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Transglutaminase 2 expression in acute myeloid leukemia: Association with adhesion molecule expression and leukemic blast motility

机译:转谷氨酰胺酶2在急性髓细胞性白血病中的表达:与黏附分子表达和白血病母细胞运动的关系。

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摘要

Acute myeloid leukemia (AML) is a heterogenous disease with differential oncogene association, outcome and treatment regimens. Treatment strategies for AML have improved outcome but despite increased molecular biological information AML is still associated with poor prognosis. Proteomic analysis on the effects of a range of leukemogenic oncogenes showed that the protein transglutaminase 2 (TG2) is expressed at greater levels as a consequence of oncogenic transformation. Further analysis of this observation was performed with 511 AML samples using reverse phase proteomic arrays, demonstrating that TG2 expression was higher at relapse than diagnosis in many cases. In addition elevated TG2 expression correlated with increased expression of numerous adhesion proteins and many apoptosis regulating proteins, two processes related to leukemogenesis. TG2 has previously been linked to drug resistance in cancer and given the negative correlation between TG2 levels and peripheral blasts observed increased TG2 levels may lead to the protection of the leukemic stem cell due to increased adhesion/reduced motility. TG2 may therefore form part of a network of proteins that define poor outcome in AML patients and potentially offer a target to sensitize AML stem cells to drug treatment.
机译:急性髓细胞性白血病(AML)是一种异源性疾病,其致癌基因关联,结果和治疗方案均不同。 AML的治疗策略改善了预后,但尽管分子生物学信息有所增加,但AML仍与不良预后相关。蛋白质组学分析一系列致白血病致癌基因的影响表明,由于致癌性转化,蛋白转谷氨酰胺酶2(TG2)的表达水平更高。使用反相蛋白质组学阵列对511个AML样品进行了进一步的观察分析,表明在许多情况下TG2表达在复发时高于诊断。另外,TG2表达升高与许多粘附蛋白和许多凋亡调节蛋白的表达增加相关,这是与白血病发生有关的两个过程。 TG2以前与癌症的耐药性有关,鉴于TG2水平与外周母细胞之间呈负相关关系,观察到的TG2水平升高可能由于粘附力增加/运动性降低而导致了白血病干细胞的保护。因此,TG2可能构成蛋白质网络的一部分,这些蛋白质定义了AML患者的不良结局,并可能提供使AML干细胞对药物治疗敏感的靶标。

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