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[Preprint]. 2024 Sep 4:2024.08.30.610457. [Version 1] doi: 10.1101/2024.08.30.610457

Temporal Genomic Dynamics Shape Clinical Trajectory in Multiple Myeloma

Francesco Maura, Marcella Kaddoura, Alexandra M Poos, Linda B Baughn, Bachisio Ziccheddu, Marc-Andrea Bärtsch, Anthony Cirrincione, Kylee Maclachlan, Monika Chojnacka, Benjamin Diamond, Marios Papadimitriou, Patrick Blaney, Lukas John, Philipp Reichert, Stefanie Huhn, Dylan Gagler, Yanming Zhang, Ahmet Dogan, Alexander M Lesokhin, Faith Davies, Hartmut Goldschmidt, Roland Fenk, Katja C Weisel, Elias K Mai, Neha Korde, Gareth J Morgan, S Vincent Rajkumar, Shaji Kumar, Saad Usmani, Ola Landgren, Marc S Raab, Niels Weinhold
PMCID: PMC11398314  PMID: 39282268

ABSTRACT

To comprehensively unravel the temporal relationship between initiating and driver events and its impact on clinical outcomes, we analyzed 421 whole-genome sequencing profiles from 382 patients. Using clock-like mutational signatures, we estimated a time lag of 2-4 decades between initiating events and diagnosis. In patients with hyperdiploidy, we demonstrate that trisomies of odd-numbered chromosomes can be acquired simultaneously with other chromosomal gains, such as 1q gain. We provide evidence that hyperdiploidy is acquired after canonical IGH translocation when both events are present. Finally, patients with early 1q gain had adverse outcomes similar to those with 1q amplification (>1 extra-copies), but faring worse than those with late 1q gain. This underscores that the prognostic impact of 1q gain/amp depends more on the timing of acquisition than on the number of extra copies gained. Overall, this study contributes to a better understanding of the life history of MM and may have prognostic implications.

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