Prolonged EVLP Using OCS Lung

Loor, Gabriel; Howard, Brian T.; Spratt, John R.; Mattison, Lars M.; Panoskaltsis‐Mortari, Angela; Brown, Roland; Iles, Tinen L.; Meyer, Carolyn; Helms, Haylie R.; Price, Alex; Iaizzo, Paul A.

doi:10.1097/tp.0000000000001616

Cited by 70 publications

(43 citation statements)

References 30 publications

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“…Perfusion times in clinical EVLP range from 4 to 11 h. For functional assessment of lungs after donation after circulatory death (DCD) or of marginal lungs after donation after brain death usually shorter time periods are used, while for reconditioning purposes or therapeutic interventions an extension of perfusion times up to 6–12 h or even beyond might be necessary [ 30 – 32 ]. In experimental EVLP, perfusion times of up to 24 h have been performed [ 17 , 33 ].…”

Section: Discussionmentioning

confidence: 99%

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Cellular and acellular ex vivo lung perfusion preserve functional lung ultrastructure in a large animal model: a stereological study

et al. 2018

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BackgroundEx vivo lung perfusion (EVLP) is used by an increasing number of transplant centres. It is still controversial whether an acellular or cellular (erythrocyte enriched) perfusate is preferable. The aim of this paper was to evaluate whether acellular (aEVLP) or cellular EVLP (cEVLP) preserves functional lung ultrastructure better and to generate a hypothesis regarding possible underlying mechanisms.MethodsLungs of 20 pigs were assigned to 4 groups: control, ischaemia (24 h), aEVLP and cEVLP (both EVLP groups: 24 h ischaemia + 12 h EVLP). After experimental procedures, whole lungs were perfusion fixed, samples for light and electron microscopic stereology were taken, and ventilation, diffusion and perfusion related parameters were estimated.ResultsLung structure was well preserved in all groups. Lungs had less atelectasis and higher air content after EVLP. No significant group differences were found in alveolar septum composition or blood-air barrier thickness. Small amounts of intraalveolar oedema were detected in both EVLP groups but significantly more in aEVLP than in cEVLP.ConclusionsBoth EVLP protocols supported lungs well for up to 12 h and could largely prevent ischaemia ex vivo reperfusion associated lung injury. In both EVLP groups, oedema volume remained below the level of functional relevance. The group difference in oedema formation was possibly due to inferior septal perfusion in aEVLP.Electronic supplementary materialThe online version of this article (10.1186/s12931-018-0942-5) contains supplementary material, which is available to authorized users.

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Section: Discussionmentioning

confidence: 99%

“…erythrocyte addition to perfusate. Previous studies mainly focusing on functional parameters gave differential and sometimes conflicting results regarding the superiority of any one of the techniques [ 13 – 17 ]. However, uncertainties about preferable strategies limit further expansion of EVLP usage.…”

Section: Introductionmentioning

confidence: 99%

Cellular and acellular ex vivo lung perfusion preserve functional lung ultrastructure in a large animal model: a stereological study

et al. 2018

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“…To our knowledge, EVLP for more than 12h has not been reported so far using the three widely used EVLP protocols in the clinical setting. Several studies have been performed to optimize the EVLP protocols looking at the roles of atrial pressure, 9 synchronous bronchial artery circulation, 10 cellular and acellular perfusates, 11 continued perfusate exchange, 12 negative pressure ventilation, 13 perfusate oxygen concentration, 14 continuous perfusate adsorption, 15 and positioning of donor lungs. 16 Combination of these strategies may result in prolonged EVLP times.…”

Section: Glossary Of Abbreviationsmentioning

confidence: 99%

Perfusate adsorption during ex vivo lung perfusion improves early post-transplant lung function

Arni

Maeyashiki

Çıtak

et al. 2021

The Journal of Thoracic and Cardiovascular Surgery

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Objective: Improvement in ex vivo lung perfusion (EVLP) protocols could increase the number of donors available for transplantation and protect the lungs from primary graft dysfunction. We hypothesize that perfusate adsorption during EVLP reconditions the allograft to ischemia-reperfusion injury after lung transplantation. Methods: Donor pig lungs were preserved for 24h at 4°C, followed by 6h of EVLP according to the Toronto protocol. The perfusate was additionally adsorbed through a CytoSorb adsorber in the treatment group, whereas control lungs were perfused according to the standard protocol (n = 5, each). EVLP physiology and biochemistry were monitored. Upon completion of EVLP, a left single lung transplantation was performed. Oxygenation function and lung mechanics were assessed during a 4-hour reperfusion period. The inflammatory response was determined during EVLP and reperfusion. Results: The cytokine concentrations in the perfusate were markedly lower with the adsorber, resulting in improved EVLP physiology and biochemistry during the 6-hour perfusion period. Post-transplant dynamic lung compliance was markedly better during the 4-hour reperfusion period in the treatment group. Isolated allograft oxygenation function and dynamic compliance were continued to be superior in the adsorber group at the end of reperfusion accompanied by a markedly decreased local inflammatory response. Conclusions: Implementation of an additional cytokine adsorber has refined the standard EVLP protocol. Furthermore, cytokine removal during EVLP improved immediate post-transplant graft function together with a less intense inflammatory response to reperfusion in pigs. Further studies are warranted to understand the beneficial effects of perfusate adsorption during EVLP in the clinical setting.

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“…Fluid exchange depends on the balance of hydrostatic and oncotic pressure differences between the lumen of the microvasculature and the interstitial space, and the selective permeability of the endothelium to molecules of different sizes, as described in the classic Starling hypothesis (27). The essential roles of the normal electrolyte composition, pH, nutrient, hormonal and colloid osmotic pressure of the perfusion solution in maintaining vascular function have been well characterized in the classic isolated organ preparations such as the isolated heart, lung, and kidney, and more recently in ex vivo perfusion protocols used to recondition donor lungs before transplantation (6,16,22,25,27,35). However, these isolated organ preparations develop edema after relatively brief periods (hours).…”

Section: Introductionmentioning

confidence: 99%

“…However, these isolated organ preparations develop edema after relatively brief periods (hours). To further increase the period for which isolated organs can be maintained viable, nonphysiological modifications of classic perfusion media have been introduced such as increasing concentrations of albumin and globulins substantially above normal in vivo values to increase colloid osmotic pressure, and addition of pharmacological vasodilators and oxidant scavengers (25,35). Nonetheless, development of edema after relatively restricted periods of time remains a problem (6,35).…”

Section: Introductionmentioning

confidence: 99%

Pulmonary endothelial permeability and tissue fluid balance depend on the viscosity of the perfusion solution

Rowan

Rochfort

Piouceau

et al. 2018

American Journal of Physiology-Lung Cellular and Molecular Phys

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Fluid filtration in the pulmonary microcirculation depends on the hydrostatic and oncotic pressure gradients across the endothelium and the selective permeability of the endothelial barrier. Maintaining normal fluid balance depends both on specific properties of the endothelium and of the perfusing blood. Although some of the essential properties of blood needed to prevent excessive fluid leak have been identified and characterized, our understanding of these remains incomplete. The role of perfusate viscosity in maintaining normal fluid exchange has not previously been examined. We prepared a high-viscosity perfusion solution (HVS) with a relative viscosity of 2.5, i.e., within the range displayed by blood flowing in vessels of different diameters in vivo (1.5-4.0). Perfusion of isolated murine lungs with HVS significantly reduced the rate of edema formation compared with perfusion with a standard solution (SS), which had a lower viscosity similar to plasma (relative viscosity 1.5). HVS did not alter capillary filtration pressure. Increased endothelial shear stress produced by increasing flow rates of SS, to mimic the increased shear stress produced by HVS, did not reduce edema formation. HVS significantly reduced extravasation of Evans blue-labeled albumin compared with SS, indicating that it attenuated endothelial leak. These findings demonstrate for the first time that the viscosity of the solution perfusing the pulmonary microcirculation is an important physiological property contributing to the maintenance of normal fluid exchange. This has significant implications for our understanding of fluid homeostasis in the healthy lung, edema formation in disease, and reconditioning of donor organs for transplantation.

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Prolonged EVLP Using OCS Lung

Cited by 70 publications

References 30 publications

Cellular and acellular ex vivo lung perfusion preserve functional lung ultrastructure in a large animal model: a stereological study

Cellular and acellular ex vivo lung perfusion preserve functional lung ultrastructure in a large animal model: a stereological study

Perfusate adsorption during ex vivo lung perfusion improves early post-transplant lung function

Pulmonary endothelial permeability and tissue fluid balance depend on the viscosity of the perfusion solution

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