Germinal center‐derived lymphomas: The darkest side of humoral immunity

Mlynarczyk, Coraline; Fontán, Lorena; Melnick, Ari

doi:10.1111/imr.12755

Cited by 116 publications

(133 citation statements)

References 226 publications

(477 reference statements)

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“…The hope is that more detailed knowledge of the cellular and molecular mechanisms that underlie the generation of protective, long-lived antibody responses and B cell memory will allow the development of safe, effective vaccines for pathogens for which we currently have none. Moreover, such knowledge may have broader benefits; for example, for the development of therapies for both systemic autoimmune disease and B cell tumours that may be, in part, unintended consequences of the drive to generate B cell memory 6,7 .…”

mentioning

confidence: 99%

B cell memory: building two walls of protection against pathogens

2019

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Surviving a single infection often results in lifelong immunity to the infecting pathogen. Such protection is mediated, in large part, by two main B cell memory 'walls'-namely , longlived plasma cells and memory B cells. The cellular and molecular processes that drive the production of long-lived plasma cells and memory B cells are subjects of intensive research and have important implications for global health. Indeed, although nearly all vaccines in use today depend on their ability to induce B cell memory , we have not yet succeeded in developing vaccines for some of the world's most deadly diseases, including AIDS and malaria. Here, we describe the two-phase process by which antigen drives the generation of long-lived plasma cells and memory B cells and highlight the challenges for successful vaccine development in each phase.

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confidence: 99%

B cell memory: building two walls of protection against pathogens

2019

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“…The intrinsic force of B cell development—the sequence of V(D)J recombination, CSR, and SHM—can lead to somatic mutations within numerous oncogenes that are associated with lymphomagenesis and their cell-of-origin stemming from the pre-GC, GC, or the post-GC [ 35 , 36 ]. The GC B cell, for instance, is at high risk of undergoing malignant transformation due to genetic lesions that occur in GC-specific DNA remodeling events for Ig affinity maturation [ 37 ]. Beyond mere B cell development, several alterations in DNA repair pathways have been linked to lymphoma susceptibility [ 38 ].…”

Section: Role Of Dna Repair In B Cell Development and Lymphomagenementioning

confidence: 99%

Targeting DNA Repair, Cell Cycle, and Tumor Microenvironment in B Cell Lymphoma

Bröckelmann

Jong

Jachimowicz

2020

Cells

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The DNA double-strand break (DSB) is the most cytotoxic lesion and compromises genome stability. In an attempt to efficiently repair DSBs, cells activate ATM kinase, which orchestrates the DNA damage response (DDR) by activating cell cycle checkpoints and initiating DSB repair pathways. In physiological B cell development, however, programmed DSBs are generated as intermediates for effective immune responses and the maintenance of genomic integrity. Disturbances of these pathways are at the heart of B cell lymphomagenesis. Here, we review the role of DNA repair and cell cycle control on B cell development and lymphomagenesis. In addition, we highlight the intricate relationship between the DDR and the tumor microenvironment (TME). Lastly, we provide a clinical perspective by highlighting treatment possibilities of defective DDR signaling and the TME in mantle cell lymphoma, which serves as a blueprint for B cell lymphomas.

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“…Cell signaling pathways are critical in B‐NHL pathophysiology . B‐NHL cells are, in most instances, dependent on constitutively active cascades that transmit survival and proliferation inputs from the surface membrane to the nucleus, where transcriptional and epigenetic processes translate the signals in effective outputs, like cell cycle progression, apoptosis inhibition, and invasiveness . On the basis of this, aberrant signal transduction is genetic and epigenetic mechanisms as well as the origination of an abnormal tumor microenvironment.…”

Section: Signaling In Nhlmentioning

confidence: 99%

New responsibilities for aged kinases in B‐lymphomas

Manni

Arjomand

Visentin

et al. 2019

Hematological Oncology

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The knowledge accumulated over the last decade on B-cell-derived non-Hodgkin lymphoma (B-NHL) pathogenesis has led to the identification of several molecular abnormalities, opening new perspectives in the design of novel therapies. Indeed, drugs targeting specific biochemical pathways critical for B-NHL cell survival, proliferation, and fitness within the malignant microenvironment are now available to the clinician: the B-cell receptor signaling inhibitors of BTK, PI3Kδ, ζ, γ, and SYK or the pro-apoptotic BH3-mimetics are clear examples of it. Moreover, it is emerging that malignant B-cell growth is sustained not only by mutations in oncogenes/tumor suppressors but also by the "addiction" to nononcogene (ie, nonstructurally altered) molecules. In this regard, a consistent body of data has established that the Ser/Thr kinases CK1, CK2, and GSK3 are involved in malignant lymphocyte biology and act as pro-survival and signaling-boosting molecules, both in precursor and mature B-cell tumors. Currently, an experimental and clinical groundwork is available, upon which to design CK1-, CK2-, and GSK3-directed antilymphoma/leukemia therapies. In this review, we have examined the main features of CK1, CK2, and GSK3 kinases, summarized the data in B-NHL supporting them as suitable therapeutic targets, and proposed a perspective on potential future research development. K E Y W O R D S B lymphocytes, CK1, CK2, GSK3, lymphoma, protein kinase 1 | EVOLVING PARADIGMS IN NON-HODGKIN LYMPHOMAS Non-Hodgkin lymphomas (NHL) are collectively the most frequent hematologic cancer, among the top 10 most frequent malignant tumors worldwide. 1 B-cell-derived NHL (B-NHL) are by far more frequent than T-cell-derived NHL, and between them, tumors arising from the mature B cell are more frequent. The 2016 World Health Organization (WHO) classification of NHL has recognized approximately 60 distinct entities. 2 In the group of B-NHL, diffuse large B-cell lymphoma (DLBCL) is the most frequent subtype, accounting for 35% of all B-NHL, followed by follicular lymphoma (FL), which accounts for up to 20% to 25% of B-NHL. These two B-NHL subtypes originate from germinal center (GC) centrocytes/centroblasts. 3 However, a proportion of DLBCL are from post-GC origin, the so called "activated B-cell" (ABC)-type DLBCL. Patients affected by this latter subtype are believed to be subjected to a more dismal prognosis as compared with those with GC B-cell (GCB) type. 4 Other less frequent B-NHL are mantle cell lymphoma (MCL, approximately 10% of all B-NHL), marginal zone lymphoma (MZL, about 5% of all B-NHL), small lymphocyte lymphoma/chronic lymphocytic leukemia (SLL/CLL, 5%), lymphoplasmacytic lymphoma (LPL, 3%). 2 Deep sequencing of the genome and the transcriptome has provided a great amount of data describing mutations and aberrant expression of cell signaling molecules. For instance, the molecular classification of DLBCL has been progressively refined from the seminal paper of Alizadeh describing the GCB/ABC/undetermined subtypes, 4 based on gene expres...

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Germinal center‐derived lymphomas: The darkest side of humoral immunity

Cited by 116 publications

References 226 publications

B cell memory: building two walls of protection against pathogens

B cell memory: building two walls of protection against pathogens

Targeting DNA Repair, Cell Cycle, and Tumor Microenvironment in B Cell Lymphoma

New responsibilities for aged kinases in B‐lymphomas

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