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Prognostic models in myelodysplastic syndromes

机译:骨髓增生异常综合症的预后模型

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Establishing the prognosis for patients with myelodysplastic syndromes (MDS) is a key element of their care. It helps patients understand the severity of their disease and set expectations for their future. For physicians, an accurate estimate of prognosis drives decisions about the timing and choice of therapeutic options to consider. The International Prognostic Scoring System (IPSS) has been the standard tool for MDS risk stratification since it was released in 1997. It has been used to describe patients in pivotal clinical trials and is a key element of practice guidelines. Subsequent changes to the classification scheme for MDS and an underestimation of risk in some patients from the low and intermediate-1 categories have led to the development of several newer prognostic models. The most recent is the revised IPSS (IPSS-R), which addresses several of the perceived deficiencies of its predecessor. Despite their utility, none of the available prognostic systems incorporates disease-related molecular abnormalities such as somatic mutations. These lesions are present in the nearly all cases and many have been shown to improve upon existing prognostic models. However, the interpretation of somatic mutations can be challenging and it is not yet clear how best to combine them with clinical predictors of outcome. Here I review several prognostic scoring systems developed after the IPSS and describe the emerging use of molecular markers to refine risk stratification in the MDS patient population.
机译:建立骨髓增生异常综合症(MDS)患者的预后是其护理的关键要素。它可以帮助患者了解疾病的严重性并设定对未来的期望。对于医生而言,对预后的准确估计将决定要考虑的治疗方案的时机和选择。自1997年发布以来,国际预后评分系统(IPSS)一直是MDS风险分层的标准工具。它已被用于描述关键临床试验中的患者,并且是实践指南的关键要素。随后对MDS分类方案的更改以及一些低级和中级1类患者对风险的低估导致了几种新的预后模型的发展。最新的是修订后的IPSS(IPSS-R),它解决了其前身的一些公认缺陷。尽管具有实用性,但现有的预后系统均未包含与疾病相关的分子异常,例如体细胞突变。这些病变几乎存在于所有病例中,并且许多病变已显示可改善现有的预后模型。然而,对体细胞突变的解释可能具有挑战性,目前尚不清楚如何最好地将它们与临床预后指标结合起来。在这里,我回顾了IPSS之后开发的几种预后评分系统,并描述了分子标记物在MDS患者人群中改善风险分层的新兴应用。

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