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在实验性肺自体移植模型中,七氟醚麻醉预处理可保护肺内皮糖萼免受缺血再灌注损伤。

Sevoflurane anesthetic preconditioning protects the lung endothelial glycocalyx from ischemia reperfusion injury in an experimental lung autotransplant model.

作者信息

Casanova Javier, Simon Carlos, Vara Elena, Sanchez Guillermo, Rancan Lisa, Abubakra Selma, Calvo Alberto, Gonzalez Francisco Jose, Garutti Ignacio

机构信息

Anesthesiologist in cardiothoracic section, Anesthesiology Department, Gregorio Marañon Hospital, Doctor Esquerdo Street 46, 28007, Madrid, Spain.

Thoracic Surgery Department, Gregorio Marañon Hospital, Madrid, Spain.

出版信息

J Anesth. 2016 Oct;30(5):755-62. doi: 10.1007/s00540-016-2195-0. Epub 2016 Jun 2.

Abstract

PURPOSE

The glycocalyx is a glycoprotein-polysaccaride layer covering the endothelium luminal surface, and plays a key regulatory role in several endothelial functions. Lung ischemia reperfusion (IR) is a clinical entity that occurs in everyday thoracic surgery and causes glycocalix destruction and a florid local and systemic immune response. Moreover, sevoflurane is able to modulate the inflammatory response triggered by IR lung injury. In this study, we evaluated the protective effects of sevoflurane on the pulmonary endothelial glycocalyx in an in-vivo lung autotransplant model in pigs.

METHODS

Sixteen Large White pigs underwent pneumonectomy plus lung autotransplant. They were divided into two groups depending on the hypnotic agent received (propofol or anesthetic preconditioning with sevoflurane). Glycocalyx components (syndecan-1 and heparan sulphate), cathepsin B, chemokines (MCP-1, MIP-1, and MIP-2) and adhesion molecules (VCAM and ICAM-1) were measured at four different timepoints using porcine-specific enzyme-linked immunosorbent assay (ELISA) kits.

RESULTS

There were no differences between groups in weight or in surgical and one-lung ventilation time. Greater glycocalyx destruction and higher chemokine and adhesion molecule expression were observed in the group that did not receive sevoflurane. Heparan sulphate and serum syndecan levels were higher in the propofol group (P < 0.0001) after reperfusion, as was cathepsin B activity (P < 0.015). MCP-1, MIP-1, MIP-2, VCAM, and ICAM-1 levels were also higher in the propofol group (P < 0.006).

CONCLUSION

Sevoflurane preconditioning protects pulmonary glycocalyx and reduces expression of leukocyte chemokines in an in-vivo model of pulmonary IR.

摘要

目的

糖萼是覆盖在内皮细胞腔面的糖蛋白 - 多糖层,在多种内皮功能中起关键调节作用。肺缺血再灌注(IR)是日常胸外科手术中出现的一种临床情况,会导致糖萼破坏以及明显的局部和全身免疫反应。此外,七氟醚能够调节由IR肺损伤引发的炎症反应。在本研究中,我们在猪的体内肺自体移植模型中评估了七氟醚对肺内皮糖萼的保护作用。

方法

16只大白猪接受了肺切除术加肺自体移植。根据所接受的催眠药物(丙泊酚或七氟醚麻醉预处理)将它们分为两组。使用猪特异性酶联免疫吸附测定(ELISA)试剂盒在四个不同时间点测量糖萼成分(多配体蛋白聚糖 -1和硫酸乙酰肝素)、组织蛋白酶B、趋化因子(MCP -1、MIP -1和MIP -2)以及黏附分子(VCAM和ICAM -1)。

结果

两组在体重、手术时间和单肺通气时间方面无差异。在未接受七氟醚的组中观察到更严重的糖萼破坏以及更高的趋化因子和黏附分子表达。再灌注后,丙泊酚组的硫酸乙酰肝素和血清多配体蛋白聚糖水平更高(P < 0.0001),组织蛋白酶B活性也是如此(P < 0.015)。丙泊酚组的MCP -1、MIP -1、MIP -2、VCAM和ICAM -1水平也更高(P < 0.006)。

结论

在肺IR的体内模型中,七氟醚预处理可保护肺糖萼并降低白细胞趋化因子的表达。

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