The Npl3 hnRNP prevents R-loop-mediated transcription–replication conflicts and genome instability

JM Santos-Pereira, AB Herrero… - Genes & …, 2013 - genesdev.cshlp.org
Genes & development, 2013genesdev.cshlp.org
Transcription is a major obstacle for replication fork (RF) progression and a cause of
genome instability. Part of this instability is mediated by cotranscriptional R loops, which are
believed to increase by suboptimal assembly of the nascent messenger ribonucleoprotein
particle (mRNP). However, no clear evidence exists that heterogeneous nuclear RNPs
(hnRNPs), the basic mRNP components, prevent R-loop stabilization. Here we show that
yeast Npl3, the most abundant RNA-binding hnRNP, prevents R-loop-mediated genome …
Transcription is a major obstacle for replication fork (RF) progression and a cause of genome instability. Part of this instability is mediated by cotranscriptional R loops, which are believed to increase by suboptimal assembly of the nascent messenger ribonucleoprotein particle (mRNP). However, no clear evidence exists that heterogeneous nuclear RNPs (hnRNPs), the basic mRNP components, prevent R-loop stabilization. Here we show that yeast Npl3, the most abundant RNA-binding hnRNP, prevents R-loop-mediated genome instability. npl3Δ cells show transcription-dependent and R-loop-dependent hyperrecombination and genome-wide replication obstacles as determined by accumulation of the Rrm3 helicase. Such obstacles preferentially occur at long and highly expressed genes, to which Npl3 is preferentially bound in wild-type cells, and are reduced by RNase H1 overexpression. The resulting replication stress confers hypersensitivity to double-strand break-inducing agents. Therefore, our work demonstrates that mRNP factors are critical for genome integrity and opens the option of using them as therapeutic targets in anti-cancer treatment.
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