A swine model of pulmonary embolism with human-derived thrombi

Author:

Larco Jorge Luis Arturo1,Madhani Sarosh Irfan2,Liu Yang3,Abbasi Mehdi1,Shahid Adnan Hussain4,Yasin Omar Ziad5,Moreno Cristina6,Vadlamudi Venu7,Savastano Luis Emilio2

Affiliation:

1. Department of Radiology, Mayo Clinic, Rochester, United States,

2. Department of Neurosurgery, UCSF, San Francisco, United States,

3. Global Institute of Future Technology, Shanghai Jiao Tong University, Shanghai, China,

4. Department of Neurosurgery, PGIMER, Chandigarh, India,

5. Department of Internal Medicine, Mayo Clinic, Rochester, United States,

6. Department of Infectology, Hospital Metropolitano, Quito, Ecuador,

7. Endovascular Engineering, Menlo Park, United States,

Abstract

Objectives: The development and evaluation of percutaneous thrombectomy devices for pulmonary embolism (PE) pose a need for standardized large in vivo models with representative anatomical and physiological conditions and clots analogs. In this study, we present a swine model of PE model employing human-derived clot analogs. Material and Methods: Baseline angiographic and physiological pressure measurements were obtained in six adult Yorkshire pigs (45–65 kg) and results were benchmarked for interspecies comparison with published human data using fluoroscopic examinations, intra-arterial pressure measurements, and histologic studies. Then, clot analogs were created ex vivo employing banked human blood and a subset incubated in iodinated contrast for fluoroscopic visualization. Clot analogs were then embolized via a femoral venous access and angiographic/physiological consequences were evaluated. Results: The main, right, and left pulmonary artery diameters were 24 ± 1.1 mm, 16.5 ± 0.8 mm, and 12.6 ± 1.2 mm, respectively. The angle between the main pulmonary artery at the bifurcation point was approximately 90–95°. The clot analogs were heterogeneous and had increased fibrin content along the clot length. The overall composition was 96.63% red blood cell (RBC)/3.37% fibrin in the initial section, 48.85% RBC/51.15% fibrin in the intermediate section, and 3.44% RBC/96.56% fibrin in the final section. Embolization of the clot analogs resulted in distal occlusion of the right and left pulmonary arteries. Conclusions: This swine model coupled with clot analog is able to accurately mimic human anatomical and physiological conditions in PE making it feasible for the evaluation of pulmonary thrombectomy devices.

Publisher

Scientific Scholar

Subject

Computer Networks and Communications,Hardware and Architecture,Software

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