Increased aggregation of polyleucine compared with that of polyglutamine in dentatorubral-pallidoluysian atrophy protein.

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Polyglutamine (polyQ ) diseases result from expansion of CAG trinucleotide repeats in their responsible genes . Although gene products with polyQ expansions undergo conformational changes to aggregate in neurons , the relationship between inclusions and neurotoxicity remains unclear . Dentatorubral-pallidoluysian atrophy (DRPLA ) is a polyQ disease , and DRPLA protein , also known as atrophin-1 (ATN 1 ), carries an expanded polyQ tract . To investigate how an expanded polyQ tract influences ATN 1 aggregation and localization , we compared the aggregation of ATN 1 with a polyQ tract to that of ATN 1 with a polyleucine (polyL ) tract . In COS -7 cells , polyL-ATN 1 triggered more aggregation than polyQ-ATN 1 of similar repeat sizes . Immunocytochemical and biochemical studies revealed that replacement of the polyQ tract with polyL alters ATN 1 localization , leading to retention of polyL-ATN 1 in the cytoplasm . Despite this change in localization , polyL-ATN 1 and polyQ-ATN 1 demonstrate comparable repeat length dependent toxicity . These results suggest that expanded polyQ repeats in ATN 1 may contribute to neurodegeneration via alterations in both protein aggregation and intracellular localization .