Focused transhepatic electroporation mediated by hypersaline infusion through the portal vein in rat model. Preliminary results on differential conductivity

Author:

Pañella Clara1,Castellví Quim2,Moll Xavier3,Quesada Rita1,Villanueva Alberto4,Iglesias Mar5,Naranjo Dolores5,Sánchez-Velázquez Patricia1,Andaluz Anna3,Grande Luís1,Ivorra Antoni2,Burdío Fernando1

Affiliation:

1. General Surgery Department, Hospital del Mar Medical Research Institute (IMIM) , Universitat Pompeu Fabra , Barcelona , Spain

2. Department of Informatics and Communication Technologies , Universitat Pompeu Fabra , Barcelona , Spain

3. Department of Pathological Anatomy, Hospital del Mar Medical Research Insitute (IMIM) , Universitat Pompeu Fabra , Barcelona , Spain

4. Chemoresistance and Predictive Factors Group, Program Against Cancer Therapeutic Resistance (ProCURE), Catalan Institute of Oncology (ICO), Bellvitge Biomedical Research Institute (IDIBELL), Hospitalet de Llobregat , Barcelona , Spain

5. Medical and Surgery Animal Department, Faculty of Veterinary , Universitat Autònoma de Barcelona , Cerdanyola del Vallès Barcelona , Spain

Abstract

Abstract Background Spread hepatic tumours are not suitable for treatment either by surgery or conventional ablation methods. The aim of this study was to evaluate feasibility and safety of selectively increasing the healthy hepatic conductivity by the hypersaline infusion (HI) through the portal vein. We hypothesize this will allow simultaneous safe treatment of all nodules by irreversible electroporation (IRE) when applied in a transhepatic fashion. Material and methods Sprague Dawley (Group A, n = 10) and Athymic rats with implanted hepatic tumour (Group B, n = 8) were employed. HI was performed (NaCl 20%, 3.8 mL/Kg) by trans-splenic puncture. Deionized serum (40 mL/Kg) and furosemide (2 mL/Kg) were simultaneously infused through the jugular vein to compensate hypernatremia. Changes in conductivity were monitored in the hepatic and tumour tissue. The period in which hepatic conductivity was higher than tumour conductivity was defined as the therapeutic window (TW). Animals were monitored during 1-month follow-up. The animals were sacrificed and selective samples were used for histological analysis. Results The overall survival rate was 82.4% after the HI protocol. The mean maximum hepatic conductivity after HI was 2.7 and 3.5 times higher than the baseline value, in group A and B, respectively. The mean maximum hepatic conductivity after HI was 1.4 times higher than tumour tissue in group B creating a TW to implement selective IRE. Conclusions HI through the portal vein is safe when the hypersaline overload is compensated with deionized serum and it may provide a TW for focused IRE treatment on tumour nodules.

Publisher

Walter de Gruyter GmbH

Subject

Radiology, Nuclear Medicine and imaging,Oncology

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