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人衰变加速因子及人衰变加速因子/血红素加氧酶-1转基因在猪主动脉内皮细胞中对台湾猕猴血清的体外保护作用

The in vitro protection of human decay accelerating factor and hDAF/heme oxygenase-1 transgenes in porcine aortic endothelial cells against sera of Formosan macaques.

作者信息

Tu C-F, Tai H-C, Wu C-P, Ho L-L, Lin Y-J, Hwang C-S, Yang T-S, Lee J-M, Tseng Y-L, Huang C-C, Weng C-N, Lee P-H

机构信息

Division of Biotechnoloy, Animal Technology Institute Taiwan, Ding-Pu Lii, Zhunan, Miaoli, Taiwan, ROC.

出版信息

Transplant Proc. 2010 Jul-Aug;42(6):2138-41. doi: 10.1016/j.transproceed.2010.05.104.

Abstract

To mitigate hyperacute rejection, pigs have been generated with alpha-Gal transferase gene knockout and transgenic expression of human decay accelerating factor (hDAF), MCP, and CD59. Additionally, heme-oxygenase-1 (HO-1) has been suggested to defend endothelial cells. Sera (MS) (0%, 1%, 5%, 10%, and 15%) from Formosan macaques (Macaca cyclopis, MC), an Old World monkey wildly populated in Taiwan, was used to test the protective in vitro, effects of hDAF or hDAF/hHO-1 on porcine aortic endothelial cells (pAEC) derived from hDAF(+), hDAF(+)/hHO-1(+), and hDAF(+)/hHO-1(-) and 1 nontransgenic pAEC. Ten percent human serum (HS) served as a positive control. When MS addition increased to 10% or 15%, all transgenic pAEC exhibited a greater survival than nontransgenic pAEC. Noticeably, 15% MS reduced survived to <10% versus >40% in nontransgenic and transgenic pAEC, respectively. These results revealed that hDAF exerted protective effects against MC complement activation. However, comparing with 10% MS and HS in pAEC of nontransgenic pigs, the survivability was higher in HS, suggesting that complement activation by MS was more toxic than that by HS. Furthermore, hDAF(+)/hHO-1(+) showed no further protection against effects of MS on transgenic pAEC.

摘要

为减轻超急性排斥反应,已培育出敲除α - 半乳糖转移酶基因并转染人衰变加速因子(hDAF)、膜辅蛋白(MCP)和CD59基因的猪。此外,有人提出血红素加氧酶 - 1(HO - 1)可保护内皮细胞。使用来自台湾野生的旧大陆猴——台湾猕猴(Macaca cyclopis,MC)的血清(MS)(0%、1%、5%、10%和15%),来体外测试hDAF或hDAF/hHO - 1对源自hDAF(+)、hDAF(+)/hHO - 1(+)和hDAF(+)/hHO - 1( - )的猪主动脉内皮细胞(pAEC)以及1株非转基因pAEC的保护作用。10%的人血清(HS)用作阳性对照。当MS添加量增加到10%或15%时,所有转基因pAEC的存活率均高于非转基因pAEC。值得注意的是,15% MS使非转基因和转基因pAEC的存活率分别降至<10%和>40%。这些结果表明,hDAF对MC补体激活具有保护作用。然而,与非转基因猪pAEC中的10% MS和HS相比,HS中的细胞存活率更高,这表明MS引起的补体激活比HS更具毒性。此外,hDAF(+)/hHO - 1(+)对MS对转基因pAEC的影响没有进一步的保护作用。

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