诱导t细胞耗竭的新试剂抗cd3 - crm9。

D M Neville, J Scharff, H Z Hu, K Rigaut, J Shiloach, W Slingerland, M Jonker
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引用次数: 73

摘要

我们开发了一种新的诱导体内t细胞耗竭的试剂,并在恒河猴身上进行了试验。该试剂是一种基于白喉毒素结合位点突变体CRM9的抗cd3 epsilon免疫毒素。在给猴子注射后,T细胞从血液和淋巴结区室中被消耗到初始值的< 1%。t细胞耗损与短暂性免疫抑制有关,这可以通过rhla错配皮肤移植的延迟排斥反应来判断。T细胞在两个隔室中重新填充;然而,再繁殖率是年龄相关的。幼龄动物发病迅速(12天),老龄动物发病需要> 30天。再生率和年龄之间的相关性表明,再生率依赖于胸腺,再生率的T细胞可能是幼稚的T细胞。该试剂将成为研究记忆T细胞在自身免疫性疾病恒河猴模型中的作用和器官移植后耐受诱导方案的有价值的工具。
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A new reagent for the induction of T-cell depletion, anti-CD3-CRM9.

We have developed a new reagent for inducing in vivo T-cell depletion and have tested this reagent in rhesus monkeys. The reagent is an anti-CD3 epsilon immunotoxin based on a diphtheria toxin binding-site mutant, CRM9. After administration to monkeys, T cells are depleted from both the blood and lymph node compartments to < 1% of their initial values. T-cell depletion is associated with transient immunosuppression, as judged by delayed rejection of RhLA-mismatched skin allografts. T cells are repopulated in both compartments; however, the rate of repopulation is age dependent. The rate is rapid in juvenile animals (12 days) and requires > 30 days in old animals. The correlation between repopulation rate and age suggests that the repopulation is thymus dependent and that the repopulated T cells are probably naive T cells. This reagent should be a valuable tool in studying the role of memory T cells in rhesus models of autoimmune diseases and protocols of tolerance induction after organ transplantation.

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