Combination of Alcohol and EVOH as a New Embolic Agent: Midterm Tissue and Inflammatory Effects in a Swine Model

Author:

Hak Jean-François123ORCID,Tradi Farouk123,Bobot Mickael345,Brige Pauline23,Habert Paul123ORCID,Chopinet Sophie236,Haffner Aurélie7,Soulez Gilles8,Guillet Benjamin359,Vidal Vincent123

Affiliation:

1. Diagnostic and Interventional Radiology Section, Department of Medical Imaging, University Hospital Timone APHM, 278 Rue Saint-Pierre, Marseille 13005, France

2. Aix-Marseille University, LIIE, Marseille, France

3. Aix-Marseille University, CERIMED, Marseille, France

4. Department of Nephrology, University Hospital Conception APHM, Marseille 13005, France

5. INSERM 1263, INRA 1260, C2VN, Aix Marseille University, Marseille 13005, Timone APHM, France

6. Department of Digestive Surgery, University Hospital Timone APHM, Marseille 13005, France

7. Department of Pathological Anatomy, University Hospital Timone APHM, Marseille 13005, France

8. Department of Radiology, Centre Hospitalier de L’Université de Montréal, Sherbrooke East, Montreal H2L 4M1, Montreal 1560, Canada

9. Department of Radiopharmacy, University Hospital Conception APHM, Marseille 13005, France

Abstract

Objective. To evaluate the vascular occlusion and midterm tissue toxicity properties of a combination of ethylene-vinyl alcohol (EVOH) (Squid 18®) (75%) and alcohol (25%)—Alco-Squid 18—in a swine model. Materials and Methods. Alco-Squid 18 (75% Squid 18® mixed with 25% alcohol) (AS18) was compared to embolization with 96% alcohol alone and to embolization with Squid 18® (S18®) alone. An arteriovenous malformation (AVM) model was created in group 1 (n = 2). Each AVM model was then embolized with AS18 or S18® alone with evaluation of a ratio between the volume of embolic agent divided by the volume of the AVM (evaluated by CT). For group 2 (n = 5), each agent was tested on three different kidneys (upper pole kidney artery). Pre- and postinterventional CTs, angiographies, blood alcohol content dosages, and histological studies (3 months postintervention) were performed. Results. AS18 has better distal distribution than S18® alone, both in the kidneys (mean capsule-S18® distance: 3.9 mm (±0.23) and mean capsule-AS18 distance: 2.3 mm (±0.11) ( p = 0.029 ) and in the AVM model. Histological exploration found a higher rate of tubular necrosis with AS18 compared with S18® alone and alcohol alone (3.78 ± 0.44 compared to 2.33 ± 1.22 p =  0 . 012 and 1.22 ± 0.67 p < 0 . 0001 ). The blood alcohol content was negligible in all cases. Conclusion. AS18 can suggest a better distal sclerotic and embolic character as compared with S18® alone without systemic toxicity.

Funder

Balt Extrusion

Publisher

Hindawi Limited

Subject

Radiology, Nuclear Medicine and imaging,Radiological and Ultrasound Technology

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