, San Francisco, CA 94110, USA and ²Department of Neurology, University of California, San Francisco, CA, USA

Received February 6, 2003; Accepted April 7, 2003

Chronic exposure of cells to expanded polyglutamine proteinsresults in eventual cell demise. We constructed mouse cell linesexpressing either the full-length androgen receptor (AR), ortruncated forms of AR containing 25 or 65 glutamines to studythe cellular consequences of chronic low-level exposure to theseproteins. Expression of the polyglutamine-expanded truncatedAR protein, but not the full-length expanded protein, resultedin the formation of cytoplasmic and nuclear aggregates and eventualcell death. Nuclear aggregates preferentially stained positivefor heat shock protein (hsp)72, a sensitive indicator of a cellularstress response. Biochemical studies revealed that the presenceof nuclear aggregates correlated with activation of the c-junNH2-terminal kinase (JNK). Different metabolic insults, includingheat shock treatment, and exposure to sodium arsenite or menadione,proved more toxic to those cells expressing the polyglutamine-expandedtruncated protein than to cells expressing the non-expandedform. Cells containing cytoplasmic polyglutamine–proteinaggregates exhibited a delayed expression of hsp72 after heatshock. Once expressed, hsp72 failed to localize normally andinstead was sequestered within the protein aggregates. Thiswas accompanied by an inability of the aggregate-containingcells to cease their stress response as evidenced by the continuedpresence of activated JNK. Finally, activation of the cellularstress response increased the overall extent of polyglutamineprotein aggregation, especially within the nucleus. Inclusionof a JNK inhibitor reduced this stress-dependent increase innuclear aggregates. Abnormal stress responses may contributeto enhanced cell vulnerability in cells expressing polyglutamine-expandedproteins and may increase the propensity of such cells to formcytoplasmic and nuclear inclusions.

^* To whom correspondence should be addressed. Tel: +1 4152066948;Fax: +1 4152066997; Email: welch{at}itsa.ucsf.edu

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