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恒河猴骨髓中否决活性与同种异体移植耐受性和嵌合现象的进一步研究。

Further studies of veto activity in rhesus monkey bone marrow in relation to allograft tolerance and chimerism.

作者信息

Thomas J M, Carver F M, Kasten-Jolly J, Haisch C E, Rebellato L M, Gross U, Vore S J, Thomas F T

机构信息

Department of Surgery, East Carolina University School of Medicine, Greenville, North Carolina 27858.

出版信息

Transplantation. 1994 Jan;57(1):101-15. doi: 10.1097/00007890-199401000-00018.

Abstract

Infusing the DR-/dim fraction of bone marrow cells (BMC) from an allogeneic kidney donor into rabbit antithymocyte globulin-treated transplant recipients delivers a tolerogenic signal, leading to functional allograft tolerance in rhesus monkeys without additional drug therapy. Our updated results in an expanded series show a median 131-day graft survival of recipients given DR-/dim donor BMC with a 23% 1-year survival (P < 0.00001 vs. rabbit antithymocyte globulin controls). Removing DRbright cells from donor BMC appeared to have a significant effect (P < 0.05). We have further investigated the tolerogenic mechanism within the experimental framework of the veto hypothesis in this preclinical model. In limiting dilution assays, we demonstrated the donor specificity of clonal inactivation of CTL precursors (CTLp) after in vitro or in vivo exposure to DR-/dim donor BMC, confirming specific tolerance. Additionally, in vitro studies confirmed the allogeneic specificity of CTLp inactivation in 3-cell MLR assays; minimal bystander effects were seen on normal CTLp responses to third party stimulator cells, while CTLp responses to the BMC donor's cells were abrogated in the same cultures. BMC mediating the veto effect were found to be resistant to L-leucyl-L-leucine methyl ester (Leu-leu-OMe), which excluded BMC-mediated cytotoxicity by NK or lymphokine-activated killer cells, CTL, or activated macrophages. In contrast, veto activity was abolished if the BMC were pretreated with either high dose UV-B light irradiation, mitomycin, or gamma-irradiation, indicating that BMC contained a UV-B-sensitive precursor of the veto effector, and that a proliferative step separated the two. Irradiation of DR-/dim donor BMC or administration of cyclophosphamide after infusion of nonirradiated BMC prevented the tolerogenic effect. Only recipients given nonirradiated DR-/dim donor BMC demonstrated PBL chimerism, which associated with functional deletion of antidonor CTLp and duration of graft survival. The Leu-leu-OMe resistance and the other properties of the allogeneic monkey CD3- CD2+ CD8+ BMC subpopulation that exhibits tolerance-promoting activity in vitro and in vivo lead us to postulate that a donor BMC-derived precursor population, possibly a dendritic cell population, may induce allogeneic unresponsiveness in this model.

摘要

将来自同种异体肾供体的骨髓细胞(BMC)的DR - /dim亚群输注到经兔抗胸腺细胞球蛋白治疗的移植受者体内,可传递一种致耐受性信号,从而在恒河猴中实现功能性同种异体移植耐受,而无需额外的药物治疗。我们在一个扩大队列中的最新结果显示,接受DR - /dim供体BMC的受者移植中位存活期为131天,1年生存率为23%(与兔抗胸腺细胞球蛋白对照组相比,P < 0.00001)。从供体BMC中去除DRbright细胞似乎有显著效果(P < 0.05)。我们在这个临床前模型的否决假说实验框架内进一步研究了致耐受机制。在有限稀释试验中,我们证明了体外或体内暴露于DR - /dim供体BMC后,CTL前体(CTLp)克隆失活的供体特异性,证实了特异性耐受。此外,体外研究在3细胞混合淋巴细胞反应(MLR)试验中证实了CTLp失活的同种异体特异性;在正常CTLp对第三方刺激细胞的反应中观察到最小的旁观者效应,而在相同培养物中CTLp对BMC供体细胞的反应被消除。发现介导否决效应的BMC对L - 亮氨酰 - L - 亮氨酸甲酯(Leu - leu - OMe)具有抗性,这排除了BMC通过NK或淋巴因子激活的杀伤细胞、CTL或活化巨噬细胞介导的细胞毒性。相反,如果BMC用高剂量UV - B光照射、丝裂霉素或γ射线照射预处理,否决活性就会被消除,这表明BMC含有否决效应器的UV - B敏感前体,并且一个增殖步骤将两者分开。在输注未照射的BMC后,照射DR - /dim供体BMC或给予环磷酰胺可阻止致耐受效应。只有接受未照射的DR - /dim供体BMC的受者表现出外周血淋巴细胞嵌合现象,这与抗供体CTLp的功能性缺失和移植存活期相关。Leu - leu - OMe抗性以及在体外和体内表现出促进耐受活性的同种异体猴CD3 - CD2 + CD8 + BMC亚群的其他特性,使我们推测,一个供体BMC衍生的前体细胞群,可能是一个树突状细胞群,可能在这个模型中诱导同种异体无反应性。

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