The development of a clinically relevant canine model of postperfusion syndrome. Academic Article uri icon

abstract

  • Investigation into the complex etiology of the postperfusion syndrome (PPS) has been limited by access to only retrospective human case studies, and performance of animal studies that examine biochemical predictors of injury rather than the PPS itself. To determine whether a reproducible canine model of the clinical syndrome was possible, seven dogs underwent cardiopulmonary bypass (CPB) with a bubble oxygenator for 0 (n = 1, sham), 2 (n = 1), 4 (n = 1), and 6 (n = 4) hours. Arterial oxygenation, chest radiographs, serum creatinine, and total leukocyte and platelet counts continued to change through the second postoperative day, illustrating the need for prolonged follow-up (48 hours) to accurately detect postperfusion organ dysfunction. The dogs that did not undergo CPB for 6 hours (n = 3) did not develop important pulmonary dysfunction postoperatively, but three of the four dogs undergoing 6 hours of CPB developed profound, persistent, arterial hypoxemia associated with radiographic, histologic, and hemodynamic evidence of severe PPS. Early evidence of renal dysfunction was also apparent within 84 hours of 6 hour CPB. It is concluded that the canine long duration (6 hour) CPB model, with prolonged (48 hour) postoperative monitoring, generates a reproducible, clinically relevant model of human PPS.

published proceedings

  • ASAIO Trans

author list (cited authors)

  • Baldwin, R. T., Kadipasaoglu, K. A., Radovancevic, B., Gordon, L. L., Furusho, N., Matsuwaka, R., ... Clubb, F. J.

citation count

  • 1

complete list of authors

  • Baldwin, RT||Kadipasaoglu, KA||Radovancevic, B||Gordon, LL||Furusho, N||Matsuwaka, R||Conger, JL||Parnis, SM||Hare, WD||Clubb, FJ

publication date

  • July 1991