美国食品药品监督管理局批准的第一个转基因猪心脏移植到人类的道路。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2022-09-01 Epub Date: 2022-09-20 DOI:10.1111/xen.12776
Avneesh K Singh, Bartley P Griffith, Corbin E Goerlich, David Ayares, Muhammad M Mohiuddin
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引用次数: 0

摘要

自2005年以来,我们一直在非人类灵长类动物(NHP)中测试基因工程(GE)猪心并优化免疫抑制(IS)。我们展示了我们如何将这项临床前研究转化为美国食品药品监督管理局(FDA)批准的临床心脏异种移植。首先,将基因工程(GE)猪心脏与包括抗CD20和抗CD40共刺激阻断抗体的IS一起移植到NHP的腹部。我们报道了三个基因的GE猪心脏在NHP中存活945天。基于这一概念验证,我们在支持生命的原位模型中测试了3-10个基因修饰的GE猪心脏(为了进一步提高异种移植物的免疫相容性),但由于围手术期心脏异种移植物功能障碍(PCXD),成功率有限。采用新型非缺血性持续灌注保存(NICP),使用XVIVO心脏溶液(XHS),维持生命的生存期延长至9个月。我们向美国食品药品监督管理局申请了“扩大获取”(EA),为一名终末期非缺血性心肌病患者移植GE猪心脏。他没有其他治疗选择,并且依赖VA-ECMO。美国食品药品监督管理局的一个审查小组审查了我们的临床前研究经验和数据,并允许我们继续进行。进行了该临床异种心脏移植,患者存活了60天,证明了异种心脏移植从台架到床边的转化临床前研究。移植物衰竭的最终病因目前是一个研究主题,吸取的经验教训将推动该领域的发展。
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The road to the first FDA-approved genetically engineered pig heart transplantation into human.

We have been testing genetically engineered (GE) pig hearts and optimizing immunosuppression (IS) in non-human primates (NHPs) since 2005. We demonstrate how we translated this preclinical investigation into a US Food and Drug Administration (FDA)-approved clinical cardiac xenotransplantation. First, genetically engineered (GE) pig hearts were transplanted into the abdomen of NHP along with IS, which included anti-CD20 and anti-CD40-based co-stimulation blockade antibodies. We reported 945 days of survival of three gene GE pig hearts in NHPs. Building on this proof-of-concept, we tested 3-10 gene-modified GE pig hearts (in order to improve the immunocompatibility of the xenograft further) in a life-supporting orthotopic model, but had limited success due to perioperative cardiac xenograft dysfunction (PCXD). With novel non-ischemic continuous perfusion preservation (NICP), using the XVIVO Heart solution (XHS), life-supporting survival was extended to 9 months. We approached the FDA under an application for "Expanded Access" (EA), to transplant a GE pig heart in a patient with end-stage non-ischemic cardiomyopathy. He was without other therapeutic options and dependent on VA-ECMO. A team of FDA reviewers reviewed our preclinical research experience and data and allowed us to proceed. This clinical cardiac xenotransplantation was performed, and the patient survived for 60 days, demonstrating the translational preclinical investigation of cardiac xenotransplantation from bench to bedside. The ultimate etiology of graft failure is currently a topic of investigation and lessons learned will progress the field forward.

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567
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