Raphaël CeccaldiGénétique des cancers - Institut Curie / INSERM

ATIP-Avenir 2016

Mieux comprendre les processus fondamentaux régulant la réparation de l’ADN dans les cancers

Mes recherches

Raphael Ceccaldi received dual degrees in Pharmacy (Pharm D) and Hematology (PhD) at the University of Paris V and Paris Diderot-Paris 7 in France. He completed a postdoctoral fellowship in the laboratory of Professor Alan D. D’Andrea at Dana-Farber Cancer Institute in Boston in the US. Ceccaldi’s main research focus is to understand the molecular basis of the DNA repair mechanisms that are essential for the survival of cancer cells.

Mon projet ATIP-Avenir

Characterisation of DNA Double-Strand Break Repair by Alternative End-Joining:

Potential Targets for Cancer Therapy

altEJrepair

DNA repair pathways evolved as an intricate network that senses DNA damage and resolves it in order to minimise genetic lesions and thus preventing tumour formation. Gaining in recognition the last few years, the alternative end-joining (alt-EJ) DNA repair pathway was recently shown to be up-regulated and required for cancer cell viability in the absence of homologous recombination-mediated repair (HR). Despite this integral role, the alt-EJ repair pathway remains poorly characterised in humans. As such, its molecular composition, regulation and crosstalk with HR and other repair pathways remain elusive. Additionally, the contribution of the alt-EJ pathway to tumour progression as well as the identification of a mutational signature associated with the use of alt-EJ has not yet been investigated. Moreover, the clinical relevance of developing small-molecule inhibitors targeting players in the alt-EJ pathway, such as the polymerase Pol Theta (Polθ), is of importance as current anticancer drug treatments have shown limited effectiveness in achieving cancer remission in patients with HR-deficient (HRD) tumours.

Here, we propose a novel, multidisciplinary approach that aims to characterise the players and mechanisms of action involved in the utilisation of alt-EJ in cancer. This understanding will better elucidate the changing interplay between different DNA repair pathways, thus shedding light on whether and how the use of alt-EJ contributes to the pathogenic history and survival of HRD tumours, eventually paving the way for the development of novel anticancer therapeutics.

For all the abovementioned reasons, we are convinced this project will have important implications in :

1) elucidating critical interconnections between DNA repair pathways
2) improving the basic understanding of the composition, regulation and function of the alt-EJ pathway,
3) facilitating the development of new synthetic lethality-based chemotherapeutics for the treatment of HRD tumours.

Raphaël Ceccaldi est également lauréat Starting Grant 2016

Contact

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Imprimer

https://www.insb.cnrs.fr/fr/personne/raphael-ceccaldi