169 research outputs found
Acute Respiratory Distress Syndrome (ARDS): Pathophysiological Insights and Lung Imaging
Acute respiratory distress syndrome (ARDS) is in the center of the scientific debate both
for its complex pathophysiology and for the discussion about the remedies that could contribute to
its healing. The intricate interplay of different body systems that characterizes ARDS is mirrored
by two main research threads, one centered on the pathophysiological mechanisms of the disease
and the other on the new approaches to lung imaging. In this Special Issue of the Journal of
Clinical Medicine are presented studies using imaging technologies based on electrical impedance
tomography, synchrotron radiation computed tomography and intravital probe-based confocal laser
endomicroscopy. The studies on the pathophysiological mechanisms pertain to the evaluation of the
biomarkers of the disease and the platelet disfunction during extracorporeal membrane oxygenation.
These contributions witness the intensity of ARDS research as many of the key problems of the disease
are only in part resolved
Spontaneous breathing with airway pressure release ventilation favors ventilation in dependent lung regions and counters cyclic alveolar collapse in oleic-acid-induced lung injury: a randomized controlled computed tomography trial
INTRODUCTION: Experimental and clinical studies have shown a reduction in intrapulmonary shunt with spontaneous breathing during airway pressure release ventilation (APRV) in acute lung injury. This reduction was related to reduced atelectasis and increased aeration. We hypothesized that spontaneous breathing will result in better ventilation and aeration of dependent lung areas and in less cyclic collapse during the tidal breath. METHODS: In this randomized controlled experimental trial, 22 pigs with oleic-acid-induced lung injury were randomly assigned to receive APRV with or without spontaneous breathing at comparable airway pressures. Four hours after randomization, dynamic computed tomography scans of the lung were obtained in an apical slice and in a juxtadiaphragmatic transverse slice. Analyses of regional attenuation were performed separately in nondependent and dependent halves of the lungs on end-expiratory scans and end-inspiratory scans. Tidal changes were assessed as differences between inspiration and expiration of the mechanical breaths. RESULTS: Whereas no differences were observed in the apical slices, spontaneous breathing resulted in improved tidal ventilation of dependent lung regions (P < 0.05) and less cyclic collapse (P < 0.05) in the juxtadiaphragmatic slices. In addition, with spontaneous breathing, the end-expiratory aeration increased and nonaerated tissue decreased in dependent lung regions close to the diaphragm (P < 0.05 for the interaction ventilator mode and lung region). CONCLUSION: Spontaneous breathing during APRV redistributes ventilation and aeration to dependent, usually well-perfused, lung regions close to the diaphragm, and may thereby contribute to improved arterial oxygenation. Spontaneous breathing also counters cyclic collapse, which is a risk factor for ventilation-associated lung injury
Tigecycline Soft Tissue Penetration in Obese and Non-obese Surgical Patients Determined by Using In Vivo Microdialysis
Background and Objective
Tigecycline, a broad-spectrum glycylcycline antibiotic, is approved for use at a fixed dose irrespective of body weight. However, its pharmacokinetics may be altered in obesity, which would impact on the antibiotic’s effectiveness. The objective of this study was to investigate the plasma and subcutaneous tissue concentrations of tigecycline in obese patients compared with those in a non-obese control group.
Methods
Fifteen obese patients (one class II and 14 class III) undergoing bariatric surgery and 15 non-obese patients undergoing intra-abdominal surgery (mainly tumour resection) received a single dose of 50 or 100 mg tigecycline as an intravenous short infusion. Tigecycline concentrations were measured up to 8 h after dosing in plasma (total concentration), in ultrafiltrate of plasma (free concentration), and in microdialysate from subcutaneous tissue, respectively.
Results
In obese patients, total peak plasma concentration (1.31 ± 0.50 vs 2.27 ± 1.40 mg/L) and the area under the concentration–time curve from 0 to 8 h (AUC8h,plasma: 2.15 ± 0.42 vs 2.74 ± 0.73 h⋅mg/L), as normalized to a 100 mg dose, were significantly lower compared with those of non-obese patients. No significant differences were observed regarding the free plasma concentration, as determined by ultrafiltration, or the corresponding AUC8h (fAUC8h,plasma). Concentrations in interstitial fluid (ISF) of subcutaneous tissue were lower than the free plasma concentrations in both groups, and they were lower in obese compared to non-obese patients: the AUC8h in ISF (AUC8h,ISF) was 0.51 ± 0.22 h⋅mg/L in obese and 0.79 ± 0.23 h⋅mg/L in non-obese patients, resulting in a relative tissue drug exposure (AUC8h,ISF/fAUC8h,plasma) of 0.38 ± 0.19 and 0.63 ± 0.24, respectively.
Conclusion
Following a single dose of tigecycline, concentrations in the ISF of subcutaneous adipose tissue are decreased in heavily obese subjects, calling for an increased loading dose
Methods for determination of individual PEEP for intraoperative mechanical ventilation using a decremental PEEP trial
(1) Background: Individual PEEP settings (PEEP(IND)) may improve intraoperative oxygenation and optimize lung mechanics. However, there is uncertainty concerning the optimal procedure to determine PEEP(IND). In this secondary analysis of a randomized controlled clinical trial, we compared different methods for PEEP(IND) determination. (2) Methods: Offline analysis of decremental PEEP trials was performed and PEEP(IND) was retrospectively determined according to five different methods (EIT-based: RVD(I) method, Global Inhomogeneity Index [GI], distribution of tidal ventilation [EIT VT]; global dynamic and quasi-static compliance). (3) Results: In the 45 obese and non-obese patients included, PEEP(IND) using the RVD(I) method (PEEP(RVD)) was 16.3 ± 4.5 cm H(2)O. Determination of PEEP(IND) using the GI and EIT VT resulted in a mean difference of −2.4 cm H(2)O (95%CI: −1.2;−3.6 cm H(2)O, p = 0.01) and −2.3 cm H(2)O (95% CI: −0.9;3.7 cm H(2)O, p = 0.01) to PEEP(RVD), respectively. PEEP(IND) selection according to quasi-static compliance showed the highest agreement with PEEP(RVD) (p = 0.67), with deviations > 4 cm H(2)O in 3/42 patients. PEEP(RVD) and PEEP(IND) according to dynamic compliance also showed a high level of agreement, with deviations > 4 cm H(2)O in 5/42 patients (p = 0.57). (4) Conclusions: High agreement of PEEP(IND) determined by the RVD(I) method and compliance-based methods suggests that, for routine clinical practice, PEEP selection based on best quasi-static or dynamic compliance is favorable
Influence of different thorax models on anatomical precision of EIT
To study the anatomical precision of EIT images, we compared 2D, 2.5D and 3D thorax models of varying complexity for EIT data of a healthy and an injured lung. We determined the lung shape as the averaged tidal image for several breaths. The overlap was computed for a reference CT shape. A 3D subvolume of the lung with large anatomical complexity achieves the best overlap scores for most cases
Linezolid Concentrations in Plasma and Subcutaneous Tissue are Reduced in Obese Patients, Resulting in a Higher Risk of Underdosing in Critically Ill Patients: A Controlled Clinical Pharmacokinetic Study
Background: Linezolid is used for the treatment of soft tissue infections in critically ill patients. However, data for characterizing the pharmacokinetics (PK) and assessing whether effective concentrations are reached at the target site are lacking. We hypothesized that current dosing regimens do not lead to effective concentrations in the plasma and interstitial fluid (ISF) of subcutaneous tissue in obese patients. Methods: As a controlled clinical model, critically ill obese and non-obese patients undergoing intra-abdominal surgery received 600 mg linezolid as a single infusion. Concentrations in the plasma and microdialysate from the ISF of subcutaneous tissue were determined up to 8 h after dosing. Pharmacokinetic analysis was performed by non-compartmental methods. As a therapeutic target, we used fAUC/MIC > 80. Results: Fifteen obese (BMI: 48.7 +/- 11.2 kg/m(2)) and 15 non-obese (23.9 +/- 2.1 kg/m(2)) patients were analyzed. AUC(0-8) in ISF decreased by -1.69 mg*h/L (95% CI: -2.59 to -0.79, p = 1 mg/L in ISF and >= 2 mg/L in plasma. Conclusions: Increasing the weight led to a decrease of linezolid concentrations in the plasma and subcutaneous tissue. The current dosing regimen does not seem to produce sufficient concentrations to kill bacteria with MIC >= 2 mg/L, especially as empirical antimicrobial therapy in critically ill obese patients
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