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意义未明的单克隆丙种球蛋白病:介绍与当前临床问题

Monoclonal gammopathy of undeterminated significance: introduction and current clinical issues.

作者信息

Klincová M, Sandecká V, Mikuláiová A, Radocha J, Maisnar V, Hájek R

机构信息

Department of Internal Medicine-Hematooncology, University Hospital Brno, Czech Republic.

出版信息

Klin Onkol. 2011;24 Suppl:S14-7.

PMID:21923058
Abstract

Monoclonal gammopathy of undetermined significance (MGUS) is a precancerosis comprising two different kinds of cancer: lymphoid/lymphoplasmocytoid MGUS and plasma cell MGUS that represents about 85% of all MGUS cases. This type of MGUS has low but persistent tendency to transform to malignant disease, mainly multiple myeloma (MM), with frequency of about 1% per year. Using known risk stratification models based on clinical parameters, it is possible to identify patients' groups with average rates of progression as low as 0.26% and as high as 12% per year. However, due to the lack of clear genetic and/or phenotypic markers distinguishing MGUS from MM, we are not able to predict if and when MGUS will progress to MM in individual patients. There are partially overlapping molecular pathogenic events shared by MGUS and MM. Better understanding of pathogenesis of MGUS and MM using molecular-genetic approaches will help disclose the mechanisms of myeloma genesis; it can be also useful for identification of novel molecular targets. The ultimate goal for the near future is to develop better markers for definition of high-risk MGUS patients who will be candidates for early treatment intervention.

摘要

意义未明的单克隆丙种球蛋白病(MGUS)是一种癌前病变,包括两种不同类型的癌症:淋巴样/淋巴浆细胞样MGUS和浆细胞MGUS,后者约占所有MGUS病例的85%。这种类型的MGUS虽有转变为恶性疾病的可能性,但概率较低且持续存在,主要转变为多发性骨髓瘤(MM),每年的转变频率约为1%。利用基于临床参数的已知风险分层模型,可以识别出每年进展率低至0.26%和高达12%的患者群体。然而,由于缺乏区分MGUS与MM的明确遗传和/或表型标志物,我们无法预测个体患者中的MGUS是否以及何时会进展为MM。MGUS和MM存在部分重叠的分子致病事件。使用分子遗传学方法更好地理解MGUS和MM的发病机制将有助于揭示骨髓瘤的发生机制;这对于识别新的分子靶点也可能有用。近期的最终目标是开发更好的标志物,以确定将成为早期治疗干预候选者的高危MGUS患者。

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