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Review

Hepatic Arterial Infusion Chemotherapy for Advanced Hepatocellular Carcinoma in Japan

Department of Gastroenterology and Hepatology, Osaka Red Cross Hospital, 5-30 Fudegasaki-cho, Tennoji-ku, Osaka 543-0027, Japan
*
Author to whom correspondence should be addressed.
Cancers 2012, 4(1), 165-183; https://doi.org/10.3390/cancers4010165
Submission received: 16 January 2012 / Revised: 8 February 2012 / Accepted: 16 February 2012 / Published: 21 February 2012

Abstract

:
Transcatheter methods such as transcatheter arterial chemoembolization (TACE) and hepatic arterial infusion chemotherapy (HAIC) have an important role in the treatment for advanced hepatocellular carcinoma (HCC). Recently, sorafenib, an inhibitor of tyrosine kinases, has been found to obtain survival benefits in patients with HCC, leading to major advances in the treatment of advanced HCC. However, it is associated with a low tumor response rate, minimal survival advantage, and high rates of adverse events. On the other hand, high rates of objective treatment response with HAIC for advanced HCC have been reported, although convincing evidence of it contributing to overall survival in HAIC has been lacking. In Japan, HAIC still tends to be the preferred method for the treatment of advanced HCC, even in patients with poor liver function. However, the choice of chemotherapeutic agents in TACE/HAIC for HCC varies between institutions. In this review, based on studies reported to date in the literature, we refer to current knowledge regarding the chemotherapeutic agents used for TACE/HAIC for HCC in Japan and consider the future perspectives for HAIC for this cancer.

1. Introduction

Hepatocellular carcinoma (HCC) is a problem worldwide, especially in Asian countries [1,2,3] Unlike most solid cancers, the incidence and mortality rates for HCC are projected to increase substantially in many countries over the next 20 years, mostly as a result of viral infections with hepatitis C and hepatitis B [4]. It has become possible to identify a group of patients with chronic liver disease who are at a high risk of developing HCC. In addition, improvements in diagnostic imaging have allowed early diagnosis of HCC. However, unfortunately, most HCC patients are first seen when the disease has reached an advanced stage at which curative treatment is no longer possible [4].
Potentially curative treatments for HCC include hepatic resection and liver transplantation [5,6]. Several non-surgical treatment options, including percutaneous ethanol injection, microwave coagulation, and radiofrequency ablation (RFA) have also been developed and are widely used for the treatment of HCC [4]. However, in general, these modalities are not indicated for patients with multiple tumors, invasion or thrombosis of major vessels, extrahepatic metastases, or poor liver function. Various anticancer agents have been employed for transcatheter arterial chemoembolization (TACE) and hepatic arterial infusion chemotherapy (HAIC) in these patients with advanced HCC, in whom effective chemotherapy is required.
Regarding systemic chemotherapy for advanced HCC, no agent has reproducibly shown a high response rate, and few chemotherapeutic regimens have a meaningful impact on patient survival, although numerous clinical trials have been performed to establish effective systemic treatment for patients with advanced HCC [7,8,9,10,11].
Sorafenib, an inhibitor of tyrosine kinases, was the first systemic chemotherapeutic agent found to improve the survival time of patients with advanced HCC, in the SHARP trial [12]. However, it is associated with a low tumor response rate, minimal survival advantage, and high rates of adverse events [12]. Moreover, because most patients enrolled in this study had Child–Pugh A cirrhosis with well-preserved liver function, the benefits and safety profile of sorafenib in advanced HCC patients with poor liver function such as Child–Pugh B/C cirrhosis or other poor prognostic factors remain unclear. Alternative approaches to the treatment of advanced HCC are needed, especially in patients with poor liver function.
Transcatheter arterial iodized oil chemoembolization has become established as an effective treatment for unresectable HCC. However, it is generally suitable only for patients with well-preserved liver function and multiple tumors without major vascular invasion [13,14]. HAIC is one of the few remaining options for advanced HCC patients with poor liver function [15]. In general, patients with HCC are less tolerant to chemotherapy than patients with other malignancies owing to poor liver function. In most HCC patients, pancytopenia may already be present because of concomitant liver cirrhosis, and myelosuppression and a bleeding tendency are likely to occur when performing chemotherapy. Owing to these clinical features of cirrhotic patients, HAIC is not commonly used for HCC in North America and Europe. However, in cases in which extrahepatic spread is minimal and local control of liver tumors is considered more important, HAIC is useful and may offer survival benefits, even when there are extrahepatic metastases. HAIC has often been used in these cases in Japan [16,17].
Compared with systemic chemotherapy, HAIC requires several technical procedures, including catheterization, and is associated with a risk of vascular disorders related to catheter placement and reservoir management [17]. However, it is a useful therapeutic modality because higher concentrations of the anticancer agent are obtained in the targeted tumor. The agent is administered directly into the liver via the hepatic artery, increasing the antitumor effect while being associated with a lower rate of incidence of systemic adverse events, and numerous clinical studies have reported that HAIC has moderate chemotherapeutic effect with favorable toxicity profiles in selected patients with advanced HCC [17]. However, there have been no large randomized studies and convincing clinical evidence is lacking for HAIC in advanced HCC. Therefore, HAIC is not yet a well-established treatment for advanced HCC, and its further investigation is required.
Several intra-arterial chemotherapy regimens, using doxorubicin, epirubicin, mitomycin C, 5-fluorouracil (5-FU), zinostatin stimalamer (SMANCS), cisplatin, miriplatin and oxaliplatin administered singly or in combination, have been reported as treatments for HCC. However, the optimal regimen for intra-arterial chemotherapy for HCC remains unknown. In this review, based primarily on clinical studies reported to date in the literature regarding transcatheter chemotherapeutic agents in HAIC for advanced HCC, we refer to current knowledge regarding the chemotherapeutic agents used in Japan for HCC and consider the future perspectives for hepatic arterial chemotherapy for this cancer.

2. Chemotherapeutic Agents

2.1. Doxorubicin

Doxorubicin (Adriacin; Kyowa Hakko Kogyo, Tokyo, Japan) is an anthracycline-based anticancer drug that had been conventionally used as a first-line therapy for HCC. In 1982, Hirose et al. reported that one shot of high-dose doxorubicin intra-arterial infusion therapy showed useful chemotherapeutic effects against HCC [18]. In 1994, Yasui et al. reported that of 86 patients with unresectable or recurrent HCC who underwent doxorubicin containing HAIC, 21 (34.4%) showed an objective response, and responders to doxorubicin containing HAIC achieved longer survival than non-responders [19]. In 1999, Tzoracoleftherakis et al. reported a randomized comparative study between HAIC with doxorubicin and systemic chemotherapy with doxorubicin involving 72 patients with unresectable (Stage IVA) HCC; patients who received HAIC with doxorubicin had a higher rate of objective and subjective remission and greater Karnofsky performance status improvement than did those in the systemic chemotherapy with doxorubicin group [20]. However, previous studies of systemic chemotherapy with doxorubicin had confirmed the minimal efficacy of this anticancer drug in HCC [9,10,11]. In Japan, doxorubicin is used for both HAIC and TACE in the treatment of advanced HCC [21].

2.2. Epirubicin

Epirubicin (Farmorubicin; Nihon Kayaku, Tokyo, Japan) is the 4-epimer of doxorubicin. It has a more favorable toxicity profile with less myelosuppression and cardiotoxicity than doxorubicin, and is routinely used for HCC. Because epirubicin easily undergoes glucuronidation, it is less toxic than doxorubicin. In 1986, the Japan Epirubicin Study Group for Hepatocellular Carcinoma reported that of 53 HCC patients who received HAIC with epirubicin, eight patients (15.1%) showed an objective response (complete response [CR] or partial response [PR]) [22]. Furthermore, a retrospective comparison with intra-arterial administration of doxorubicin showed that epirubicin was more effective than doxorubicin in terms of survival rate. Since then, epirubicin has been routinely used in HAIC for HCC in Japan [22]. Additional clinical trials have been performed in several faculties. Epirubicin alone or in combination with other chemotherapeutic agents such as mitomycin C or 5-FU has been used in HAIC for HCC in various Asian countries including Japan, with objective response rates ranging from 5% to 78% [22,23,24,25,26,27,28,29]. Reports of HAIC with anthracycline-based chemotherapeutic agents are listed in Table 1.
Table 1. Reports of HAIC with anthracycline-based chemotherapeutic agents for advanced hepatocellular carcinoma.
Table 1. Reports of HAIC with anthracycline-based chemotherapeutic agents for advanced hepatocellular carcinoma.
Authors (year) [ref.]CountryNumber of patientsAgentsCharacteristicsResponse rate (%)
Nagasue et al. (1986) [22]Japan53EpirubicinUnresectable15.1
Yoshikawa et al. (1994) [23]Japan17EpirubicinUnresectable12
Yasui et al. (1994) [19]Japan86Doxorubicin, MMC, 5-FUUnresectable34.4
Tzoracoleftherakis et al. (1999) [20]Greece72DoxorubicinUnresectable60
Hwang et al. (2005) [24]Korea18Epirubicin, MMC, 5-FUUnresectable38.9
Ikeda et al. (2007) [25]Japan45EpirubicinPV invasion9
Tanaka et al. (2008) [26]Japan20EpirubicinTAE refractory5
Ikushima et al. (2009) [27]Japan18EpirubicinUnresectable77.8
Kim et al. (2010) [30]Korea36DoxorubicinUnresectable16.7
HAIC: hepatic arterial infusion chemotherapy; MMC: mitomycin C; 5-FU: 5-fluorouracil; PV: portal vein; TAE: transcatheter arterial embolization.

2.3. Mitomycin C

Mitomycin C is an antineoplastic antibiotic isolated from the culture fluid of Streptomyces caespitosus. The objective response rate of intra-arterial chemotherapy with mitomycin C alone has been reported as 25% (9/36) [31]. However, this agent has recently been used in HAIC as a combination therapeutic agent. In Japan, mitomycin C alone has never been used in HAIC [21,24,32].

2.4. 5-FU

The pyrimidine antimetabolite 5-FU was the first reported chemotherapeutic agent used in the treatment of HCC. Monotherapy with intra-arterial 5-FU has a relatively low objective response rate, ranging from 13% to 22%, with a median survival of only 3.5 to 14 months [33,34]; therefore, 5-FU is often used in combination in HAIC for HCC.
Combined therapy comprising intra-arterial infusion of 5-FU and systemic interferon-α (IFN-α) (FAIT) has been reported to be useful as a palliative treatment for HCC patients with major vascular invasion, although monotherapy with IFN-α had minimal objective response rate against HCC [35,36,37]. In 2002, Sakon et al. reported that of 11 advanced HCC patients with portal vein tumor thrombus (PVTT), eight patients (73%) showed an objective response to FAIT [38]. In 2006, Obi et al. reported that in 116 advanced HCC patients with PVTT who received FAIT, 19 (16%) showed a CR and another 42 (36%) showed a PR; adverse events were limited to nausea and appetite loss, and the overall survival rates at 1 and 2 years were 34% and 18%, respectively [39]. In 2011, Nagano et al. reported that of 102 HCC patients with PVTT, 40 (39.2%) showed an objective response to FAIT, and no major treatment-related complications were noted [40]. In 2006, Kondo et al. reported that a combination of 5-FU and IFN-α strongly inhibited the growth of human HCC cells, and suggested that the effects of this combination therapy may be attributable to changes in the induction of apoptosis through IFN-α/β receptors [41]. In 2009, Kasai et al. reported that intra-arterial 5-FU and systemic pegylated (PEG)-IFN-α2b combination therapy for advanced HCC had an objective response rate of 71.4% [42]. In 1999, Yano et al. compared the in vivo antitumor effects of PEG-IFN-α2b and IFN-α in nude mice injected with cultured HCC cells, and found that PEG-IFN-α2b induced apoptosis more strongly than IFN-α [43]. Intra-arterial 5-FU infusion and systemic PEG-IFN-α2b combination therapy appears to be highly promising, although further prospective studies are required [42,44]. Reports of the use of HAIC with 5-FU combined with systemic IFN in advanced HCC are listed in Table 2.
Table 2. Reports of hepatic arterial infusion chemotherapy with 5-FU combined with systemic interferon for advanced hepatocellular carcinoma.
Table 2. Reports of hepatic arterial infusion chemotherapy with 5-FU combined with systemic interferon for advanced hepatocellular carcinoma.
Authors (year) [ref.]CountryNumber of patientsCharacteristicsIFNResponse rate (%)
Sakon et al. (2002) [38]Japan8PV invasionIFN-α62.5
Enjoji et al. (2005) [45]Japan28PV invasion or unresectableIFN-α21.5
Ota et al. (2005) [46]Japan55PV invasionIFN-α43.6
Obi et al. (2006) [39]Japan116PV invasionIFN-α52.5
Uka et al. (2007) [47]Japan31PV invasionIFN-α29.1
Kuroda et al. (2007) [48]Japan10PV invasionIFN-α10
Katamura et al. (2009) [49]Japan16PV invasionIFN-α25
Kasai et al. (2009) [44]Japan9PV invasionPeg-IFN α2b77.8
Kasai et al. (2011) [42]Japan21PV invasionPeg-IFN α2b71.4
Nagano et al. (2011) [40]Japan102PV invasionIFN-α39.2
IFN: interferon; PV: portal vein; Peg-IFN: pegylated interferon.
Low-dose cisplatin (CDDP) combined with 5-FU (low-dose FP therapy) has synergistic effects. This combination is often used in the treatment of gastrointestinal tract malignancies. In combination with 5-FU, cisplatin is a modulator rather than an effector, and increases the antitumor efficacy of 5-FU by increasing the intracellular concentration of reduced folate [37,50]. In 2002, Ando et al. reported that of 48 HCC patients with PVTT, 23 (48.0%) showed an objective response to low-dose FP therapy and concluded that HAIC using low-dose FP might be a useful therapeutic option for patients with advanced HCC with PVTT [51]. In 2010, Ueshima et al. reported that of 52 advanced HCC patients, 20 (38.5%) showed an objective response to low-dose FP therapy [52]. However, there are few reports of favorable objective response rates with the use of high-dose CDDP combined with 5-FU therapy for the treatment of advanced HCC [53,54,55]. Reports of intra-arterial 5-FU and CDDP combination therapy in HAIC are listed in Table 3.
Table 3. Reports of hepatic arterial infusion chemotherapy with 5-FU and CDDP for advanced hepatocellular carcinoma.
Table 3. Reports of hepatic arterial infusion chemotherapy with 5-FU and CDDP for advanced hepatocellular carcinoma.
Author (year) [ref.]CountryNumber of patientsCharacteristicsDoseResponse rate (%)
Ando et al. (2002) [51]Japan48PV invasionLow48
Itamoto et al. (2002) [56]Japan7PV invasionLow33
Lai et al. (2003) [57]China18PV invasionLow33
Sumie et al. (2003) [58]Japan16PV invasionLow56.3
Yamasaki et al. (2005) [59]Japan15UnresectableLow20
Park et al. (2007) [54]Korea41UnresectableHigh22
Kim et al. (2010) [53]Korea36UnresectableHigh16.7
Ueshima et al. (2010) [52]Japan52PV invasion or unresectableLow38.5
Woo et al. (2010) [55]Korea32PV invasionLow0
Woo et al. (2010) [55]Korea36PV invasionHigh16.7
PV: portal vein.

2.5. CDDP

Clinical investigation of cisplatin (cis-diamminedichloroplatinum; CDDP) had been started in 1972. The usefulness of CDDP as an anticancer agent was first confirmed in the treatment of urinary tract cancers. Currently, CDDP is a key chemotherapeutic agent for the treatment of various cancers, including tumors of the respiratory, genitourinary, and digestive systems [60]. The anticancer effect of CDDP is characterized by both time-dependent and concentration-dependent features.
The response rate of CDDP monotherapy administered by HAIC for advanced HCC ranges from 14% to 42% [61,62,63,64]. Reported objective response rates to arterial infusion regimens containing CDDP, such as low-dose FP therapy, range from 0% to 56%, although high efficacy of systemic chemotherapy with CDDP has not been reported in HCC [17,51,52,53,65,66,67,68,69,70,71].
Microfine powder CDDP preparations (DDP-H) (IA-call; Nippon Kayaku Co., Ltd., Japan) for arterial infusion were approved for its use in Japan in 2004. Recently in Japan, favorable results have been obtained using DDP-H in the treatment of advanced HCC patients. In 2008, Yoshikawa et al. conducted a phase II study in advanced HCC patients, reporting that in 80 patients who received HAIC with DDP-H, the overall response rate was 33.8%, the 1-year and the 2-year survival rates were 67.5% and 50.8%; respectively, they concluded that DDP-H has higher antitumor effect than other anticancer drugs when administered by HAIC [62]. The usefulness of DDP-H as a second-line treatment for advanced HCC refractory to TACE using an epirubicin-lipiodol emulsion has also been reported [72,73].
Systemic combination therapy with S-1 and CDDP is a promising treatment for advanced HCC. In 2010, Katamura et al. reported that of 16 HCC patients with extrahepatic metastases who received S-1 and CDDP combination therapy, two (13%), none (0%), five (31%), and nine (56%) showed CR, PR, stable disease, and progressive disease, respectively, with an overall objective response rate of 13% (2/16) and an overall survival rate at 1 year of 77% [74].
There is one report that RFA with sequential HAIC using cisplatin contributed to a longer disease-free interval [16]. HAIC using cisplatin before RFA might prevent an increase in the size of pre-existing microscopic tumor foci.

2.6. SMANCS

SMANCS is a lipophilic intra-arterial chemotherapeutic agent for HCC. In 1983, Konno et al. reported a reduction in tumor size and tumor markers in 13 of 14 patients with HCC following arterial infusion of SMANCS-lipiodol emulsion [75]. A subsequent study of 124 patients with HCC or metastatic liver tumors showed significantly higher survival rate following infusion of a SMANCS-lipiodol emulsion [76].
In 2002, Okusaka et al. reported a phase II study of TACE using SMANCS in which the overall response rate was 32% (16/50); they concluded that TACE using SMANCS, which was well tolerated, might be a useful treatment for advanced HCC [77]. However, hepatic arterial infusion with SMANCS caused severe vascular endothelial damage and loss of the hepatic artery for infusion [77,78]. SMANCS is thus unsuitable for repeated TACE/HAIC in HCC and is not widely used for this purpose in Japan.

2.7. Miriplatin

Miriplatin (Miripla; Dainippon Sumitomo Co., Ltd., Tokyo, Japan), a cisplatin derivative, is a novel chemotherapeutic agent designed for use in transarterial infusion chemotherapy for HCC [79]. Miriplatin: (1) inhibits cell proliferation in a similar manner to cisplatin and has superior solubility in ethyl esters of iodized fatty acids derived from poppy seed oil; (2) releases its platinum constituent continuously, together with the ethyl esters (sustained release), by remaining at the site of the tumor; and (3) has fewer adverse effects, because of its sustained release and its minimal presence in the general circulation [80,81,82,83]. In Japan, miriplatin was approved for use in October 2009.
In 2004, Okusaka et al. conducted a phase II study of miriplatin to assess its antitumor effect and toxicity in treatment-naive patients with HCC. They reported that the CR rate was 56% (9/16) and that none of the patients exhibited grade 4 toxicity or episodes of renal dysfunction, and concluded that miriplatin was well tolerated and showed promising antitumor effect in patients with HCC [84]. In 2011, Okusaka et al. reported their phase II comparative study of miriplatin and SMANCS, in which HAIC with miriplatin had a similar efficacy to HAIC with SMANCS, and repeated dosing with miriplatin was possible without hepatic vascular injury in cases of relapse, whereas HAIC with SMANCS caused hepatic vascular injury [78]. In 2011, Imai et al. reported that in 162 unresectable HCC patients who underwent transcatheter arterial chemotherapy using miriplatin with or without embolization, the objective response rates to HAIC with miriplatin and TACE with miriplatin were 33% (13/40) and 57% (70/120), respectively; they concluded that an objective response was achieved in a significantly higher number of patients treated with TACE with miriplatin than with HAIC with miriplatin [85].
It is well known that HAIC with CDDP causes renal dysfunction [86]. However, in 2011, Imai et al. reported that HAIC with miriplatin could be used safely in HCC patients with chronic renal failure, probably owing to its minimal presence in the general circulation [87]. In terms of renal toxicity, HAIC with miriplatin is considered safer than HAIC with CDDP.
In an animal experiment comparing the antitumor effects of two platinum agents (miriplatin and DDP-H), Watanabe et al. reported no significant difference between miriplatin-lipiodol emulsion and DDP-H-lipiodol emulsion after 7 days post-administration [88]. To date, however, there is no convincing clinical evidence regarding the antitumor effects of these drugs. In Japan, several clinical studies comparing the antitumor effects of miriplatin and other chemotherapeutic agents such as CDDP and epirubicin for advanced HCC are ongoing. If the results for miriplatin are positive in these studies, it will become a key chemotherapeutic drug in the treatment of unresectable HCC.

2.8. Oxaliplatin

The platinum-based chemotherapeutic agent oxaliplatin (L-OHP) displays a wide range of antitumor activities [89]. Oxaliplatin has often been used for the treatment of advanced colorectal cancer, in which its effectiveness has been confirmed in many clinical studies [90]. To date, however, few detailed clinical data are available concerning the effects of HAIC with oxaliplatin in advanced HCC. In Japan, oxaliplatin has not been used for the treatment of advanced HCC. In 2010, Rathore et al. reported that in their phase I trial, HAIC with oxaliplatin was feasible, well tolerated, and had demonstrated activity in patients with advanced HCC [91]. A phase II prospective randomized study of the effectiveness of HAIC with oxaliplatin in unresectable HCC is underway. If positive results are obtained, oxaliplatin could become a key chemotherapeutic agent in the treatment of advanced HCC.

3. Discussion

There are four main reasons why HAIC may be well suitable for the treatment of advanced HCC compared with systemic chemotherapy. First, because HCC derives almost all of its blood supply from the hepatic artery, high anticancer drug concentrations can be obtained while hepatic perfusion is maintained via the portal vein [17,92,93]. Second, normal hepatic tissue metabolizes various agents, such that first pass metabolism leads to higher local drug concentrations in the liver, reducing systemic adverse effects [17,93]. Third, prolonged drug exposure, which may increase the antitumor effect, is easily obtained with HAIC [17,93]. Fourth, unlike other locoregional therapies for HCC, HAIC is not limited by tumor size, tumor number, or proximity to major vascular structures, all of which preclude surgical resection or RFA in general.
There are two methods for administration of HAIC: one-shot hepatic arterial infusion and continuous hepatic arterial infusion. In one-shot hepatic arterial infusion, concentration-dependent agents such as anthracycline-based agents, mitomycin C, CDDP, and miriplatin are suitable for HAIC. In continuous hepatic arterial infusion, 5-FU, which exerts its antitumor effects time-dependently, anthracycline-based agents, mitomycin C, and intermittent administration of CDDP based on the concept of biochemical modulation are suitable for HAIC. In continuous hepatic arterial infusion, an implantable port system is required. Several recent studies indicate that probably owing to technical improvements of angiographic procedure, only 0–4% of patients develop catheter-related complications such as breakage of the reservoir device, catheter dislocation, artery dissection, artery occlusion, subcutaneous hematoma, and infection [38,56]. Therefore, HAIC using an implantable port system can be performed safely.
In general, HCC responds poorly to chemotherapy. The possible explanations are tumor heterogeneity, inducible overexpression of the multidrug resistance gene, and/or inherent resistance due to an unknown mechanism [94,95,96,97]. Combination therapy is therefore considered to be more effective than monotherapy. Synergistic cooperative effects have been observed in experiments on HCC cell lines [96].
In sorafenib treatment for advanced HCC, as mentioned above, because most patients enrolled in the SHARP trial had Child–Pugh A cirrhosis with well-preserved liver function, the benefits and safety profile of sorafenib in advanced HCC patients with Child–Pugh B/C or other poor prognostic factors remains unclear [12]. However, even patients with poor performance status or reduced hepatic functional reserve could be eligible for HAIC. Indeed, as shown in Table 2 and Table 3, many studies of HAIC have focused on HCC patients with PVTT. Moreover, the objective response rate of sorafenib treatment is low in general. In the SHARP trial, it was very low (CR and PR were 0% and 2%, respectively) [12]. In Japan, however, there have been many reports of high rates of response to HAIC in advanced HCC, although most of these studies were not randomized and few demonstrated any survival benefit using controls. The clinical response reflects the survival benefits [14,37,38,39,52,98,99]. Probably, chemosensitive subgroups of patients with advanced HCC are present, and it is therefore important to identify optimal candidates for HAIC as well as to investigate novel therapeutic strategies. A novel method using gene expression profiling has recently been reported for the prediction of treatment response in advanced HCC [100]. In practice, however, responders and non-responders should be distinguishable after the first session of HAIC by evaluating tumor size using imaging modalities and the levels of tumor markers. In early non-responders, HAIC should not be continued; instead, different therapeutic options, including sorafenib, should be explored. We have experience of a case of advanced HCC with PVTT refractory to epirubicin that showed a marked decrease in tumor markers after HAIC with miriplatin [101].

4. Future Perspectives

The favorable objective response rate reported for HAIC in advanced HCC in Japan provides a sound basis for its clinical use. In the era of molecular targeted anticancer therapies such as sorafenib, incorporating such agents into HAIC regimens may obtain further improvement of treatment effect. However, the effects of combination therapy of sorafenib and HAIC are unclear. According to a subgroup analysis of the SHARP trial, it is speculated that sorafenib in combination with resection, ablation, TACE or HAIC will prolong overall survival in various stages of HCC [12,102]. There are several case reports showing a favorable response of advanced HCC to combination therapy with sorafenib and HAIC [103,104], although in 2011 Kemeny et al. reported that in 22 primary liver cancer patients, addition of systemic bevacizumab to HAI floxuridine/dexamethasone appeared to increase biliary toxicity without any clear improvement in outcome [105]. To elucidate this issue, a randomized clinical trial of sorafenib alone versus sorafenib combined with maintenance TACE/HAIC and/or HAIC in intermediate and advanced HCC was initiated in Japan in 2009 [102]. If favorable results are obtained by these trials, the treatment strategy for HCC will be drastically changed.

5. Conclusions

As shown in Table 1, Table 2, and Table 3, many clinical studies with favorable response rates for HAIC in advanced HCC have been reported in Japan, and the improvement of survival can be ascribed to treatment-related effects. We believe that HAIC as well as sorafenib should be considered an effective treatment for advanced HCC.

Conflict of Interests

The authors declare that they have no conflicts of interest. In addition, none of the authors had any financial relationship (within the past 12 months) with a biotechnology manufacturer, a pharmaceutical company, or other commercial entity that has any interest in the subject matter, materials, or processes discussed in the manuscript.

References

  1. Curley, S.A.; Izzo, F.; Ellis, L.M.; Nicolas Vauthey, J.; Vallone, P. Radiofrequency ablation of hepatocellular carcinoma in 110 patients with cirrhosis. Ann. Surg. 2000, 232, 1694–1702. [Google Scholar]
  2. Allgaier, H.P.; Deibert, P.; Zuber, I.; Olschewski, M.; Blum, H.E. Percutaneous radiofrequency interstitial thermal ablation of small hepatocellular carcinoma. Lancet 1999, 353, 1676–1677. [Google Scholar]
  3. Okuda, K. Hepatocellular carcinoma: Recent progress. Hepatology 1992, 15, 948–963. [Google Scholar] [CrossRef]
  4. Lencioni, R. Loco-regional treatment of hepatocellular carcinoma. Hepatology 2010, 52, 762–773. [Google Scholar] [CrossRef]
  5. Lai, E.C.; Lau, W.Y. The continuing challenge of hepatic cancer in Asia. Surgeon 2005, 3, 210–215. [Google Scholar] [CrossRef]
  6. Lau, W.Y.; Leung, T.W.; Yu, S.C.; Ho, S.K. Percutaneous local ablative therapy for hepatocellular carcinoma: A review and look into the future. Ann. Surg. 2003, 237, 171–179. [Google Scholar]
  7. Boucher, E.; Corbinais, S.; Brissot, P.; Boudjema, K.; Raoul, J.L. Treatment of hepatocellular carcinoma (HCC) with systemic chemotherapy combining epirubicin, cisplatinum and infusional 5-fluorouracil (ECF regimen). Cancer Chemother. Pharmacol. 2002, 50, 305–308. [Google Scholar] [CrossRef]
  8. Okusaka, T.; Ueno, H.; Ikeda, M. Chemotherapy for hepatocellular carcinoma [in Japanese]. Gan To Kagaku Ryoho 2004, 31, 2122–2128. [Google Scholar]
  9. Yeo, W.; Mok, T.S.; Zee, B.; Leung, T.W.; Lai, P.B.; Lau, W.Y.; Koh, J.; Mo, F.K.; Yu, S.C.; Chan, A.T.; et al. A randomized phase III study of doxorubicin versus cisplatin/interferon alpha-2b/doxorubicin/fluorouracil (PIAF) combination chemotherapy for unresectable hepatocellular carcinoma. J. Natl. Cancer Inst. 2005, 97, 1532–1538. [Google Scholar] [CrossRef]
  10. Gish, R.G.; Porta, C.; Lazar, L.; Ruff, P.; Feld, R.; Croitoru, A.; Feun, L.; Jeziorski, K.; Leighton, J.; Gallo, J.; Kennealey, G.T. Phase III randomized controlled trial comparing the survival of patients with unresectable hepatocellular carcinoma treated with nolatrexed or doxorubicin. J. Clin. Oncol. 2007, 25, 3069–3075. [Google Scholar]
  11. Edeline, J.; Raoul, J.L.; Vauleon, E.; Guillygomac’h, A.; Boudjema, K.; Boucher, E. Systemic chemotherapy for hepatocellular carcinoma in non-cirrhotic liver: A retrospective study. World J. Gastroenterol. 2009, 15, 713–716. [Google Scholar]
  12. Llovet, J.M.; Ricci, S.; Mazzaferro, V.; Hilgard, P.; Gane, E.; Blanc, J.F.; de Oliveira, A.C.; Santoro, A.; Raoul, J.L.; Forner, A.; et al. SHARP Investigators Study Group. Sorafenib in advanced hepatocellular carcinoma. N. Engl. J. Med. 2008, 359, 378–390. [Google Scholar] [CrossRef]
  13. Llovet, J.M.; Bruix, J. Systematic review of randomized trials for unresectable hepatocellular carcinoma: Chemoembolization improves survival. Hepatology 2003, 37, 429–442. [Google Scholar] [CrossRef]
  14. Llovet, J.M.; Real, M.I.; Montaña, X.; Planas, R.; Coll, S.; Aponte, J.; Ayuso, C.; Sala, M.; Muchart, J.; Solà, R.; et al. Barcelona Liver Cancer Group. Arterial embolisation or chemoembolisation versus symptomatic treatment in patients with unresectable hepatocellular carcinoma: A randomised controlled trial. Lancet 2002, 359, 1734–1739. [Google Scholar]
  15. Nagai, H.; Sumino, Y. Therapeutic strategy of advanced hepatocellular carcinoma by using combined intra-arterial chemotherapy. Recent Pat. Anticancer Drug Discov. 2008, 3, 220–226. [Google Scholar] [CrossRef]
  16. Ishikawa, T.; Higuchi, K.; Kubota, T.; Seki, K.; Honma, T.; Yoshida, T.; Kamimura, T. Prevention of intrahepatic distant recurrence by transcatheter arterial infusion chemotherapy with platinum agents for stage I/II hepatocellular carcinoma. Cancer 2011, 117, 4018–4025. [Google Scholar] [CrossRef]
  17. Ishikawa, T. Future perspectives on the treatment of hepatocellular carcinoma with cisplatin. World J. Hepatol. 2009, 1, 8–16. [Google Scholar] [CrossRef]
  18. Hirose, H.; Aoyama, M.; Oshima, K.; Udo, K.; Kobayashi, S.; Adachi, N.; Nonaka, T.; Yamada, T. Chemotherapy of hepatocellular carcinoma—With special reference to one-shot intra-arterial infusion of a high dose of adriamycin (in Japanese). Gan To Kagaku Ryoho 1982, 9, 2216–2221. [Google Scholar]
  19. Yasui, M.; Nonami, T.; Kurokawa, T.; Nakao, A.; Harada, A.; Hashimoto, S.; Kajikawa, M.; Hiraoka, E.; Takagi, H. Effects of hepatic arterial infusion chemotherapy on unresectable or recurrent hepatocellular carcinoma. Cancer Chemother. Pharmacol. 1994, 33, S139–S141. [Google Scholar] [CrossRef]
  20. Tzoracoleftherakis, E.E.; Spiliotis, J.D.; Kyriakopoulou, T.; Kakkos, S.K. Intra-arterial versus systemic chemotherapy for non-operable hepatocellular carcinoma. Hepatogastroenterology 1999, 46, 1122–1125. [Google Scholar]
  21. Osuga, K.; Murakami, T.; Nakata, S.; Tomoda, K.; Nagano, H.; Monden, M.; Nakamura, H. Hepatic arterial infusion chemotherapy (HAIC)—Hepatocellular carcinoma (in Japanese). Gan To Kagaku Ryoho 2004, 31, 2114–2117. [Google Scholar]
  22. Ando, K.; Hirai, K.; Kubo, Y. Intra-arterial administration of epirubicin in the treatment of nonresectable hepatocellular carcinoma. Cancer Chemother. Pharmacol. 1987, 19, 183–188. [Google Scholar]
  23. Yoshikawa, M.; Saisho, H.; Ebara, M.; Iijima, T.; Iwama, S.; Endo, F.; Kimura, M.; Shimamura, Y.; Suzuki, Y.; Nakano, T. A randomized trial of intrahepatic arterial infusion of 4'-epidoxorubicin with Lipiodol versus 4'-epidoxorubicin alone in the treatment of hepatocellular carcinoma. Cancer Chemother. Pharmacol. 1994, 33, S149–S152. [Google Scholar] [CrossRef]
  24. Hwang, J.Y.; Jang, B.K.; Kwon, K.M.; Chung, W.J.; Park, K.S.; Cho, K.B.; Hwang, J.S.; Ahn, S.H.; Kim, G.C.; Kim, Y.H.; et al. Efficacy of hepatic arterial infusion therapy for advanced hepatocellular carcinoma using 5-fluorouracil, epirubicin and mitomycin-C (in Korean). Korean J. Gastroenterol. 2005, 45, 118–124. [Google Scholar]
  25. Ikeda, M.; Okusaka, T.; Ueno, H.; Morizane, C.; Iwasa, S.; Hagihara, A.; Kojima, Y. Hepatic arterial infusion chemotherapy with epirubicin in patients with advanced hepatocellular carcinoma and portal vein tumor thrombosis. Oncology 2007, 72, 188–193. [Google Scholar] [CrossRef]
  26. Tanaka, T.; Ikeda, M.; Okusaka, T.; Ueno, H.; Morizane, C.; Ogura, T.; Hagihara, A.; Iwasa, S. A phase II trial of transcatheter arterial infusion chemotherapy with an epirubicin-Lipiodol emulsion for advanced hepatocellular carcinoma refractory to transcatheter arterial embolization. Cancer Chemother. Pharmacol. 2008, 61, 683–688. [Google Scholar]
  27. Ikushima, I.; Higashi, S.; Seguchi, K.; Ishii, A.; Ota, Y.; Shima, M.; Kanemaru, M.; Hidaka, Y. Transarterial infusion chemotherapy with epirubicin in water-in-oil-in-water emulsion for recurrent hepatocellular carcinoma in the residual liver after hepatectomy. Eur. J. Radiol. 2009, 69, 114–119. [Google Scholar]
  28. Sahara, S.; Kawai, N.; Sato, M.; Minamiguchi, H.; Nakai, M.; Takasaka, I.; Nakata, K.; Ikoma, A.; Sawa, N.; Sonomura, T.; et al. Prospective comparison of transcatheter arterial chemoembolization with Lipiodol-epirubicin and Lipiodol-cisplatin for treatment of recurrent hepatocellular carcinoma. Jpn. J. Radiol. 2010, 28, 362–368. [Google Scholar] [CrossRef]
  29. Yamanaka, K.; Hatano, E.; Narita, M.; Taura, K.; Yasuchika, K.; Nitta, T.; Arizono, S.; Isoda, H.; Shibata, T.; Ikai, I.; et al. Comparative study of cisplatin and epirubicin in transcatheter arterial chemoembolization for hepatocellular carcinoma. Hepatol. Res. 2011, 41, 303–309. [Google Scholar] [CrossRef]
  30. Kim, H.Y.; Kim, J.D.; Bae, S.H.; Park, J.Y.; Han, K.H.; Woo, H.Y.; Choi, J.Y.; Yoon, S.K.; Jang, B.K.; Hwang, J.S.; et al. Korean Liver Cancer Study Group. A comparative study of high-dose hepatic arterial infusion chemotherapy and transarterial chemoembolization using doxorubicin for intractable, advanced hepatocellular carcinoma. Korean J. Hepatol. 2010, 16, 355–361. [Google Scholar] [CrossRef]
  31. Mäkelä, J.T.; Kantola, R.; Kairaluoma, M.I. Superselective intra-arterial chemotherapy with mitomycin C for hepatocellular carcinoma. Surg. Oncol. 1993, 2, 99–104. [Google Scholar] [CrossRef]
  32. Lu, W.; Li, Y.H.; Yu, Z.J.; He, X.F.; Chen, Y.; Zhao, J.B.; Zhu, Z.Y. A comparative study of damage to liver function after TACE with use of low-dose versus conventional-dose of anticancer drugs in hepatocellular carcinoma. Hepatogastroenterology 2007, 54, 1499–1502. [Google Scholar]
  33. Doci, R.; Bignami, P.; Bozzetti, F.; Bonfanti, G.; Audisio, R.; Colombo, M.; Gennari, L. Intrahepatic chemotherapy for unresectable hepatocellular carcinoma. Cancer 1988, 61, 1983–1987. [Google Scholar]
  34. Iwamiya, T.; Sawada, S.; Ohta, Y. Repeated arterial infusion chemotherapy for inoperable hepatocellular carcinoma using an implantable drug delivery system. Cancer Chemother. Pharmacol. 1994, 33, S134–S138. [Google Scholar] [CrossRef]
  35. Patt, Y.Z.; Hassan, M.M.; Lozano, R.D.; Brown, T.D.; Vauthey, J.N.; Curley, S.A.; Ellis, L.M. Phase II trial of systemic continuous fluorouracil and subcutaneous recombinant interferon alpha-2b for treatment of hepatocellular carcinoma. J. Clin. Oncol. 2003, 21, 421–427. [Google Scholar] [CrossRef]
  36. Llovet, J.M.; Sala, M.; Castells, L.; Suarez, Y.; Vilana, R.; Bianchi, L.; Ayuso, C.; Vargas, V.; Rodés, J.; Bruix, J. Randomized controlled trial of interferon treatment for advanced hepatocellular carcinoma. Hepatology 2000, 31, 54–58. [Google Scholar] [CrossRef]
  37. Lai, Y.C.; Shih, C.Y.; Jeng, C.M.; Yang, S.S.; Hu, J.T.; Sung, Y.C.; Liu, H.T.; Hou, S.M.; Wu, C.H.; Chen, T.K. Hepatic arterial infusion chemotherapy for hepatocellular carcinoma with portal vein tumor thrombosis. World J. Gastroenterol. 2003, 9, 2666–2670. [Google Scholar]
  38. Sakon, M.; Nagano, H.; Dono, K.; Nakamori, S.; Umeshita, K.; Yamada, A.; Kawata, S.; Imai, Y.; Iijima, S.; Monden, M. Combined intraarterial 5-fluorouracil and subcutaneous interferon-alpha therapy for advanced hepatocellular carcinoma with tumor thrombi in the major portal branches. Cancer 2002, 94, 435–442. [Google Scholar]
  39. Obi, S.; Yoshida, H.; Toune, R.; Unuma, T.; Kanda, M.; Sato, S.; Tateishi, R.; Teratani, T.; Shiina, S.; Omata, M. Combination therapy of intraarterial 5-fluorouracil and systemic interferon-alpha for advanced hepatocellular carcinoma with portal venous invasion. Cancer 2006, 106, 1990–1997. [Google Scholar] [CrossRef]
  40. Nagano, H.; Wada, H.; Kobayashi, S.; Marubashi, S.; Eguchi, H.; Tanemura, M.; Tomimaru, Y.; Osuga, K.; Umeshita, K.; Doki, Y.; et al. Long-term outcome of combined interferon-α and 5-fluorouracil treatment for advanced hepatocellular carcinoma with major portal vein thrombosis. Oncology 2011, 80, 63–69. [Google Scholar] [CrossRef]
  41. Kondo, M.; Nagano, H.; Wada, H.; Damdinsuren, B.; Yamamoto, H.; Hiraoka, N.; Eguchi, H.; Miyamoto, A.; Yamamoto, T.; Ota, H.; et al. Combination of IFN-α and 5-fluorouracil induces apoptosis through IFN-α/β receptor in human hepatocellular cells. Clin. Cancer Res. 2005, 11, 1277–1286. [Google Scholar]
  42. Kasai, K.; Ushio, A.; Kasai, Y.; Sawara, K.; Miyamoto, Y.; Oikawa, K.; Kuroda, H.; Takikawa, Y.; Suzuki, K. Combination therapy of intra-arterial 5-fluorouracil and systemic pegylated interferon α-2b for advanced hepatocellular carcinoma. Int J. Clin. Oncol. 2011, 16, 221–229. [Google Scholar] [CrossRef]
  43. Yano, H.; Iemura, A.; Haramaki, M.; Ogasawara, S.; Takayama, A.; Akiba, J.; Kojiro, M. Interferon alfa receptor expression and growth inhibition by interferon alfa in human liver cancer cell lines. Hepatology 1999, 29, 1708–1717. [Google Scholar] [CrossRef]
  44. Kasai, K.; Kuroda, H.; Ushio, A.; Sawara, K.; Takikawa, Y.; Suzuki, K. Evaluation of newly developed combination therapy of intra-arterial 5-fluorouracil and systemic pegylated interferon alpha-2b for advanced hepatocellular carcinoma with portal venous invasion: Preliminary results. Hepatol. Res. 2009, 39, 117–125. [Google Scholar] [CrossRef]
  45. Enjoji, M.; Morizono, S.; Kotoh, K.; Kohjima, M.; Miyagi, Y.; Yoshimoto, T.; Nakamuta, M. Re-evaluation of antitumor effects of combination chemotherapy with interferon-alpha and 5-fluorouracil for advanced hepatocellular carcinoma. World J. Gastroenterol. 2005, 11, 5685–5687. [Google Scholar]
  46. Ota, H.; Nagano, H.; Sakon, M.; Eguchi, H.; Kondo, M.; Yamamoto, T.; Nakamura, M.; Damdinsuren, B.; Wada, H.; Marubashi, S.; et al. Treatment of hepatocellular carcinoma with major portal vein thrombosis by combined therapy with subcutaneous interferon-alpha and intra-arterial 5-fluorouracil; role of type 1 interferon receptor expression. Br. J. Cancer 2005, 93, 557–564. [Google Scholar] [CrossRef]
  47. Uka, K.; Aikata, H.; Takaki, S.; Miki, D.; Kawaoka, T.; Jeong, S.C.; Takahashi, S.; Toyota, N.; Ito, K.; Chayama, K. Pretreatment predictor of response, time to progression, and survival to intraarterial 5-fluorouracil/interferon combination therapy in patients with advanced hepatocellular carcinoma. J. Gastroenterol. 2007, 42, 845–853. [Google Scholar] [CrossRef]
  48. Kuroda, M.; Kobayashi, Y.; Urawa, N.; Yamamoto, M.; Mifuji, R.; Araki, J.; Tanaka, H.; Horiike, S.; Itani, T.; Furjita, N.; et al. Hepatic arterial infusion of 5-fluorouracil in combination with subcutaneous interferon-alpha for advanced hepatocellular carcinoma. Hepatogastroenterology 2007, 54, 518–521. [Google Scholar]
  49. Katamura, Y.; Aikata, H.; Takaki, S.; Azakami, T.; Kawaoka, T.; Waki, K.; Hiramatsu, A.; Kawakami, Y.; Takahashi, S.; Kenjo, M.; et al. Intra-arterial 5-fluorouracil/interferon combination therapy for advanced hepatocellular carcinoma with or without three-dimensional conformal radiotherapy for portal vein tumor thrombosis. J. Gastroenterol. 2009, 44, 492–502. [Google Scholar] [CrossRef]
  50. Scanlon, K.J.; Safirstein, R.L.; Thies, H.; Gross, R.B.; Waxman, S.; Guttenplan, J.B. Inhibition of amino acid transport by cis-diamminedichloroplatinum(II) derivatives in L1210 murine leukemia cells. Cancer Res. 1983, 43, 4211–4215. [Google Scholar]
  51. Ando, E.; Tanaka, M.; Yamashita, F.; Kuromatsu, R.; Yutani, S.; Fukumori, K.; Sumie, S.; Yano, Y.; Okuda, K.; Sata, M. Hepatic arterial infusion chemotherapy for advanced hepatocellular carcinoma with portal vein tumor thrombosis: Analysis of 48 cases. Cancer 2002, 95, 588–595. [Google Scholar] [CrossRef]
  52. Ueshima, K.; Kudo, M.; Takita, M.; Nagai, T.; Tatsumi, C.; Ueda, T.; Kitai, S.; Ishikawa, E.; Yada, N.; Inoue, T.; et al. Hepatic arterial infusion chemotherapy using low-dose 5-fluorouracil and cisplatin for advanced hepatocellular carcinoma. Oncology 2010, 78, 148–153. [Google Scholar] [CrossRef]
  53. Kim, N.Y.; Sun, J.M.; Kim, Y.J.; Lee, K.W.; Kim, J.H.; Bang, S.M.; Kim, J.W.; Jeong, S.H.; Lee, J.S. Cisplatin-based combination chemotherapy for advanced hepatocellular carcinoma: A single center experience before the Sorafenib Era. Cancer Res. Treat. 2010, 42, 203–209. [Google Scholar] [CrossRef]
  54. Park, J.Y.; Ahn, S.H.; Yoon, Y.J.; Kim, J.K.; Lee, H.W.; Lee do, Y.; Chon, C.Y.; Moon, Y.M.; Han, K.H. Repetitive short-course hepatic arterial infusion chemotherapy with high-dose 5-fluorouracil and cisplatin in patients with advanced hepatocellular carcinoma. Cancer 2007, 110, 129–137. [Google Scholar] [CrossRef]
  55. Woo, H.Y.; Bae, S.H.; Park, J.Y.; Han, K.H.; Chun, H.J.; Choi, B.G.; Im, H.U.; Choi, J.Y.; Yoon, S.K.; Cheong, J.Y.; et al. Korean Liver Cancer Study Group. A randomized comparative study of high-dose and low-dose hepatic arterial infusion chemotherapy for intractable, advanced hepatocellular carcinoma. Cancer Chemother. Pharmacol. 2010, 65, 373–382. [Google Scholar] [CrossRef]
  56. Itamoto, T.; Nakahara, H.; Tashiro, H.; Haruta, N.; Asahara, T.; Naito, A.; Ito, K. Hepatic arterial infusion of 5-fluorouracil and cisplatin for unresectable or recurrent hepatocellular carcinoma with tumor thrombus of the portal vein. J. Surg. Oncol. 2002, 80, 143–148. [Google Scholar] [CrossRef]
  57. Lai, Y.C.; Shih, C.Y.; Jeng, C.M.; Yang, S.S.; Hu, J.T.; Sung, Y.C.; Liu, H.T.; Hou, S.M.; Wu, C.H.; Chen, T.K. Hepatic arterial infusion chemotherapy for hepatocellular carcinoma with portal vein tumor thrombosis. World J. Gastroenterol. 2003, 9, 2666–2670. [Google Scholar]
  58. Sumie, S.; Yamashita, F.; Ando, E.; Tanaka, M.; Yano, Y.; Fukumori, K.; Sata, M. Interventional radiology for advanced hepatocellular carcinoma: Comparison of hepatic artery infusion chemotherapy and transcatheter arterial lipiodol chemoembolization. Am. J. Roentgenol. 2003, 181, 1327–1334. [Google Scholar]
  59. Yamasaki, T.; Kimura, T.; Kurokawa, F.; Aoyama, K.; Ishikawa, T.; Tajima, K.; Yokoyama, Y.; Takami, T.; Omori, K.; Kawaguchi, K.; et al. Prognostic factors in patients with advanced hepatocellular carcinoma receiving hepatic arterial infusion chemotherapy. J. Gastroenterol. 2005, 40, 70–78. [Google Scholar]
  60. Go, R.S.; Adjei, A.A. Review of the comparative pharmacology and clinical activity of cisplatin and carboplatin. J. Clin. Oncol. 1999, 17, 409–422. [Google Scholar]
  61. Court, W.S.; Order, S.E.; Siegel, J.A.; Johnson, E.; DeNittis, A.S.; Principato, R.; Martz, K.; Zeiger, L.S. Remission and survival following monthly intraarterial cisplatinum in nonresectable hepatoma. Cancer Invest. 2002, 20, 613–625. [Google Scholar] [CrossRef]
  62. Yoshikawa, M.; Ono, N.; Yodono, H.; Ichida, T.; Nakamura, H. Phase II study of hepatic arterial infusion of a fine-powder formulation of cisplatin for advanced hepatocellular carcinoma. Hepatol. Res. 2008, 38, 474–483. [Google Scholar] [CrossRef]
  63. Carr, B.I. Hepatic artery chemoembolization for advanced stage HCC: Experience of 650 patients. Hepatogastroenterology 2002, 49, 79–86. [Google Scholar]
  64. Chung, Y.H.; Song, I.H.; Song, B.C.; Lee, G.C.; Koh, M.S.; Yoon, H.K.; Lee, Y.S.; Sung, K.B.; Suh, D.J. Combined therapy consisting of intraarterial cisplatin infusion and systemic interferon-alpha for hepatocellular carcinoma patients with major portal vein thrombosis or distant metastasis. Cancer 2000, 88, 1986–1991. [Google Scholar]
  65. Murata, K.; Shiraki, K.; Kawakita, T.; Yamamoto, N.; Okano, H.; Nakamura, M.; Sakai, T.; Deguchi, M.; Ohmori, S.; Nakano, T. Low-dose chemotherapy of cisplatin and 5-fluorouracil or doxorubicin via implanted fusion port for unresectable hepatocellular carcinoma. Anticancer Res. 2003, 23, 1719–1722. [Google Scholar]
  66. Koizumi, Y.; Hirooka, M.; Uehara, T.; Kisaka, Y.; Uesugi, K.; Kumagi, T.; Abe, M.; Matsuura, B.; Hiasa, Y.; Onji, M. Transcatheter arterial chemoembolization with fine-powder cisplatin-lipiodol for HCC. Hepatogastroenterology 2011, 58, 512–515. [Google Scholar]
  67. Kim, B.K.; Park, J.Y.; Choi, H.J.; Kim do, Y.; Ahn, S.H.; Kim, J.K.; Lee do, Y.; Lee, K.H.; Han, K.H. Long-term clinical outcomes of hepatic arterial infusion chemotherapy with cisplatin with or without 5-fluorouracil in locally advanced hepatocellular carcinoma. J. Cancer Res. Clin. Oncol. 2011, 137, 659–667. [Google Scholar]
  68. Nagamatsu, H.; Hiraki, M.; Mizukami, N.; Yoshida, H.; Iwamoto, H.; Sumie, S.; Torimura, T.; Sata, M. Intra-arterial therapy with cisplatin suspension in lipiodol and 5-fluorouracil for hepatocellular carcinoma with portal vein tumour thrombosis. Aliment Pharmacol. Ther. 2010, 32, 543–550. [Google Scholar] [CrossRef]
  69. Ikeda, M.; Maeda, S.; Shibata, J.; Muta, R.; Ashihara, H.; Tanaka, M.; Fujiyama, S.; Tomita, K. Transcatheter arterial chemotherapy with and without embolization in patients with hepatocellular carcinoma. Oncology 2004, 66, 24–31. [Google Scholar] [CrossRef]
  70. Ikeda, M.; Maeda, S.; Ashihara, H.; Nagahama, H.; Tanaka, M.; Sasaki, Y. Transcatheter arterial infusion chemotherapy with cisplatin-lipiodol suspension in patients with hepatocellular carcinoma. J. Gastroenterol. 2010, 45, 60–67. [Google Scholar] [CrossRef]
  71. Okuda, K.; Tanaka, M.; Shibata, J.; Ando, E.; Ogata, T.; Kinoshita, H.; Eriguchi, N.; Aoyagi, S.; Tanikawa, K. Hepatic arterial infusion chemotherapy with continuous low dose administration of cisplatin and 5-fluorouracil for multiple recurrence of hepatocellular carcinoma after surgical treatment. Oncol. Rep. 1999, 6, 587–591. [Google Scholar]
  72. Maeda, N.; Osuga, K.; Higashihara, H.; Tomoda, K.; Mikami, K.; Nakazawa, T.; Nakamura, H.; Tomiyama, N. Transarterial chemoembolization with cisplatin as second-line treatment for hepatocellular carcinoma unresponsive to chemoembolization with epirubicin-lipiodol emulsion. Cardiovasc. Intervent. Radiol. 2011, 35, 82–89. [Google Scholar]
  73. Kawamura, Y.; Ikeda, K.; Kumada, H. Strategy for advanced hepatocellular carcinoma unresponsive to transcatheter arterial chemoembolization using epirubicin (in Japanese). Gan To Kagaku Ryoho 2010, 37, 402–407. [Google Scholar]
  74. Katamura, Y.; Aikata, H.; Hashimoto, Y.; Kimura, Y.; Kawaoka, T.; Takaki, S.; Waki, K.; Hiramatsu, A.; Kawakami, Y.; Takahashi, S.; et al. Pilot study of systemic combination therapy with S-1, an oral fluoropyrimidine, and cisplatin for hepatocellular carcinoma with extrahepatic metastases. Hepatogastroenterology 2010, 57, 1272–1278. [Google Scholar]
  75. Konno, T.; Maeda, H.; Iwai, K.; Tashiro, S.; Maki, S.; Morinaga, T.; Mochinaga, M.; Hiraoka, T.; Yokoyama, I. Effect of arterial administration of high-molecular-weight anticancer agent SMANCS with lipid lymphographic agent on hepatoma: A preliminary report. Eur. J. Cancer Clin. Oncol. 1983, 19, 1053–1065. [Google Scholar]
  76. Tashiro, S.; Maeda, H. Clinical evaluation of arterial administration of SMANCS in oily contrast medium for liver cancer. Jpn. J. Med. 1985, 24, 79–80. [Google Scholar] [CrossRef]
  77. Okusaka, T.; Okada, S.; Ueno, H.; Ikeda, M.; Iwata, R.; Furukawa, H.; Takayasu, K.; Moriyama, N.; Sato, T.; et al. Transcatheter arterial embolization with zinostatin stimalamer for hepatocellular carcinoma. Oncology 2002, 62, 228–233. [Google Scholar]
  78. Okusaka, T.; Kasugai, H.; Ishii, H.; Kudo, M.; Sata, M.; Tanaka, K.; Shioyama, Y.; Chayama, K.; Kumada, H.; Yoshikawa, M.; et al. A randomized phase II trial of intra-arterial chemotherapy using SM-11355 (Miriplatin) for hepatocellular carcinoma. Invest. New Drugs 2011. [Google Scholar]
  79. Maeda, M.; Uchida, U.A.; Sasaki, T. Liposoluble platinum (II) complexes with antitumor activity. Jpn. J. Cancer Res. 1986, 77, 523–525. [Google Scholar]
  80. Kishimoto, S.; Noguchi, T.; Yamaoka, T.; Fukushima, S.; Takeuchi, Y. Antitumor effects of a novel lipophilic platinum complex (SM-11355) against a slowly growing rat hepatic tumor after intra-hepatic arterial administration. Biol. Pharm. Bull. 2000, 23, 344–348. [Google Scholar] [CrossRef]
  81. Hanada, M.; Baba, A.; Tsutsumishita, Y.; Noguchi, T.; Yamaoka, T.; Chiba, N.; Nishikaku, F. Intra-arterial administration with miriplatin suspended in an oily lymphographic agent inhibits the growth of tumors implanted in rat livers by inducing platinum-DNA adducts to form and massive apoptosis. Cancer Chemother. Pharmacol. 2009, 64, 473–483. [Google Scholar] [CrossRef]
  82. Imai, Y.; Chikayama, T.; Nakazawa, M.; Watanabe, K.; Ando, S.; Mizuno, Y.; Yoshino, K.; Sugawara, K.; Hamaoka, K.; Fujimori, K.; et al. Usefulness of miriplatin as an anticancer agent for transcatheter arterial chemoembolization in patients with unresectable hepatocellular carcinoma. J. Gastroenterol. 2011. [Google Scholar]
  83. Hanada, M.; Baba, A.; Tsutsumishita, Y.; Noguchi, T.; Yamaoka, T. Intra-arterial administration with miriplatin suspended in an oily lymphographic agent inhibits the growth of human hepatoma cells orthotopically implanted in nude rats. Cancer Sci. 2009, 100, 189–194. [Google Scholar] [CrossRef]
  84. Okusaka, T.; Okada, S.; Nakanishi, T.; Fujiyama, S.; Kubo, Y. Phase II trial of intra-arterial chemotherapy using a novel lipophilic platinum derivative (SM-11355) in patients with hepatocellular carcinoma. Invest. New Drugs 2004, 22, 169–176. [Google Scholar] [CrossRef]
  85. Imai, N.; Ikeda, K.; Kawamura, Y.; Sezaki, H.; Hosaka, T.; Akuta, N.; Kobayashi, M.; Saitoh, S.; Suzuki, F.; Suzuki, Y.; et al. Transcatheter arterial chemotherapy using miriplatin-lipiodol suspension with or without embolization for unresectable hepatocellular carcinoma. Jpn. J. Clin. Oncol. 2011. [Google Scholar]
  86. Uyama, N.; Hatano, E.; Maetani, Y.; Isoda, H.; Shibata, T.; Taura, K.; Oe, S.; Naito, M.; Yasuchika, K.; Fujii, H.; et al. Efficacy and toxicity of transcatheter arterial chemoembolization with Cisplatin suspended in lipiodol for unresectable hepatocellular carcinoma (in Japanese). Gan To Kagaku Ryoho 2008, 35, 775–780. [Google Scholar]
  87. Imai, N.; Ikeda, K.; Seko, Y.; Matsumoto, N.; Kawamura, Y.; Hosaka, T.; Kobayashi, M.; Saitoh, S.; Sezaki, H.; Akuta, N.; et al. Transcatheter arterial chemotherapy with miriplatin for patients with hepatocellular carcinoma and chronic renal failure. Nihon Shokakibyo Gakkai Zasshi 2011, 108, 1872–1878. [Google Scholar]
  88. Watanabe, S.; Nitta, N.; Ohta, S.; Sonoda, A.; Otani, H.; Tomozawa, Y.; Nitta-Seko, A.; Tsuchiya, K.; Tanka, T.; Takahashi, M.; Murata, K. Comparison of the anti-tumor effects of two platinum agents (miriplatin and fine-powder cisplatin). Cardiovasc. Intervent. Radiol. 2011. [Google Scholar]
  89. Wang, Z.; Zhou, J.; Fan, J.; Qiu, S.J.; Yu, Y.; Huang, X.W.; Sun, J.; Tan, C.J.; Dai, Z. Oxaliplatin induces apoptosis in hepatocellular carcinoma cells and inhibits tumor growth. Expert Opin. Investig. Drugs 2009, 18, 1595–1604. [Google Scholar] [CrossRef]
  90. Lombardi, L.; Morelli, F.; Cinieri, S.; Santini, D.; Silvestris, N.; Fazio, N.; Orlando, L.; Tonini, G.; Colucci, G.; Maiello, E. Adjuvant colon cancerchemotherapy: Where we are and where we’ll go. Cancer Treat. Rev. 2010, 36, S34–S41. [Google Scholar] [CrossRef]
  91. Rathore, R.; Safran, H.; Soares, G.; Dubel, G.; McNulty, B.; Ahn, S.; Iannitti, D.; Kennedy, T. Phase I study of hepatic arterial infusion of oxaliplatin in advanced hepatocellular cancer: A brown university oncology group study. Am. J. Clin. Oncol. 2010, 33, 43–46. [Google Scholar] [CrossRef]
  92. Breedis, C.; Young, G. The blood supply of neoplasms in the liver. Am. J. Pathol. 1954, 30, 969–977. [Google Scholar]
  93. Okada, S. Chemotherapy in hepatocellular carcinoma. Hepatogastroenterology 1998, 45, 1259–1263. [Google Scholar]
  94. Di Maio, M.; de Maio, E.; Perrone, F.; Pignata, S.; Daniele, B. Hepatocellular carcinoma: Systemic treatments. J. Clin. Gastroenterol. 2002, 35, S109–S114. [Google Scholar] [CrossRef]
  95. Aguayo, A.; Patt, Y.Z. Nonsurgical treatment of hepatocellular carcinoma. Semin. Oncol. 2001, 28, 503–513. [Google Scholar] [CrossRef]
  96. Eguchi, H.; Nagano, H.; Yamamoto, H.; Miyamoto, A.; Kondo, M.; Dono, K.; Nakamori, S.; Umeshita, K.; Sakon, M.; Monden, M. Augmentation of antitumor activity of 5-fluorouracil by IFN-α is associated with upregulation of p27Kip1 in human hepatocellular carcinoma cells. Clin. Cancer Res. 2000, 6, 2881–2890. [Google Scholar]
  97. Nagano, H. Treatment of advanced hepatocellular carcinoma: Intraarterial infusion chemotherapy combined with interferon. Oncology 2010, 78, 142–147. [Google Scholar] [CrossRef]
  98. Jang, J.W.; Bae, S.H.; Choi, J.Y.; Oh, H.J.; Kim, M.S.; Lee, S.Y.; Kim, C.W.; Chang, U.I.; Nam, S.W.; Cha, S.B.; et al. A combination therapy with transarterial chemo-lipiodolization and systemic chemo-infusion for large extensive hepatocellular carcinoma invading portal vein in comparison with conservative management. Cancer Chemother. Pharmacol. 2007, 59, 9–15. [Google Scholar]
  99. Kasugai, H.; Kojima, J.; Tatsuta, M.; Okuda, S.; Sasaki, Y.; Imaoka, S.; Fujita, M.; Ishiguro, S. Treatment of hepatocellular carcinoma by transcatheter arterial embolization combined with intraarterial infusion of a mixture of cisplatin and ethiodized oil. Gastroenterology 1989, 97, 965–971. [Google Scholar]
  100. Kurokawa, Y.; Matoba, R.; Nagano, H.; Sakon, M.; Takemasa, I.; Nakamori, S.; Dono, K.; Umeshita, K.; Ueno, N.; Ishii, S.; et al. Molecular prediction of response to 5-fluorouracil and IFN-α combination chemotherapy in advanced hepatocellular carcinoma. Clin. Cancer Res. 2004, 10, 6029–6038. [Google Scholar]
  101. Nishikawa, H.; Inuzuka, T.; Takeda, H.; Nakajima, J.; Sakamoto, A.; Henmi, S.; Ishikawa, T.; Saito, S.; Kita, R.; Kimura, T.; et al. A case of advanced hepatocellular carcinoma with portal vein tumor thrombus refractory to epirubicin that showed marked decrease in tumor markers after transcatheter arterial infusion with miriplatin. Case Rep. Oncol. 2011, 4, 327–335. [Google Scholar] [CrossRef]
  102. Kudo, M. Current status of molecularly targeted therapy for hepatocellular carcinoma: Clinical practice. Int. J. Clin. Oncol. 2010, 15, 242–255. [Google Scholar] [CrossRef]
  103. Ishizaki, M.; Kaibori, M.; Matsui, K.; Yanagimoto, Y.; Nakatake, R.; Kwon, A.H. The effect of sorafenib and intermittent hepaticarterialinfusionchemotherapy using cisplatin for advanced hepatocellular carcinoma with portal vein tumor thrombus—A pilot study (in Japanese). Gan To Kagaku Ryoho 2010, 37, 2679–2682. [Google Scholar]
  104. Yang, M.Y.; Jeong, S.W.; Kim, D.K.; Kim, S.G.; Jang, J.Y.; Kim, Y.S.; Lee, J.S.; Kim, B.S.; Kim, J.H.; Kim, Y.J.; et al. Treatment of hepatocellular carcinoma with portal vein thrombosis by sorafenib combined with hepatic arterial infusion chemotherapy. Gut Liver 2010, 4, 423–427. [Google Scholar] [CrossRef]
  105. Kemeny, N.E.; Schwartz, L.; Gönen, M.; Yopp, A.; Gultekin, D.; D’Angelica, M.I.; Fong, Y.; Haviland, D.; Gewirtz, A.N.; Allen, P.; et al. Treating primary liver cancer with hepatic arterial infusion of floxuridine and dexamethasone: Does the addition of systemic bevacizumab improve results? Oncology 2011, 80, 153–159. [Google Scholar] [CrossRef]

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MDPI and ACS Style

Nishikawa, H.; Osaki, Y.; Kita, R.; Kimura, T. Hepatic Arterial Infusion Chemotherapy for Advanced Hepatocellular Carcinoma in Japan. Cancers 2012, 4, 165-183. https://doi.org/10.3390/cancers4010165

AMA Style

Nishikawa H, Osaki Y, Kita R, Kimura T. Hepatic Arterial Infusion Chemotherapy for Advanced Hepatocellular Carcinoma in Japan. Cancers. 2012; 4(1):165-183. https://doi.org/10.3390/cancers4010165

Chicago/Turabian Style

Nishikawa, Hiroki, Yukio Osaki, Ryuichi Kita, and Toru Kimura. 2012. "Hepatic Arterial Infusion Chemotherapy for Advanced Hepatocellular Carcinoma in Japan" Cancers 4, no. 1: 165-183. https://doi.org/10.3390/cancers4010165

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