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小鼠γδTCR⁺NK1.1⁺胸腺细胞特异性产生白细胞介素-4,不依赖主要组织相容性复合体I类,并且在发育上与αβTCR⁺NK1.1⁺胸腺细胞相关。

Mouse gamma delta TCR+NK1.1+ thymocytes specifically produce interleukin-4, are major histocompatibility complex class I independent, and are developmentally related to alpha beta TCR+NK1.1+ thymocytes.

作者信息

Vicari A P, Mocci S, Openshaw P, O'Garra A, Zlotnik A

机构信息

DNAX Research Institute, Palo Alto, CA 94304-1104, USA.

出版信息

Eur J Immunol. 1996 Jul;26(7):1424-9. doi: 10.1002/eji.1830260704.

DOI:10.1002/eji.1830260704
PMID:8766542
Abstract

Mouse T cells co-expressing an alpha beta T cell receptor (TCR) and the NK1.1 antigen have been shown to be major interleukin (IL)-4-producing cells and could therefore regulate cell-mediated immune responses. We have identified a related sub-set of thymocytes co-expressing a gamma delta TCR and NK1.1 which also produce IL-4. Unlike alpha beta +NK1.1+ thymocytes, the selection of gamma delta +NK1.1+ thymocytes is not dependent upon beta 2-microglobulin (beta 2m)-associated class I molecule expression because these cells are present in beta 2m-deficient mice. This suggests that gamma delta +NK1.1+ T cells may regulate immune responses to a different variety of antigens. However, the development of alpha beta +NK1.1+ and gamma delta +NK1.1+ thymocytes appears to be related. Analysis of different mutant mice lacking alpha beta +NK1.1+ thymocytes revealed a specific increase in gamma delta +NK1.1+ thymocyte production when the block in alpha beta +NK1.1+ thymocyte differentiation occurs after beta TCR rearrangement.

摘要

已证明共表达αβ T细胞受体(TCR)和NK1.1抗原的小鼠T细胞是主要产生白细胞介素(IL)-4的细胞,因此可能调节细胞介导的免疫反应。我们已鉴定出一个共表达γδ TCR和NK1.1的胸腺细胞相关亚群,它们也产生IL-4。与αβ +NK1.1+胸腺细胞不同,γδ +NK1.1+胸腺细胞的选择不依赖于与β2-微球蛋白(β2m)相关的I类分子表达,因为这些细胞存在于β2m缺陷小鼠中。这表明γδ +NK1.1+ T细胞可能调节对不同种类抗原的免疫反应。然而,αβ +NK1.1+和γδ +NK1.1+胸腺细胞的发育似乎相关。对缺乏αβ +NK1.1+胸腺细胞的不同突变小鼠的分析显示,当αβ +NK1.1+胸腺细胞分化的阻滞发生在β TCR重排之后时,γδ +NK1.1+胸腺细胞的产生会特异性增加。

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