Cutting Edge: Dual TCRα Expression Poses an Autoimmune Hazard by Limiting Regulatory T Cell Generation

Nathaniel J. Schuldt; Jennifer L. Auger; Justin A. Spanier; Tijana Martinov; Elise R. Breed; Brian T. Fife; Kristin A. Hogquist; Bryce A. Binstadt

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Cutting Edge: Dual TCRα Expression Poses an Autoimmune Hazard by Limiting Regulatory T Cell Generation

机译：前沿：双重TCRα表达通过限制调节性T细胞生成而构成自身免疫危险

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Despite accounting for 10–30% of the T cell population in mice and humans, the role of dual TCR-expressing T cells in immunity remains poorly understood. It has been hypothesized that dual TCR T cells pose an autoimmune hazard by allowing self-reactive TCRs to escape thymic selection. We revisited this hypothesis using the NOD murine model of type 1 diabetes. We bred NOD mice hemizygous at both TCRα and β (TCRα+/? β+/?) loci, rendering them incapable of producing dual TCR T cells. We found that the lack of dual TCRα expression skewed the insulin-specific thymocyte population toward greater regulatory T (Treg) cell commitment, resulting in a more tolerogenic Treg to conventional T cell ratio and protection from diabetes. These data support a novel hypothesis by which dual TCR expression can promote autoimmunity by limiting agonist selection of self-reactive thymocytes into the Treg cell lineage.

机译：尽管占小鼠和人类T细胞总数的10％至30％，但表达双重TCR的T细胞在免疫中的作用仍然知之甚少。已经假设双TCR T细胞通过允许自反应性TCR逃避胸腺选择而构成自身免疫危害。我们使用1型糖尿病的NOD鼠模型重新审视了这一假设。我们在TCRα和β（TCRα+ /？β+ /？）基因座上杂合了NOD小鼠，使其无法产生双重TCR T细胞。我们发现，缺乏双重TCRα表达使胰岛素特异性胸腺细胞群体偏向更大的调节性T（Treg）细胞，从而导致Treg与常规T细胞的比例更具有耐受性，并能预防糖尿病。这些数据支持了一种新的假说，通过该假说，双TCR表达可通过限制自身反应性胸腺细胞的激动剂选择进入Treg细胞谱系来促进自身免疫。

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《The journal of immunology》 |2017年第1期|共6页
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Nathaniel J. Schuldt; Jennifer L. Auger; Justin A. Spanier; Tijana Martinov; Elise R. Breed; Brian T. Fife; Kristin A. Hogquist; Bryce A. Binstadt;
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1. Cutting Edge: Dual TCR alpha Expression Poses an Autoimmune Hazard by Limiting Regulatory T Cell Generation [J] . Schuldt Nathaniel J., Auger Jennifer L., Spanier Justin A., The Journal of Immunology: Official Journal of the American Association of Immunologists . 2017,第1期

机译：尖端：双TCRα表达通过限制调节性T细胞产生自身免疫危害
2. Cutting edge: Low-Affinity TCRs support regulatory t cell function in autoimmunity [J] . Sprouse, Shevchenko, I.a, The Journal of Immunology: Official Journal of the American Association of Immunologists . 2018,第3期

机译：切削刃：低亲和力TCR支持自身免疫中的调节T细胞功能
3. Cutting Edge: Low-Affinity TCRs Support Regulatory T Cell Function in Autoimmunity [J] . Maran L. Sprouse, Ivan Shevchenko, Marissa A. Scavuzzo, The journal of immunology . 2018,第3期

机译：前沿：低亲和力TCR支持自身免疫中的调节性T细胞功能
4. ENGINEERING T CELL RECEPTORS (TCRS) FOR IMPROVED THERAPEUTIC T REGULATORY CELL (TREG) FUNCTION [C] . Elissa Leonard, Jennifer Maynard Biochemical and molecular engineering XX: the next generation of biochemical engineering: from nanoscale to industrial scale . 2017

机译：用于改善治疗性T调节细胞（TREG）功能的工程T细胞受体（TCRS）
5. TCR dependent thymic Treg differentiation and Th17 cells in experimental autoimmune encephalomyelitis. [D] . Leung, Monica W. L. 2010

机译：实验性自身免疫性脑脊髓炎中，TCR依赖性胸腺Treg分化和Th17细胞。
6. Dual TCRα expression poses an autoimmune hazard by limiting Treg cell generation [O] . Nathaniel J. Schuldt, Jennifer L. Auger, Justin A. Spanier, -1

机译：TCRα的双重表达通过限制Treg细胞的产生而引起自身免疫危险
7. Cutting Edge: Low-Affinity TCRs Support Regulatory T Cell Function in Autoimmunity [O] . Maran L. Sprouse, Ivan Shevchenko, Marissa A. Scavuzzo, 2017

机译：切削刃：低亲和力TCR支持自身免疫中的调节T细胞功能

Cutting Edge: Dual TCRα Expression Poses an Autoimmune Hazard by Limiting Regulatory T Cell Generation

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