Recurrent recruitment manoeuvres improve lung mechanics and minimize lung injury during mechanical ventilation of healthy mice

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Abstract

Introduction: Mechanical ventilation (MV) of mice is increasingly required in experimental studies, but the conditions that allow stable ventilation of mice over several hours have not yet been fully defined. In addition, most previous studies documented vital parameters and lung mechanics only incompletely. The aim of the present study was to establish experimental conditions that keep these parameters within their physiological range over a period of 6 h. For this purpose, we also examined the effects of frequent short recruitment manoeuvres (RM) in healthy mice. Methods: Mice were ventilated at low tidal volume V T = 8 mL/kg or high tidal volume V T = 16 mL/kg and a positive end-expiratory pressure (PEEP) of 2 or 6 cmH 2O. RM were performed every 5 min, 60 min or not at all. Lung mechanics were followed by the forced oscillation technique. Blood pressure (BP), electrocardiogram (ECG), heart frequency (HF), oxygen saturation and body temperature were monitored. Blood gases, neutrophil-recruitment, microvascular permeability and pro-inflammatory cytokines in bronchoalveolar lavage (BAL) and blood serum as well as histopathology of the lung were examined. Results: MV with repetitive RM every 5 min resulted in stable respiratory mechanics. Ventilation without RM worsened lung mechanics due to alveolar collapse, leading to impaired gas exchange. HF and BP were affected by anaesthesia, but not by ventilation. Microvascular permeability was highest in atelectatic lungs, whereas neutrophil-recruitment and structural changes were strongest in lungs ventilated with high tidal volume. The cytokines IL-6 and KC, but neither TNF nor IP-10, were elevated in the BAL and serum of all ventilated mice and were reduced by recurrent RM. Lung mechanics, oxygenation and pulmonary inflammation were improved by increased PEEP. Conclusions: Recurrent RM maintain lung mechanics in their physiological range during low tidal volume ventilation of healthy mice by preventing atelectasis and reduce the development of pulmonary inflammation. © 2011 Reiss et al.

Figures

  • Table 1. Comparison of mouse ventilation models.
  • Table 2. Experimental groups.
  • Figure 1. Lung mechanics. Mice were ventilated for six hours with low VT = 8 mL/kg or high VT = 16 mL/kg, PEEP = 2 cmH2O and RM every five minutes (RM5), every 60 minutes (RM60) or without RM (noRM). Lung mechanics were measured every ten minutes by the forced oscillation technique. (LowVTRM5: n = 6, highVTRM5: n = 6, lowVTnoRM: n = 5, highVTnoRM: n = 4, lowVTRM60: n = 5). P-values for group comparisons are shown in supplementary Table S1. doi:10.1371/journal.pone.0024527.g001
  • Figure 2. Heart rate and blood pressure. Electrocardiogram (ECG) was recorded permanently. A. Heart frequency (HF) was calculated simultaneously from the ECG and is displayed in beats per minute (bpm). B. Mean arterial blood pressure (BP) was measured via a catheter in the carotid artery.(LowVTRM5 n = 6, highVTRM5 n = 6, lowVTnoRM n = 5, highVTnoRM n = 4, lowVTRM60 n = 5). doi:10.1371/journal.pone.0024527.g002
  • Figure 3. Blood gas results. Arterial blood was analysed after six hours of ventilation. A. pO2/FiO2 ratio was calculated, FiO2 was 0.5. B. Comparison of pCO2 levels. (LowVTRM5 n = 6, highVTRM5 n = 6, lowVTnoRM n = 5, highVTnoRM n = 4, lowVTRM60 n = 5). * p,0.05, ** p,0.01, *** p,0.001. doi:10.1371/journal.pone.0024527.g003
  • Figure 4. Protein leakage. A. Total protein levels were measured with DC protein assay. (Unventilated n = 5, lowVTRM5 n = 6, highVTRM5 n = 6, lowVTnoRM n = 4, highVTnoRM n = 4, lowVTRM60 n = 5). B. BSA was quantified in BAL and serum by ELISA and the ratio was calculated. (Unventilated n = 5, lowVTRM5 n = 5, highVTRM5 n = 5, lowVTnoRM n = 4, highVTnoRM n = 4, lowVTRM60 n = 5). * p,0.05, ** p,0.01, *** p,0.001. doi:10.1371/journal.pone.0024527.g004
  • Figure 6. Neutrophils in BAL fluid. BAL fluid was subjected to cytospin preparation, followed by Diff-Quick staining. From each preparation 400 cells were counted and percentage of neutrophils was calculated. (Unventilated: n = 5, lowVTRM5 n = 5, highVTRM5 n = 5, lowVTnoRM n = 4, highVTnoRM n = 4, lowVTRM60 n = 5). 1 *** p,0.001 versus all other groups. doi:10.1371/journal.pone.0024527.g006
  • Figure 7. Lung histopathology. Representative lung sections stained with hematoxylin and eosin from: A. unventilated control, B. lowVTRM60, C. lowVTRM5, D. highVTRM5, E. lowVTnoRM and F. highVTnoRM mice. Black arrows indicate neutrophils; blue arrows indicate intra-alveolar monocytes and macrophages, scale bars 100 mm; magnification 200x. Insets in A and D contain enlarged images of exemplary leukocytes. doi:10.1371/journal.pone.0024527.g007

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Reiss, L. K., Kowallik, A., & Uhlig, S. (2011). Recurrent recruitment manoeuvres improve lung mechanics and minimize lung injury during mechanical ventilation of healthy mice. PLoS ONE, 6(9). https://doi.org/10.1371/journal.pone.0024527

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