| Literature DB >> 30682861 |
Romana Butova1, Petra Vychytilova-Faltejskova2, Adela Souckova3, Sabina Sevcikova4, Roman Hajek5.
Abstract
Multiple myeloma (MM) is the second most common hematooncological disease of malignant plasma cells in the bone marrow. While new treatment brought unprecedented increase of survival of patients, MM pathogenesis is yet to be clarified. Increasing evidence of expression of long non-coding RNA molecules (lncRNA) linked to development and progression of many tumors suggested their important role in tumorigenesis. To date, over 15,000 lncRNA molecules characterized by diversity of function and specificity of cell distribution were identified in the human genome. Due to their involvement in proliferation, apoptosis, metabolism, and differentiation, they have a key role in the biological processes and pathogenesis of many diseases, including MM. This review summarizes current knowledge of non-coding RNAs (ncRNA), especially lncRNAs, and their role in MM pathogenesis. Undeniable involvement of lncRNAs in MM development suggests their potential as biomarkers.Entities:
Keywords: biomarker; long non-coding RNAs; multiple myeloma
Year: 2019 PMID: 30682861 PMCID: PMC6468639 DOI: 10.3390/ncrna5010013
Source DB: PubMed Journal: Noncoding RNA ISSN: 2311-553X
Figure 1Four archetypes of long non-coding RNA (lncRNA) molecular mechanisms.
Specific long non-coding RNAs found in multiple myeloma cells.
| Specific lncRNA | Expression in MM vs. Normal | Results of Changed Expression in MM | Effect of Reversed Expression Profile | References |
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| Cell cycle positive regulation via CREB regulation | [ | |
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| Increased DEX resistance | Sensitivity to DEX | [ |
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| Increased proliferation | Decreased proliferation, proteasome inhibition | [ |
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| Negative effect to osteogenesis of mesenchymal stem cells (MSC) | MM–MSC differentiation | [ |
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| Chemoresistance | Inhibition of myeloma autophagy | [ |
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| Increased cell proliferation | Cell inhibition, cell arrest, and apoptosis induction | [ |
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| Increased tumor growth | Tumor growth inhibition, promotion of apoptosis, and sensitivity to bortezomib | [ |
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| Oncogenic role via positive regulation of HOXA1 expression | Cell proliferation inhibition, promotion of apoptosis, and tumor growth suppression in vivo | [ |
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| Increased cell proliferation via miR-410 accumulation | [ | |
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| Increased tumor progression via negative regulation of miR-451 | Cell proliferation inhibition, promotion of apoptosis | [ |
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| Increased proliferation through NF-κB pathway | Inhibition of proliferation and viability | [ |
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| Promoting of proliferation, migration, and invasion | Suppression of cell proliferation, invasion, and colony formation | [ |
lncRNA: long non-coding RNA; MM: multiple myeloma; DEX: dexamethasone; CREB: cyclic AMP response element binding protein; MSC: mesenchymal stem cells; HOXA1: homeobox A1.