A virtual approach to evaluate therapies for management of multiple myeloma induced bone disease

被引:2
|
作者
Ji, Bing [1 ]
Genever, Paul G. [2 ]
Fagan, Michael J. [3 ]
机构
[1] Shandong Univ, Sch Control Sci & Engn, Jinan 250061, Peoples R China
[2] Univ York, Dept Biol, York YO10 5DD, N Yorkshire, England
[3] Univ Hull, Sch Engn, Kingston Upon Hull HU6 7RX, N Humberside, England
基金
中国国家自然科学基金; 英国工程与自然科学研究理事会;
关键词
multiple myeloma; bone disease; therapies; mathematical model; KAPPA-B LIGAND; RECEPTOR ACTIVATOR; ZOLEDRONIC ACID; GROWTH-FACTOR; TUMOR; BISPHOSPHONATES; OSTEOPROTEGERIN; INTERLEUKIN-6; MARROW; DIFFERENTIATION;
D O I
10.1002/cnm.2735
中图分类号
R318 [生物医学工程];
学科分类号
0831 ;
摘要
Multiple myeloma bone disease is devastating for patients and a major cause of morbidity. The disease leads to bone destruction by inhibiting osteoblast activity while stimulating osteoclast activity. Recent advances in multiple myeloma research have improved our understanding of the pathogenesis of multiple myeloma-induced bone disease and suggest several potential therapeutic strategies. However, the effectiveness of some potential therapeutic strategies still requires further investigation and optimization. In this paper, a recently developed mathematical model is extended to mimic and then evaluate three therapies of the disease, namely: bisphosphonates, bortezomib and TGF- inhibition. The model suggests that bisphosphonates and bortezomib treatments not only inhibit bone destruction, but also reduce the viability of myeloma cells. This contributes to the current debate as to whether bisphosphonate therapy has an anti-tumour effect. On the other hand, the analyses indicate that treatments designed to inhibit TGF- do not reduce bone destruction, although it appears that they might reduce the viability of myeloma cells, which again contributes to the current controversy regarding the efficacy of TGF- inhibition in multiple myeloma-induced bone disease. (c) 2015 The Authors. International Journal for Numerical Methods in Biomedical Engineering published by John Wiley & Sons Ltd.
引用
收藏
页码:1 / 18
页数:18
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