Loss of T cell receptor-induced Bmi-1 in the KLRG1~+ senescent CD8~+ T lymphocyte

Maike Heffner; Douglas T. Fearon

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Loss of T cell receptor-induced Bmi-1 in the KLRG1~+ senescent CD8~+ T lymphocyte

机译：T细胞受体诱导的KLRG1〜+衰老CD8〜+ T淋巴细胞中Bmi-1的丢失

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Clones of CD8~+ T cells specific for viral antigens must avoid replicative senescence to maintain continuous production of new effector cells during chronic viral infections. In the present study, we have determined whether this capability may be related to Bmi-1, a transcriptional repressor that is required for the maintenance of hematopoietic stem cells and certain neural stem cells and that mediates its antisenescence function by inhibiting transcription of the Ink4a/Arf tumor suppressor locus. Ligation of the T cell receptor increased the levels of Bmi-1 mRNA and protein in primary CD8~+ T cells. The increased expression was reversible upon removal of antigen but could be maintained by using stimulation with the IL-2 receptor. Specific suppression of Bmi-1 by using a lentivirally encoded short hairpin RNA inhibited the proliferation of IL-2-stimulated CTLL-2 cytotoxic T cells and primary CD8~+ T cells. Ectopically expressed Bmi-1 enhanced the expansion of primary CD8~+ T cells stimulated by IL-2 and IL-7 in vitro and by homeostatic signals in vivo. Taken together, these findings indicate that Bmi-1 is required for CD8~+ T cell clonal expansion and is positively regulated by receptors that mediate this response. Therefore, the observation that the ability of the T cell receptor to induce Bmi-1 is maintained in the subset of replication-competent, antigen-experienced CD8~+ T cells that do not express the killer cell lectin-like receptor G1 (KLRG1) but is developmentally switched off in the senescent, KLRG1~+ subset suggests that Bmi-1 is a molecular determinant of the capacity of a CD8~+ T cell clone to persist during chronic viral infections.

机译：病毒抗原特异的CD8〜+ T细胞克隆必须避免复制性衰老，以在慢性病毒感染期间维持新效应细胞的连续产生。在本研究中，我们已经确定了这种能力是否与Bmi-1有关，Bmi-1是维持造血干细胞和某些神经干细胞所必需的转录阻遏物，并通过抑制Ink4a /介导其抗衰老功能。 Arf抑癌基因座。 T细胞受体的连接增加了原代CD8〜+ T细胞中Bmi-1 mRNA和蛋白的水平。去除抗原后增加的表达是可逆的，但是可以通过使用IL-2受体刺激来维持。通过使用慢病毒编码的短发夹RNA特异性抑制Bmi-1可以抑制IL-2刺激的CTLL-2细胞毒性T细胞和原代CD8 + T细胞的增殖。异位表达的Bmi-1增强了体外受IL-2和IL-7和体内稳态信号刺激的CD8 + T细胞的扩增。综上所述，这些发现表明Bmi-1是CD8〜+ T细胞克隆扩增所必需的，并且受介导此反应的受体正调控。因此，观察到T细胞受体诱导Bmi-1的能力在不表达杀伤细胞凝集素样受体G1（KLRG1）的具有复制能力的抗原经历的CD8〜+ T细胞的子集中得以维持但在衰老过程中发育关闭，KLRG1〜+亚群提示Bmi-1是CD8〜+ T细胞克隆在慢性病毒感染期间持续存在的能力的分子决定因素。

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来源
《Proceedings of the National Academy of Sciences of the United States of America》 |2007年第33期|13414-13419|共6页
作者
Maike Heffner; Douglas T. Fearon;
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作者单位

Wellcome Trust Immunology Unit, Department of Medicine, University of Cambridge, Medical Research Council Centre, Hills Road, Cambridge CB2 2QH, United Kingdom;

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收录信息美国《科学引文索引》(SCI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
原文格式 PDF
正文语种 eng
中图分类自然科学总论;
关键词
Ink4a; senescence; IL-2;

机译：Ink4a;衰老;白介素2;

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机译：衰老的牙齿间充质干细胞的牙源性分化受损与Bmi-1表达的丧失有关。
2. Non-regulatory CD8(+)CD45RO(+)CD25(+) T-lymphocytes may compensate for the loss of antigen-inexperienced CD8(+)CD45RA(+) T-cells in old [J] . Herndier-Brandstetter D, Veel E, Laschober GT, Biological chemistry . 2008,第5期

机译：非调节性CD8（+）CD45RO（+）CD25（+）T淋巴细胞可能补偿了抗原缺乏的CD8（+）CD45RA（+）T细胞的丢失
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4. Analysis of T cell receptor V beta diversity in peripheral CD8(+) T lymphocytes in patients with hepatitis B infection [C] . Yuguo Song, Lei Xiang, Shengli Bi 2011 International Conference on Human Health and Biomedical Engineering . 2011

机译：乙型肝炎感染患者外周血CD8（+）T淋巴细胞中T细胞受体Vβ多样性的分析
5. Essential discrimination of vascular and tissue lymphocytes redefines CD8 T cell responses to respiratory infection. [D] . Anderson, Kristin Gail. 2014

机译：血管和组织淋巴细胞的基本区分重新定义了CD8 T细胞对呼吸道感染的反应。
6. Loss of T cell receptor-induced Bmi-1 in the KLRG1+ senescent CD8+ T lymphocyte [O] . Maike Heffner, Douglas T. Fearon 2007

机译：T细胞受体诱导的KLRG1 +衰老CD8 + T淋巴细胞中Bmi-1的丢失
7. Loss of T cell receptor-induced Bmi-1 in the KLRG1+ senescent CD8+ T lymphocyte [O] . Heffner, Maike, Fearon, Douglas T. 2007

机译：T细胞受体诱导的Bmi-1在KLRG1 +衰老CD8 + T淋巴细胞中的丢失

Loss of T cell receptor-induced Bmi-1 in the KLRG1~+ senescent CD8~+ T lymphocyte

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