人胸腺细胞TNF受体的表征。

Thymus Pub Date : 1994-01-01
M Murphy, L Pike-Nobile, V W Soo, L B Epstein
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引用次数: 0

摘要

尽管肿瘤坏死因子- α (TNF)在人和小鼠胸腺中组成性表达,但TNF对胸腺细胞增殖、分化和存活的影响表明其在胸腺中的影响是复杂的。为了确定这种复杂性是否源于胸腺细胞分化过程中两种TNF受体表达的变化,我们检测了出生后人类胸腺细胞中55 kDa TNF受体(TNF- r1)和75 kDa TNF受体(TNF- r2)的表达。逆转录聚合酶链式反应(RT-PCR)在人胸腺细胞中检测到TNF-R1和TNF-R2 mRNA。利用与各自TNF受体特异性反应的mAb和高度敏感的三步免疫荧光法,在绝大多数胸腺细胞上检测到细胞表面TNF- r1。相比之下,平均只有12.9%的胸腺细胞存在可检测到的细胞表面TNF-R2。结合植红蛋白(TNF- pe)的TNF也与少量胸腺细胞发生反应,并被发现特异性阻断TNF- r2单抗的结合,而不是TNF- r1单抗,暗示TNF- pe优先结合TNF- r2。使用双色免疫荧光与TNF-PE,我们发现表达TNF-R2的细胞群体也表达高水平的TCR α, β - cd3复合物,CD4或CD8,和IL-2受体α链。因此,未成熟(TCRneg/low)胸腺细胞表达TNF-R1,而成熟(TCRhigh)胸腺细胞也可以表达TNF-R2。TNF受体的差异表达为TNF对未成熟胸腺细胞的不同作用提供了一种机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Characterization of TNF receptors on human thymocytes.

Although tumor necrosis factor-alpha (TNF) is constitutively expressed in human and mouse thymus, the effects of TNF on thymocyte proliferation, differentiation and survival suggest that its influence in the thymus is complex. To determine if this complexity results from changes in the expression of the two TNF receptors during thymocyte differentiation, we examined the expression of the 55 kDa TNF receptor (TNF-R1) and the 75 kDa TNF receptor (TNF-R2) on postnatal human thymocytes. Both TNF-R1 and TNF-R2 mRNA were found in resting human thymocytes by reverse transcriptase-polymerase chain reaction (RT-PCR). Using mAb which specifically react with the respective TNF receptors and a highly sensitive, three-step method of immunofluorescence, cell surface TNF-R1 was detected on the vast majority of thymocytes. In contrast, detectable cell surface TNF-R2 was present on a mean of only 12.9% of thymocytes. TNF conjugated to phycoerythrin (TNF-PE) also reacted with a small population of thymocytes and was found to specifically block binding of the TNF-R2 mAb and not the TNF-R1 mAb, implicating preferential binding of TNF-PE to TNF-R2. Using dual-color immunofluorescence with TNF-PE we found that the population of cells which express TNF-R2 also express high levels of the TCR alpha, beta-CD3 complex, CD4 or CD8, and IL-2 receptor alpha chain. Thus, immature (TCRneg/low) thymocytes express TNF-R1 while mature (TCRhigh) thymocytes can also express TNF-R2. This differential expression of TNF receptors provides a mechanism for distinct effects of TNF on immature vs. mature thymocytes.

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