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Immunomodulatory drugs in multiple myeloma

机译:多发性骨髓瘤的免疫调节药物

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Immunomodulatory drugs(IMiDs)are thalidomide analogues that retain the direct anticancer cytotoxic and immunological activity of their parent compound,but with a different toxicity profile.In vitro studies show that IMiDs have a more potent antitumour effect than thalidomide on multiple myeloma(MM)cell lines.This activity is mediated by multiple mechanisms:direct antiproliferative effect;inhibition of angiogenesis due to reduced IL-6 and vascular endothelial growth factor secretion;inhibition of cytokines production,especially TNF-alpha;and stimulation of T-cell activity.Two IMiDs,CC-5013 and CC-4047,have been tested in clinical trials in MM patients with progressive or refractory disease,and one trial is ongoing in newly diagnosed MM patients.Observed toxicities include thrombocytopoenia,neutropoenia and cardiovascular events,but no significant neurotoxicity has been reported.Partial responses(>= 50% reduction in M-protein)ranged from 20 to 71% in different studies depending on the pretreatment status of the patients.The combination of IMiDs with dexamethasone may be beneficial.
机译:免疫调节药物(IMiDs)是沙利度胺类似物,保留了其母体化合物的直接抗癌细胞毒性和免疫活性,但毒性谱不同。体外研究表明,IMiDs在多发性骨髓瘤(MM)细胞方面比沙利度胺更有效的抗肿瘤作用该活性由多种机制介导:直接的抗增殖作用;由于IL-6和血管内皮生长因子分泌减少而抑制血管生成;抑制细胞因子产生,特别是TNF-α;以及刺激T细胞活性。两个IMiDs ,CC-5013和CC-4047已在进行性或难治性MM病患的临床试验中进行了测试,一项正在新诊断的MM病患中进行的试验正在进行中。在不同的研究中,部分反应(M蛋白减少> == 50%)的范围从20%到71%不等。 IMiDs与地塞米松的组合可能是有益的。

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