Dana-Farber Cancer Institute, Boston, MA, USA.
Blood. 2011 May 5;117(18):4696-700. doi: 10.1182/blood-2010-10-300970. Epub 2011 Feb 3.
A panel of members of the 2009 International Myeloma Workshop developed guidelines for risk stratification in multiple myeloma. The purpose of risk stratification is not to decide time of therapy but to prognosticate. There is general consensus that risk stratification is applicable to newly diagnosed patients; however, some genetic abnormalities characteristic of poor outcome at diagnosis may suggest poor outcome if only detected at the time of relapse. Thus, in good-risk patients, it is necessary to evaluate for high-risk features at relapse. Although detection of any cytogenetic abnormality is considered to suggest higher-risk disease, the specific abnormalities considered as poor risk are cytogenetically detected chromosomal 13 or 13q deletion, t(4;14) and del17p, and detection by fluorescence in situ hybridization of t(4;14), t(14;16), and del17p. Detection of 13q deletion by fluorescence in situ hybridization only, in absence of other abnormalities, is not considered a high-risk feature. High serum β(2)-microglobulin level and International Staging System stages II and III, incorporating high β(2)-microglobulin and low albumin, are considered to predict higher risk disease. There was a consensus that the high-risk features will change in the future, with introduction of other new agents or possibly new combinations.
一个由 2009 年国际骨髓瘤工作组的成员组成的小组制定了多发性骨髓瘤风险分层的指南。风险分层的目的不是决定治疗时间,而是进行预后。人们普遍认为,风险分层适用于新诊断的患者;然而,一些在诊断时就具有不良预后特征的遗传异常,如果仅在复发时检测到,也可能提示预后不良。因此,在低危患者中,有必要在复发时评估高危特征。虽然任何细胞遗传学异常的检测都被认为提示疾病具有更高的风险,但被认为是不良风险的具体异常包括细胞遗传学检测到的染色体 13 或 13q 缺失、t(4;14)和 del17p,以及通过荧光原位杂交检测到的 t(4;14)、t(14;16)和 del17p。仅通过荧光原位杂交检测到 13q 缺失,而没有其他异常,不被认为是高危特征。高血清β(2)-微球蛋白水平和国际分期系统的 II 期和 III 期,包括高β(2)-微球蛋白和低白蛋白,被认为预测疾病具有更高的风险。有共识认为,随着新药物或新的联合治疗方法的引入,高危特征将在未来发生变化。
