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首页> 美国卫生研究院文献>British Journal of Pharmacology and Chemotherapy >Induction of apoptosis in human mitogen-activated peripheral blood T-lymphocytes by the ether phospholipid ET-18-OCH3: Involvement of the Fas receptor/ligand system
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Induction of apoptosis in human mitogen-activated peripheral blood T-lymphocytes by the ether phospholipid ET-18-OCH3: Involvement of the Fas receptor/ligand system

机译:醚磷脂ET-18-OCH3诱导人促分裂原激活的外周血T淋巴细胞凋亡:Fas受体/配体系统的参与

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class="enumerated" style="list-style-type:decimal">Activated T-cells constitute a target for treatment of autoimmune diseases. We have found that the antitumour ether phospholipid 1-O-octadecyl-2-O-methyl-rac-glycero-3-phosphocholine (ET-18-OCH3; edelfosine) induced dose- and time-dependent apoptosis in human mitogen-activated peripheral blood T-lymphocytes, but not in resting T-cells. T-lymphocytes were stimulated with phytohemagglutinin and interleukin-2 or with concanavalin A. Apoptosis was assessed by DNA fragmentation through cell cycle and TUNEL analyses, as well as through visualization of internucleosomal DNA fragmentation in agarose gels.The ET-18-OCH3-mediated apoptotic response in activated T-lymphocytes was less intense than in human leukaemic T cell lines, such as Jurkat cells and Peer cells; namely about 25% apoptosis in activated T-cells versus about 46–61% apoptosis in T leukaemic cells after 24 h treatment with 10 μM ET-18-OCH3.The ET-18-OCH3 thioether analogue BM 41.440 (ilmofosine) showed a similar apoptotic capacity to that found with ET-18-OCH3 in activated T-cells, whereas the phospholipid analogue hexadecylphosphocholine (miltefosine) failed to promote this response.The uptake of [3H]-ET-18-OCH3 was much larger in activated T-cells than in resting lymphocytes.Using a cytofluorimetric approach we have found that ET-18-OCH3 induced disruption of the mitochondrial transmembrane potential and production of reactive oxygen species in activated T-cells, but not in resting lymphocytes.ET-18-OCH3 induced an increase in Fas (APO-1/CD95) ligand mRNA expression in activated T-cells, and incubation with a blocking anti-Fas (APO-1/CD95) antibody partially inhibited the ET-18-OCH3-induced apoptosis of activated T-lymphocytes.These results demonstrate that mitogen-activated T-cells, unlike resting lymphocytes, are able to take up significant amounts of ET-18-OCH3, and are susceptible to undergo apoptosis by the ether lipid via, in part, the Fas (APO-1/CD95) receptor/ligand system. This ET-18-OCH3 apoptotic action can be of importance in the therapeutic action of this ether lipid in certain autoimmune diseases.
机译:class =“ enumerated” style =“ list-style-type:decimal”> <!-list-behavior =枚举前缀-word = mark-type = decimal max-label-size = 0-> 活化的T细胞构成治疗自身免疫性疾病的靶标。我们已经发现抗肿瘤醚磷脂1-O-十八烷基-2-O-甲基-rac-甘油-3-磷酸胆碱(ET-18-OCH3; edelfosine)在人促分裂原激活的外周血中诱导了剂量和时间依赖性凋亡血液中的T淋巴细胞,但不在静止的T细胞中。用植物血凝素和白介素-2或伴刀豆球蛋白A刺激T淋巴细胞。通过细胞周期和TUNEL分析,以及通过可视化琼脂糖凝胶中核小体间DNA片段的DNA片段化来评估细胞凋亡。 ET-18-OCH3介导的活化T淋巴细胞的凋亡反应强度不及人类白血病T细胞系(如Jurkat细胞和Peer细胞)强烈。即用10μmET-18-OCH3处理24 h后,活化T细胞的凋亡约占25%,而白血病T细胞的凋亡约46-61%。 ET-18-OCH3硫醚类似物BM 41.440(ilmofosine)在活化的T细胞中显示出与ET-18-OCH3类似的凋亡能力,而磷脂类似物十六烷基磷酸胆碱(miltefosine)未能促进这种反应。 [[< sup> 3 H] -ET-18-OCH3在活化的T细胞中比静止的淋巴细胞大得多。 使用细胞荧光法,我们发现ET-18-OCH3诱导了破坏活化的T细胞中线粒体跨膜电位和活性氧的产生,而不是静止的淋巴细胞中。 ET-18-OCH3诱导Fas(APO-1 / CD95)配体mRNA表达的增加在活化的T细胞中,并与抗Fas(APO-1 / CD95)抗体一起孵育可部分抑制ET-18-OCH3诱导的活化T淋巴细胞的凋亡。 < li>这些结果表明,有丝分裂原激活的T细胞与静止的淋巴细胞不同,能够吸收大量的ET-18-OCH3,并且易受醚脂质通过部分Fas(APO -1 / CD95)受体/配体系统。 ET-18-OCH3的凋亡作用可能在某些自身免疫性疾病中对该醚脂质的治疗作用中具有重要意义。

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