The enrichment of breakpoints in late-replicating chromatin provides novel insights into chromoanagenesis mechanisms
Chatron N., Giannuzzi G., Rollat-Farnier P-A., Diguet F., Porcu E., Yammine T., Uguen K., Bellil Z-L., Zillhardt JL., Sorlin A., Ader F., Afenjar A., Andrieux J., Bardel C., Calpena E., Chantot-Bastaraud S., Callier P., Chelloug N., Chopin E., Cordier M-P., Dubourg C., Faivre L., Girard F., Heide S., Herenger Y., Jaillard S., Keren B., Knight SJL., Lespinasse J., Lohmann L., Marle N., Maroofian R., Masurel-Paulet A., Mathieu-Dramard M., Metay C., Pagnamenta AT., Portnoï M-F., Prieur F., Rio M., Siffroi J-P., Valence S., Taylor JC., Wilkie AOM., Edery P., Reymond A., Sanlaville D., Schluth-Bolard C.
AbstractThe rise of pangenomic molecular assays allowed uncovering complex rearrangements namedchromoanagenesisthat were hypothesized to result from catastrophic shattering events. Constitutional cases have typically been reported individually preventing identification of common features and uncovering the mechanisms at play. We characterized 20 newchromoanagenesisand discovered yet undescribed features. While literature differentiateschromothripsisand its shattering event repaired through non-homologous end joining fromchromoanasynthesisborn to aberrant replicative processes, we identified shattered chromosomes repaired through a combination of mechanisms. In particular, three samples present with “rearrangement hubs” comprising a fragmented kilobase-long sequence threaded throughout the rearrangement.To assess the mechanisms at play, we merged our data with those of 20 published constitutional complex chromosomal rearrangement cases. We evaluated if the distribution of their 1032 combined breakpoints was distinctive using bootstrap simulations and found that breakpoints tend to keep away from haplosensitive genes suggesting selective pressure. We then compared their distribution with that of 13,310 and 468 breakpoints of cancer complex chromosomal rearrangements and constitutional simple rearrangement samples, respectively. Both complex rearrangement groups showed breakpoint enrichment in late replicating regions suggesting similar origins for constitutional and cancer cases. Simple rearrangement breakpoints but not complex ones were depleted from lamina-associated domains (LADs), possibly as a consequence of reduced mobility of DNA ends bound to lamina.The enrichment of breakpoints in late-replicating chromatin for both constitutional and cancerchromoanagenesisprovides an orthogonal support to the premature chromosome condensation hypothesis that was put forward to explainchromoanagenesis.