Cutting Edge: De Novo Induction of Functional Foxp3+ Regulatory CD4 T Cells in Response to Tissue-Restricted Self Antigen

Lucas J. Thompson; Andrea C. Valladao; Steven F. Ziegler

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Cutting Edge: De Novo Induction of Functional Foxp3+ Regulatory CD4 T Cells in Response to Tissue-Restricted Self Antigen

机译：前沿：从头诱导功能性Foxp3 +调节性CD4 T细胞对组织限制性自身抗原的反应

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Naive CD4 T cells can differentiate into a number of functional subsets in response to Ag, including Foxp3+ induced regulatory T cells (iTregs). The in vivo development and function of iTregs has been primarily demonstrated in systems involving Ag encountered systemically or delivered via the intestinal mucosa. In this study, we demonstrate that de novo Foxp3 expression in naive CD4 T cells is a critical mechanism for establishing tolerance for a tissue-restricted neo-self Ag. Naive CD4 T cells lacking a functional Foxp3 gene cannot achieve tolerance, but can be suppressed in vivo in the presence of wild type naive CD4 T cells. Exposure to nonspecific inflammation during priming undermines tolerance through impaired Foxp3 induction, suggesting that the microenvironment also has a role. These data show that de novo Foxp3 expression is an integral component of establishing and maintaining tolerance among naive peripheral CD4 T cells.

机译：幼稚的CD4 T细胞可响应Ag而分化为许多功能性亚型，包括Foxp3 +诱导的调节性T细胞（iTregs）。 iTregs的体内发育和功能已在涉及全身或通过肠道粘膜递送的银的系统中得到了初步证明。在这项研究中，我们证明了新生CD4 T细胞中的从头Foxp3表达是建立对组织限制性新自我Ag耐受的关键机制。缺乏功能性Foxp3基因的幼稚CD4 T细胞不能达到耐受性，但是在野生型幼稚CD4 T细胞存在的情况下可以在体内被抑制。在启动过程中暴露于非特异性炎症会通过削弱Foxp3诱导而破坏耐受性，这表明微环境也有作用。这些数据表明，从头开始的Foxp3表达是在幼稚的外周CD4 T细胞中建立和维持耐受性的组成部分。

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《The journal of immunology》 |2011年第8期|共5页
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Lucas J. Thompson; Andrea C. Valladao; Steven F. Ziegler;
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1. Cutting edge: De novo induction of functional Foxp3+ regulatory CD4 T cells in response to tissue-restricted self antigen. [J] . Thompson LJ, Valladao AC, Ziegler SF The Journal of Immunology: Official Journal of the American Association of Immunologists . 2011,第8期

机译：尖端技术：从头诱导功能性Foxp3 +调节性CD4 T细胞响应组织受限的自身抗原。
2. Cutting edge: CD4-independent development of functional FoxP3+ regulatory T cells. [J] . Blache C, Adriouch S, Calbo S, The Journal of Immunology: Official Journal of the American Association of Immunologists . 2009,第7期

机译：前沿：功能性FoxP3 +调节性T细胞的CD4独立开发。
3. Cutting edge: CD4-independent development of functional FoxP3+ regulatory T cells. [J] . Blache C, Adriouch S, Calbo S, The Journal of Immunology: Official Journal of the American Association of Immunologists . 2009,第7期

机译：前沿：功能性FoxP3 +调节性T细胞的CD4独立开发。
4. CD40-ACTIVATED B (CD40-B) CELLS LOADED WITH AUTOLOGOUS TUMOR RNA AS A NOVEL ANTIGEN-PRESENTING CELL VACCINE FOR CANINE LYMPHOMA [C] . Amy LaBlanc, Erika L Krick, Beth Overley, Annual conference of the Veterinary Cancer Society . 2008

机译：CD40-活化的B（CD40-B）用自体肿瘤RNA负载，作为犬淋巴瘤的新型抗原呈递细胞疫苗
5. Regulation of gastritis and gastric cancer by CD4+ Foxp3+ regulatory T cells. [D] . Nguyen, Thanh-Long M. 2015

机译：CD4 + Foxp3 +调节性T细胞调节胃炎和胃癌。
6. De Novo Induction of Functional Foxp3+ Regulatory CD4 T Cells in Response to Tissue-Restricted Self Antigen [O] . Lucas J. Thompson, Andrea C. Valladao, Steven F. Ziegler -1

机译：功能Foxp3 +调节性CD4T细胞的从头诱导响应于组织限制性自身抗原
7. Cutting Edge: De Novo Induction of Functional Foxp3+ Regulatory CD4 T Cells in Response to Tissue-Restricted Self Antigen [O] . Lucas J. Thompson, Andrea C. Valladao, Steven F. Ziegler 2011

机译：切削刃：官能团FoxP3 +调节CD4 T细胞的Novo诱导响应组织限制的自抗原

Cutting Edge: De Novo Induction of Functional Foxp3+ Regulatory CD4 T Cells in Response to Tissue-Restricted Self Antigen

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