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Human membrane cofactor protein (MCP, CD 46) protects transgenic pig hearts from hyperacute rejection in primates.

作者信息

Adams D H, Kadner A, Chen R H, Farivar R S

机构信息

Division of Cardiac Surgery, Brigham & Women's Hospital, Harvard Medical School, Boston, MA 02115, USA.

出版信息

Xenotransplantation. 2001 Feb;8(1):36-40. doi: 10.1046/j.0908-665x.2000.00085.x.

DOI:10.1046/j.0908-665x.2000.00085.x
PMID:11208189
Abstract

Recently, we and others have shown the prolongation of xenograft survival with the use of transgenic pigs bearing human CD 59 and DAF complement regulatory proteins (CRP). We now report heart transplantation using a new line of transgenic pigs bearing a different human CRP, membrane cofactor protein (MCP, CD 46). We transplanted three MCP transgenic and three wild-type porcine hearts into baboons suppressed with cyclosporine, methylprednisone, and rapamycin or cyclophosphamide. In addition, recipients were treated with extracorporeal plasma perfusion to remove alpha-Gal reactivity. The wild-type grafts were rapidly rejected at 60 to 80 min. Two functioning MCP hearts were removed after 5 and 46 h for histological examination. One MCP heart showed vigorous function until postoperative day 16. Immunohistochemistry of both wild-type and MCP-transgenic hearts showed strong deposition of IgM. In contrast, there was less MAC deposition in the transgenic graft as compared to the wild-type control. MCP is another CRP capable of decreasing the features of hyperacute rejection of cardiac xenografts in baboon recipients.

摘要

相似文献

1
Human membrane cofactor protein (MCP, CD 46) protects transgenic pig hearts from hyperacute rejection in primates.
Xenotransplantation. 2001 Feb;8(1):36-40. doi: 10.1046/j.0908-665x.2000.00085.x.
2
Hearts from transgenic pigs constructed with CD59/DAF genomic clones demonstrate improved survival in primates.用CD59/DAF基因组克隆构建的转基因猪的心脏在灵长类动物中显示出存活率提高。
Xenotransplantation. 1999 Aug;6(3):194-200. doi: 10.1034/j.1399-3089.1999.00017.x.
3
Mechanism of delayed rejection in transgenic pig-to-primate cardiac xenotransplantation.转基因猪至灵长类动物心脏异种移植中延迟性排斥反应的机制
J Surg Res. 2000 May 15;90(2):119-25. doi: 10.1006/jsre.2000.5864.
4
Life-supporting human complement regulator decay accelerating factor transgenic pig liver xenograft maintains the metabolic function and coagulation in the nonhuman primate for up to 8 days.具有维持生命功能的人补体调节因子衰变加速因子转基因猪肝异种移植可在非人灵长类动物中维持代谢功能和凝血功能长达8天。
Transplantation. 2000 Oct 15;70(7):989-98. doi: 10.1097/00007890-200010150-00001.
5
A human CD46 transgenic pig model system for the study of discordant xenotransplantation.用于研究非协调性异种移植的人CD46转基因猪模型系统。
Transplantation. 2001 Jan 15;71(1):132-42. doi: 10.1097/00007890-200101150-00021.
6
Characterization of a CD46 transgenic pig and protection of transgenic kidneys against hyperacute rejection in non-immunosuppressed baboons.CD46转基因猪的特性及转基因肾脏在未免疫抑制狒狒中免受超急性排斥反应的保护作用
Xenotransplantation. 2004 Mar;11(2):171-83. doi: 10.1046/j.1399-3089.2003.00103.x.
7
Transgenic porcine valves show no signs of delayed cardiac xenograft rejection.转基因猪瓣膜未显示出心脏异种移植延迟排斥的迹象。
Ann Thorac Surg. 2001 May;71(5 Suppl):S389-92. doi: 10.1016/s0003-4975(01)02505-x.
8
Protection against hyperacute xenograft rejection of transgenic rat hearts expressing human decay accelerating factor (DAF) transplanted into primates.对移植到灵长类动物体内的表达人衰变加速因子(DAF)的转基因大鼠心脏超急性异种移植排斥反应的防护。
Mol Med. 1999 Sep;5(9):617-30.
9
Transgenic expression of human complement regulatory proteins in mice results in diminished complement deposition during organ xenoperfusion.人类补体调节蛋白在小鼠中的转基因表达导致器官异种灌注期间补体沉积减少。
Transplantation. 1995 Apr 27;59(8):1177-82.
10
Transgenic expression in pig hearts of both human decay-accelerating factor and human membrane cofactor protein does not provide an additional benefit to that of human decay-accelerating factor alone in pig-to-baboon xenotransplantation.在猪心脏中同时转基因表达人衰变加速因子和人膜辅因子蛋白,在猪到狒狒的异种移植中,相较于单独表达人衰变加速因子,并未带来额外益处。
Transplantation. 2004 Sep 27;78(6):930-3. doi: 10.1097/01.tp.0000133309.82387.8c.

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