Robson S C, Schulte am Esch J, Bach F H
Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, Massachusetts 02215, USA.
Ann N Y Acad Sci. 1999 Jun 18;875:261-76. doi: 10.1111/j.1749-6632.1999.tb08509.x.
Important mechanisms underlying immediate xenograft loss by hyperacute rejection (HAR), in the pig-to-primate combination, have been recently delineated. There are now several proposed therapies that deal with the problem of complement activation and xenoreactive natural antibody (XNA) binding to the vasculature that have been shown to prevent HAR. However, vascularized xenografts are still lost, typically within days, by delayed xenograft rejection (DXR), alternatively known as acute vascular rejection (AVR). This process is characterized by endothelial cell (EC) perturbation, localization of XNA within the graft vasculature, host NK cell and monocyte activation with platelet sequestration and vascular thrombosis. Alternative immunosuppressive strategies, additive anti-complement therapies with the control of any resulting EC activation processes and induction of protective responses have been proposed to ameliorate this pathological process. In addition, several potentially important molecular incompatibilities between activated human coagulation factors and the natural anticoagulants expressed on porcine EC have been noted. Such incompatibilities may be analogous to cross-species alterations in the function of complement regulatory proteins important in HAR. Disordered thromboregulation is potentially relevant to the progression of inflammatory events in DXR and the disseminated intravascular coagulation seen in primate recipients of porcine renal xenografts. We have recently demonstrated the inability of porcine tissue factor pathway inhibitor (TFPI) to adequately neutralize human factor Xa (FXa), the aberrant activation of both human prothrombin and FXa by porcine EC and the failure of the porcine natural anticoagulant, thrombomodulin to bind human thrombin and hence activate human protein C. The enhanced potential of porcine von Willebrand factor to associate with human platelet GPIb has been demonstrated to be dependent upon the isolated A1 domain of von Willebrand factor. In addition, the loss of TFPI and vascular ATPDase/CD39 activity following EC activation responses would potentiate any procoagulant changes within the xenograft. These developments could exacerbate vascular damage from whatever cause and enhance the activation of platelets and coagulation pathways within xenografts resulting in graft infarction and loss. Analysis of these and the other putative factors underlying DXR should lead to the development and testing of genetic approaches that, in conjunction with selected pharmacological means, may further prolong xenograft survival to a clinically relevant extent.
最近已经阐明了猪 - 灵长类动物组合中因超急性排斥反应(HAR)导致异种移植立即丧失的重要机制。现在有几种针对补体激活和异种反应性天然抗体(XNA)与血管系统结合问题的治疗方法,这些方法已被证明可以预防HAR。然而,血管化异种移植仍然会在数天内因延迟性异种移植排斥反应(DXR)而丧失,DXR也被称为急性血管排斥反应(AVR)。这个过程的特征是内皮细胞(EC)紊乱、XNA在移植血管系统内定位、宿主NK细胞和单核细胞激活以及血小板扣押和血管血栓形成。已经提出了替代免疫抑制策略、控制任何由此产生的EC激活过程的附加抗补体疗法以及诱导保护性反应,以改善这一病理过程。此外,已经注意到活化的人类凝血因子与猪EC上表达的天然抗凝剂之间存在一些潜在的重要分子不相容性。这种不相容性可能类似于HAR中重要的补体调节蛋白功能的跨物种改变。血栓调节紊乱可能与DXR中的炎症事件进展以及猪肾异种移植灵长类受体中出现的弥散性血管内凝血有关。我们最近证明了猪组织因子途径抑制剂(TFPI)无法充分中和人类因子Xa(FXa),猪EC对人类凝血酶原和FXa的异常激活,以及猪天然抗凝剂血栓调节蛋白无法结合人类凝血酶从而激活人类蛋白C。已经证明猪血管性血友病因子与人类血小板糖蛋白Ib结合的增强潜力取决于血管性血友病因子的分离A1结构域。此外,EC激活反应后TFPI和血管ATP酶/CD39活性的丧失会增强异种移植内的任何促凝变化。这些进展可能会加剧任何原因引起的血管损伤,并增强异种移植内血小板和凝血途径的激活,导致移植梗死和丧失。对这些以及DXR背后的其他假定因素的分析应该会导致开发和测试基因方法,这些方法与选定的药理学手段相结合,可能会将异种移植存活期进一步延长至临床相关程度。
