Multiple Myeloma Exemplifies a Model of Cancer Based on Tissue Disruption as the Initiator Event

Capp, Jean‐Pascal; Bataille, Régis

doi:10.3389/fonc.2018.00355

Cited by 22 publications

(31 citation statements)

References 90 publications

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“…This process could only initiate with a loss of the environmental constraints present in the healthy tissue, whatever genetic alterations are present or not in the cells, because they are known to control the level of cellular stochasticity. This TiDiS theory is supported by much experimental evidence that has been reviewed elsewhere [63][64][65]71], especially in the context of MM [60].…”

Section: General Scheme Of the Tidis Theorymentioning

confidence: 53%

“…During the malignant transition from MGUS to overt MM, both mechanisms interact to accentuate the disruption, and facilitate the occurrence of the MM bone disease, not only LBL, but also generalized bone loss, the second component of the MM bone disease (Table 3). We and others have previously emphasized that the natural history of MM includes a pre-MGUS phase, characterized by a hyper-gammaglobulinemia, reactive plasmacytosis (excess of circulating plasmablasts) or even transient MGUS in a context of immune deficiency [60,61]. Genetically altered memory B cells and plasmablasts could expand during such a pre-MGUS stage, because they remain sensitive to both polyclonal B cell activation and specific antigenic activation.…”

Section: Extended Model To the Bmementioning

confidence: 99%

“…Much experimental evidence indicates that the normal microenvironment is able to control genetically altered cells and reduce phenotypic plasticity [21,[63][64][65]71]. Thus, mimicking this normal micro-environment with molecules that would mimic healthy cellular interactions, together with molecules stimulating the re-expression of the proteins necessary to interact with these partners, would be efficient in stopping cell proliferation and cancer evolution [60,74].…”

Section: Perspectives For the Management Of MMmentioning

confidence: 99%

“…In the future, epigenetic-based treatments are clearly adequate for the first step that is to re-establish the initial interactions of MM cells with the BME. In MM, knowing the role of decorins and other interaction proteins in the inhibitory effects of osteoblasts over MM cells [79], providing decorins or "pseudo-decorins" as soluble proteins, and/or promoting osteoblast activity [80][81][82] would be good candidates for the second step [60], which is to mimic their inhibitory effects. Providing such peptides that mimic interactions domains of key environmental proteins could substitute for normal osteoblasts.…”

Section: Perspectives For the Management Of MMmentioning

confidence: 99%

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Multiple Myeloma as a Bone Disease? The Tissue Disruption-Induced Cell Stochasticity (TiDiS) Theory

Capp¹,

Bataille

2020

Cancers

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The standard model of multiple myeloma (MM) relies on genetic instability in the normal counterparts of MM cells. MM-induced lytic bone lesions are considered as end organ damages. However, bone is a tissue of significance in MM and bone changes could be at the origin/facilitate the emergence of MM. We propose the tissue disruption-induced cell stochasticity (TiDiS) theory for MM oncogenesis that integrates disruption of the microenvironment, differentiation, and genetic alterations. It starts with the observation that the bone marrow endosteal niche controls differentiation. As decrease in cellular stochasticity occurs thanks to cellular interactions in differentiating cells, the initiating role of bone disruption would be in the increase of cellular stochasticity. Thus, in the context of polyclonal activation of B cells, memory B cells and plasmablasts would compete for localizing in endosteal niches with the risk that some cells cannot fully differentiate if they cannot reside in the niche because of a disrupted microenvironment. Therefore, they would remain in an unstable state with residual proliferation, with the risk that subclones may transform into malignant cells. Finally, diagnostic and therapeutic perspectives are provided.

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Section: General Scheme Of the Tidis Theorymentioning

confidence: 53%

Section: Extended Model To the Bmementioning

confidence: 99%

Section: Perspectives For the Management Of MMmentioning

confidence: 99%

Section: Perspectives For the Management Of MMmentioning

confidence: 99%

See 2 more Smart Citations

Multiple Myeloma as a Bone Disease? The Tissue Disruption-Induced Cell Stochasticity (TiDiS) Theory

Capp¹,

Bataille

2020

Cancers

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“…The perturbation in PMDs occurs at the epigenetic, transcriptomic and 3D organization levels and is responsible for interpatient variability. This disturbance in PMDs could explain, in part, some aberrant and heterogeneous phenotypes across MM samples [57,58]. In addition, the lack of accurate global DNA methylation maintenance also drives intrapatient DNA methylation heterogeneity, which can contribute to intrapatient variability, allowing cell-to-cell diversity in transcriptional programs and opening multiple trajectories in response to therapy (Additional file 3: Figure S25).…”

Section: Resultsmentioning

confidence: 99%

The DNA methylation landscape of multiple myeloma shows extensive inter- and intrapatient heterogeneity that fuels transcriptomic variability

Derrien

Guérin‐Charbonnel

Gaborit

et al. 2020

Preprint

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Background: Cancer evolution depends on epigenetic and genetic diversity. Historically, in multiple myeloma (MM), subclonal diversity and tumor evolution have been investigated mostly from a genetic perspective. Results: Here, we combined the notions of epipolymorphism and epiallele switching to analyze DNA methylation heterogeneity in MM patients. We show that MM is characterized by the continuous accumulation of stochastic methylation at the promoters of development-related genes. High entropy change is associated with poor outcomes and depends predominantly on partially methylated domains (PMDs). These PMDs, which represent the major source of inter- and intrapatient DNA methylation heterogeneity in MM, are linked to other key epigenetic aberrations, such as CpG island (CGI)/transcription start site (TSS) hypermethylation and H3K27me3 redistribution as well as 3D organization alterations. In addition, transcriptome analysis revealed that intratumor methylation heterogeneity was associated with low-level expression and high variability. Conclusion: We propose that disordered methylation in MM is responsible for high epigenetic and transcriptomic instability allowing tumor cells to adapt to environmental changes by tapping into a pool of evolutionary trajectories.

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Overexpression of wild type or a Q311E mutant MB21D2 promotes a pro‐oncogenic phenotype in HNSCC

et al. 2020

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Cadherin-mediated cell-cell contacts regulated by intracellular binders play critical roles in tissue homeostasis and tumorigenesis. Here, we screened mutational profiles of 312 annotated genes involved in cadherin binding in human squamous cell carcinomas and found MB21D2 to carry a unique recurrent Q311E mutation. MB21D2 overexpression was also frequently found in head and neck cancer (HNSCC) and was associated with poor clinical outcomes. Cell-based characterizations revealed pro-oncogenic roles for MB21D2 wild-type (WT) and its Q311E mutant (Q311E) in cell proliferation, colony formation, sphere growth, and migration/invasion by promoting epithelial-mesenchymal transition. Conversely, MB21D2 knockdown in MB21D2-overexpressing cells resulted in cell growth arrest and apoptosis. Xenograft tumor models with Q311E-expressing cells formed larger and more aggressive lesions, compared to models with WT-MB21D2-expressing cells or an empty vector. Transcriptome and protein interactome analyses revealed enrichment of KRAS signaling by MB21D2 expression. Immunoblotting confirmed RAS elevation, along with upregulation/phosphorylation of PI3K, AKT, and CREB. Blocking RAS signaling in MB21D2-expressing cells by manumycin significantly reduced cell growth and survival. Our study thus defined RAS signaling-dependent prooncogenic roles for MB21D2 overexpression and Q311E MB21D2 expression in HNSCC development. Abbreviations GEPIA, gene expression profiling interactive analysis; HNSCC, head and neck squamous cell carcinoma; KRAS, Kirsten rat sarcoma viral oncogene homolog (KRAS proto-oncogene, GTPase); MB21D2, Mab-21-containing domain 2; PI3K, phospho-inositol kinase 3; Q311E, change in glutamine at the position 311 to glutamic acid; SCCs, squamous cell carcinoma(s; TCGA, The Cancer Genome Atlas; WT, in this study, wild-type MB21D2.

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Multiple Myeloma Exemplifies a Model of Cancer Based on Tissue Disruption as the Initiator Event

Cited by 22 publications

References 90 publications

Multiple Myeloma as a Bone Disease? The Tissue Disruption-Induced Cell Stochasticity (TiDiS) Theory

Multiple Myeloma as a Bone Disease? The Tissue Disruption-Induced Cell Stochasticity (TiDiS) Theory

The DNA methylation landscape of multiple myeloma shows extensive inter- and intrapatient heterogeneity that fuels transcriptomic variability

Overexpression of wild type or a Q311E mutant MB21D2 promotes a pro‐oncogenic phenotype in HNSCC

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