(Hepatology 2014;60:1674-1685.) Even if metastases tend
to occur late in the natural history of HCC, their presence radically changes the therapeutic options. Little is known about the molecular mechanisms underlying the HCC metastatic process. For other tumor types, it has been shown that cross-linking of collagen by lysyl oxidases favors colonization of potential metastatic sites. Wong et al. report increased expression of lysyl oxidase-like Selleck Roxadustat 2 (LOXL-2) in HCC samples, compared to nontumor tissues, and in the sera of patients with HCC, compared to the sera of those without HCC. In vitro, media from hepatocytes expressing LOXL2 favors invasion of bone marrow cells through Matrigel-coated transwell. Hepatic implantation of HCC cells expressing LOXL2 resulted in intra- and extrahepatic metastases. The investigators identified Fulvestrant cell line factors regulating the expression of LOXL2; among them, hypoxia increased the expression of LOXL2. This illuminating work has many implications, one of which is to suggest how transarterial chemoembolization (TACE), a major hypoxia inducer, may negatively affect tumor biology.
(Hepatology 2014;60:1645-1658.) Patients with intermediary-stage HCC are treated with TACE. This is a palliative treatment that may profit from combination with a systemic therapy. Evidence in support of this is lacking, at least with sorafenib. Kudo et al. report the results of a randomized, control trial testing brivanib in combination with TACE. When it came to light that the trials testing brivanib in first and second lines were negative, this third trial was stopped. Consequently, the results are based on only 32% of the required events, which represents a major limitation of this work. Nevertheless, patients receiving brivanib after the first TACE needed fewer TACE sessions and had a delayed time to extrahepatic spread or vascular invasion. Unfortunately, this did not translate into an improvement of overall
survival. The upshot of this is that we are left with a negative, terminated trial, and so, support for combination treatment with TACE is still lacking. (Hepatology 2014;60:1697-1707.) What has been the evolution in HCC stage at diagnosis and which treatments have been selected at the beginning of this century? Ulahannan et al. Y-27632 2HCl studied the cases identified in the Surveillance, Epidemiology, and End Results (SEER 18) cancer registries from January 2000 to December 2010. They assembled an impressive collection of more than 47,000 cases, which covers approximately 28% of the cases in the U.S. population. Until 2005, more tumors >5 cm were diagnosed, but, in the second half of the decade, more tumors ≤5 cm were diagnosed. In terms of treatment selection, 52% (at best) of the patients eligible for a curative option received it. Resection was the most common treatment over the years. Transplantation increased up to 2006 only.