Gene-modified pig-to-human liver xenotransplantation

Kaishan Tao(Xijing Hospital), Zhao-Xu Yang(Xijing Hospital), Xuan Zhang(Xijing Hospital), Hongtao Zhang(Xijing Hospital), Shuqiang Yue(Xijing Hospital), Yanling Yang(Xijing Hospital), Wenjie Song(Xijing Hospital), Desheng Wang(Xijing Hospital), Zhengcai Liu(Xijing Hospital), Haimin Li(Xijing Hospital), Yong Chen(Xijing Hospital), Rui Ding(Xijing Hospital), Shiren Sun(Xijing Hospital), Ming Yu(Xijing Hospital), Jipeng Li(Xijing Hospital), Weixun Duan(Xijing Hospital), Zhe Wang(Xijing Hospital), Jingwen Wang(Xijing Hospital), Jiayun Liu(Xijing Hospital), Minwen Zheng(Xijing Hospital), Xijing Zhang(Xijing Hospital), Wen‐Jin Yin(Xijing Hospital), Wei-Jun Qin(Xijing Hospital), Donglong Bian(Xijing Hospital), Lin Li(Xijing Hospital), Min Li(Xijing Hospital), Zhibin Lin(Xijing Hospital), Haojie Xu(Xijing Hospital), Dan Wei(Xijing Hospital), Hong Zhang(Xijing Hospital), Juanli Duan(Xijing Hospital), Dengke Pan, Hailong Dong(Xijing Hospital), Lin Wang(Xijing Hospital), Kefeng Dou(Xijing Hospital)
Nature
March 26, 2025
Cited by 89Open Access
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Abstract

The shortage of donors is a major challenge for transplantation; however, organs from genetically modified pigs can serve as ideal supplements1,2. Until now, porcine hearts and kidneys have been successively transplanted into humans3–7. In this study, heterotopic auxiliary transplantation was used to donate a six-gene-edited pig liver to a brain-dead recipient. The graft function, haemodynamics, and immune and inflammatory responses of the recipient were monitored over the subsequent 10 days. Two hours after portal vein reperfusion of the xenograft, goldish bile was produced, increasing to 66.5 ml by postoperative day 10. Porcine liver-derived albumin also increased after surgery. Alanine aminotransferase levels remained in the normal range, while aspartate aminotransferase levels increased on postoperative day 1 and then rapidly declined. Blood flow velocity in the porcine hepatic artery and portal and hepatic veins remained at an acceptable level. Although platelet numbers decreased early after surgery, they ultimately returned to normal levels. Histological analyses showed that the porcine liver regenerated capably with no signs of rejection. T cell activity was inhibited by anti-thymocyte globulin administration, and B cell activation increased 3 days after surgery and was then inhibited by rituximab. There were no significant peri-operative changes in immunoglobulin G or immunoglobulin M levels. C-reactive protein and procalcitonin levels were initially elevated and then quickly declined. The xenograft remained functional until study completion. A gene-edited pig liver transplanted into a human recipient remains functional after 10 days and indicates that porcine organs could help meet the growing demand for liver transplants.


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