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Clinical implications of gene expression profiling in myelodysplastic syndromes: recognition of ribosomal and translational gene dysregulation and development of predictive assays.

机译:骨髓增生异常综合症中基因表达谱的临床意义:核糖体和翻译基因失调的认识和预测性测定的发展。

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摘要

Myelodysplastic syndromes (MDS) are a group of haematopoietic stem cell disorders that pose a unique challenge for gene expression profiling by virtue of their inherent heterogeneity. Despite monoclonality of MDS, the marrow picture is complicated by the presence of not only stromal cells but also by varying stages of differentiating diseased cells belonging to all three lineages. Now that reproducible results can be obtained from nanograms of RNA, it is possible to derive useful information from even a limited number of cells; for example, dysregulation of ribosomal and translational genes was detected in MDS patients compared to controls using a small number of CD34+ cells. Gene expression profiling in MDS patients treated with lenalidomide or 5-azacitidine+thalidomide yielded signatures which differentiated responders from non-responders. These biologic and clinical insights are providing the framework on which to build a new model of these diseases which, despite their heterogeneity, manifest certain unifying themes.
机译:骨髓增生异常综合症(MDS)是一组造血干细胞疾病,由于其固有的异质性,它们对基因表达谱构成了独特的挑战。尽管MDS具有单克隆性,但骨髓基质细胞不仅由于基质细胞的存在而复杂化,而且由于分化属于所有三个谱系的患病细胞的不同阶段而变得复杂。现在,可以从纳克的RNA中获得可重复的结果,甚至可以从有限数量的细胞中获得有用的信息。例如,与使用少量CD34 +细胞的对照组相比,在MDS患者中检测到核糖体和翻译基因的失调。在来那度胺或5-氮杂胞苷+沙利度胺治疗的MDS患者中的基因表达谱产生了区分反应者和非反应者的特征。这些生物学和临床方面的见识为建立这些疾病的新模型提供了框架,这些模型尽管具有异质性,但仍表现出某些统一的主题。

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