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使用抗(肿瘤坏死因子-α)抗体或3-去氮腺苷作为添加剂,以促进威斯康星大学溶液在缺血/再灌注损伤中的保护作用。

Use of anti-(tumour necrosis factor-alpha) antibody or 3-deaza-adenosine as additives to promote protection by University of Wisconsin solution in ischaemia/reperfusion injury.

作者信息

Chiang C H, Wu C P, Perng W C, Yan H C, Yu C P

机构信息

Pulmonary Division, Tri-Service General Hospital, National Defense Medical Center, Taipei, Taiwan, Republic of China.

出版信息

Clin Sci (Lond). 2000 Sep;99(3):215-22.

PMID:11787474
Abstract

Experimental interventions that reduce ischaemia/reperfusion (I/R) lung injury can be used to improve the properties of preservation solutions. We attempted to increase the attenuation of I/R injury by University of Wisconsin solution (UW) by adding an antibody against tumour necrosis factor-alpha (TNF-alpha), to neutralize TNF-alpha, and/or by adding 3-deaza-adenosine (c3-Ado), to inhibit leucocyte adhesion and the biosynthesis of ICAM-1 (intercellular cell-adhesion molecule 1). We examined I/R injury using an isolated rat lung model. Six different solutions were perfused individually, followed by evaluation of I/R injury: (1) 0.9% NaCl (normal saline; NS), (2) NS+anti-TNF-alpha antibody, (3) UW alone, (4) UW+anti-TNF-alpha, (5) UW+c3-Ado and (6) UW+anti-TNF-alpha+c3-Ado. Haemodynamic changes, lung weight gain, capillary filtration coefficient, TNF-alpha levels and lung pathology were analysed in order to evaluate I/R injury. Compared with lungs perfused with NS, lungs treated with NS+anti-TNF-alpha showed less I/R injury. The addition of anti-TNF-alpha and/or c3-Ado to UW reduced I/R injury compared with unmodified UW. Among the six solutions tested, UW containing anti-TNF-alpha antibody reduced I/R injury to the greatest extent. We conclude that addition of anti-TNF-alpha antibody or c3-Ado protects against I/R lung injury when using UW. Further investigation of the improved properties of modified UWs would be beneficial with regard to lung transplantation research.

摘要

可采用减少缺血/再灌注(I/R)肺损伤的实验性干预措施来改善保存液的性能。我们尝试通过在威斯康星大学溶液(UW)中添加抗肿瘤坏死因子-α(TNF-α)抗体以中和TNF-α,和/或添加3-脱氮腺苷(c3-Ado)以抑制白细胞黏附和细胞间黏附分子-1(ICAM-1)的生物合成,来增强UW对I/R损伤的减轻作用。我们使用离体大鼠肺模型研究I/R损伤。分别灌注六种不同的溶液,随后评估I/R损伤:(1)0.9%氯化钠(生理盐水;NS),(2)NS +抗TNF-α抗体,(3)单纯UW,(4)UW +抗TNF-α,(5)UW + c3-Ado,(6)UW +抗TNF-α + c3-Ado。分析血流动力学变化、肺重量增加、毛细血管滤过系数、TNF-α水平和肺病理学,以评估I/R损伤。与灌注NS的肺相比,用NS +抗TNF-α处理的肺I/R损伤较轻。与未改良的UW相比,在UW中添加抗TNF-α和/或c3-Ado可减轻I/R损伤。在所测试的六种溶液中,含抗TNF-α抗体的UW对I/R损伤的减轻作用最大。我们得出结论,在使用UW时添加抗TNF-α抗体或c3-Ado可预防I/R肺损伤。关于改良UW的性能改进的进一步研究对肺移植研究将是有益的。

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