Evidence of human non-alpha-galactosyl antibodies involved in the hyperacute rejection of pig lungs and their removal by pig organ perfusion.

Macchiarini P; Oriol R; Azimzadeh A; de-Montpreville V; Rieben R; Bovin N; Mazmanian M; Dartevelle P

首页> 外文期刊>The Journal of Thoracic and Cardiovascular Surgery >Evidence of human non-alpha-galactosyl antibodies involved in the hyperacute rejection of pig lungs and their removal by pig organ perfusion.

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Evidence of human non-alpha-galactosyl antibodies involved in the hyperacute rejection of pig lungs and their removal by pig organ perfusion.

机译：人类非α-半乳糖基抗体参与猪肺超急性排斥和通过猪器官灌注清除的证据。

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BACKGROUND: Human natural xenoantibodies represent a major hurdle to the clinical application of pig lungs in transplantation by initiating hyperacute rejection within minutes to hours. OBJECTIVE: The object was to compare pig organ perfusion and specific depletion of anti-alpha-galactosyl xenoantibodies for prevention of hyperacute rejection in the pig to human lung combination. METHODS: Large White pig (20-25 kg) left lungs were removed and continuously ventilated and reperfused ex vivo either with (1) whole human blood previously perfused in situ through pig right lung (group I), liver (group II), or spleen (group III) or with (2) human plasma in vitro immunoabsorbed on columns containing alpha-galactosyl disaccharide (Gal-alpha-(1-3)Gal-beta-(CH2)3NH2; B disaccharide) (group IV). Each study group included 6 animals. RESULTS: The in situ and in vitro preperfusions depleted anti-alpha-galactosyl xenoantibodies and all in situ perfused pig organs showed histologic signs of hyperacute rejection. After the ex vivo reperfusion, group I xenografts had a significantly (P < .001) longer functional and histologic survival than did xenografts in groups II, III, and IV. Human blood reperfusing group I xenografts had a significantly (P < 0.05) lower (1) decline of clotting factors and total circulating immunoglobulins, (2) total and membrane attack complex (C5b,6,7,8,9) complement activation, and (3) hemolysis. By Western blot analysis, the in situ lung preperfusion removed antibodies against non-alpha-galactosyl proteins of low molecular weight that were not eliminated by the alpha-galactosyl column. CONCLUSIONS: Results demonstrate that specific depletion of anti-alpha-galactosyl antibodies alone incompletely protects pig lungs from hyperacute rejection. It is speculated that the more complete prevention of this rejection afforded by pig lung preperfusion relates to the removal of other, non-alpha-galactosyl antibodies.

机译：背景：人类天然异种抗体是在几分钟至几小时内引发超急性排斥反应而成为猪肺移植临床应用的主要障碍。目的：比较猪器官灌注和抗α-半乳糖基异种抗体的特定消耗量，以预防猪对人肺的超急性排斥反应。方法：取出大白猪（20-25公斤）左肺，并连续通气并离体再灌注（1）事先通过猪右肺（I组），肝脏（II组）原位灌注的全人血或脾脏（III组）或与（2）人血浆在体外免疫吸附在含有α-半乳糖基二糖（Gal-α-（1-3）Gal-β-（CH2）3NH2; B二糖）的色谱柱上（IV组）。每个研究组包括6只动物。结果：原位和体外预灌注耗尽了抗α-半乳糖基异种抗体，所有原位灌注的猪器官均表现出超急性排斥的组织学迹象。离体再灌注后，与第二，第三和第四组相比，第一组异种移植的功能和组织学存活时间显着延长（P <.001）。人血再灌注组I异种移植物具有显着（P <0.05）更低（1）凝血因子和总循环免疫球蛋白下降，（2）总膜攻击复合物（C5b，6,7,8,9）补体激活，和（3）溶血。通过蛋白质印迹分析，原位肺预灌注去除了抗低分子量非α-半乳糖基蛋白的抗体，这些抗体没有被α-半乳糖基柱消除。结论：结果表明，仅抗α-半乳糖基抗体的特异性消耗不能完全保护猪肺免受超急性排斥。据推测，猪肺预灌注所提供的这种排斥的更完全预防与去除其他非α-半乳糖基抗体有关。

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《The Journal of Thoracic and Cardiovascular Surgery 》 |1998年第5期| 共13页
作者
Macchiarini P; Oriol R; Azimzadeh A; de-Montpreville V; Rieben R; Bovin N; Mazmanian M; Dartevelle P;
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正文语种 eng
中图分类心脏、血管（循环系）疾病 ; 外科学各论 ;
关键词
Antibodies; Heterophile; Graft Rejection; Lung Transplantation; Organ Preservation; 抗体; 嗜异性; 移植物排斥; 肺移植; 器官保存; 三糖类;

机译：Antibodies;Heterophile;Graft Rejection;Lung Transplantation;Organ Preservation;抗体;嗜异性;移植物排斥;肺移植;器官保存;三糖类;

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1. Evidence of human non-alpha-galactosyl antibodies involved in the hyperacute rejection of pig lungs and their removal by pig organ perfusion. [J] . Macchiarini P, Oriol R, Azimzadeh A, The Journal of Thoracic and Cardiovascular Surgery . 1998 ,第5期

机译：人类非α-半乳糖基抗体参与猪肺超急性排斥和通过猪器官灌注清除的证据。
2. Hyperacute Lung Rejection in the Pig-to-Human Model 4: Evidence for Complement and Antibody Independent Mechanisms. [J] . Pfeiffer S, Blair KS, Wu G, Transplantation: Official Journal of the Transplantation Society . 2005 ,第6期

机译：猪到人模型4中的超急性肺排斥：补体和抗体独立机制的证据。
3. Hyperacute lung rejection in a pig-to-human transplant model: the role of anti-pig antibody and complement. [J] . Pierson RN 3rd, Kasper Konig W, Tew DN, Transplantation: Official Journal of the Transplantation Society . 1997 ,第4期

机译：猪到人移植模型中的超急性肺排斥：抗猪抗体和补体的作用。
4. DETECTION OF PCV-2 ANTIBODY AND DNA IN STILLBORN PIG SERA FROM FARMS WITH A HISTORY OF HIGH BORN-DEAD PIGS [C] . MW Farnham, YK Choi, HS Joo Congress of the International Pig Veterinary Society . 2002

机译：从历史悠久的死猪历史的农场检测病史的病史血清中PCV-2抗体和DNA
5. Study of the pathogenesis of hyperacute and delayed xenograft rejection in the guinea pig-to-rat model [D] . Leventhal, Joseph Ross. 1996

机译：豚鼠大鼠模型中超急性和延迟异种移植排斥反应的发病机理研究
6. Expression of a functional human complement inhibitor in a transgenic pig as a model for the prevention of xenogeneic hyperacute organ rejection. [O] . W L Fodor, B L Williams, L A Matis, 1994

机译：功能性人类补体抑制剂在转基因猪中的表达作为预防异种超急性器官排斥的模型。
7. Evidence of human non-α-galactosyl antibodies involved in the hyperacute rejection of pig lungs and their removal by pig organ perfusion [O] . Macchiarini Paolo, Oriol Rafael, Azimzadeh Agnès, 1998

机译：人类非α-半乳糖基抗体参与猪肺超急性排斥反应以及通过猪器官灌注清除的证据
8. Analyzing Protein Changes in Guinea Pig Tissue Lysates Using Non-guinea Pig Specific Antibodies: Procedures for Western Blotting and Examples Using 16 Individual Antibodies for Common CNS Proteins [R] . Johnson, E. A. , Daugherty, K. S. 2006

机译：使用非豚鼠特异性抗体分析豚鼠组织裂解液中的蛋白质变化：Western印迹和实施例16用于常见CNs蛋白质的单个抗体的程序

Evidence of human non-alpha-galactosyl antibodies involved in the hyperacute rejection of pig lungs and their removal by pig organ perfusion.

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