Cutting edge: LFA-1 is required for liver NK1.1+TCR alpha beta+ cell development: evidence that liver NK1.1+TCR alpha beta+ cells originate from multiple pathways.

Ohteki T; Maki C; Koyasu S; Mak TW; Ohashi PS

首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Cutting edge: LFA-1 is required for liver NK1.1+TCR alpha beta+ cell development: evidence that liver NK1.1+TCR alpha beta+ cells originate from multiple pathways.

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Cutting edge: LFA-1 is required for liver NK1.1+TCR alpha beta+ cell development: evidence that liver NK1.1+TCR alpha beta+ cells originate from multiple pathways.

机译：尖端技术：肝脏NK1.1 + TCRαβ+细胞发育需要LFA-1：证据表明肝脏NK1.1 + TCRαβ+细胞起源于多种途径。

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Using mice deficient for LFA-1, CD44, and ICAM-1, we examined the role of these adhesion molecules in NK1.1+TCR alpha beta+ (NKT) cell development. Although no defect in NKT cell development was observed in CD44-/- and ICAM-1-/- mice, a dramatic reduction of liver NKT cells was observed in LFA-1-/- mice. Normal numbers of NKT cells were present in other lymphoid organs in LFA-1-/- mice. When LFA-1-/- splenocytes were injected i.v. into wild-type mice, the frequency of NKT cells among donor-derived cells in the recipient liver was normal. In contrast, when LFA-1-/- bone marrow (BM) cells were injected i.v. into irradiated wild-type mice, the frequency of liver NKT cells was significantly lower than that of mice injected with wild-type BM cells. Collectively, these data indicate that LFA-1 is required for the development of liver NKT cells, rather than the migration to and/or subsequent establishment of mature NKT cells in the liver.

机译：使用缺乏LFA-1，CD44和ICAM-1的小鼠，我们检查了这些粘附分子在NK1.1 + TCRαβ+（NKT）细胞发育中的作用。尽管在CD44-/-和ICAM-1-/-小鼠中未观察到NKT细胞发育的缺陷，但在LFA-1-/-小鼠中观察到肝NKT细胞的显着减少。正常数量的NKT细胞存在于LFA-1-/-小鼠的其他淋巴器官中。当静脉内注射LFA-1-/-脾细胞时。在野生型小鼠中，受体肝脏供体来源细胞中NKT细胞的频率正常。相反，当LFA-1-/-骨髓（BM）细胞被静脉内注射时。辐射的野生型小鼠中，肝NKT细胞的频率显着低于注射野生型BM细胞的小鼠。总体而言，这些数据表明，LFA-1是肝脏NKT细胞发育所必需的，而不是肝脏中成熟NKT细胞的迁移和/或随后的建立。

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来源
《The Journal of Immunology: Official Journal of the American Association of Immunologists》 |1999年第7期|共4页
作者
Ohteki T; Maki C; Koyasu S; Mak TW; Ohashi PS;
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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; Liver; Lymphocyte Function-Associated Antigen-1; Proteins; Receptors; Antigen; T-Cell; alpha-beta; 抗原; 肝; 淋巴细胞功能相关抗原1; 蛋白质类; 受体; 抗原; T细胞; α-β; T淋巴细胞;

机译：Antigens;Liver;Lymphocyte Function-Associated Antigen-1;Proteins;Receptors;Antigen;T-Cell;alpha-beta;抗原;肝;淋巴细胞功能相关抗原1;蛋白质类;受体;抗原;T细胞;α-β;T淋巴细胞;

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1. Cutting edge: LFA-1 is required for liver NK1.1+TCR alpha beta+ cell development: evidence that liver NK1.1+TCR alpha beta+ cells originate from multiple pathways. [J] . Ohteki T, Maki C, Koyasu S, The Journal of Immunology: Official Journal of the American Association of Immunologists . 1999,第7期

机译：尖端技术：肝脏NK1.1 + TCRαβ+细胞发育需要LFA-1：证据表明肝脏NK1.1 + TCRαβ+细胞起源于多种途径。
2. Stringent V beta requirement for the development of NK1.1+ T cell receptor-alpha/beta+ cells in mouse liver. [J] . T Ohteki, H R MacDonald The Journal of Experomental Medicine . 1996,第3期

机译：小鼠肝脏中NK1.1 + T细胞受体-α/β+细胞发育的严格V beta要求。
3. Major histocompatibility complex class I related molecules control the development of CD4+8- and CD4-8- subsets of natural killer 1.1+ T cell receptor-alpha/beta+ cells in the liver of mice. [J] . T Ohteki, H R MacDonald The Journal of Experomental Medicine . 1994,第2期

机译：主要的组织相容性复杂的I类相关分子控制着小鼠肝脏中自然杀手1.1+ T细胞受体α/β+细胞的CD4 + 8-和CD4-8-亚型的发育。
4. COMPARISON OF FUNGAL CELL SUSCEPTIBILITY TO EXTERNAL ALPHA PARTICLE BEAM RADIATION VERSUS ALPHA PARTICLES DELIVERED BY 213-BISMUTH-LABELED ANTIBODY [C] . Ruth Bryan, Igor Shuryak, Alfred Morgenstern, 8th International Conference on Isotopes 2014 . 2014

机译：213-双铋抗体合成的真菌对体外α粒子束辐射与α粒子的敏感性比较
5. Prostate cancer cell-derived exosomes enable androgen production by patients derived stem cells: Exploring racial disparity and targeting residual androgen through stem cell-based selective delivery of 3alpha-HSD. [D] . Ranjan, Manish. 2015

机译：前列腺癌细胞衍生的外来体使患者衍生的干细胞能够产生雄激素：通过基于干细胞的3alpha-HSD选择性递送，探索种族差异并靶向残余雄激素。
6. Stringent V beta requirement for the development of NK1.1+ T cell receptor-alpha/beta+ cells in mouse liver [O] . 1996

机译：小鼠肝脏中NK1.1 + T细胞受体-α/β+细胞发育的严格V beta要求
7. Stringent V beta requirement for the development of NK1.1+ T cell receptor-alpha/beta+ cells in mouse liver [O] . 1996

机译：小鼠肝脏中NK1.1 + T细胞受体-α/β+细胞发育的严格V beta要求

Cutting edge: LFA-1 is required for liver NK1.1+TCR alpha beta+ cell development: evidence that liver NK1.1+TCR alpha beta+ cells originate from multiple pathways.

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