PaO2oscillations caused by cyclic alveolar recruitment can be monitored in pig buccal mucosa microcirculation

6533b857fe1ef96bd12b4e1f

RESEARCH PRODUCT

PaO2oscillations caused by cyclic alveolar recruitment can be monitored in pig buccal mucosa microcirculation

Kristin Engelhard Klaus Ulrich Klein Klaus Ulrich Klein Tanghua Liu Erik K. Hartmann Klaus Markstaller Klaus Markstaller Christian Werner Matthias David Line Heylen M. Szczyrba Stefan Boehme Stefan Boehme

subject

medicine.medical_specialty Pathology Respiratory rate business.industry chemistry.chemical_element General Medicine Blood flow Lung injury Laser Doppler velocimetry Oxygen Microcirculation Anesthesiology and Pain Medicine Respiratory failure chemistry Internal medicine Cardiology Medicine business Oxygen saturation (medicine)

description

BACKGROUND Cyclic alveolar recruitment and derecruitment play a role in the pathomechanism of acute lung injury and may lead to arterial partial pressure of oxygen (PaO(2) ) oscillations within the respiratory cycle. It remains unknown, however, if these PaO(2) oscillations are transmitted to the microcirculation. The present study investigates if PaO(2) oscillations can be detected in the pig buccal mucosa microcirculation. METHODS Respiratory failure was induced by surfactant depletion in seven pigs. PaO(2) oscillations caused by cyclic recruitment and derecruitment were measured in the thoracic aorta by fast fluorescence quenching of oxygen technology. Haemoglobin oxygen saturation, haemoglobin amount and blood flow in the buccal mucosa microcirculation were determined by combined fast white light spectrometry and laser Doppler flowmetry additionally to systolic arterial pressure. Measurements were performed during baseline conditions and during cyclic recruitment and derecruitment. RESULTS Measurements remained stable during baseline. Respiratory-dependent oscillations occurred in the systemic circulation [PaO(2) oscillations 92 (69-172) mmHg; systolic arterial pressure oscillations 33 (13-35) %] and were related to the respiratory rate (5.0 ± 0.2/min) as confirmed by Fourier analysis. Synchronised oscillations were detected to the pig buccal mucosa microcirculation [haemoglobin oxygen saturation oscillations 3.4 (2.7-4.9) %; haemoglobin amount oscillations 8.5 (2.3-13.3) %; blood flow oscillations 66 (18-87) %]. The delay between PaO(2) -\ and microcirculatory oxygen oscillations was 7.2 ± 2.8 s. CONCLUSION The present study suggests that PaO(2) oscillations caused by cyclic recruitment and derecruitment were transmitted to the buccal mucosa microcirculation. This non-invasive approach of measuring oxygen waves as a surrogate parameter of cyclic recruitment and derecruitment could be used to monitor PaO(2) oscillations at the bedside.

year	journal	country	edition	language
2012-11-21	Acta Anaesthesiologica Scandinavica

https://doi.org/10.1111/aas.12019