Service of Thoracic Surgery, Lausanne University Hospital, Lausanne, Switzerland.
Service of Adult Intensive Care Medicine, Lausanne University Hospital, Lausanne, Switzerland.
Front Immunol. 2024 May 14;15:1390026. doi: 10.3389/fimmu.2024.1390026. eCollection 2024.
The pulmonary endothelium is the primary target of lung ischemia-reperfusion injury leading to primary graft dysfunction after lung transplantation. We hypothesized that treating damaged rat lungs by a transient heat stress during ex-vivo lung perfusion (EVLP) to elicit a pulmonary heat shock response could protect the endothelium from severe reperfusion injury.
Rat lungs damaged by 1h warm ischemia were reperfused on an EVLP platform for up to 6h at a constant temperature (T°) of 37°C (EVLP group), or following a transient heat stress (HS) at 41.5°C from 1 to 1.5h of EVLP (EVLP group). A group of lungs exposed to 1h EVLP only (pre-heating conditions) was added as control (Baseline group). In a first protocol, we measured lung heat sock protein expression (HSP70, HSP27 and Hsc70) at selected time-points (n=5/group at each time). In a second protocol, we determined (n=5/group) lung weight gain (edema), pulmonary compliance, oxygenation capacity, pulmonary artery pressure (PAP) and vascular resistance (PVR), the expression of PECAM-1 (CD31) and phosphorylation status of Src-kinase and VE-cadherin in lung tissue, as well as the release in perfusate of cytokines (TNFα, IL-1β) and endothelial biomarkers (sPECAM, von Willebrand Factor -vWF-, sE-selectin and sICAM-1). Histological and immunofluorescent studies assessed perivascular edema and formation of 3-nitrotyrosine (a marker of peroxinitrite) in CD31 lung endothelium.
HS induced an early (3h) and persisting expression of HSP70 and HSP27, without influencing Hsc70. Lungs from the EVLP group developed massive edema, low compliance and oxygenation, elevated PAP and PVR, substantial release of TNFα, IL-1β, s-PECAM, vWF, E-selectin and s-ICAM, as well as significant Src-kinase activation, VE-cadherin phosphorylation, endothelial 3-NT formation and reduced CD31 expression. In marked contrast, all these alterations were either abrogated or significantly attenuated by HS treatment.
The therapeutic application of a transient heat stress during EVLP of damaged rat lungs reduces endothelial permeability, attenuates pulmonary vasoconstriction, prevents src-kinase activation and VE-cadherin phosphorylation, while reducing endothelial peroxinitrite generation and the release of cytokines and endothelial biomarkers. Collectively, these data demonstrate that therapeutic heat stress may represent a promising strategy to protect the lung endothelium from severe reperfusion injury.
肺内皮细胞是肺缺血再灌注损伤的主要靶标,导致肺移植后原发性移植物功能障碍。我们假设,在体外肺灌注(EVLP)期间通过短暂的热应激处理受损的大鼠肺,引发肺热休克反应,可以保护内皮免受严重的再灌注损伤。
用 1 小时热缺血损伤大鼠的肺,在 37°C 的恒定温度(T°)下进行 EVLP (EVLP 组),或在 EVLP 期间进行 1 至 1.5 小时的短暂热应激(HS)(EVLP 组)进行再灌注。添加一组仅接受 1 小时 EVLP 暴露的肺(预热条件)作为对照(基础组)。在第一个方案中,我们在选定的时间点(每组 5 个样本)测量肺热休克蛋白表达(HSP70、HSP27 和 Hsc70)。在第二个方案中,我们测定(每组 5 个样本)肺湿重增加(水肿)、肺顺应性、氧合能力、肺动脉压(PAP)和血管阻力(PVR)、PECAM-1(CD31)的表达和肺组织中Src-激酶和 VE-钙粘蛋白的磷酸化状态,以及细胞因子(TNFα、IL-1β)和内皮生物标志物(sPECAM、血管性血友病因子-vWF-、sE-选择素和 sICAM-1)在灌流液中的释放。组织学和免疫荧光研究评估了肺内皮细胞中血管周围水肿和 3-硝基酪氨酸(过氧亚硝酸盐的标志物)的形成。
HS 诱导 HSP70 和 HSP27 的早期(3 小时)和持续表达,而不影响 Hsc70。EVLP 组的肺发生大量水肿、顺应性和氧合能力降低、PAP 和 PVR 升高、TNFα、IL-1β、s-PECAM、vWF、E-选择素和 sICAM 大量释放,以及 Src-激酶的显著激活、VE-钙粘蛋白的磷酸化、内皮 3-NT 的形成和 CD31 表达的减少。相比之下,HS 处理完全消除或显著减轻了所有这些改变。
在受损大鼠肺 EVLP 期间应用短暂的热应激可降低内皮通透性,减轻肺血管收缩,防止 Src-激酶的激活和 VE-钙粘蛋白的磷酸化,同时减少内皮过氧亚硝酸盐的产生和细胞因子和内皮生物标志物的释放。综上所述,这些数据表明,治疗性热应激可能是保护肺内皮免受严重再灌注损伤的一种有前途的策略。
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