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表达高水平CD94的CD8 T细胞和自然杀伤细胞的优先存活。

Preferential survival of CD8 T and NK cells expressing high levels of CD94.

作者信息

Gunturi Anasuya, Berg Rance E, Forman James

机构信息

Center for Immunology, University of Texas Southwestern Medical Center, 6000 Harry Hines Boulevard, Dallas, TX 75390-9093, USA.

出版信息

J Immunol. 2003 Feb 15;170(4):1737-45. doi: 10.4049/jimmunol.170.4.1737.

Abstract

The Qa-1(b)/Qdm tetramer binds to CD94/NKG2 receptors expressed at high levels on approximately 50% of murine NK cells. Although very few CD8 T cells from naive mice express CD94/NKG2 receptors, approximately 50% of CD8 T cells taken from mice undergoing a secondary response against Listeria monocytogenes (LM) are CD94(high) and bind the tetramer. Although CD94(int) NK cells do not bind the tetramer, CD94(int) CD8 T cells do, and this binding is dependent on the CD8 coreceptor. We found that the extent of apoptosis in CD8 T and NK cells was inversely related to the expression of CD94, with lower levels of apoptosis seen in CD94(high) cells after 1-3 days of culture. The difference in CD8 T cell survival was evident as early as 6 h after culture and persisted until nearly all the CD94(neg/int) cells were apoptotic by 48 h. In contrast, expression of inhibitory Ly-49A,G2,C/I molecules was associated with higher levels of apoptosis. Cross-linking CD94/NKG2 receptors on CD8 T cells from a mouse undergoing an LM infection further reduced the percentage of apoptotic cells on the CD94-expressing populations, while cross-linking Ly-49I had no effect on CD8 T cells expressing Ly-49I. Cross-linking CD3 on CD8 T cells from a mouse undergoing a secondary LM infection increases the extent of apoptosis, but this is prevented by cross-linking CD94/NKG2 receptors at the same time. Similar results were observed with NK cells in that the CD94(high) population displayed less apoptosis than CD94(int) cells after 1-3 days in culture. Therefore, the expression of CD94/NKG2 is correlated with a lower level of apoptosis and may play an important role in the maintenance of CD8 T and NK cells.

摘要

Qa-1(b)/Qdm四聚体与约50%的小鼠NK细胞上高水平表达的CD94/NKG2受体结合。虽然来自未接触过抗原小鼠的CD8 T细胞中极少表达CD94/NKG2受体,但取自经历针对单核细胞增生李斯特菌(LM)二次应答小鼠的CD8 T细胞中,约50%为CD94(高表达)且能结合该四聚体。虽然CD94(中表达)的NK细胞不结合该四聚体,但CD94(中表达)的CD8 T细胞能结合,且这种结合依赖于CD8共受体。我们发现,CD8 T细胞和NK细胞中的凋亡程度与CD94的表达呈负相关,培养1 - 3天后,CD94(高表达)细胞中的凋亡水平较低。CD8 T细胞存活的差异在培养6小时后就很明显,并一直持续到48小时时几乎所有CD94(阴性/中表达)细胞都发生凋亡。相反,抑制性Ly-49A、G2、C/I分子的表达与较高的凋亡水平相关。对来自感染LM小鼠的CD8 T细胞上的CD94/NKG2受体进行交联,可进一步降低表达CD94群体中凋亡细胞的百分比,而对表达Ly-49I的CD8 T细胞交联Ly-49I则没有影响。对来自经历LM二次感染小鼠的CD8 T细胞交联CD3会增加凋亡程度,但同时交联CD94/NKG2受体会阻止这种情况。在NK细胞中也观察到了类似结果,即培养1 - 3天后,CD94(高表达)群体的凋亡比CD94(中表达)细胞少。因此,CD94/NKG2的表达与较低的凋亡水平相关,可能在维持CD8 T细胞和NK细胞方面发挥重要作用。

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