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Computer-based monitoring of global cardiovascular dynamics during acute pulmonary embolism and septic shock in swine

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Academic year: 2021

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Computer-based monitoring of global cardiovascular dynamics during acute pulmonary embolism and septic shock in swine

JA Revie1; DJ Stevenson1; JG Chase1; CE Hann1; BC Lambermont2; A Ghuysen2; P Kolh2; GM Shaw3; T Desaive3.

1: Univ of Canterbury, Christchurch, NZ 2: Univ of Liege, Belgium

3: Christchurch Hospital, Christchurch, NZ

Introduction: Acute pulmonary embolism (APE) and septic shock (SS) are highly prevalent dysfunctions in intensive care due to the immunocompromised and immobile state of ICU patients. This research retrospectively tests the ability of a computer-based method to monitor acute hemodynamic changes in pigs. If proven, this method could assist ICU staff by providing a clear physiological, patient-specific picture of cardiovascular status for diagnosis and decision support. Method: In 2 porcine studies, APE (N=5) and SS (N=4) were induced using autologous blood clots and endotoxin infusions. Hemodynamic measurements were recorded every 30 minutes for 4hrs (N=80). Subject-specific models of the cardiovascular system were identified from typical ICU measurements obtained from each of these data sets, including aortic and pulmonary artery pressure, stroke volume, heart rate, global end diastolic volume, and mitral and tricuspid valve closure times. Model outputs and identified parameters were compared to experimentally derived indices, measurements not used in the identification process, and known trends to validate the accuracy of the subject-specific models.

Results: Identified models accurately predicted maximum ventricular pressures and volumes, not used in the identification process, to mean percentage errors of 7.1% and 6.7% (less than measurement error ~10%). Mean modelled pulmonary vascular resistances (PVR) compared well (R2=0.81 for APE and R2=0.95 for SS) to experimentally derived values. Importantly, in the APE study a 91% rise from baseline in the mean PVR was identified with an 89% increase seen in the SS pigs. Contrasting behaviour between the two studies was observed for systemic vascular resistance (SVR) with a maximum drop of 40% from baseline recorded at T120 for SS, indicating a loss of vascular tone as expected, where at the same time in the APE study the average SVR had increased by 13%. An increase in the ratio of right to left ventricle end volume was identified in all 9 pigs, indicating right ventricular distension and a leftward shift in the intra-ventricular septum.

Conclusion: These results indicate that subject-specific CVS models are capable of tracking well known global hemodynamic trends of two common forms of shock in the ICU. The method shows potential and could provide a means for continuous cardiovascular monitoring at little extra cost as no extra measurements or expensive devices are required. However, further human trials are needed to validate this model-based approach.

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