Towards Stratified Medicine in Plasma Cell Myeloma

被引:13
作者
Egan, Philip [1 ]
Drain, Stephen [1 ]
Conway, Caroline [1 ]
Bjourson, Anthony J. [1 ]
Alexander, H. Denis [1 ]
机构
[1] Univ Ulster, Northern Ireland Ctr Stratified Med, Biomed Sci Res Inst, Altnagelvin Area Hosp, C TRIC Bldg,Glenshane Rd, Derry Londonderry BT47 6SB, North Ireland
关键词
plasma cell myeloma; multiple myeloma; plasma cell dyscrasias; personalised medicine; flow cytometry; Next Generation Sequencing; proteasome inhibitors; immunomodulatory drugs; microRNAs; MINIMAL RESIDUAL DISEASE; INTERNATIONAL STAGING SYSTEM; UPDATED MAYO STRATIFICATION; PROGRESSION-FREE SURVIVAL; RISK MULTIPLE-MYELOMA; LONG-TERM SURVIVAL; FREE LIGHT-CHAIN; MONOCLONAL GAMMOPATHY; UNDETERMINED SIGNIFICANCE; CLINICAL-SIGNIFICANCE;
D O I
10.3390/ijms17101760
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Plasma cell myeloma is a clinically heterogeneous malignancy accounting for approximately one to 2% of newly diagnosed cases of cancer worldwide. Treatment options, in addition to long-established cytotoxic drugs, include autologous stem cell transplant, immune modulators, proteasome inhibitors and monoclonal antibodies, plus further targeted therapies currently in clinical trials. Whilst treatment decisions are mostly based on a patient's age, fitness, including the presence of co-morbidities, and tumour burden, significant scope exists for better risk stratification, sub-classification of disease, and predictors of response to specific therapies. Clinical staging, recurring acquired cytogenetic aberrations, and serum biomarkers such as beta-2 microglobulin, and free light chains are in widespread use but often fail to predict the disease progression or inform treatment decision making. Recent scientific advances have provided considerable insight into the biology of myeloma. For example, gene expression profiling is already making a contribution to enhanced understanding of the biology of the disease whilst Next Generation Sequencing has revealed great genomic complexity and heterogeneity. Pathways involved in the oncogenesis, proliferation of the tumour and its resistance to apoptosis are being unravelled. Furthermore, knowledge of the tumour cell surface and its interactions with bystander cells and the bone marrow stroma enhance this understanding and provide novel targets for cell and antibody-based therapies. This review will discuss the development in understanding of the biology of the tumour cell and its environment in the bone marrow, the implementation of new therapeutic options contributing to significantly improved outcomes, and the progression towards more personalised medicine in this disorder.
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页数:21
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