Genomic profiling for clinical decision making in lymphoid neoplasms

Leval, Laurence de; Alizadeh, Ash A.; Bergsagel, P. Leif; Campo, Elı́as; Davies, Andrew; Doğan, Ahmet; Fitzgibbon, Jude; Horwitz, Steven M.; Melnick, Ari; Morice, William G.; Morin, Ryan D.; Nadel, Bertrand; Pileri, Stefano; Rosenquist, Richard; Rossi, Davide; Salaverría, Itziar; Steidl, Christian; Treon, Steven P.; Zelenetz, Andrew D.; Advani, Ranjana H.; Allen, Carl E.; Ansell, Stephen M.; Chan, Wing C.; Cook, James R.; Cook, Lucy; d’Amore, Francesco; Dirnhofer, Stefan; Dreyling, Martin; Dunleavy, Kieron; Feldman, Andrew L.; Fend, Falko; Gaulard, Philippe; Ghia, Paolo; Gribben, John G.; Hermine, Olivier; Hodson, Daniel J.; Hsi, Eric D.; Inghirami, Giorgio; Jaffe, Elaine S.; Karube, Kennosuke; Kataoka, Keisuke; Klapper, Wolfram; Kim, Won Seog; King, Rebecca; Ko, Young Hyeh; LaCasce, Ann S.; Lenz, Georg; Martin-Subero, Iñaki; Piris, Miguel Á.; Pittaluga, Stefania; Pasqualucci, Laura; Quintanilla-Martı́nez, Leticia; Rodig, Scott J.; Rosenwald, Andreas; Salles, Gilles; Miguel, Jesús F. San; Savage, Kerry J.; Sehn, Laurie H.; Semenzato, Gianpietro; Staudt, Louis M.; Swerdlow, Steven H.; Tam, Constantine S.; Trotman, Judith; Vose, Julie M.; Weigert, Oliver; Wilson, Wyndham H.; Winter, Jane N.; Wu, Catherine J.; Zinzani, Pier Luigi; Zucca, Emanuele; Bagg, Adam; Scott, David W.

doi:10.1182/blood.2022015854

Cited by 70 publications

(65 citation statements)

References 505 publications

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“…Emavusertib showed the strongest dose-dependent anti-proliferative activity in the Karpas1718 cell line bearing mutated MYD88. Albeit a fraction of MZL patients present MYD88 abnormalities [ 2 , 10 , 11 , 12 , 13 , 14 ], the prevalence of these mutations, in particular the L265P, is much higher in LPL, [ 2 , 10 , 11 , 12 , 13 , 14 , 15 , 16 , 17 ] and we cannot rule out the possibility that the cell line derives from a LPL rather than from MZL. Nonetheless, our results are in line with the previously reported activity of emavusertib in MYD88 L265P mutated ABC DLBCL cell lines [ 26 ], and they indicate that emavusertib as single agent could be explored in the population of patients with MYD88 mutated LPL or MZL.…”

Section: Discussionmentioning

confidence: 99%

“…Mutations of proteins within the TLR/IL-1R pathway can lead to an increased NF-κB activity and the promotion of cancer. For example, MYD88-L265P encoding mutations are known to occur in a fraction of the activated B cell (ABC) diffuse large B-cell lymphomas (DLBCL), in the vast majority of LPL, and in rare MZL, with differences based on the primary anatomical site [ 2 , 10 , 11 , 12 , 13 , 14 , 15 , 16 , 17 ]. In ABC DLBCL, MYD88-L265P leads to oncogenic activation of NF-κB through TLR-MYD88-IRAK1/4-TRAF6, independent of B cell receptor (BCR)–BTK activity and establishes a pathway for potential ibrutinib resistance [ 10 ].…”

Section: Introductionmentioning

confidence: 99%

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Targeting IRAK4 with Emavusertib in Lymphoma Models with Secondary Resistance to PI3K and BTK Inhibitors

Guidetti

Arribas

Sartori

et al. 2023

JCM

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Inhibitors of phosphatidylinositol 3-kinase (PI3K) and Bruton tyrosine kinase (BTK) represent a recognized option for the treatment of patients affected by indolent B cell lymphomas. However, small molecules as single agents show limited success in their ability in inducing complete responses, with only partial remission achieved in most patients, suggesting the need for combination therapies. IRAK4 is a protein kinase downstream of the Toll-like receptor signaling (TLR), a driver pathway of secondary tumor° resistance in both hematological and solid tumor malignancies. Activation of IRAK4 upon TLRs and IL-1 receptor (IL-1R) stimulation and through the adaptor protein MYD88 initiates a signaling cascade that induces cytokine and survival factor expression mediated by the transcription factor NF-κB. MYD88-L265P encoding mutations occur in diffuse large B-cell lymphomas, in lymphoplasmacytic lymphomas and in few marginal zone lymphomas (MZL). The IRAK4 inhibitor emavusertib (CA-4948) has shown early safety and clinical activity in lymphoma and leukemia patients. In this preclinical study, we assessed emavusertib effectiveness in MZL, both as single agent and in combination with targeted agents, with a particular focus on its capability to overcome resistance to BTK and PI3K inhibitors. We showed that the presence of MYD88 L265P mutation in bona fide MZL cell lines confers sensitivity to the IRAK4 inhibitor emavusertib as single agent. Emavusertib-based combinations improved the sensitivity of MZL cells to BTK and PI3K inhibitors, including cells with a secondary resistance to these agents. Emavusertib exerted its activity via inhibition of NF-κB signaling and induction of apoptosis. Considering the early safety data from clinical trials, our study identifies the IRAK4 inhibitor emavusertib as a novel compound to be explored in trials for patients with MYD88-mutated indolent B cell lymphomas as single agent and as combination partner with BTK or PI3K inhibitors in unselected populations of patients.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Targeting IRAK4 with Emavusertib in Lymphoma Models with Secondary Resistance to PI3K and BTK Inhibitors

Guidetti

Arribas

Sartori

et al. 2023

JCM

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“…Extensive genomic profiling of lymphomas is becoming more common; however, it is still not widely employed and the utility of genomic testing to predict response to therapy is limited. 24 With further genomic characterization of these tumors, we may be better equipped to individualize treatment to improve outcomes.…”

Section: Discussionmentioning

confidence: 99%

Successful CNS-Centric Therapeutic Management and Genomic Profiling of Primary Cranial Vault Diffuse Large B-Cell Lymphoma

Davis

Kimbrough

Moustafa

et al. 2023

JBM

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Primary cranial vault lymphoma (PCVL) is a rare lymphoma involving the skull with or without extra- and intracranial extension. Most cases of PCVL are diffuse large B-cell lymphoma (DLBCL). We report a case of primary cranial vault diffuse large B-cell lymphoma (PCV-DLBCL) that was successfully treated with anthracycline-based chemoimmunotherapy (CIT) alternating with central nervous system (CNS)-directed CIT with high-dose methotrexate and high-dose cytarabine. CNS-centric therapy was given for suspected cerebral cortical involvement and presumed elevated risk of CNS recurrence. The patient has remained in complete remission for 4.25 years following treatment. We suggest that PCV-DLBCL is potentially curable with CNS-directed therapy. Additionally, we provide genomic profiling results indicating an indeterminate cell of origin and multiple genetic mutations which are not frequently seen in DLBCL.

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“…MYD88 mutations in the TIR domain are found in > 90% of LPL predominantly L265P, although rarely non-L265P variants may be present [28,72]. Molecular studies for MYD88 L265P should be performed using a sensitive method as some sequencing methods may yield false negative results, especially in cases with low tumor volume [18]. A small percentage of LPL are MYD88 wild-type with alternative mutations downstream of MYD88 in the NFKB signaling pathway.…”

Section: Lymphoplasmacytic Lymphomamentioning

confidence: 99%

Plasma cell neoplasms and related entities—evolution in diagnosis and classification

2022

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Plasma cell neoplasms including multiple myeloma (MM) and related terminally differentiated B-cell neoplasms are characterized by secretion of monoclonal immunoglobulin and stepwise development from a preneoplastic clonal B and/or plasma cell proliferation called monoclonal gammopathy of undetermined significance (MGUS). Diagnosis of these disorders requires integration of clinical, laboratory, and morphological features. While their classification mostly remains unchanged compared to the revised 2016 WHO classification and the 2014 International Myeloma Working Group consensus, some changes in criteria and terminology were proposed in the 2022 International Consensus Classification (ICC) of mature lymphoid neoplasms. MGUS of IgM type is now divided into IgM MGUS of plasma cell type, precursor to the rare IgM MM and characterized by MM-type cytogenetics, lack of clonal B-cells and absence of MYD88 mutation, and IgM MGUS, NOS including the remaining cases. Primary cold agglutinin disease is recognized as a new entity. MM is now formally subdivided into cytogenetic groups, recognizing the importance of genetics for clinical features and prognosis. MM with recurrent genetic abnormalities includes MM with CCND family translocations, MM with MAF family translocations, MM with NSD2 translocation, and MM with hyperdiploidy, with the remaining cases classified as MM, NOS. For diagnosis of localized plasma cell tumors, solitary plasmacytoma of bone, and primary extraosseous plasmacytoma, the importance of excluding minimal bone marrow infiltration by flow cytometry is emphasized. Primary systemic amyloidosis is renamed immunoglobulin light chain amyloidosis (AL), and a localized AL amyloidosis is recognized as a distinct entity. This review summarizes the updates on plasma cell neoplasms and related entities proposed in the 2022 ICC. Key points • Lymphoplasmacytic lymphoma can be diagnosed with lymphoplasmacytic aggregates in trephine biopsies < 10% of cellularity and evidence of clonal B-cells and plasma cells. • IgM MGUS is subdivided into a plasma cell type and a not otherwise specified (NOS) type. • Primary cold agglutinin disease is recognized as a new entity. • The term “multiple myeloma” replaces the term “plasma cell myeloma” used in the 2016 WHO classification. • Multiple myeloma is subdivided into 4 mutually exclusive cytogenetic groups and MM NOS. • Minimal bone marrow infiltration detected by flow cytometry is of major prognostic importance for solitary plasmacytoma of bone and to a lesser extent for primary extraosseous plasmacytoma. • Localized IG light chain amyloidosis is recognized as a separate entity, distinct from systemic immunoglobulin light chain (AL) amyloidosis.

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Genomic profiling for clinical decision making in lymphoid neoplasms

Cited by 70 publications

References 505 publications

Targeting IRAK4 with Emavusertib in Lymphoma Models with Secondary Resistance to PI3K and BTK Inhibitors

Targeting IRAK4 with Emavusertib in Lymphoma Models with Secondary Resistance to PI3K and BTK Inhibitors

Successful CNS-Centric Therapeutic Management and Genomic Profiling of Primary Cranial Vault Diffuse Large B-Cell Lymphoma

Plasma cell neoplasms and related entities—evolution in diagnosis and classification

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