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首页> 外文期刊>Clinical cancer research: an official journal of the American Association for Cancer Research >A gene expression-based predictor for myeloma patients at high risk of developing bone disease on bisphosphonate treatment.
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A gene expression-based predictor for myeloma patients at high risk of developing bone disease on bisphosphonate treatment.

机译:一种基于基因表达的预测因子,用于双膦酸盐治疗时罹患骨病高风险的骨髓瘤患者。

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摘要

PURPOSE: Myeloma bone disease impairs quality of life and is associated with impaired survival. Even with effective bisphosphonate treatment, a significant proportion of patients still develop skeletal-related events (SRE). Identifying such patients at presentation would allow treatment modification. EXPERIMENTAL DESIGN: To investigate the molecular basis of bone disease at presentation and to develop a predictive signature for patients at high risk of developing SREs on bisphosphonates, 261 presenting myeloma samples were analyzed by global gene expression profiling. The derived "SRE gene signature" was complemented by the integration of associated clinical parameters to generate an optimal predictor. RESULTS: Fifty genes were significantly associated with presenting bone disease, including the WNT signaling antagonist DKK1 and genes involved in growth factor signaling and apoptosis. Higher serum calcium level and the presence of bone disease and hyperdiploidy at presentation were associated with high risk of SRE development. A gene signature derived from the fourteen genes overexpressed in the SRE group was able to identify patients at high risk of developing an SRE on treatment. These genes either belonged to the IFN-induced family or were involved in cell signaling and mitosis. Multivariate logistic model selection yielded an optimal SRE predictor comprising seven genes and calcium level, which was validated as an effective predictor in a further set of patients. CONCLUSIONS: The simple expression-based SRE predictor can effectively identify individuals at high risk of developing bone disease while being on bisphosphonates. This predictor could assist with developing future trials on novel therapies aimed at reducing myeloma bone disease.
机译:目的:骨髓瘤骨病损害生活质量,并与生存受损有关。即使采用有效的双膦酸盐治疗,仍有相当一部分患者仍会发生骨骼相关事件(SRE)。在就诊时识别此类患者将允许进行治疗修改。实验设计:为了研究呈现时骨骼疾病的分子基础,并为在双膦酸盐上发生SRE的高风险患者建立预测特征,通过整体基因表达谱分析了261个存在的骨髓瘤样品。衍生的“ SRE基因签名”通过相关临床参数的整合得到补充,以生成最佳预测因子。结果:五十个基因与当前的骨病显着相关,包括WNT信号转导拮抗剂DKK1和涉及生长因子信号转导和凋亡的基因。出现时较高的血清钙水平以及骨骼疾病和双倍体的存在与SRE发生的高风险相关。来自SRE组中过表达的14个基因的基因签名能够识别出在治疗中发展SRE的高风险患者。这些基因要么属于IFN诱导的家族,要么参与细胞信号转导和有丝分裂。多变量逻辑模型选择产生了包含七个基因和钙水平的最佳SRE预测因子,这在另一组患者中被确认为有效的预测因子。结论:基于简单表达的SRE预测因子可以有效地识别使用双膦酸盐治疗时处于发生骨病高风险的个体。该预测因子可以协助开发针对减少骨髓瘤骨病的新疗法的未来试验。

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