首页> 外文期刊>Leukemia Research: A Forum for Studies on Leukemia and Normal Hemopoiesis >CD44 isoforms are differentially regulated in plasma cell dyscrasias and CD44v9 represents a new independent prognostic parameter in multiple myeloma.
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CD44 isoforms are differentially regulated in plasma cell dyscrasias and CD44v9 represents a new independent prognostic parameter in multiple myeloma.

机译:CD44亚型在浆细胞异常中受到差异调节,而CD44v9代表多发性骨髓瘤的新独立预后参数。

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摘要

To evaluate the role of CD44 variant isoforms (CD44v) in plasma cell dyscrasias, CD44v expression was analysed in bone marrow (BM) biopsies of multiple myeloma (MM) and monoclonal gammopathy of undetermined significance (MGUS) patients, in biopsies of soft tissue infiltration by MM and in extramedullary plasmacytoma samples. Expression of CD44 isoforms containing the 3v, 4v, 6v or 10v domain was observed in 15, 7, 13 and 5% of 87 samples from 49 consecutive MM cases, but could not be detected in ten normal persons or 11 MGUS patients. In contrast, CD44v9 revealed a broader pattern of expression and was observed in plasma cells in three out of ten normal persons and in three out of 11 MGUS cases. In MM, CD44v9 was detected in 32 out of 87 samples (37%) of BM infiltrates and was associated with an advanced Durie and Salmon stage (P<0.03), a progressive disease (P<0.01) and an IgA subtype (P<0.01). Furthermore, CD44v9 expression was observed in three out of five cases of MM soft tissue infiltrates, was often upregulated during disease progression, was significantly correlated with a shorter overall survival (P<0.03) and emerged as an independent prognostic factor in multivariate analysis (stage: relative risk 1.36, P<0.02; CD44v9 expression: relative risk 1.45, P<0.04). These results substantiate the clinical relevance of CD44v domains in plasma cell disorders and establish CD44v9 as a new independent prognostic parameter in MM.
机译:为了评估CD44变异同工型(CD44v)在浆细胞发育不良中的作用,在多发性骨髓瘤(MM)的骨髓活检和不明重要性的单发性乳腺病(MGUS)患者的软组织浸润活检中分析了CD44v的表达。 MM和髓外浆细胞瘤样本在来自49例连续MM病例的87个样本中,分别在15、7、13和5%中观察到包含3v,4v,6v或10v域的CD44亚型的表达,但在10名正常人或11名MGUS患者中未检测到。相反,CD44v9显示了更广泛的表达模式,在浆细胞中,十分之三的正常人和11%的MGUS病例中的三者都观察到CD44v9。在MM中,在87例BM浸润样本中,有32例(37%)检测到CD44v9,并与晚期Durie和Salmon期(P <0.03),进行性疾病(P <0.01)和IgA亚型(P < 0.01)。此外,在五分之三的MM软组织浸润中观察到CD44v9表达,在疾病进展过程中常常被上调,与较短的总生存期显着相关(P <0.03),并且在多变量分析中作为独立的预后因素出现(阶段:相对危险度1.36,P <0.02; CD44v9表达:相对危险度1.45,P <0.04)。这些结果证实了CD44v结构域在浆细胞疾病中的临床相关性,并建立了CD44v9作为MM中新的独立预后参数。

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