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Immunosuppressant deoxyspergualin induces apoptotic cell death in dividing cells.

机译:免疫抑制剂脱氧精银蛋白可诱导分裂细胞中凋亡细胞的死亡。

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摘要

Deoxyspergualin (DSG) has been found to have an antitumour and immunosuppressive activity. However, the precise mechanism of action of DSG has not been clarified. We have used its analogue, methyldeoxyspergualin (MeDSG) for in vitro culture studies of DSG since it shows good stability in aqueous solution and retains strong immunosuppressive activity. In the present study, we found that MeDSG inhibited proliferation of rapidly dividing murine T-cell hybridomas, resulting in cell death. The cell death was accompanied by chromatin condensation and DNA cleavage at the linker regions between nucleosomes. Furthermore, MeDSG induced a reduction in mitochondrial transmembrane potential. When murine thymocytes were treated with MeDSG for 48 hr, a slight increase of DNA fragmentation was constantly observed, and selective depletion of CD4- CD8- cells was noticed. In contrast, CD4+ CD8+ cells were hardly affected. Moreover, splenic T-cells are resistant to MeDSG-induced apoptosis, as evaluated by measuring DNA cleavage. Our findings may account for the immunosuppressive and antitumour properties of DSG which were described in a number of previous studies.
机译:已发现脱氧精豆素(DSG)具有抗肿瘤和免疫抑制活性。但是,DSG的确切作用机理尚未阐明。我们已经使用了其类似物甲基脱氧精豆素(MeDSG)进行DSG的体外培养研究,因为它在水溶液中显示出良好的稳定性并保留了强大的免疫抑制活性。在本研究中,我们发现MeDSG抑制快速分裂的鼠T细胞杂交瘤的增殖,从而导致细胞死亡。细胞死亡伴随着核小体之间连接区域的染色质浓缩和DNA裂解。此外,MeDSG诱导线粒体跨膜电位降低。当用MeDSG处理鼠胸腺细胞48小时时,不断观察到DNA片段的轻微增加,并且观察到CD4-CD8-细胞的选择性消耗。相反,CD4 + CD8 +细胞几乎不受影响。而且,如通过测量DNA切割所评估的,脾T细胞对MeDSG诱导的凋亡具有抗性。我们的发现可能解释了DSG的免疫抑制和抗肿瘤特性,这在先前的许多研究中都有描述。

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