Constitutive expression of a chimeric receptor that delivers IL-2/IL-15 signals allows antigen-independent proliferation of CD8+CD44high but not other T cells.

Gasser S; Corthesy P; Beerman F; MacDonald HR; Nabholz M

首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Constitutive expression of a chimeric receptor that delivers IL-2/IL-15 signals allows antigen-independent proliferation of CD8+CD44high but not other T cells.

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Constitutive expression of a chimeric receptor that delivers IL-2/IL-15 signals allows antigen-independent proliferation of CD8+CD44high but not other T cells.

机译：传递IL-2 / IL-15信号的嵌合受体的组成型表达允许CD8 + CD44high高抗原依赖性增殖，但其他T细胞则不能。

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We have prepared transgenic mice whose T cells constitutively express a chimeric receptor combining extracellular human IL-4R and intracellular IL-2Rbeta segments. This receptor can transmit IL-2/IL-15-like signals in response to human, but not mouse, IL-4. We used these animals to explore to what extent functional IL-2R/IL-15R expression controls the capacity of T cells to proliferate in response to IL-2/IL-15-like signals. After activation with Con A, naive transgenic CD8+ and CD4+ T cells respond to human IL-4 as well as to IL-2. Without prior activation, they failed to proliferate in response to human IL-4, although human IL-4 did prolong their survival. Thus, IL-2-induced proliferation of activated T cells requires at least one other Ag-induced change apart from the induction of a functional IL-2R. However, a fraction of CD8+CD44high T cells proliferate in human IL-4 without antigenic stimulation or syngeneic feeder cells. In contrast, CD4+CD44high T cells are not constitutively responsive to human IL-4. We conclude that although all transgenic T cells express a functional chimeric receptor, only some CD8+CD44high T cells contain all molecules required for entry into the cell cycle in response to human IL-4 or IL-15.

机译：我们准备了转基因小鼠，其T细胞组成型表达嵌合受体，结合了细胞外人IL-4R和细胞内IL-2Rbeta片段。该受体可以响应人类（而非小鼠）IL-4传递类似IL-2 / IL-15的信号。我们使用这些动物来探索功能性IL-2R / IL-15R表达在多大程度上控制了T细胞响应IL-2 / IL-15样信号而增殖的能力。用Con A激活后，幼稚的转基因CD8 +和CD4 + T细胞对人IL-4和IL-2产生反应。没有人激活，它们就无法响应人IL-4增殖，尽管人IL-4确实延长了生存期。因此，除了诱导功能性IL-2R之外，IL-2诱导的活化T细胞的增殖还需要至少一种其他的Ag诱导的改变。但是，一部分CD8 + CD44high T细胞在没有抗原刺激或同系饲养细胞的情况下在人IL-4中增殖。相比之下，CD4 + CD44high T细胞对人IL-4的组成型反应不明显。我们得出的结论是，尽管所有转基因T细胞均表达功能性嵌合受体，但只有某些CD8 + CD44high T细胞包含响应人类IL-4或IL-15进入细胞周期所需的所有分子。

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来源
《The Journal of Immunology: Official Journal of the American Association of Immunologists 》 |2000年第11期| 共9页
作者
Gasser S; Corthesy P; Beerman F; MacDonald HR; Nabholz M;
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正文语种 eng
中图分类医学免疫学 ; 免疫遗传学 ;
关键词
Antigens; CD44; Antigens; CD8; Chimeric Proteins; Interleukin-15; Receptors; Interleukin-2; 抗原; CD44; 抗原; CD8; 嵌合体蛋白质类; 白细胞介素15; 受体; 白细胞介素2; 受体; 白细胞介素4;

机译：Antigens;CD44;Antigens;CD8;Chimeric Proteins;Interleukin-15;Receptors;Interleukin-2;抗原;CD44;抗原;CD8;嵌合体蛋白质类;白细胞介素15;受体;白细胞介素2;受体;白细胞介素4;

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专利

1. Constitutive expression of a chimeric receptor that delivers IL-2/IL-15 signals allows antigen-independent proliferation of CD8+CD44high but not other T cells. [J] . Gasser S, Corthesy P, Beerman F, The Journal of Immunology: Official Journal of the American Association of Immunologists . 2000 ,第11期

机译：传递IL-2 / IL-15信号的嵌合受体的组成型表达允许CD8 + CD44high高抗原依赖性增殖，但其他T细胞则不能。
2. Antigen-Independent Induction of Tim-3 Expression on Human T Cells by the Common γ-Chain Cytokines IL-2, IL-7, IL-15, and IL-21 Is Associated with Proliferation and Is Dependent on the Phosphoinositide 3-Kinase Pathway. [J] . Shariq Mujib, R Brad Jones, Calvin Lo, The Journal of Immunology: Official Journal of the American Association of Immunologists . 2012 ,第8期

机译：常见的γ链细胞因子IL-2，IL-7，IL-15和IL-21对人类T细胞Tim-3表达的抗原非依赖性诱导与增殖相关，并依赖于磷酸肌醇3-激酶途径。
3. Antigen-Independent Induction of Tim-3 Expression on Human T Cells by the Common γ-Chain Cytokines IL-2, IL-7, IL-15, and IL-21 Is Associated with Proliferation and Is Dependent on the Phosphoinositide 3-Kinase Pathway [J] . Shariq Mujib, R. Brad Jones, Calvin Lo, The journal of immunology . 2012 ,第8期

机译：常见的γ链细胞因子IL-2，IL-7，IL-15和IL-21对人类T细胞Tim-3表达的抗原非依赖性诱导与增殖相关，并依赖于磷酸肌醇3-激酶途径
4. Selective Expansion of Genetically Modified T Cells Using a Chimeric IL-2 Receptor for Cancer Therapy [C] . Takahiro Sogo, Masahiro Kawahara, Hiroshi Ueda, Annual Meeting of the Japanese Association for Animal Cell Technology . 2009

机译：使用嵌合IL-2受体进行癌症治疗的基因改性T细胞的选择性扩张
5. Preferential estrogen receptor beta ligands inhibit proliferation and reduce Bcl-2 expression in Fulvestrant-resistant breast cancer cells. [D] . Ruddy, Samantha C. 2013

机译：优先的雌激素受体β配体抑制耐富夫司特的乳腺癌细胞增殖并降低Bcl-2表达。
6. Membrane Potential Distinctly Modulates Mobility and Signaling of IL-2 and IL-15 Receptors in T Cells [O] . Éva Nagy, Gábor Mocsár, Veronika Sebestyén, 2018

机译：膜电位显着调节T细胞中IL-2和IL-15受体的移动性和信号传导
7. Constitutive Expression of a Chimeric Receptor That Delivers IL-2/IL-15 Signals Allows Antigen-Independent Proliferation of CD8+CD44high But Not Other T Cells [O] . Stephan Gasser, Patricia Corthésy, Friedrich Beerman, 2000

机译：嵌合受体的组成型表达，其递送IL-2 / IL-15信号，允许抗原无关的CD8 + CD44High的增殖，但不是其他T细胞

Constitutive expression of a chimeric receptor that delivers IL-2/IL-15 signals allows antigen-independent proliferation of CD8+CD44high but not other T cells.

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