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10.1245/s10434-007-9714-z
Annals of Surgical Oncology 15:1367-1374 (2008)
© 2008 Society of Surgical Oncology
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Original Article

Isolated Hypoxic Hepatic Perfusion with Retrograde Outflow in Patients with Irresectable Liver Metastases; A New Simplified Technique in Isolated Hepatic Perfusion

Cornelis Verhoef, MD1, Johannes H. W. deWilt, MD, PhD1, Flavia Brunstein, MD, PhD1, Andreas W. K. S. Marinelli, MD, PhD1, Boudewijn vanEtten, MD, PhD1, Maarten Vermaas, MD1, Gunther Guetens, PhD2, Gert de Boeck, PhD2, Ernst A. de Bruijn, PhD2 and Alexander M. M. Eggermont, MD, PhD1

1 Department of Surgical Oncology, Erasmus University Medical Centre—Daniel den Hoed Cancer Centre, PO Box 5201, 3008 AE, Rotterdam, The Netherlands
2 Laboratory of Experimental Oncology, University of Leuven—UZ Gasthuisberg, CDG building, Herestraat 49, B-3000, Leuven, Belgium

Correspondence: Address correspondence and reprint requests to: Cornelis Verhoef, MD; E-mail: c.verhoef{at}erasmusmc.nl

Background: Isolated hepatic perfusion with high-dose chemotherapy is a treatment option for patients with irresectable metastases confined to the liver. Prolonged local control and impact on survival have been claimed. Major drawbacks are magnitude and costs of the procedure. We developed an isolated hypoxic hepatic perfusion (IHHP) with retrograde outflow without the need for a heart-lung machine.

Patients and Methods: Twenty-four consecutive patients with irresectable metastases of various origins were treated. IHHP inflow was via the hepatic artery, outflow via the portal vein with occlusion of the retrohepatic caval vein. Radiolabeled albumine was used for leakage monitoring. Melphalan was used at 1–2 mg/kg. A 25-minute perfusion period was followed by a complete washout. Local and systemic melphalan concentrations were determined.

Results: Compared with oxygenated classical IHP, the IHPP procedure reduced operation time from >8 h to 4 hours, blood loss from >4000 to 900 cc and saved material and personnel costs. Leakage was 0% with negligible systemic toxicity and 0% perioperative mortality. Tumor response: complete response (CR) in 4%, partial response (PR) in 58%, and stable disease (SD) in 13%. Median time to progression was 9 months (2–24 months); pharmacokinetics demonstrated intrahepatic melphalan concentrations more than 9 fold higher than postperfusion systemic concentrations.

Conclusions: IHPP is a relatively simple procedure with reduced costs, reduced blood loss, no mortality, limited toxicity, and response rates comparable to classic IHP. The median duration of 9 months of tumor control should be improved. Hereto, vasoactive drugs, will be explored in further studies.

Key Words: Isolated hepatic perfusion • Retrograde outflow • Hypoxic • Metastasis • Melphalan







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