The genetic heterogeneity and drug resistance mechanisms of relapsed refractory multiple myeloma

Author:

Vo Josh N.,Wu Yi-Mi,Mishler Jeanmarie,Hall Sarah,Mannan RahulORCID,Wang Lisha,Ning Yu,Zhou Jin,Hopkins Alexander C.,Estill James C.,Chan Wallace K. B.ORCID,Yesil Jennifer,Cao Xuhong,Rao Arvind,Tsodikov Alexander,Talpaz Moshe,Cole Craig E.,Ye Jing C.,Ailawadhi Sikander,Berdeja Jesus G.,Hofmeister Craig C.,Jagannath Sundar,Jakubowiak Andrzej,Krishnan Amrita,Kumar Shaji,Levy Moshe Yair,Lonial Sagar,Orloff Gregory J.,Siegel David,Trudel Suzanne,Usmani Saad Z.,Vij Ravi,Wolf Jeffrey L.,Zonder Jeffrey A.,Bergsagel P. LeifORCID,Auclair Daniel,Cho Hearn Jay,Robinson Dan R.ORCID,Chinnaiyan Arul M.ORCID,

Abstract

AbstractMultiple myeloma is the second most common hematological malignancy. Despite significant advances in treatment, relapse is common and carries a poor prognosis. Thus, it is critical to elucidate the genetic factors contributing to disease progression and drug resistance. Here, we carry out integrative clinical sequencing of 511 relapsed, refractory multiple myeloma (RRMM) patients to define the disease’s molecular alterations landscape. The NF-κB and RAS/MAPK pathways are more commonly altered than previously reported, with a prevalence of 45–65% each. In the RAS/MAPK pathway, there is a long tail of variants associated with the RASopathies. By comparing our RRMM cases with untreated patients, we identify a diverse set of alterations conferring resistance to three main classes of targeted therapy in 22% of our cohort. Activating mutations in IL6ST are also enriched in RRMM. Taken together, our study serves as a resource for future investigations of RRMM biology and potentially informs clinical management.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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