Fas(CD95)/FasL interactions required for programmed cell death after T-cell activation.

Ju ST; Panka DJ; Cui H; Ettinger R; el Khatib M; Sherr DH; Stanger BZ; Marshak Rothstein A

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Fas(CD95)/FasL interactions required for programmed cell death after T-cell activation.

机译：T细胞活化后程序性细胞死亡所需的Fas（CD95）/ FasL相互作用。

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Receptor crosslinking of T-cell hybridomas induces cell activation followed by apoptosis. This activation-induced cell death requires de novo synthesis of RNA and proteins, but the actual gene products that provide the death signal have not been identified. We show here that receptor crosslinking induces Fas ligand and upregulates Fas, and that the ensuing engagement of Fas by Fas ligand activates the cell-death programme. Cell death, but not activation, can be selectively prevented by a soluble Fas-immunoglobulin fusion protein. Thus, Fas and Fas ligand are the death-gene products, and their interaction accounts for the molecular mechanism of activation-induced T-cell death.

机译：T细胞杂交瘤的受体交联诱导细胞活化，然后凋亡。这种激活诱导的细胞死亡需要从头合成RNA和蛋白质，但尚未确定提供死亡信号的实际基因产物。我们在这里显示受体交联诱导Fas配体并上调Fas，并且随后Fas配体与Fas的结合会激活细胞死亡程序。可以通过可溶性Fas-免疫球蛋白融合蛋白选择性地防止细胞死亡，但不能激活。因此，Fas和Fas配体是死亡的基因产物，它们的相互作用解释了激活诱导T细胞死亡的分子机制。

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来源
《Nature》 |1995年第6513期|P.444-448|共5页
作者
Ju ST; Panka DJ; Cui H; Ettinger R; el Khatib M; Sherr DH; Stanger BZ; Marshak Rothstein A;
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作者单位

Arthritis Center, Boston University School of Medicine, Massachusetts 02118.;

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收录信息美国《科学引文索引》(SCI);美国《工程索引》(EI);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
Antigens; Surface; Apoptosis; Lymphocyte Transformation; Membrane Glycoproteins; 抗原; 表面; 脱噬作用; 淋巴细胞转化; 膜糖蛋白类; T淋巴细胞;

机译：Antigens;Surface;Apoptosis;Lymphocyte Transformation;Membrane Glycoproteins;抗原;表面;脱噬作用;淋巴细胞转化;膜糖蛋白类;T淋巴细胞;

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1. T-cell factor (TCF/LEF1) binding elements (TBEs) of FasL (Fas ligand or CD95 ligand) bind and cluster Fas (CD95) and form complexes with the TCF-4 and b-catenin transcription factors in vitro and in vivo which result in triggering cell death and/or cell activation [J] . Liu Xia, Huang Yuwei, Zhang Yuanyuan, Cellular and Molecular Neurobiology . 2016,第6期

机译：FasL（Fas配体或CD95配体）的T细胞因子（TCF / LEF1）结合元件（TBEs）在体外和体内与Fas（CD95）结合并成簇，并与TCF-4和b-catenin转录因子形成复合物，导致触发细胞死亡和/或细胞活化
2. Immunohistochemical characterization of Fas (CD95) and Fas Ligand (FasL/CD95L) expression in the injured brain: relationship with neuronal cell death and inflammatory mediators. [J] . Grosjean MB, Lenzlinger PM, Stahel PF, Histology and histopathology . 2007,第3期

机译：Fas（CD95）和Fas Ligand（FasL / CD95L）在受伤的大脑中表达的免疫组织化学表征：与神经元细胞死亡和炎症介质的关系。
3. Close Association between Fas Ligand (FasL; CD95L)-positive Tumor-associated Macrophages and Apoptotic Cancer Cells along Invasive Margin of Colorectal Carcinoma: A Proposal on Tumor-Host Interactions. [J] . Sugita J, Ohtani H, Mizoi T, Japanese Journal of Cancer Research . 2002,第3期

机译：Fas配体（FasL; CD95L）阳性的肿瘤相关巨噬细胞与大肠癌浸润边缘的凋亡癌细胞之间的密切联系：关于肿瘤与宿主相互作用的建议。
4. Modulation of CD95 (APO-1/Fas)-induced hepatocyte death by NO [C] . P. R. GALLE, D. STRAND, Z. SU, International Symposium on the Maillard Reaction . 2002

机译：CD95（APO-1 / Fas）的调节 - 诱导肝细胞死亡
5. CD30-Redirected Chimeric Antigen Receptor T Cells Target Embryonal Carcinoma via Antigen-Dependent and Fas/FasL Interactions [D] . Hong, Lee Kyung. 2018

机译：CD30-重定向的嵌合抗原受体T细胞通过抗原依赖性和FAS / FASL相互作用靶向胚胎癌
6. The Nef-Mediated AIDS-Like Disease of CD4C/Human Immunodeficiency Virus Transgenic Mice Is Associated with Increased Fas/FasL Expression on T Cells and T-Cell Death but Is Not Prevented in Fas- FasL- Tumor Necrosis Factor Receptor 1- or Interleukin-1β-Converting Enzyme-Deficient or Bcl2-Expressing Transgenic Mice [O] . Elena Priceputu, Isabelle Rodrigue, Pavel Chrobak, 2005

机译：CD4C /人类免疫缺陷病毒转基因小鼠的Nef介导的艾滋病样疾病与T细胞上Fas / FasL表达增加和T细胞死亡相关但在Fas-FasL-肿瘤坏死因子受体1 、、或白介素1β转化酶缺陷或表达Bcl2的转基因小鼠
7. The Nef-Mediated AIDS-Like Disease of CD4C/Human Immunodeficiency Virus Transgenic Mice Is Associated with Increased Fas/FasL Expression on T Cells and T-Cell Death but Is Not Prevented in Fas-, FasL-, Tumor Necrosis Factor Receptor 1-, or Interleukin-1β-Converting Enzyme-Deficient or Bcl2-Expressing Transgenic Mice [O] . Priceputu, Elena, Rodrigue, Isabelle, Chrobak, Pavel, 2005

机译：CD4C /人类免疫缺陷病毒转基因小鼠的Nef介导的艾滋病样疾病与T细胞上Fas / FasL表达增加和T细胞死亡相关，但在Fas-，FasL-，肿瘤坏死因子受体1 、、或白介素1β转化酶缺陷或表达Bcl2的转基因小鼠

Fas(CD95)/FasL interactions required for programmed cell death after T-cell activation.

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