A damaged genome’s transcriptional landscape through multilayered expression profiling around in situ-mapped DNA double-strand breaks

Fabio Iannelli(IFOM), Alessandro Galbiati(IFOM), Ilaria Capozzo(Istituto di Genetica Molecolare), Quan Nguyen, Brian Magnuson(University of Michigan), Flavia Michelini(IFOM), Giuseppina D’Alessandro(IFOM), Matteo Cabrini(Istituto di Genetica Molecolare), Marco Roncador(Istituto di Genetica Molecolare), Sofia Francia(IFOM), Nicola Crosetto(Science for Life Laboratory), Mats Ljungman(University of Michigan), Piero Carninci, Fabrizio d’Adda di Fagagna(IFOM)
Nature Communications
May 31, 2017
Cited by 134Open Access
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Abstract

Of the many types of DNA damage, DNA double-strand breaks (DSBs) are probably the most deleterious. Mounting evidence points to an intricate relationship between DSBs and transcription. A cell system in which the impact on transcription can be investigated at precisely mapped genomic DSBs is essential to study this relationship. Here in a human cell line, we map genome-wide and at high resolution the DSBs induced by a restriction enzyme, and we characterize their impact on gene expression by four independent approaches by monitoring steady-state RNA levels, rates of RNA synthesis, transcription initiation and RNA polymerase II elongation. We consistently observe transcriptional repression in proximity to DSBs. Downregulation of transcription depends on ATM kinase activity and on the distance from the DSB. Our study couples for the first time, to the best of our knowledge, high-resolution mapping of DSBs with multilayered transcriptomics to dissect the events shaping gene expression after DSB induction at multiple endogenous sites.


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