Cells have evolved several DNA repair mechanisms to maintain their genetic information unaltered and a DNA damage response pathway (DDR) coordinates DNA repair with several cellular events including a cell-cycle arrest until damaged DNA is repaired. When cells fail to repair DNA lesions, they undergo either apoptosis or cellular senescence. Tools commonly used to detect DNA lesions rely on indirect, antibody-based recognition of proteins associated to DNA breaks. Unfortunately, these tools do not allow direct and precise localization of the breaks, leaving several biological questions unanswered. I validated and optimized BLESS and BLISS, two methods that allow genome-wide single-nucleotide resolution mapping of DNA double strand-breaks (DSBs). Using these techniques, I studied the impact of DSBs on transcription. I characterized a DDR-dependent transcription inhibition around breaks. Differently, I observed that following macrophages LPS-stimulation, a transient wave of DSBs is induced at LPS-specific enhancers and it correlates with their transcription activation, thus suggesting a new mechanism for transcription activation involving controlled DNA damage generation. BLESS and BLISS cannot be applied to single-cell studies. Thus, I developed a new method, named DI-PLA, for the detection and imaging of DSBs in fixed cells and tissues. I applied DI-PLA to demonstrate that senescence cells and aged tissues accumulate DSBs, which are associated with persistent DDR activation, that is known to fuel cellular senescence. Finally, I developed a modification of BLESS to discriminate between DSB bearing telomeres and deprotected telomeres which could be applied to further characterize the mechanisms of DDR activation at telomeres.

NEW APPROACHES TO STUDY DNA DOUBLE-STRAND BREAKS GENOME-WIDE AND IN SINGLE-CELLS / A. Galbiati ; supervisore interno: G. Natoli, Humanitas University; supervisore esterno: J. Hoeijmakersm, Erasmus University MC ; supervisor: F. D'Adda di Fagagna. DIPARTIMENTO DI ONCOLOGIA ED EMATO-ONCOLOGIA, Università degli Studi di Milano, 2018 Mar 26. 29. ciclo, Anno Accademico 2017. [10.13130/galbiati-alessandro_phd2018-03-26].

NEW APPROACHES TO STUDY DNA DOUBLE-STRAND BREAKS GENOME-WIDE AND IN SINGLE-CELLS

A. Galbiati
2018

Abstract

Cells have evolved several DNA repair mechanisms to maintain their genetic information unaltered and a DNA damage response pathway (DDR) coordinates DNA repair with several cellular events including a cell-cycle arrest until damaged DNA is repaired. When cells fail to repair DNA lesions, they undergo either apoptosis or cellular senescence. Tools commonly used to detect DNA lesions rely on indirect, antibody-based recognition of proteins associated to DNA breaks. Unfortunately, these tools do not allow direct and precise localization of the breaks, leaving several biological questions unanswered. I validated and optimized BLESS and BLISS, two methods that allow genome-wide single-nucleotide resolution mapping of DNA double strand-breaks (DSBs). Using these techniques, I studied the impact of DSBs on transcription. I characterized a DDR-dependent transcription inhibition around breaks. Differently, I observed that following macrophages LPS-stimulation, a transient wave of DSBs is induced at LPS-specific enhancers and it correlates with their transcription activation, thus suggesting a new mechanism for transcription activation involving controlled DNA damage generation. BLESS and BLISS cannot be applied to single-cell studies. Thus, I developed a new method, named DI-PLA, for the detection and imaging of DSBs in fixed cells and tissues. I applied DI-PLA to demonstrate that senescence cells and aged tissues accumulate DSBs, which are associated with persistent DDR activation, that is known to fuel cellular senescence. Finally, I developed a modification of BLESS to discriminate between DSB bearing telomeres and deprotected telomeres which could be applied to further characterize the mechanisms of DDR activation at telomeres.
26-mar-2018
supervisore interno: G. Natoli, Humanitas University; supervisore esterno: J. Hoeijmakersm, Erasmus University MC ; supervisor: F. D'Adda di Fagagna
DIPARTIMENTO DI ONCOLOGIA ED EMATO-ONCOLOGIA
English
29
2017
MEDICINA DEI SISTEMI
Settore BIO/11 - Biologia Molecolare
Ricerca di base
Pubblicazione scientifica
DNA damage; DDR; senescence; ageing; transcription
D'ADDA DI FAGAGNA, FABRIZIO
FOIANI, MARCO
Doctoral Thesis
Prodotti della ricerca::Tesi di dottorato
-2.0
open
Università degli Studi di Milano
info:eu-repo/semantics/doctoralThesis
1
A. Galbiati
NEW APPROACHES TO STUDY DNA DOUBLE-STRAND BREAKS GENOME-WIDE AND IN SINGLE-CELLS / A. Galbiati ; supervisore interno: G. Natoli, Humanitas University; supervisore esterno: J. Hoeijmakersm, Erasmus University MC ; supervisor: F. D'Adda di Fagagna. DIPARTIMENTO DI ONCOLOGIA ED EMATO-ONCOLOGIA, Università degli Studi di Milano, 2018 Mar 26. 29. ciclo, Anno Accademico 2017. [10.13130/galbiati-alessandro_phd2018-03-26].
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/562490
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