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FAS system deregulation in T-cell lymphoblastic lymphoma

机译:T细胞淋巴母细胞淋巴瘤的FAS系统失调

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摘要

The acquisition of resistance towards FAS-mediated apoptosis may be required for tumor formation. Tumors from various histological origins exhibit FAS mutations, the most frequent being hematological malignancies. However, data regarding FAS mutations or FAS signaling alterations are still lacking in precursor T-cell lymphoblastic lymphomas (T-LBLs). The available data on acute lymphoblastic leukemia, of precursor origin as well, indicate a low frequency of FAS mutations but often report a serious reduction in FAS-mediated apoptosis as well as chemoresistance, thus suggesting the occurrence of mechanisms able to deregulate the FAS signaling pathway, different from FAS mutation. Our aim at this study was to determine whether FAS-mediated apoptotic signaling is compromised in human T-LBL samples and the mechanisms involved. This study on 26 T-LBL samples confirms that the FAS system is impaired to a wide extent in these tumors, with 57.7% of the cases presenting any alteration of the pathway. A variety of mechanisms seems to be involved in such alteration, in order of frequency the downregulation of FAS, the deregulation of other members of the pathway and the occurrence of mutations at FAS. Considering these results together, it seems plausible to think of a cumulative effect of several alterations in each T-LBL, which in turn may result in FAS/FASLG system deregulation. Since defective FAS signaling may render the T-LBL tumor cells resistant to apoptotic cell death, the correct prognosis, diagnosis and thus the success of anticancer therapy may require such an in-depth knowledge of the complete scenario of FAS-signaling alterations.
机译:肿瘤形成可能需要获得对FAS介导的细胞凋亡的抗性。来自各种组织学来源的肿瘤均表现出FAS突变,最常见的是血液系统恶性肿瘤。但是,在前体T细胞淋巴母细胞淋巴瘤(T-LBLs)中仍然缺少有关FAS突变或FAS信号改变的数据。关于前体起源的急性淋巴细胞白血病的可用数据也表明,FAS突变的频率较低,但经常报告FAS介导的细胞凋亡以及化学抗药性的严重降低,因此表明存在能够解除FAS信号通路调控机制的现象。 ,不同于FAS突变。我们在这项研究中的目的是确定FAS介导的细胞凋亡信号在人T-LBL样品中是否被破坏及其机制。这项针对26个T-LBL样本的研究证实,在这些肿瘤中,FAS系统受到很大程度的损害,其中57.7%的病例表现出该途径的任何改变。这种改变似乎涉及多种机制,按照频率顺序,FAS的下调,途径其他成员的失调和FAS突变的发生频率。综合考虑这些结果,似乎可以想到每个T-LBL中若干变更的累积影响,这反过来可能导致FAS / FASLG系统解除管制。由于有缺陷的FAS信号传导可能使T-LBL肿瘤细胞对凋亡细胞死亡具有抵抗力,因此正确的预后,诊断以及抗癌治疗的成功可能需要对FAS信号改变的完整方案有如此深入的了解。

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