Affiliation:
1. Indiana University
2. Center for Computational Biology and Bioinformatics, Indiana University School of Medicine
3. Department of Medical and Molecular Genetics, Indiana University School of Medicine
4. Translational Genomics Research Institute
5. NYU Langone Health
Abstract
Abstract
Alternative splicing plays a pivotal role in tumorigenesis and proliferation. However, its pattern and pathogenic role has not been systematically analyzed in multiple myeloma or its subtypes. Alternative splicing profiles for 598 newly diagnosed myeloma patients with comprehensive genomic annotation identified primary translocations and DIS3 events to have more differentially spliced events than those without. Splicing levels were correlated with expression of splicing factors. Moreover, the non-homologous end joining pathway was an independent factor that was highly associated with splicing frequency via Prp19C, a component of spliceosome, as well as an increased number of structural variants. We therefore identify an axis of high-risk disease encompassing expression of the non-homologous end joining pathway, increase structural variants, and increased alternative splicing that are linked together. This indicates a joint pathogenic role for DNA damage response and alternative RNA processing in myeloma.
Publisher
Research Square Platform LLC