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作为威斯康星大学溶液添加剂使用的保护剂,用于促进对大鼠肺缺血再灌注损伤的保护。

Protective agents used as additives in University of Wisconsin solution to promote protection against ischaemia-reperfusion injury in rat lung.

作者信息

Chiang C H, Wu K, Yu C P, Perng W C, Yan H C, Wu C P, Chang D M, Hsu K

机构信息

Pulmonary Division, Tri-Service General Hospital, No. 8 Section 3, Ting-Chow Road, Taipei, Taiwan, Republic of China.

出版信息

Clin Sci (Lond). 1998 Sep;95(3):369-76.

PMID:9730858
Abstract
  1. An intervention to reduce ischaemia-reperfusion lung injury will be an important advance in transplant medicine. Although the mechanisms associated with producing ischaemia-reperfusion endothelial injury have not been completely elucidated, many of the injury mediators have been studied in detail. While no single pharmacological therapy is likely to be totally effective in eliminating this complex injury, we have developed a mixture of agents that are known to block pathways involved in producing ischaemia-reperfusion-associated lung vascular injury.2. The present study modified University of Wisconsin solution (UW) by adding one of the protective agents prostaglandin E1 (PGE1), dexamethasone (Dex) or dibutyryl cAMP (Bt2-cAMP), or a combination of these, to the perfusate of rat lungs exposed to 4 h of cold ischaemia followed by 1 h of reperfusion. Nine modified UW solutions were studied: (1) UW+Dex, (2) UW+PGE1, (3) UW+Bt2-cAMP, (4) UW+Dexx3, (5) UW+PGE1x3, (6) UW+Bt2-cAMPx3, (7) UW+Dex+PGE1, (8) UW+Dex+Bt2-cAMP, (9) UW+PGE1+Bt2-cAMP. These solutions were utilized in individual experiments to assess haemodynamic changes, lung weight gain, the capillary filtration coefficient (Kfc) and pathology in all lungs.3. The results indicate that lung weight gain and Kfc values were significantly lower than with UW alone in groups 1, 2 and 3, which contained only one additional protective agent. In groups 4, 5 and 6, which contain three times the concentration of each protective agent, both Kfc and lung weight gain were similar to those measured in groups 1, 2 and 3, i.e. lungs were protected but the protection was not dose dependent. In groups 7, 8 and 9, which contained two protective agents, lung weight gain and Kfc were greatly reduced compared with UW alone. Histopathological studies showed similar decreases in the injury profiles of lungs.4. Although UW contains several antioxidant protective agents such as allopurinol and glutathione, it did not provide effective protection in our ischaemia-reperfusion lung injury model. UW modified with an additive of PGE1, Dex or Bt2-cAMP attenuated ischaemia-reperfusion injury. Furthermore, UW containing two of these protective agents augmented the protection. Among the modified solutions, it appears that UW+PGE1+Bt2-cAMP protects the lungs to a greater extent than all other solutions used in our study. We suggest that preservation solutions containing PGE1-Bt2-cAMP will provide additional protective effects to organs stored for transplantation.
摘要
  1. 减少缺血再灌注肺损伤的干预措施将是移植医学的一项重要进展。尽管与缺血再灌注内皮损伤相关的机制尚未完全阐明,但许多损伤介质已得到详细研究。虽然没有单一的药物疗法可能完全有效地消除这种复杂损伤,但我们已开发出一种混合制剂,已知其可阻断参与产生缺血再灌注相关肺血管损伤的途径。

  2. 本研究通过向经历4小时冷缺血后再灌注1小时的大鼠肺灌注液中添加一种保护剂前列腺素E1(PGE1)、地塞米松(Dex)或二丁酰环磷腺苷(Bt2-cAMP),或这些的组合,对威斯康星大学溶液(UW)进行了改良。研究了9种改良的UW溶液:(1)UW+Dex,(2)UW+PGE1,(3)UW+Bt2-cAMP,(4)UW+Dex×3,(5)UW+PGE1×3,(6)UW+Bt2-cAMP×3,(7)UW+Dex+PGE1,(8)UW+Dex+Bt2-cAMP,(9)UW+PGE1+Bt2-cAMP。这些溶液在各个实验中用于评估所有肺的血流动力学变化、肺重量增加、毛细血管滤过系数(Kfc)和病理学情况。

  3. 结果表明,仅含有一种额外保护剂的第1、2和3组中,肺重量增加和Kfc值显著低于单独使用UW的情况。在每种保护剂浓度为其三倍的第4、5和6组中,Kfc和肺重量增加与第1、2和3组中测得的相似,即肺得到了保护,但保护不具有剂量依赖性。在含有两种保护剂的第7、8和9组中,与单独使用UW相比,肺重量增加和Kfc大大降低。组织病理学研究显示肺损伤情况有类似程度的减轻。

  4. 尽管UW含有几种抗氧化保护剂,如别嘌醇和谷胱甘肽,但在我们的缺血再灌注肺损伤模型中它并未提供有效的保护。添加PGE1、Dex或Bt2-cAMP改良后的UW减轻了缺血再灌注损伤。此外,含有其中两种保护剂的UW增强了保护作用。在改良溶液中,UW+PGE1+Bt2-cAMP似乎比我们研究中使用的所有其他溶液在更大程度上保护肺。我们建议含有PGE1-Bt2-cAMP的保存溶液将为储存用于移植的器官提供额外的保护作用。

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