Identification of novel mutational drivers reveals oncogene dependencies in multiple myeloma

Walker, Brian A.; Mavrommatis, Konstantinos; Wardell, Christopher P.; Ashby, Cody; Bauer, Michael; Davies, Faith E.; Rosenthal, Adam; Wang, Hongwei; Qu, Pingping; Hoering, Antje; Samur, Mehmet K.; Towfic, Fadi; Ortiz, María; Flynt, Erin; Yu, Zhinuan; Yang, Zhihong; Rozelle, Dan; Obenauer, John C.; Trotter, Matthew; Auclair, Daniel; Keats, Jonathan J.; Bolli, Niccolò; Fulciniti, Mariateresa; Szalat, Raphaël; Moreau, Philippe; Durie, Brian G.M.; Stewart, A. Keith; Goldschmidt, Hartmut; Raab, Marc-Steffen; Einsele, Hermann; Sonneveld, Pieter; Miguel, Jesús F. San; Lonial, Sagar; Jackson, Graham; Anderson, Kenneth C.; Avet-Loiseau, Hervé; Munshi, Nikhil C.; Thakurta, Anjan; Morgan, Gareth J.

doi:10.1182/blood-2018-03-840132

Cited by 352 publications

(514 citation statements)

References 54 publications

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“…Data analysis was performed as described previously, with minor differences between sequencing modalities. 32 For details see Supplementary Methods.…”

Section: Resultsmentioning

confidence: 99%

Microhomology-mediated end joining drives complex rearrangements and over-expression of MYC and PVT1 in multiple myeloma

Mikulášová

Ashby

Tytarenko

et al. 2019

Preprint

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MYC is a widely acting transcription factor and its deregulation is a crucial event in many human cancers. MYC is important biologically and clinically in multiple myeloma, but the mechanisms underlying its dysregulation are poorly understood. We show that MYC rearrangements are present in 36.0% of newly diagnosed myeloma patients, as detected in the largest set of next generation sequencing data to date (n=1267). Rearrangements were complex and associated with increased expression of MYC and PVT1, but not other genes at 8q24. The highest effect on gene expression was detected in cases where the MYC locus is juxtaposed next to superenhancers associated with genes such as IGH, IGK, IGL, TXNDC5/BMP6, FAM46C and FOXO3.We identified three hotspots of recombination at 8q24, one of which is enriched for IGH-MYC translocations. Breakpoint analysis indicates primary myeloma rearrangements involving the IGH locus occur through non-homologous end joining, whereas secondary MYC rearrangements occur through microhomology-mediated end joining. This mechanism is different to lymphomas, where non-homologous end joining generates MYC rearrangements. Rearrangements resulted in over-expression of key genes and ChIP-seq identified that HK2, a member of the glucose metabolism pathway, is directly over-expressed through binding of MYC at its promoter.

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“…Data analysis was performed as described previously, with minor differences between sequencing modalities. 32 For details see Supplementary Methods.…”

Section: Resultsmentioning

confidence: 99%

Microhomology-mediated end joining drives complex rearrangements and over-expression of MYC and PVT1 in multiple myeloma

Mikulášová

Ashby

Tytarenko

et al. 2019

Preprint

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“…This strong association was likely missed in earlier studies given that PHF19 expression is not associated with any cytogenetic feature while several therapeutic advances over the last 20 years have made it difficult to model outcome across multiple studies from different periods. Furthermore, PHF19 has not been found to be significantly mutated in sequencing-based studies 28,29 , suggesting that its overexpression is not directly related to genomic alterations within the PHF19 gene. We also show that a simple four feature predictor composed of age, ISS, and expression of PHF19 and MMSET performs similarly to more complex models with many more gene expression features included (Supplemental Figure 4).…”

Section: Discussionmentioning

confidence: 98%

Multiple Myeloma DREAM Challenge Reveals Epigenetic RegulatorPHF19As Marker of Aggressive Disease

Mason

Schinke

Eng

et al. 2019

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Key points• Most comprehensive and unbiased assessment of prognostic biomarkers in MM resulting in a robust and parsimonious model. •Identification of PHF19 as the expression based biomarker most strongly associated with rapid progression in MM patients. AbstractWhile the past decade has seen meaningful improvements in clinical outcomes for multiple myeloma patients, a subset of patients do not benefit from current therapeutics for unclear reasons. Many gene expression-based models of risk have been developed, but each model uses a different combination of genes and often involve assaying many genes making them difficult to implement. We organized the Multiple Myeloma DREAM Challenge, a crowdsourced effort to develop models of rapid progression in newly diagnosed myeloma patients and to benchmark these against previously published models. This effort lead to more robust predictors and found that incorporating specific demographic and clinical features improved gene expression-based models of high risk. Furthermore, post challenge analysis identified a novel expression-based risk marker and histone modifier, PHF19, which featured prominently in several independent models. Lastly, we show that a simple four feature predictor composed of age, International Staging System stage (ISS), and expression of PHF19 and MMSET performs similarly to more complex models with many more gene expression features included.

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“…MM is a unique case study of Ras biology as approximately 40% of MM patient tumors have predicted activating mutations in KRAS or NRAS 4,5 , with an almost equal distribution between the two, but essentially none in HRAS. Notably, these KRAS and NRAS mutations are very rare in the precursor lesion monoclonal gammopathy of uncertain significance (MGUS), suggesting that RAS mutations are important for transformation to MM 16 .…”

Section: Introductionmentioning

confidence: 99%

“…In vitro overexpression studies in myeloma cell lines indicated that KRAS may lead to more rapid proliferation in the absence of interleukin-6 (IL-6) stimulation than NRAS 20,21 . More recent sequencing studies have suggested that NRAS mutations tend to cluster with specific genomic aberrations in MM 5 . Finally, immunohistochemistry studies on MM bone marrow have suggested possible differences in ERK phosphorylation depending on RAS isoform and specific mutation 22 .…”

Section: Introductionmentioning

confidence: 99%

Integrated Phosphoproteomics and Transcriptional Classifiers Reveal Hidden RAS Signaling Dynamics in Multiple Myeloma

Lin¹,

Way

Barwick

et al. 2019

Preprint

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A major driver of multiple myeloma is thought to be aberrant signaling, yet no kinase inhibitors have proven successful in the clinic. Here, we employ an integrated, systems approach combining phosphoproteomic and transcriptome analysis to dissect cellular signaling in multiple myeloma to inform precision medicine strategies. Collectively, these predictive models identify vulnerable signaling signatures and highlight surprising differences in functional signaling patterns between NRAS and KRAS mutants invisible to the genomic landscape.Transcriptional analysis suggests that aberrant MAPK pathway activation is only present in a fraction of RAS-mutated vs. WT RAS patients. These high-MAPK patients, enriched for NRAS Q61 mutations, have inferior outcomes whereas RAS mutations overall carry no survival impact.We further develop an interactive software tool to relate pharmacologic and genetic kinase dependencies in myeloma. These results may lead to improved stratification of MM patients in clinical trials while also revealing unexplored modes of Ras biology.

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Identification of novel mutational drivers reveals oncogene dependencies in multiple myeloma

Cited by 352 publications

References 54 publications

Microhomology-mediated end joining drives complex rearrangements and over-expression of MYC and PVT1 in multiple myeloma

Microhomology-mediated end joining drives complex rearrangements and over-expression of MYC and PVT1 in multiple myeloma

Multiple Myeloma DREAM Challenge Reveals Epigenetic RegulatorPHF19As Marker of Aggressive Disease

Integrated Phosphoproteomics and Transcriptional Classifiers Reveal Hidden RAS Signaling Dynamics in Multiple Myeloma

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