Spt4 is selectively required for transcription of extended trinucleotide repeats

Chia Rung Liu, Chuang Rung Chang, Yijuang Chern, Tzu Han Wang, Wen Chieh Hsieh, Wen Chuan Shen, Chi Yuan Chang, I. Chieh Chu, Ning Deng, Stanley N. Cohen*, Tzu Hao Cheng

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

84 Scopus citations

Abstract

Lengthy trinucleotide repeats encoding polyglutamine (polyQ) stretches characterize the variant proteins of Huntington's disease and certain other inherited neurological disorders. Using a phenotypic screen to identify events that restore functionality to polyQ proteins in S. cerevisiae, we discovered that transcription elongation factor Spt4 is required to transcribe long trinucleotide repeats located either in ORFs or nonprotein-coding regions of DNA templates. Mutation of SPT4 selectively decreased synthesis of and restored enzymatic activity to expanded polyQ protein without affecting protein lacking long-polyQ stretches. RNA-seq analysis revealed limited effects of Spt4 on overall gene expression. Inhibition of Supt4h, the mammalian ortholog of Spt4, reduced mutant huntingtin protein in neuronal cells and decreased its aggregation and toxicity while not altering overall cellular mRNA synthesis. Our findings identify a cellular mechanism for transcription through repeated trinucleotides and a potential target for countermeasures against neurological disorders attributable to expanded trinucleotide regions.

Original languageEnglish
Pages (from-to)690-701
Number of pages12
JournalCell
Volume148
Issue number4
DOIs
StatePublished - 17 Feb 2012

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