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Evolutionary trajectories of small cell lung cancer under therapy.

Julie GeorgeLukas MaasNima AbedpourMaria CartolanoLaura KaiserRieke N FischerAndreas H ScheelJan-Philipp WeberMartin Gunnar HellmichGraziella BoscoCaroline VolzChristian MuellerIlona DahmenFelix JohnCleidson Padua AlvesLisa WerrJens Peter PanseMartin KirschnerWalburga Engel-RiedelJessica JürgensErich StoelbenMichael BrockmannStefan J GrauMartin SebastianJan A StratmannJens KernHorst-Dieter HummelBalazs HegedüsMartin SchulerTill PlönesClemens AignerThomas ElterKarin ToepeltYon-Dschun KoSylke KurzChristian GrohéMonika SerkeKatja HöpkerLars HagmeyerFabian DoerrKhosro HekmathJudith StrapatsasKarl-Otto KambartelGeothy ChakupurakalAnnette BuschFranz-Georg BauernfeindFrank GriesingerAnne LuersWiebke DirksRainer WiewrodtAndrea LueckeErnst RodermannAndreas DielVolker HagenKai SeverinRoland T UllrichHans Christian ReinhardtAlexander QuaasMagdalena BogusCornelius CourtsPeter NürnbergKerstin BeckerViktor AchterReinhard ButtnerJürgen WolfMartin PeiferRoman K Thomas
Published in: Nature (2024)
The evolutionary processes that underlie the marked sensitivity of small cell lung cancer (SCLC) to chemotherapy and rapid relapse are unknown 1-3 . Here we determined tumour phylogenies at diagnosis and throughout chemotherapy and immunotherapy by multiregion sequencing of 160 tumours from 65 patients. Treatment-naive SCLC exhibited clonal homogeneity at distinct tumour sites, whereas first-line platinum-based chemotherapy led to a burst in genomic intratumour heterogeneity and spatial clonal diversity. We observed branched evolution and a shift to ancestral clones underlying tumour relapse. Effective radio- or immunotherapy induced a re-expansion of founder clones with acquired genomic damage from first-line chemotherapy. Whereas TP53 and RB1 alterations were exclusively part of the common ancestor, MYC family amplifications were frequently not constituents of the founder clone. At relapse, emerging subclonal mutations affected key genes associated with SCLC biology, and tumours harbouring clonal CREBBP/EP300 alterations underwent genome duplications. Gene-damaging TP53 alterations and co-alterations of TP53 missense mutations with TP73, CREBBP/EP300 or FMN2 were significantly associated with shorter disease relapse following chemotherapy. In summary, we uncover key processes of the genomic evolution of SCLC under therapy, identify the common ancestor as the source of clonal diversity at relapse and show central genomic patterns associated with sensitivity and resistance to chemotherapy.
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