Impact of rare structural variant events in newly diagnosed multiple myeloma

Author:

Chojnacka Monika,Diamond Benjamin,Ziccheddu Bachisio,Rustad Even,Maclachlan Kylee,Papadimitriou Marios,Boyle Eileen M.ORCID,Blaney Patrick,Usmani Saad,Morgan Gareth,Landgren OlaORCID,Maura FrancescoORCID

Abstract

ABSTRACTWhole genome sequencing (WGS) of newly diagnosed multiple myeloma patients (NDMM) has shown recurrent structural variant (SV) involvement in distinct regions of the genome (i.e. hotspots) and causing recurrent copy number alterations. Together with canonical immunoglobulin translocations, these SVs are recognized as “recurrent SVs”. More than half SVs were not involved in recurrent events. The significance of these “rare SVs” has not been previously examined. In this study, we utilize 752 WGS and 591 RNA-seq data from NDMM patients to determine the role of rare SVs in myeloma pathogenesis. 94% of patients harbored at least one rare SV event. Rare SVs showed an SV-class specific enrichment within genes and superenhancers associated with outlier gene expression. Furthermore, known myeloma driver genes recurrently impacted by point mutations were dysregulated by rare SVs. Overall, we demonstrate the association of rare SVs with aberrant gene expression supporting a driver role in myeloma pathogenesis.SIGNIFICANCECharacterization of multiple myeloma genome revealed that more than half structural variants are not involved in recurrent events. Here, we demonstrate that these rare SVs hold potential for myeloma pathogenesis through their gene expression impact. Rare SVs contribute to MM heterogeneity and have implications for development of individualized treatment.

Publisher

Cold Spring Harbor Laboratory

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1. An Overview of Advances in Rare Cancer Diagnosis and Treatment;International Journal of Molecular Sciences;2024-01-18

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