Portal Vein Occlusion Prior to Extensive Resection in Colorectal Liver Metastasis: A Necessity Rather than an Option!

Abstract

Preoperative portal vein occlusion (PVO) of one liver lobe is regularly used for inducing liver hypertrophy of the contralateral lobe to prevent postoperative liver failure in patients with an anticipated insufficient future liver remnant (FLR) following resection. A similar rate of hypertrophy of the liver parenchyma with preserved portal flow can be obtained either by percutaneous portal embolization using several agents or by portal vein ligation. This strategy of preoperatively manipulating the liver volume has been acclaimed as a major step in liver surgery, paving the way for extensive resection for initially unresectable tumors. It has been clearly shown that chemotherapy of colorectal liver metastases (CRLM) can provide significant downstaging of liver disease enabling curative rescue resection and translating into an improved long-term survival. Over the last decade, both PVO and chemotherapy have dramatically widened the scope of surgical resection of CRLM. Several institutions involved in the surgical treatment of CRLM have claimed that preoperative PVO has increased the number of candidates for complete tumor resection. The hypertrophy of the FLR allows the safety of major resection. In the present issue, the article by Pamecha et al. tends to dampen the early enthusiasm regarding PVO for CLRM. This well-written article, which compares the surgical outcomes of two groups of patients operated for CRLM with or without portal vein embolization (PVE), highlights the unfavorable effects of PVE. Firstly, one-third of the patients were nonoperable after PVE because of rapid progression of disease, and secondly the long-term survival for patients resected after PVE was less favorable than for the group who underwent immediate surgery. A legitimate concern is whether the stimulus for liver regeneration induced by PVO might enhance tumor growth. As reported in a recent review of this journal, experimental studies have shown that hepatectomy or portal ligation in rats induced tumor growth and in some clinical studies, after PVO, the growth rate of liver metastasis seems to be more rapid than that of the liver parenchyma including a higher proliferative activity of intrahepatic metastasis possibly induced by hyper arterializations. Although these studies clearly demonstrate that tumor progression after PVO is possible, we believe that it is not yet time to consider a restriction of preoperative modulation of the liver parenchyma by PVO. Percutaneous embolization is a safe procedure that could reduce intrahepatic recurrence rate after right hepatectomy for unilobar CRLM. Several series have shown that in patients with extensive CRLM who would otherwise be unresectable, PVO followed by surgery offers a significant benefit with a 5-year survival up to 40%. In these studies the evidence of direct stimulation of tumor growth by PVE is circumstantial, and the rate of unresectability after PVE due to intrahepatic and/or extrahepatic tumor progression is regularly around 25%, which is not very different from the results of Pamecha et al. The main problem raised by this article is the indication of PVO and its association with chemotherapy before a major liver resection. The indication of PVO should depend on several factors including the extent and expected difficulties of resection, the status of nontumorous liver parenchyma, and the exact quantification of sufficient minimal functional hepatic volume. We have clearly demonstrated that a right hepatectomy, which is the main procedure performed after PVO, can be safely performed in patients with normal parenchyma. Therefore, except in patients with a FLR less than 25% of the total volume and Society of Surgical Oncology 2009