The assessment of gas exchange by automated analysis of O2 and CO2 alveolar to arterial differences

Paoletti, P; Fornai, E.; A, Giannella Neto; Prediletto, Renato; Ruschi, S.; Pisani, P; Giuntini, C.

doi:10.1007/bf01880760

Cited by 5 publications

(7 citation statements)

References 13 publications

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“…Pulmonary gas exchange was estimated primarily by the V D/VTalv, calculated using etCO2 in the Severinghaus equation (1,14,25). Use of the etCO2 to estimate the alveolar dead space fraction as opposed to the mixed-expired CO2 was chosen because the end-tidal equation provides a more specific estimate of the alveolar dead space fraction compared with the physiological dead space fraction, which measures both airway and alveolar dead space (25).…”

Section: Methodsmentioning

confidence: 99%

“…Use of the etCO2 to estimate the alveolar dead space fraction as opposed to the mixed-expired CO2 was chosen because the end-tidal equation provides a more specific estimate of the alveolar dead space fraction compared with the physiological dead space fraction, which measures both airway and alveolar dead space (25). VD/VTalv correlates with pulmonary vascular resistance (22), and perfusion defects in humans with PE (17) decreases in parallel with reduction in perfusion defects during treatment (25) and correlates with the plasma concentration of TxB2 in dogs with PE (39).…”

Section: Methodsmentioning

confidence: 99%

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Inhibition of prostaglandin synthesis during polystyrene microsphere-induced pulmonary embolism in the rat

Jones

Watts

Debelak

et al. 2003

American Journal of Physiology-Lung Cellular and Molecular Phys

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2002.-Our objective was to test the effect of inhibition of thromboxane synthase versus inhibition of cyclooxygenase (COX)-1/2 on pulmonary gas exchange and heart function during simulated pulmonary embolism (PE) in the rat. PE was induced in rats via intrajugular injection of polystyrene microspheres (25 m). Rats were randomized to one of three posttreatments: 1) placebo (saline), 2) thromboxane synthase inhibition (furegrelate sodium), or 3) COX-1/2 inhibition (ketorolac tromethamine). Control rats received no PE. Compared with controls, placebo rats had increased thromboxane B2 (TxB2) in bronchoalveolar lavage fluid and increased urinary dinor TxB2. Furegrelate and ketorolac treatments reduced TxB2 and dinor TxB2 to control levels or lower. Both treatments significantly decreased the alveolar dead space fraction, but neither treatment altered arterial oxygenation compared with placebo. Ketorolac increased in vivo mean arterial pressure and ex vivo left ventricular pressure (LVP) and right ventricular pressure (RVP). Furegrelate improved RVP but not LVP. Experimental PE increased lung and systemic production of TxB 2. Inhibition at the COX-1/2 enzyme was equally as effective as inhibition of thromboxane synthase at reducing alveolar dead space and improving heart function after PE. thromboembolism/treatment; cyclooxygenase; thromboxane; leukotriene; ketorolac; heart failure; Langendorff; animal model PULMONARY EMBOLISM (PE) continues to be a major cause of morbidity and mortality in the United States. In one large autopsy-based study, massive PE was the second leading cause of sudden death in adults aged Ͻ65 yr (4). The primary treatment strategy for massive PE is the recanalization of occluded pulmonary vasculature by fibrinolytic agents (11), catheter fragmentation (32), or surgical removal of clot (16). However, up to one-half of patients with massive PE have contraindications to fibrinolysis (15), and few hospitals have facilities for invasive treatment of PE. Even under optimal conditions (e.g., immediate bolus infusion of a fibrinolytic agent), these interventions require Ͼ2 h to effect a significant reduction in pulmonary vascular resistance (20). PE may also cause pulmonary vasoconstriction through the liberation of vasoconstrictive agents, including PGF 2␣ and thromboxane (Tx) A 2 and B 2 (10). PE can cause hypoxemia and increased pulmonary arterial pressure in previously healthy patients (19). Both hypoxemia and increased shear forces in the pulmonary vascular bed have been found to increase expression of the cyclooxygenase (COX)-2 gene (3). In humans with PE, blood concentrations of thromboxane have been found to be elevated for up to 7 days after onset of symptoms (10). Both the mechanical vascular occlusion and release of vasoconstrictive agents from massive PE appear to produce a synergistic effect that causes acute pulmonary hypertension, worsened gas exchange, impaired right ventricular (RV) function that can culminate in acute cor pulmonale, circulatory shock, and even death (26,30,39).In the ...

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Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Inhibition of prostaglandin synthesis during polystyrene microsphere-induced pulmonary embolism in the rat

Jones

Watts

Debelak

et al. 2003

American Journal of Physiology-Lung Cellular and Molecular Phys

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“…From 13 unique candidate variables, our selection process found that end-tidal CO 2 , end-tidal O 2 , and flow yielded the genome with highest overall diagnostic accuracy. End-tidal CO 2 concentrations have previously been used to diagnose pulmonary embolism [11,20]. Similarly, higher end-tidal O 2 concentrations are associated with pulmonary embolism [11].…”

Section: Discussionmentioning

confidence: 99%

“…The D-dimer test has excellent diagnostic sensitivity but has poor specificity in most patients with risk factors for pulmonary embolism [5]. Several studies have been conducted utilizing the knowledge that pulmonary embolism increases pulmonary deadspace and affects partial pressures of exhaled CO 2 or O 2 [11,20]. Recently, development of a portable device that measures exhaled CO 2 and O 2 concentrations along with flows and volumes has shown promise in predicting thromboembolism [12].…”

Section: Introductionmentioning

confidence: 99%

Use of genetic programming to diagnose venous thromboembolism in the emergency department

Engoren

Kline

2007

Genet Program Evolvable Mach

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Pulmonary thromboembolism as a cause of respiratory complaints is frequently undiagnosed and requires expensive imaging modalities to diagnose. The objective of this study was to determine if genetic programming could be used to classify patients as having or not having pulmonary thromboembolism using exhaled ventilatory and gas indices as genetic material. Using a custom-built exhaled oxygen and carbon dioxide analyzer; exhaled flows, volumes, and gas partial pressures were recorded from patients for a series of deep exhalation and 30 s tidal volume breathing. A diagnosis of pulmonary embolism was made by contrast-enhanced computerized tomography angiography of the chest and indirect venography supplemented by 90-day follow-up. Genetic programming developed a series of genomes comprising genes of exhaled CO 2 , O 2 , flow, volume, vital signs, and patient demographics from these data and their predictions were compared to the radiological results. We found that 24 of 178 patients had pulmonary embolism. The best genome consisted of four genes: the minimum flow rate during the third 30 s period of tidal breathing, the average peak exhaled CO 2 during the first 30 s period of tidal breathing, the average peak of the exhaled O 2 during the first 30 s period of tidal breathing, and the average peak exhaled CO 2 during the fourth period of tidal breathing, which immediately followed a deep exhalation. This had 100% sensitivity and 91% specificity on the construction population and 100% and 82%, respectively when tested on the separate validation population. Genetic programming using only data obtained from exhaled breaths was very accurate in classifying patients with suspected pulmonary thromboembolism.

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“…Other drawbacks to the use of the Enghoff equation include the requirement for a painful arterial blood gas stick, and the occurrence of negative values suggesting non-steady-state collection of end-tidal CO 2 and arterial blood pCO 2 (Kline et al, 2004). Prior work has provided concept framework suggesting that end-tidal CO 2 decreases and end-tidal O 2 increases in rats subjected to experimental PE, and in humans diagnosed with pulmonary thromboembolism (Paoletti et al, 1986;Jones et al, 2003). This project was designed to non-invasively measure the effect of high ventilation-perfusion relationships imparted by pulmonary thromboembolism by measuring the decrease without the need for arterial blood gas sampling.…”

Section: Discussionmentioning

confidence: 99%

Measurement of expired carbon dioxide, oxygen and volume in conjunction with pretest probability estimation as a method to diagnose and exclude pulmonary venous thromboembolism

Kline

Hogg

2006

Clin Physio Funct Imaging

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The assessment of gas exchange by automated analysis of O2 and CO2 alveolar to arterial differences

Cited by 5 publications

References 13 publications

Inhibition of prostaglandin synthesis during polystyrene microsphere-induced pulmonary embolism in the rat

Inhibition of prostaglandin synthesis during polystyrene microsphere-induced pulmonary embolism in the rat

Use of genetic programming to diagnose venous thromboembolism in the emergency department

Measurement of expired carbon dioxide, oxygen and volume in conjunction with pretest probability estimation as a method to diagnose and exclude pulmonary venous thromboembolism

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