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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >MGUS to myeloma: a mysterious gammopathy of underexplored significance
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MGUS to myeloma: a mysterious gammopathy of underexplored significance

机译:MGU至骨髓瘤:一个神秘的血管病的巨大意义

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All cases of multiple myeloma (MM) are preceded by precursor states termed monoclonal gammopathy of undetermined significance (MGUS) or smoldering myeloma (SMM). Genetic analyses of MGUS cells have provided evidence that it is a genetically advanced lesion, wherein tumor cells carry many of the genetic changes found in MM cells. Intraclonal heterogeneity is also established early during the MGUS phase. Although the genetic features of MGUS or SMM cells at baseline may predict disease risk, transition to MM involves altered growth of preexisting clones. Recent advances in mouse modeling of MGUS suggest that the clinical dormancy of the clone may be regulated in part by growth controls extrinsic to the tumor cells. Interactions of MGUS cells with immune cells, bone cells, and others in the bone marrow niche may be key regulators of malignant transformation. These interactions involve a bidirectional crosstalk leading to both growth-supporting and inhibitory signals. Because MGUS is already a genetically complex lesion, application of new tools for earlier detection should allow delineation of earlier stages, which we term as pre-MGUS. Analyses of populations at increased risk of MGUS also suggest the possible existence of a polyclonal phase preceding the development of MGUS. Monoclonal gammopathy in several patients may have potential clinical significance in spite of low risk of malignancy. Understanding the entire spectrum of these disorders may have broader implications beyond prevention of clinical malignancy.
机译:所有多种骨髓瘤(mm)的病例都是前体状态,其称为未确定意义(MGU)的单克隆γ肠道或闷烧骨髓瘤(SMM)。 MGUS细胞的遗传分析提供了证据表明它是一种遗传先进的病变,其中肿瘤细胞携带许多在MM细胞中发现的遗传变化。在MGUS相期间也是肠内异质性。虽然基线的MGU或SMM细胞的遗传特征可以预测疾病风险,但过渡到MM涉及预先存在的克隆的增长。 MGU的近期对小鼠建模的进展表明,克隆的临床休眠可以部分地通过生长对照对肿瘤细胞的生长控制来调节。 MGUS细胞与免疫细胞,骨细胞和骨髓龛中其他细胞的相互作用可能是恶性转化的关键调节因子。这些相互作用涉及双向串扰,导致生长支撑和抑制信号。由于MGU已经是遗传复杂的病变,所以适用于早期检测的新工具应允许划分早期阶段,这是我们作为MGU的术语。 MGU的风险增加的群体的分析还表明MGUS发育前的多克隆相的存在。在几个患者中,单克隆血管病可能性尽管恶性肿瘤风险低,但仍可能具有潜在的临床意义。了解这些疾病的整个频谱可能具有更广泛的影响,无法预防临床恶性肿瘤。

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