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肺内源性封闭、其机制以及对肺封闭剂研究的有效性和转化价值的影响:动物研究的汇总分析

Intrinsic pulmonary sealing, its mechanisms and impact on validity and translational value of lung sealant studies: a pooled analysis of animal studies.

作者信息

Hermans Bob P, Li Wilson W L, Roozen Edwin A, van Dort Daniël I M, Vos Shoko, van der Heide Stefan M, van der Heijden Erik H F M, Ten Broek Richard P G, van Goor Harry, Verhagen Ad F T M

机构信息

Department of Cardio-Thoracic Surgery, Radboud University Medical Center, Radboud Institute for Health Sciences, Nijmegen, The Netherlands.

Department of General Surgery, Radboud University Medical Center, Radboud Institute for Health Sciences, Nijmegen, The Netherlands.

出版信息

J Thorac Dis. 2023 Sep 28;15(9):4703-4716. doi: 10.21037/jtd-23-180. Epub 2023 Aug 30.

Abstract

BACKGROUND

No validated and standardized animal models of pulmonary air leakage (PAL) exist for testing aerostatic efficacy of lung sealants. Lack of negative control groups in published studies and intrinsic sealing mechanisms of healthy animal lungs might contribute to a translational gap, leading to poor clinical results. This study aims to address the impact of intrinsic sealing mechanisms on the validity of PAL models, and investigate the conditions required for an ovine model of PAL for lung sealant testing.

METHODS

An ovine acute aerostasis model was developed, consisting of a bilateral thoracotomy with lesion creation, chest tube insertion and monitoring of air leaks using digital drains (≥80 minutes), under spontaneous respiration. Healthy mixed-breed adult female sheep were used and all procedures were performed under terminal anesthesia. Superficial parenchymal lesions were tested and , extended lesions including bronchioles (deep bowl-shaped and sequential lung amputation lesions) were tested . Experiment outcomes include air leakage (AL), minimal leaking pressure (MLP) and histology.

RESULTS

Two (N=4 superficial parenchymal lesions) and 10 experiments (N=5 superficial parenchymal and N=16 lesions involving bronchioles) were performed. In contrast to the model, superficial parenchymal lesions showed less air leak [mean flow ± standard deviation (SD): 760±693 42±33 mL/min, P=0.055]. All superficial parenchymal lesions sealed intrinsically within a median time of 20 minutes [interquartile range (IQR), 10-75 minutes]. Histology of the intrinsic sealing layer revealed an extended area of alveolar collapse below the incision with intra-alveolar hemorrhage. Compared to superficial parenchymal lesions , lesions involving bronchioles induced significantly higher air leak post-operatively (normalized mean flow ± SD: 459±221 mL/min, P=0.003). At termination, 5/9 (55.6%) were still leaking (median drain time: 273 minutes, IQR, 207-435 minutes), and intrinsic sealing for the remaining lungs occurred within a median of 115 minutes (IQR, 52-245 minutes).

CONCLUSIONS

Lung parenchyma of healthy sheep shows a strong intrinsic sealing mechanism, explained pathologically by an extended area of alveolar collapse, which may contribute to a translational gap in lung sealant research. A meaningful ovine model has to consist of deep lesions involving bronchioles of >⌀1.5 mm. Further research is needed to develop a standardized PAL model, to improve clinical effectiveness of lung sealants.

摘要

背景

目前尚无经过验证和标准化的肺漏气(PAL)动物模型用于测试肺密封剂的气密效果。已发表研究中缺乏阴性对照组以及健康动物肺的内在密封机制可能导致转化差距,进而导致临床效果不佳。本研究旨在探讨内在密封机制对PAL模型有效性的影响,并研究用于肺密封剂测试的绵羊PAL模型所需的条件。

方法

建立了一种绵羊急性气密模型,包括双侧开胸、制造损伤、插入胸管并使用数字引流装置监测漏气情况(≥80分钟),实验在自主呼吸下进行。使用健康的成年杂种雌性绵羊,所有操作均在终末期麻醉下进行。对浅表实质损伤进行了测试, 并对包括细支气管的扩展损伤(深碗状和连续肺切除损伤)进行了测试。实验结果包括漏气(AL)、最小漏气压力(MLP)和组织学检查。

结果

进行了2项(N = 4个浅表实质损伤)和10项实验(N = 5个浅表实质损伤和N = 16个涉及细支气管的损伤)。与 模型相比,浅表实质损伤显示漏气较少[平均流量±标准差(SD):760±693对42±33 mL/分钟,P = 0.055]。所有浅表实质损伤在中位时间20分钟内(四分位间距(IQR),10 - 75分钟)自行封闭。内在密封层的组织学检查显示切口下方肺泡萎陷区域扩大,伴有肺泡内出血。与浅表实质损伤相比,涉及细支气管的损伤术后漏气明显更高(标准化平均流量±SD:459±221 mL/分钟,P = 0.003)。在实验结束时,5/9(55.6%)仍在漏气(中位引流时间:273分钟,IQR,207 - 435分钟),其余肺的内在密封在中位时间115分钟内(IQR,52 - 245分钟)发生。

结论

健康绵羊的肺实质显示出强大的内在密封机制,病理上表现为肺泡萎陷区域扩大,这可能导致肺密封剂研究中的转化差距。一个有意义的绵羊模型必须包括涉及直径>⌀1.5 mm细支气管的深部损伤。需要进一步研究以开发标准化的PAL模型,提高肺密封剂的临床有效性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/217e/10586971/1cfafa8683c0/jtd-15-09-4703-f2.jpg

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