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免疫毒素治疗。

Treatment with immunotoxin.

作者信息

Knechtle S J

机构信息

Department of Surgery, Division of Organ Transplantation, 600 Highland Avenue, University of Wisconsin Medical School, Madison,WI 53792-7375, USA.

出版信息

Philos Trans R Soc Lond B Biol Sci. 2001 May 29;356(1409):681-9. doi: 10.1098/rstb.2001.0839.

Abstract

T-cell depletion prior to or beginning at the time of transplantation has been shown to be a valuable adjunct to the induction of immunological unresponsiveness. Both total lymphoid irradiation and anti-lymphocyte globulin have been used for this purpose in experimental models of transplantation as well as in human organ transplant recipients. However, these methods of T-cell depletion are limited in their ability to deplete T cells selectively due to non-specific targeting and limited efficacy. A new anti-CD3 immunotoxin has been developed with a far more potent ability to deplete T cells selectively as measured by flow cytometry analysis of peripheral blood T lymphocytes as well as lymph node lymphocytes. This immunotoxin is well tolerated by rhesus monkeys when administered in vivo. When administered as a single immunosuppressive agent pretransplant, it substantially promotes allograft survival, inducing tolerance in at least one-third of recipients as measured by subsequent acceptance of donor skin grafts and rejection of third-party skin grafts. When administered on the day of transplant in combination with steroid pretreatment and a brief course of deoxyspergualin or mycophenolate mofetil (4 to 14 days), long-term unresponsiveness is also produced and in a more reliable manner than using immunotoxin alone. A new immunotoxin directed at the human CD3epsilon has been developed with excellent potency in T-cell killing and lacking the Fc portion of the CD3 antibody. This construct may be useful for T-cell depletion in humans and has a potential application in tolerance induction in human organ transplantation. Lessons learned from anti-CD3 immunotoxin in the non-human primate model to date include (i) profound (2-3 log) depletion of T-cells can be accomplished safely without inducing lymphoma or infection, (ii) such depletion is a useful adjunct for tolerance induction to allogeneic organ transplants, and (iii) tolerance to both allogeneic renal transplants and xenogeneic islet transplants has been accomplished using such strategies to date in non-human primates and in pigs. Immunotoxin may be useful for the induction of chimerism using strategies that include donor bone marrow infusion. Successful strategies for tolerance induction have also been developed using immunotoxin without the adjunct of donor bone marrow or stem cell infusion. Clinical application of immunotoxin will use a newly engineered construct with the potential for causing cytokine release, less susceptibility to neutralization by anti-diphtheria antibody and not dependent on chemical conjugation of an antibody and toxin. The usefulness of immunotoxin is directly related to its tremendous potency for depleting T cells. Based on results in nonhuman primates, it is anticipated that it will become a useful agent in tolerance induction in humans.

摘要

移植前或移植时开始进行T细胞清除已被证明是诱导免疫无反应性的一种有价值的辅助手段。在移植实验模型以及人体器官移植受者中,全淋巴照射和抗淋巴细胞球蛋白都已用于此目的。然而,由于非特异性靶向和有限的疗效,这些T细胞清除方法在选择性清除T细胞的能力方面受到限制。一种新的抗CD3免疫毒素已被开发出来,通过对外周血T淋巴细胞以及淋巴结淋巴细胞进行流式细胞术分析测量,其具有更强的选择性清除T细胞的能力。当在体内给药时,这种免疫毒素在恒河猴中耐受性良好。当作为单一免疫抑制剂在移植前给药时,它能显著促进同种异体移植物存活,通过随后接受供体皮肤移植和排斥第三方皮肤移植来衡量,至少三分之一的受者可诱导出耐受性。当在移植当天与类固醇预处理以及短期(4至14天)的去氧精胍菌素或霉酚酸酯联合给药时,也能产生长期无反应性,且比单独使用免疫毒素更可靠。一种针对人CD3ε的新型免疫毒素已被开发出来,在杀伤T细胞方面具有优异的效力,并且缺乏CD3抗体的Fc部分。这种构建体可能对人体T细胞清除有用,并且在人体器官移植的耐受性诱导方面具有潜在应用。迄今为止,从非人类灵长类动物模型中的抗CD3免疫毒素获得的经验教训包括:(i)可以安全地实现T细胞的深度(2至3个对数)清除,而不会诱发淋巴瘤或感染;(ii)这种清除是同种异体器官移植耐受性诱导的一种有用辅助手段;(iii)迄今为止,在非人类灵长类动物和猪中,使用此类策略已实现对同种异体肾移植和异种胰岛移植的耐受性。免疫毒素可能对使用包括供体骨髓输注在内的策略诱导嵌合体有用。在不借助供体骨髓或干细胞输注的情况下,也已开发出使用免疫毒素的成功耐受性诱导策略。免疫毒素的临床应用将使用一种新设计的构建体,其具有引发细胞因子释放的可能性、不易被抗白喉抗体中和且不依赖于抗体与毒素的化学偶联。免疫毒素的有用性与其清除T细胞的巨大效力直接相关。基于非人类灵长类动物的结果,预计它将成为人体耐受性诱导中的一种有用药物。

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