在猪对狒狒心脏异种移植中控制炎症和凝血的方法

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Martin Bender, Bruno Reichart, Constanca Figueiredo, Jonathan M Burgmann, Maria Leuschen, Felicia Wall, Julia Radan, Elisabeth Neumann, Maren Mokelke, Ines Buttgereit, Sebastian Michel, Reinhard Ellgass, Stefanie Egerer, Andreas Lange, Andrea Baehr, Barbara Kessler, Elisabeth Kemter, Nikolai Klymiuk, Joachim Denner, Antonia W Godehardt, Ralf R Tönjes, Christian Hagl, Michaela Gebauer, Uli Binder, Arne Skerra, David Ayares, Eckhard Wolf, Michael Schmoeckel, Paolo Brenner, Matthias Längin, Jan-Michael Abicht
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引用次数: 0

摘要

导言:炎症反应和凝血障碍是心脏异种移植成功进入临床的一个相关挑战。为应对这一问题,需要一种有效且在临床上切实可行的抗炎和抗凝方案。器官来源猪的基因工程可以减少炎症和凝血反应。此外,还有几种治疗策略可以预防或减轻异种移植后的炎症反应和凝血障碍。然而,目前仍不清楚在临床环境中应使用哪种药物组合。为了阐明这一点,我们展示了猪对狒狒正位心脏异种移植实验中使用多种抗炎药物组合的数据:转基因仔猪(GGTA1-KO、hCD46/hTBM 转基因)被用于心脏异种移植到人工饲养的狒狒(14 只)。所有动物都接受了抗炎药物治疗,包括 C1 酯酶抑制剂、IL-6 受体拮抗剂、TNF-α 抑制剂和 IL-1 受体拮抗剂。作为辅助药物,还使用了乙酰水杨酸和非分细肝素。免疫抑制方案基于 CD40/CD40L 协同刺激阻断。实验期间,在多个时间点对白细胞计数、C反应蛋白(CRP)水平、全身细胞因子和趋化因子水平以及凝血参数进行了评估。由于猪巨细胞病毒/猪玫瑰酚病毒(PCMV/PRV)感染(2 只)或技术故障(2 只),有 4 只动物被排除在进一步的数据分析之外:结果:白细胞计数在围手术期明显下降,CRP水平上升。术后,白细胞计数始终保持在正常范围内,CRP 水平在术后约 35 天、50 天和 80 天后出现三个高峰。细胞因子和趋化因子的分析显示了不同的模式。一些细胞因子(如 IL-8)在围手术期增加了约 2 倍,但随后又降至与术前值相当的水平,甚至更低。其他细胞因子,如 IL-12/IL-23,在围手术期有所下降,并保持在这一水平。除了围手术期的下降,在凝血参数方面也没有观察到相关的变化。总之,心脏异种移植术后的炎症反应和凝血功能障碍方面的所有参数都没有明显变化,这表明我们的方法是有效的:结论:我们在抗炎药物治疗方面的临床前经验证明,由于 PCMV/PRV 也会诱发炎症和凝血功能障碍,因此在防止病原体(尤其是 PCMV/PRV)传播给受体的条件下,控制异种移植中的炎症和凝血功能障碍是可能的,也是切实可行的。我们的抗炎方案也应适用于心脏异种移植的临床环境,并且是有效的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
An Approach to Controlling Inflammation and Coagulation in Pig-to-Baboon Cardiac Xenotransplantation.

Introduction: Inflammatory responses and coagulation disorders are a relevant challenge for successful cardiac xenotransplantation on its way to the clinic. To cope with this, an effective and clinically practicable anti-inflammatory and anti-coagulatory regimen is needed. The inflammatory and coagulatory response can be reduced by genetic engineering of the organ-source pigs. Furthermore, there are several therapeutic strategies to prevent or reduce inflammatory responses and coagulation disorders following xenotransplantation. However, it is still unclear, which combination of drugs should be used in the clinical setting. To elucidate this, we present data from pig-to-baboon orthotopic cardiac xenotransplantation experiments using a combination of several anti-inflammatory drugs.

Methods: Genetically modified piglets (GGTA1-KO, hCD46/hTBM transgenic) were used for orthotopic cardiac xenotransplantation into captive-bred baboons (n = 14). All animals received an anti-inflammatory drug therapy including a C1 esterase inhibitor, an IL-6 receptor antagonist, a TNF-α inhibitor, and an IL-1 receptor antagonist. As an additive medication, acetylsalicylic acid and unfractionated heparin were administered. The immunosuppressive regimen was based on CD40/CD40L co-stimulation blockade. During the experiments, leukocyte counts, levels of C-reactive protein (CRP) as well as systemic cytokine and chemokine levels and coagulation parameters were assessed at multiple timepoints. Four animals were excluded from further data analyses due to porcine cytomegalovirus/porcine roseolovirus (PCMV/PRV) infections (n = 2) or technical failures (n = 2).

Results: Leukocyte counts showed a relevant perioperative decrease, CRP levels an increase. In the postoperative period, leukocyte counts remained consistently within normal ranges, CRP levels showed three further peaks after about 35, 50, and 80 postoperative days. Analyses of cytokines and chemokines revealed different patterns. Some cytokines, like IL-8, increased about 2-fold in the perioperative period, but then decreased to levels comparable to the preoperative values or even lower. Other cytokines, such as IL-12/IL-23, decreased in the perioperative period and stayed at these levels. Besides perioperative decreases, there were no relevant alterations observed in coagulation parameters. In summary, all parameters showed an unremarkable course with regard to inflammatory responses and coagulation disorders following cardiac xenotransplantation and thus showed the effectiveness of our approach.

Conclusion: Our preclinical experience with the anti-inflammatory drug therapy proved that controlling of inflammation and coagulation disorders in xenotransplantation is possible and well-practicable under the condition that transmission of pathogens, especially of PCMV/PRV to the recipient is prevented because PCMV/PRV also induces inflammation and coagulation disorders. Our anti-inflammatory regimen should also be applicable and effective in the clinical setting of cardiac xenotransplantation.

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