Binder J, Lehmann M, Graser E, Hancock W W, Watschinger B, Onodera K, Sayegh M H, Volk H D, Kupiec-Weglinski J W
Harvard Medical School, Boston, MA 02115, USA.
Transplantation. 1996 Mar 15;61(5):804-11. doi: 10.1097/00007890-199603150-00022.
The immunosuppressive effects of RIB-5/2, a nondepleting anti-rat CD4 monoclonal antibody (mAb), were analyzed in a well-defined model of accelerated cardiac allograft rejection. (LEW x BN)F1 hearts are rejected within 24 hours in LEW hosts presensitized with BN skin grafts at day -7. Treatment with RIB-5/2 mAb (3.5 mg/day i.v.) at days -7 and -1, prolonged cardiac allograft survival to the median of >62 days. The long-term recipients rejected acutely third-party (Wistar-Furth) test skin grafts, without an adverse effect on the survival of the original cardiac transplants. Lymphocytes harvested from mAb-treated hosts significantly decreased proliferative responses of donor cells in mixed leukocyte reaction. The cell activation and cytokine elaboration patterns were evaluated at the mRNA and protein levels by competitive template reverse transcriptase polymerase chain reaction and immunohistochemistry, respectively. Cardiac allografts in CD4 mAb-treated rats at 24 hours displayed reduced CD3, CD25, tumor necrosis factor-alpha, interleukin (IL)-1beta, IL-2, interferon (IFN)-gamma, and IL-10 mRNA levels as compared to those in rejecting grafts. Equal amounts of IL-4 mRNA were detected throughout in both animal groups; the expression of IL-10 mRNA increased progressively in the treated hosts. In contrast, IFN-gamma was consistently depressed after mAb therapy. The mRNA levels coding for CD3, CD25, tumor necrosis factor-alpha, IL-1-beta, and IL-2 genes were comparable in long-surviving and rejecting allografts. The staining for IL-2R, IL-2, and IFN-gamma was diminished, whereas the staining for IL-4 was either unaffected or enhanced in well-functioning grafts in RIB-5/2 mAb-treated hosts. The untreated recipients elicited strong circulating IgM allo-Ab response, which peaked around the time of cardiac rejection and then switched to IgG allo-Ab 4-7 days after heart transplantation. Treatment with RIB-5/2 mAb decreased IgM and prevented the switch into the IgG allo-Ab response. In conclusion, the ability of RIB-5/2 mAb treatment to combat accelerated rejection and to produce long-term graft acceptance is unprecedented in our experience in this model. These data provide new insights into the complexities of the cellular and humoral responsiveness, contributing to the the induction of donor-specific unresponsiveness in sensitized hosts. This study, along with our previous reports, indicate that an immune deviation in which intragraft Th1-type cytokines (primarily IFN-gamma) are diminished and Th2-type cytokines (IL-4 and IL-10) are maintained represents the common effector mechanism of CD4 mAb regimens in recipients of vascularized organ allografts.
在一个明确的加速心脏移植排斥模型中,分析了非耗竭性抗大鼠CD4单克隆抗体(mAb)RIB-5/2的免疫抑制作用。在第-7天用BN皮肤移植进行预致敏的LEW宿主中,(LEW×BN)F1心脏在24小时内被排斥。在第-7天和-1天用RIB-5/2 mAb(3.5毫克/天,静脉注射)治疗,可将心脏移植存活期延长至>62天的中位数。长期接受者急性排斥第三方(Wistar-Furth)测试皮肤移植,而对原始心脏移植的存活没有不利影响。从用mAb治疗的宿主中收获的淋巴细胞显著降低了混合淋巴细胞反应中供体细胞的增殖反应。分别通过竞争性模板逆转录聚合酶链反应和免疫组织化学在mRNA和蛋白质水平评估细胞活化和细胞因子分泌模式。与排斥移植的大鼠相比,在24小时时用CD4 mAb治疗的大鼠的心脏移植显示CD3、CD25、肿瘤坏死因子-α、白细胞介素(IL)-1β、IL-2、干扰素(IFN)-γ和IL-10 mRNA水平降低。在两个动物组中始终检测到等量的IL-4 mRNA;在治疗的宿主中,IL-10 mRNA的表达逐渐增加。相反,mAb治疗后IFN-γ持续降低。在长期存活和排斥的移植中,编码CD3、CD25、肿瘤坏死因子-α IL-1-β和IL-2基因的mRNA水平相当。在用RIB-5/2 mAb治疗的宿主中功能良好的移植中,IL-2R、IL-2和IFN-γ的染色减少,而IL-4的染色未受影响或增强。未治疗的接受者引发强烈的循环IgM同种异体抗体反应,该反应在心脏排斥时达到峰值,然后在心脏移植后4-7天转换为IgG同种异体抗体。用RIB-5/2 mAb治疗可降低IgM并阻止转换为IgG同种异体抗体反应。总之,在我们在该模型中的经验中,RIB-5/2 mAb治疗对抗加速排斥并产生长期移植接受的能力是前所未有的。这些数据为细胞和体液反应性的复杂性提供了新的见解,有助于在致敏宿主中诱导供体特异性无反应性。这项研究以及我们之前的报告表明,一种免疫偏差,即移植内Th1型细胞因子(主要是IFN-γ)减少而Th2型细胞因子(IL-4和IL-10)得以维持,代表了血管化器官移植受者中CD4 mAb方案的共同效应机制。
