Can Kushen injection combined with TACE improve therapeutic efficacy and safety in patients with advanced HCC? a systematic review and network meta-analysis

INTRODUCTION

Liver cancer (primarily hepatocellular carcinoma, HCC) is one of the most common cancers with dismal outcomes including cancer-related death [1–2]. HCC is a common disease and accounts for 54% of the total number of cancer patients worldwide, with more than 600,000 related deaths estimated each year [1]. HCC is the fifth-most common malignancy and the second leading cause of cancer-related death worldwide; the 5-year survival rate of HCC is 15–17% [3]; the incidence rates of liver cancer have continued to increase rapidly by approximately 3% per year in women and 4% per year in men, although the rates have begun to decline in adults younger than 50 years of age [4]. Only a small proportion of patients with early-stage HCC can benefit from radical treatment options, such as surgical resection and orthotopic liver transplantation. Although hepatic resection offers hope of cure in patients suffering from HCC, only a small proportion (10–15%) of HCC patients are eligible for this procedure [5]. However, surgical resection is not the first treatment choice for HCC patients with large lesions or poor liver function.

Transarterial chemoembolization (TACE) as a kind of palliative care and management that is prescribed for most patients with advanced HCC to prevent and relieve suffering and improve the quality of life. This is a standard and minimally invasive procedure developed for HCC patients who are not eligible for complete resection [6] and is the most widely used primary treatment for advanced HCC [7]. This procedure combines transcatheter delivery of chemotherapy emulsions with lipiodol, followed by vascular stagnation achieved with embolization agents. TACE results in partial responses in 15–55% of patients, and it significantly delays tumor progression and macrovascular invasion. The most common TACE regimens include one, two and three chemotherapeutic agents, such as doxorubicin (ADM), cisplatin (DDP), epirubicin (EPI), hydroxycamptothecin (HCPT) and mitomycin (MMC) [8–9]. However, sensitivity analysis of results from efficacy studies has shown a significant benefit of TACE with cisplatin or doxorubicin [10]. Thus, we included TACE treatment arms with or without adriamycins/platinum for subgroup analyses. However, regarding the morbidity and mortality rate due to advanced unresectable HCC, the efficacy of TACE alone is not satisfactory. In addition, TACE has its own limitations, as it can further affect liver functions and damage the hepatic arterial system. As a result, TACE is not appropriate for HCC patients with poor liver functions, particularly patients with cirrhosis [11]. Therefore, in recent years, increasing attention has been focused on the effectiveness of TACE therapy for liver cancer combined with other non-chemical drugs or palliative therapies, including Compound Kushen Injection (CKI).

CKI is a kind of traditional Chinese medicinal preparation that is widely used in clinics. The main components of Kushen injection are matrine (Sophorae Flavescentis Radix) and tufuling (Smilacis Glabrae Rhizoma) with inactive ingredients such as polysorbate 80, sodium hydroxide and acetic acid. Its functions include relieving fever, dampness and blood stasis, detoxification, dissolution of tumors and alleviating pain, among others” [12]. Matrine is the main active ingredient of Kushen injection. Moreover, matrine exhibits anti-tumor effects against breast cancer cells (MCF-7), gastric cancer cells (SGC-7901 and MKN45), gallbladder cancer cells (GBC-SD) and osteosarcoma cells (UMR-108), and can also significantly inhibit the proliferation of HCC cells via a mechanism that may be related to the induction of apoptosis [13]. Therefore, we speculate that CKI can be used in combination with TACE in HCC treatment to relieve the clinical symptoms of cancer, reduce the side effects of chemotherapy, improve the quality of life and prolong the survival of patients. However, there is a lack of high-quality evidence to support this notion. To further explore these issues and to identify the efficacy and safety of combination treatment with CKI and TACE, we performed a network meta-analysis of all available randomized controlled trials on patients with advanced HCC. Until now, no other review [14–15] has provided a comprehensive overview of this subject using meta-regressions and network meta-analyses.

RESULTS

Description of the network and patients

In total, 191 publications were retrieved from databases; after removing duplicates, 182 publications were screened based on the title and abstract, and 84 were excluded from further analysis. A total of 98 publications were included for full-text analysis. The network comprised 44 trials with 3778 patients, which were included in the standard meta-analysis [16–59]. There were 22 different TACE arms: 5-fluorouracil (5-FU)+doxorubicin (ADM)+hydroxycamptothecin (HCPT); 5-FU+Cisplatin (DDP); 5-FU+DDP+ADM; 5-FU+DDP+epirubicin (EPI); 5-FU+DDP+gemcitabine (GEM); 5-FU+DDP+HCPT; 5-FU+DDP+mitomycin (MMC); 5-FU+DDP+MMC+vincristine (VCR); 5-FU+EPI+HCPT; 5-FU+EPI+MMC; 5-FU+HCPT; 5-FU+MMC; 5-FU+MMC+pirarubicin (THP)+oxaliplatin (L-OHP); 5-FU+THP+MMC+HCPT; DDP+ADM+MMC; EPI; EPI+THP+L-OHP; L-OHP+GEM; THP; THP+camptothecin (CPT); THP+HCPT; and THP+MMC+HCPT. Figure 1 shows the flowchart representing the steps to screen for the relevant studies.

Table 1 summarizes the numbers of patients with advanced HCC according to treatment arms. Patients were grouped by different treatment arms (TACE arm and CKI arm). Table 1 also summarizes the differences in the fundamental characteristics between the two treatment arms (see complete information regarding characteristics in Supplementary Table 1). Statistical analyses showed that the two groups had similar baseline characteristics in terms of age, sex, tumor stage, and Child-Pugh score. The results of quality assessment of these studies are presented in Supplementary Figure 1, indicating that all included trials were of acceptable quality.

Primary efficacy outcomes - treatment responses

Standardized meta-analysis

Figure 2 and Table 2 summarize the results of treatment responses from 32 trials (2444 patients) in patients with advanced HCC. Compared with TACE alone, treatment with TACE+CKI conferred significant therapeutic advantages (odds ratios: 1.85, 95% confidence intervals: 1.56 to 2.20) with low heterogeneity (P = 0.877, I² = 0.0%; Figure 2, Table 2). Moreover, some degree of bias was observed using Begg’s test (P = 0.128) and Egger’s test (P = 0.008), and the data were of high quality according to the GRADE assessment (Table 2).

Subgroup analyses and meta-regressions were used to explore the source of heterogeneity between the TACE+CKI and TACE arms regarding therapeutic efficacy (Table 2). The meta-regression results showed that the different TACE arms might have influenced the final results with a P value of 0.113. Significant efficacy was observed in all subgroups except for the group with the treatment duration of fewer than 10 days. Low degree of heterogeneity was observed in all subgroups with strong significance. In general, meta-regression did not reveal the source of heterogeneity in our pairwise meta-analysis; however, in all subgroups of TACE+CKI vs TACE alone, positive results were observed with the combination treatment. Although meta-regression results revealed differences between the TACE arms compared to the other grouping methods (Table 2), the P values were not significant. Therefore, we need to perform further comparisons of differences in TACE arms by network meta-analysis.

Network meta-analysis

Figure 3 displays the network weight of eligible comparisons of treatment efficacy along with the available, direct comparisons and network of the trials. Network meta-analysis suggested that in comparison with the TACE-only arm, 5-FU+EPI+HCPT ranked as the best (4.04, 95% credible intervals: 1.37 to 11.96), followed by THP+HCPT (3.62, 1.88 to 6.97), 5-FU+THP+MMC+HCPT (3.26, 0.86 to 12.31), 5-FU+MMC (2.91, 1.08 to 7.84), DDP+ADM+MMC (2.63, 1.15 to 6.04), EPI (2.80, 0.73 to 10.77), 5-FU+DDP (2.27, 1.09 to 4.72), 5-FU+HCPT (2.08, 1.01 to 4.29), THP (2.26, 0.30 to 17.07), 5-FU+DDP+MMC (1.95, 1.34 to 2.83), 5-FU+ADM+HCPT (1.75, 0.92 to 3.32), 5-FU+DDP+ADM (1.66, 0.79 to 3.52), 5-FU+DDP+EPI (1.68, 0.86 to 3.30), EPI+THP+L-OHP (1.29, 0.43 to 3.88), 5-FU+EPI+MMC (1.29, 0.81 to 2.07) and L-OHP+GEM (1.18, 0.68 to 2.06).

When we assessed the comparative efficacy of CKI, 5-FU+EPI+HCPT, THP+HCPT, 5-FU+MMC, DDP+ADM+MMC, 5-FU+DDP, 5-FU+HCPT and 5-FU+DDP+MMC were superior to the TACE-only arm. Treatment arms were comparable with one another in improving responses, with a significant difference found in the 5-FU+EPI+HCPT vs L-OHP+GEM groups (3.42, 1.01 to 11.53), the THP+HCPT vs L-OHP+GEM groups (3.06, 1.30 to 7.21) and the THP+HCPT vs 5-FU+DDP+EPI groups (2.80, 1.25 to 6.27) (Figure 4).

Therefore, CKI can improve the efficacy of TACE regimens with adriamycins (EPI and THP), such as 5-FU+EPI+HCPT, THP+HCPT and 5-FU+THP+MMC+HCPT. Similar results are illustrated in Table 2 with the highest OR values in subgroup analysis.

Secondary efficacy outcomes

Table 3 summarizes the results of the secondary outcomes associated with the different TACE arms. We found that combination therapy with TACE+CKI improves the KPS score, Child-Pugh score and overall survival rate. Moreover, combination therapy with CKI can reduce the clinical symptoms, improve immune function and liver function. The differences in most of the outcomes between TACE-only and TACE-CKI groups are significant, with mostly moderate to high-quality evidence according to GRADE assessment and moderate publication bias.

Safety outcomes

Table 4 summarizes the results of toxicity associated with the different TACE arms. We found that CKI did not increase the risk of side effects, while it reduced the occurrence of nausea and vomiting, fever, hepatalgia, leukopenia, and increase in transaminase and bilirubin. Moreover, the use of TACE+CKI was safe, with mostly moderate to high-quality evidence according to GRADE assessment and moderate publication bias.

DISCUSSION

The present network meta-analysis represents the most comprehensive analysis of currently available data regarding the treatment of patients with advanced HCC with CKI combined with TACE vs TACE alone. We combined direct and indirect evidence from 44 randomized controlled trials comparing 22 different TACE arms in more than three thousand HCC patients undergoing TACE therapy to make several key observations regarding the potential efficacy and safety of CKI. First, TACE+CKI was superior to TACE-only regimens regarding overall treatment response accompanied by low heterogeneity (Figure 2). Furthermore, most of the correlations identified from subgroup analyses reached statistical significance, and heterogeneity was non-existent in most of the outcomes, with moderate to high confidence regarding the estimates (Table 2). In addition, due to the differences in treatment arms (by meta-regression), the network meta-analysis of treatment responses revealed superior efficacy for the regimens 5-FU+EPI+HCPT, THP+HCPT and 5-FU+THP+MMC+HCPT among the TACE treatment arms (Figure 4). Moreover, CKI was shown to improve the KPS score, Child-Pugh score and overall survival rate. Moreover, combination therapy with CKI could also reduce the clinical symptoms and improve immune function and liver function (Table 3). Finally, CKI did not increase the risk of adverse events but rather alleviated side effects (Table 4). Overall, compared with the TACE-only control arm, TACE+CKI was found to be both safe and efficacious for the treatment of patients with HCC.

Currently, there are a number of chemotherapeutic targeted drugs that are combined with TACE therapy to improve safety and efficacy, such as sorafenib [60–62], brivanib [63] and licartin [64], but the overall efficacy has been unsatisfactory. Additionally, the positive results reported with the multikinase inhibitor sorafenib in patients with advanced HCC need to be verified in an international cohort in the adjuvant setting. With regard to safety, the sorafenib-associated adverse events were more frequent in the combination therapy group (TACE+sorafenib). Thus, even though it may improve the treatment response and overall survival rate in patients with unresectable advanced HCC [65–66], the use of TACE+sorafenib is not recommended. Therefore, researchers have focused their attention on CKI, which can affect the immune system [67] and thus improve immune function in patients with advanced HCC, thereby enhancing therapeutic efficacy. The results can be verified in a study by Gu XB et al., in which the infusion of matrine through the hepatic artery could reduce immune function after TACE therapy and enhance the T cell immunity in the body [68–69]. In addition, in the treatment of primary HCC after surgical resection, CKI combined with TACE demonstrated a very favorable clinical efficacy, which could effectively improve the quality of life of elderly patients and prolong their survival [70]. Moreover, a study by Li showed that CKI can have a synergistic effect with TACE in killing primary HCC cells, thus alleviating the pain in the liver, improving clinical symptoms and quality of life and prolonging lifespan [71].

The current study followed the guidelines in conducting rigorous systematic reviews and network meta-analyses [72–74]. To identify as many relevant studies as possible and to decrease the risk of bias, a comprehensive search strategy was designed. Based on these considerations, we observed moderate publication bias by statistical assessment. CKI significantly increased treatment efficacy in HCC patients without increasing the incidence of adverse events. A meta-regression was performed to assess heterogeneity. Overall, the meta-regression could not identify the source of heterogeneity. In our meta-analysis, based on subgroup analyses, we obtained a negative result for only the group with a treatment duration of fewer than 10 days. The results reveal that long-term application of CKI with a standard dosage (20 ml/day) can improve therapeutic efficacy. Subgroup analyses and network meta-analyses revealed that the arms 5-FU+EPI+HCPT, THP+HCPT and 5-FU+THP+MMC+HCPT ranked best with significantly high treatment efficacies. Based on these results, we can conclude that CKI can improve the therapeutic efficacy in patients with advanced HCC undergoing TACE therapy, especially regimens with chemotherapeutic drugs with high levels of adriamycins (EPI and THP) and HCPT. This is the first study demonstrating these findings based on a meta-analysis, and there have been no other reports with similar results in the literature. Although studies on efficacy have shown a significant benefit of TACE with cisplatin or doxorubicin [10], regarding the use of chemotherapy drugs containing adriamycins (EPI and THP) and HCPT, we recommend the use of CKI as an adjuvant therapy.

Our study elaborates on the findings from primary randomization controlled trials and previous pairwise meta-analyses by systematically synthesizing efficacy and safety data [16–59]. Our meta-analysis differs from earlier studies in several ways. First, our aim was to identify the most appropriate combination of CKI and TACE, rather than simply showing that the combination is effective and safe. Second, subgroup analyses and meta-regressions were used to identify differences between the different TACE arms, CKI dosage, composition of CKI, embolizing agents and duration of treatment to determine the best options for the combination treatment. Finally, our study extends the findings from network meta-analysis and ranked the TACE treatment arms to determine the best regimen to be combined with CKI.

The network meta-analysis had some limitations that merit further discussion. First, this study was restricted to trials involving patients with advanced HCC. We excluded studies in which the patients were diagnosed with earlier stages of HCC as well as patients undergoing surgical treatment, which include a substantial number of HCC patients worldwide. In addition, the network analysis had some inconsistencies, which were mainly determined by the loop. Furthermore, positive results are more likely to be published than negative results [75]. An additional limitation of pairwise comparisons were their extensive heterogeneity (Tables 2–4), which indicated substantial variability in the outcomes reported by the included studies, even though this is often because of heterogeneity in the baseline characteristics (Table 1) and differences observed in treatment arms. Finally, there was a risk of bias. Some ways to reduce bias include defining the groups in the original studies, examining the data for each patient, and expanding the scope of the study to a global scale. In the included studies, blinding was not performed, and the quality of the studies was low (Supplementary Figure 1). The quality of most studies was only sufficient for meta-analysis.

CKI is a safe and efficacious adjuvant to TACE therapy. In addition, the use of CKI in clinical therapy is relatively new. Future trials of TACE+CKI in patients with advanced HCC should be performed on a large sample size, and their design should be robust and randomized to confirm the therapeutic efficacy and safety. Future studies should ensure that appropriate methods are used for randomization and blinding with intentions to treat. Furthermore, trials should assess outcomes using standardized or prescribed measures at similar time points. Analyses of data of each patient will be valuable for further exploration. Additional normative studies should be conducted for future network meta-analyses.

The findings of this comprehensive network meta-analysis demonstrate that combination therapy with CKI and TACE can improve treatment responses, KPS score, Child-Pugh score and overall survival rate. Moreover, combination therapy with CKI can reduce clinical symptoms and improve immune function and liver function, while reducing the risk of adverse effects. Thus, patients with advanced HCC should be encouraged to accept CKI in combination with TACE, especially with TACE regimens with high levels of adriamycins (EPI and THP) and HCPT. In patients with advanced HCC, combination therapy with CKI and TACE may be used as a first-line treatment.

MATERIALS AND METHODS

This systematic review was reported with an previously defined protocol (PROSPERO CRD 42017073181) [76] and was performed in agreement with the PRISMA (Preferred Reporting Items for Systematic Reviews and Meta-Analyses) extension statement for systematic reviews incorporating network meta-analyses for healthcare treatments and the Cochrane Collaboration recommendations [72–74].

Search strategy and selection criteria

We included large-scale randomized controlled trials on patients with a primary diagnosis of advanced hepatocellular carcinoma, comparing combination therapy with Compound Kushen Injection and TACE with TACE therapy alone. Studies published by August 2017 were searched in PubMed, Medline, EMBASE, and Cochrane Library, as well as four Chinese medical databases: China National Knowledge Infrastructure database, VIP database, Chinese Biomedical Literature database, and Wanfang database. We used the following search terms: “Compound Kushen Injection” OR “Matrine” and “advanced hepatocellular carcinoma” OR “advanced liver cancer” and “clinical trial” OR “randomized controlled trial”.

The inclusion criteria were as follows: randomized controlled trials in patients with a primary diagnosis of advanced hepatocellular carcinoma; patients of any age, sex, tumor stage, and Child-Pugh score; lipiodol or lipiodol+gelfoam as embolizing agents; and TACE arms with any chemotherapy drugs. We also excluded trials published only as abstract (with no additional data available from other sources). No language restrictions were implemented, and non-English papers were translated. We then screened the references in all selected articles to avoid the exclusion of relevant trials.

Data abstraction and assessment of risk of bias

Two investigators (ZYS and HFH) independently abstracted the data on the studies, patients, and treatment-related characteristics onto a standardized form; discrepancies were resolved by consensus, by referring back to the original study or by consulting a third reviewer (ZMY or ZQC). Data on efficacy and safety were abstracted from original studies. We extracted trial design, trial size, details of treatment arms including CKI dosage and solution, chemotherapy drugs in TACE, treatment duration, embolizing agents, and type of outcome (efficacy and safety). We extracted results from intention-to-treat analyses whenever possible.

The risk of bias of the individual studies was assessed using the Cochrane risk of bias tool [77]. We assessed the following 7 items regarding risk of bias: random sequence (selection bias), allocation concealment (selection bias), blinding of participants and personnel (performance bias), blinding of outcome assessment (detection bias), incomplete outcome data (attrition bias), selective reporting (reporting bias), and other bias. All studies were classified into low risk, high risk, or unclear risk in terms of bias. Any discrepancies were resolved by consensus and arbitration by a panel of investigators within the review team.

Outcomes

The primary efficacy outcome was treatment response. Local tumor response was measured according to the modified criteria for response evaluation in solid tumors (mRECIST) [78]; mRECIST defines the treatment response into four main categories: complete response (CR), partial response (PR), progressive disease (PD), and stable disease (SD). CR corresponds to the disappearance of intra-tumoral arterial enhancement in all target lesions, and PR corresponds to a minimum of 30% decrease in the total diameter of visible (enhancement in the arterial phase) target lesions, with reference to the total diameter of target lesions at baseline. PD is defined as an increase of at least 20% in the total diameter of viable target lesions, with reference to the smallest total diameter of viable target lesions recorded at the beginning of treatment; SD refers to the cases that do not qualify for either PR or PD.

Subgroup analyses and meta-regression were performed according to the various TACE arms (adriamycins+platinum, adriamycins and platinum), CKI dosage (20 ml/d and < 20 ml/d), composition of CKI (NS or GS, NS and GS), embolizing agents (lipiodol and lipiodol+gelfoam) and duration (≤ 10 d, 10–30 d and > 30 d). In addition, we performed a network meta-analysis according to the TACE arms (5-FU+ADM+HCPT; 5-FU+DDP; 5-FU+DDP+ADM; 5-FU+DDP+EPI; 5-FU+DDP+GEM; 5-FU+DDP+HCPT; 5-FU+DDP+MMC; 5-FU+DDP+MMC+VCR; 5-FU+EPI+HCPT; 5-FU+EPI+MMC; 5-FU+HCPT; 5-FU+MMC; 5-FU+MMC+THP+L-OHP; 5-FU+THP+MMC+HCPT; DDP+ADM+MMC; EPI; EPI+THP+L-OHP; L-OHP+GEM; THP; THP+CPT; THP+HCPT; and THP+MMC+HCPT).

The secondary efficacy outcomes were improvements in Child-Pugh score, overall survival rate, clinical symptoms, immunologic function, liver function and Karnofsky Performance Status (KPS) the KPS is considered a gold standard performance scale for cancer patients [79–80]; a significantly effective improvement in KPS score after treatment relative to that before treatment corresponds to an increase by > 20 points; an effective improvement in for KPS corresponds to an increase by 10 to 20 points; a stable KPS corresponds to an increase by < 10 points; and no change and no treatment effect is shown by a reduction in the KPS score. The safety outcomes included nausea/vomiting, fever, hepatalgia, leukopenia, increased transaminase and increased bilirubin, which were stratified by TACE arms (adriamycins+platinum, adriamycins and platinum).

Data synthesis and statistical analysis

First, a standardized meta-analysis was performed using a random-effects model, because it is the most appropriate and conservative methodology to account for heterogeneity among trials within each comparison [81–82]. To estimate pooled odds ratios (ORs) or standardized mean differences (SMDs) with their 95% confidence intervals (CIs) incorporating heterogeneity within and between studies, STATA v 14.0 was used. Statistical heterogeneity was assessed with P values and the I² statistic, with values over 50% indicating substantial heterogeneity [83]. The Begg’s and Egger’s tests were used to detect publication bias [84].

To further investigate the heterogeneity, meta-regressions and subgroup analyses were performed to assess the primary outcome data and associations according to TACE arms (adriamycins+platinum, adriamycins and platinum), CKI dosage (20 ml/d and < 20 ml/d), composition of CKI (NS or GS, NS and GS), embolizing agents (lipiodol and lipiodol+gelfoam) and treatment duration ≤ 10 d, 10–30 d and > 30 d). The P values in the meta-regression revealed the overall significance of the influence factors. Additionally, the P values were inversely proportional to the degree of heterogeneity; P values less than 0.10 indicate factors that could be an important source of heterogeneity.

Second, a random-effects network meta-analysis was performed using STATA v 14.0. The results of the network meta-analysis were summarized using ORs and their credible intervals (CrI) [85]. A common heterogeneity parameter was used for all comparisons, and the global heterogeneity was assessed using P values and the I² statistic.

The relative efficacy and safety outcomes were derived from the combination of direct and indirect evidence obtained from network meta-analysis, which was assumed to be coherent [77]. Inconsistencies between direct and indirect sources of evidence were statistically assessed globally (by comparing the fit and parsimony of consistency and inconsistency models) and locally (by calculating the difference between the direct and indirect estimates in all closed loops in the network) [86]. When a direct connection between two treatment arms was not available, the results were based on indirect evidence.

We estimated ranking probabilities for all treatments in each TACE arm. The treatment hierarchy was summarized and reported as surface under the cumulative ranking curve (SUCRA) [87], ranging from 1, indicating that the treatment has a high likelihood of being the best, to 0, indicating that the treatment has a high likelihood of being the worst. High SUCRA score corresponds to a higher ranking of the treatment method for treatment response compared with the ranking of the other treatments.

Quality of evidence

In addition, the quality of evidence for the primary outcomes was assessed based on the GRADE system using GRADEpro GDT [88–89]. The GRADE system assesses the risk of bias (study limitations), imprecision, inconsistency, indirectness of study results, and publication bias (classifying each as high, moderate, low, or very low) across the body of evidence to derive an overall summary of the quality of evidence.

Patient involvement

No patients were involved in formulating the research question or assessing the outcome measures, nor were they involved in developing plans for the design or implementation of the study. None of the patients were consulted for the interpretation or compiling of the results. There is no intention to circulate the results of the research among the study participants or the relevant patient community.

Author contributions

ZYS and HFH conceived of and designed the experiments; ZYS, HFH and YY performed the experiments; ZYS, HFH and ZMY analyzed the data; CHX, QXC and ZQC contributed materials/analysis tools; ZYS and HFH wrote the paper. All authors approved of the final version of the article, including the authorship list.

ACKNOWLEDGMENTS

We thank the authors of the primary studies for providing their data and other critical information. Additionally, we would like to thank the researchers and participants for their valuable contributions to this article.

CONFLICTS OF INTEREST

The authors have declared that there are no competing interests.

FUNDING

None.

REFERENCES

1. Forner A, Llovet JM, Bruix J. Hepatocellular carcinoma. Lancet. 2012; 379:1245–55. https://doi.org/10.1016/S0140-6736(11)61347-0.

2. Qiu J, Peng B, Tang Y, Qian Y, Guo P, Li M, Luo J, Chen B, Tang H, Lu C, Cai M, Ke Z, He W, et al. CpG Methylation Signature Predicts Recurrence in Early-Stage Hepatocellular Carcinoma: Results From a Multicenter Study. J Clin Oncol. 2017; 35:734–742. https://doi.org/10.1200/JCO.2016.68.2153.

3. Kudo M. Surveillance, diagnosis, treatment, and outcome of liver cancer in Japan. Liver Cancer. 2015; 4:39–50. https://doi.org/10.1159/000367727.

4. Siegel RL, Miller KD, Jemal A. Cancer Statistics, 2017. CA Cancer J Clin. 2017; 67:7–30. https://doi.org/10.3322/caac.21387.

5. Jia H, Yang Q, Wang T, Cao Y, Jiang QY, Ma HD, Sun HW, Hou MX, Yang YP, Feng F. Rhamnetin induces sensitization of hepatocellularcarcinoma cells to a small molecularkinase inhibitor or chemotherapeutic agents. Biochim Biophys Acta. 2016; 1860:1417–30. https://doi.org/10.1016/j.bbagen.2016.04.007.

6. Jiang BG, Wang N, Huang J, Yang Y, Sun LL, Pan ZY, Zhou WP. Tumor SOCS3 methylation status predicts the treatment response to TACE and prognosis in HCC patients. Oncotarget. 2017; 8:28621–28627. https://doi.org/10.18632/oncotarget.16157.

7. Takayasu K, Arii S, Ikai I, Omata M, Okita K, Ichida T, Matsuyama Y, Nakanuma Y, Kojiro M, Makuuchi M, Yamaoka Y; Liver Cancer Study Group of Japan. Prospective cohort study of transarterial chemoembolization for unresectable hepatocellular carcinoma in 8510 patients. Gastroenterology. 2006; 131:461–9.

8. Marelli L, Stigliano R, Triantos C, Senzolo M, Cholongitas E, Davies N, Tibballs J, Meyer T, Patch DW, Burroughs AK. Transarterial therapy for hepatocellular carcinoma: which technique is more effective? A systematic review of cohort and randomized studies. Cardiovasc Intervent Radiol. 2007; 30:6–25.

9. Sun JH, Zhou TY, Zhang YL, Zhou GH, Nie CH, Zhu TY, Chen SQ, Wang BQ, Ye S, Shen Y, Guo H, Wang WL, Zheng SS. Efficacy of transcatheter arterial chemoembolization for liver metastases arising from pancreatic cancer. Oncotarget. 2017; 8:39746–39755. https://doi.org/10.18632/oncotarget.14642.

10. European Association For The Study Of The Liver; European Organisation For Research And Treatment Of Cancer. EASL-EORTC clinical practice guidelines: management of hepatocellular carcinoma. J Hepatol. 2012; 56:908–43. https://doi.org/10.1016/j.jhep.2011.12.001.

11. Zhao J, Zhang H, Wei L, Xie S, Suo Z. Comparing the long-term efficacy of standard and combined minimally invasive procedures for unresectable HCC: a mixed treatment comparison. Oncotarget. 2017; 8:15101–15113. https://doi.org/10.18632/oncotarget.13145.

12. Wang W, You RL, Qin WJ, Hai LN, Fang MJ, Huang GH, Kang RX, Li MH, Qiao YF, Li JW, Li AP. Anti-tumor activities of active ingredients in Compound Kushen Injection. Acta Pharmacol Sin. 2015; 36:676–9. https://doi.org/10.1038/aps.2015.24.

13. Wang K, Gao L, Zhou Y, Zhang J, Qin X, Du G. Network pharmacology-based study of anti-hepatoma effects and mechanisms of matrine. Acta Pharmaceutica Sinica. 2017; 52:888–896.

14. Ma X, Li RS, Wang J, Huang YQ, Li PY, Wang J, Su HB, Wang RL, Zhang YM, Liu HH, Zhang CE, Ma ZJ, Wang JB, et al. The Therapeutic Efficacy and Safety of Compound Kushen Injection Combined with Transarterial Chemoembolization in Unresectable Hepatocellular Carcinoma: An Update Systematic Review and Meta-Analysis. Front Pharmacol. 2016; 7:70. https://doi.org/10.3389/fphar.2016.00070.

15. Sun Q, Ma W, Gao Y, Zheng W, Zhang B, Peng Y. Meta-analysis: therapeutic effect of transcatheter arterial chemoembolization combined with compound kushen injection in hepatocellular carcinoma. Afr J Tradit Complement Altern Med. 2011; 9:178–88.

16. Dong WH, Hu LR, Chen S, Chen JB, Li HJ, Chen HS, Yang M, Wu J. Clinical Study on Treatment of Primary Hepatocellular Carcinoma with Compound Kushen Injection Combined with Arterial Chemoembolization. Liaoning journal of traditional chinese medicine. 2016; 43:2564–2565.

17. Wang Y. Clinical Study on Treatment of Primary Hepatocellular Carcinoma with Compound Kushen Injection Combined with Hepatic Artery Infusion Chemotherapy Embolization. Journal of China Prescription Drug. 2016; 14:91–92.

18. Yan WH, Sun CH, Sun QW, Liu HM, Wu GQ. Compound Matrine Injection Combined with Interventional Operation for 38 Cases of Hepatocellular Carcinoma. Liaoning journal of traditional chinese medicine. 2016; 43:314–315.

19. Zhang ZD, Jia GZ, Guan LJ, Wang ZX. Clinical Observation on 60 Cases of Primary Liver Cancer Treated by Compound Kushen Injection Combined with Hepatic Artery Intervention. Guiding Journal of Traditional Chinese Medicine and Pharmacy. 2015; 21:50–52.

20. Cao L, Guo YW, Wang ZW, Liu C, Liu Y, Pan J. Clinical Observation on Prevention and Treatment of Liver Injury in Patients with Advanced Hepatocellular Carcinoma Treated by Compound Kushen Injection in Prevention and Treatment of Hepatic Arterial Embolization. Chinese Journal of Information on TCM. 2014; 21:98–99.

21. Li RJ. Observation on the Therapeutic Effect of Compound Kushen Injection Combined with Double Intervention on Primary Liver Cancer. Chin J Mod Drug Appl. 2014; 8:116–117.

22. Sun MY. Clinical observation of TACE combined with compound Kushen injection in the treatment of primary HCC. Asia-Pacific Traditional Medicine. 2014; 10:45–46.

23. Tian YY. Clinical study on the treatment of primary liver cancer patients with compound Kushen injection combined with chemotherapy. Contemporary Medicine Forum. 2014; 12:45–46.

24. Wang S, Lin HS, Zhou XW, Ma CW, Xu RC, Zhang QY, Hou W, Liu J. A randomized and multicenter clinical trial of compound matrine injection combined with hepatic artery interventional therapy in treatment of primary liver cancer. Chin J Clin Oncol Rehabil. 2014; 21:331–335.

25. Yi YB, Xie KH, Liu XC, Bai J. Clinical Effects of Sophora Combined Arterial Embolization on Hepatocellular Carcinoma. Anti-tumor Pharmacy. 2014; 4:229–232.

26. Zuo L, Meng DJ, Zhao L, Xu H. Clinical Observation of intravenous infhsion of sophora after transcatheter arterial chemoembolization in treatment of mid-term liver cancer. Practical hospitals are clinical miscellaneous. 2014; 11:96–98.

27. Li B, Liu ZW, Li L, Ma LB, Zhou ZX, Hu WN. Therapeutic effect of hepatic artery embolization combined with compound Kushen injection on 98 cases of primary liver cancer. Journal of Guiyang College of Traditional Chinese. 2013; 35:90–92.

28. Liu JQ. Evaluation of the effect of compound Kushen injection on hepatic artery infusion chemotherapy plus embolization in the treatment of primary liver cancer. Guide of China Medicine. 2013; 11:261–262.

29. Wang QC, Chen W, Chen DQ, Xu YP, Yan RH, Wu YY. Influence of toad venom, salvia miltiorrhiza and matrine combined with transcatheter arterialchemoembolization on the immune function of the patients with hepatocellular carcinoma. Chin J Gastroenterol Hepatol. 2013; 22:632–634.

30. Zhong W, Tang CW, Bao Y. Protective effect of oxymatrine on hepatic and immune function after transhepatic arterial chemoembolization on liver cancer. Chinese medicine. 2013; 51:99–103.

31. Han WL, Yuan CY, Zhang TS. Efficacy of Compound Kushen Injection Combined with Chemotherapy in Primary Hepatocellular Carcinoma and Its Effect on Immune Function. Chinese traditional Chinese medicine technology. 2012; 19:61–62.

32. Xu P, Wang WD, Lu J, Fan C. Effect of Compound Kushen Injection on TACE Lymphocyte Subsets in Primary Liver Cancer. Modern Journal of Integrated Traditional Chinese and Western Medicine. 2012; 21:1313–1314.

33. Cao J, Liu HQ, He Y, Xia N, Zhang HL. Clinical analysis of TACE combined with compound Kushen injection in the treatment of primary HCC. Hebei Medical Journal. 2012; 33:2783–2784.

34. Hou JX, He M, Liu BK. Therapeutic effect of transhepatic arterial chemoembolization combined with compound Kushen injection on primary liver cancer. Chin J Misdiagn. 2011; 11:5097–5098.

35. Lu J, Wang WD, Fan C, Xu P, Wang WT, Ding Y. Clinical Observation of Compound Kushen Injection in Treating Primary Hepatocellular Carcinoma with Hepatic Artery Infusion Chemotherapy and Embolization. Modern Journal of Integrated Traditional Chinese and Western Medicine. 2011; 20:4661–4662.

36. Qu Y, Tian SJ, Zhang WJ, Li ZX, Mao WW, Gong YX, Yang JJ, Yu XL, Guo HG. Therapeutic Effect of TACE Combined with Compound Sophora flavescensInjection in Mid and Advanced Stage Primary Liver Cancer. China Pharmacy. 2011; 22:1072–1074.

37. Wang YL, Fang H, Wang XC, Zhou KM. Clinical Observation on the Treatment of Advanced Primary Hepatocellular Carcinoma with Compound Kushen Injection Combined with Implantation. Shandong medicine. 2011; 51:88–89.

38. Wang ZF, Song YP, Wang P. Clinical Observation on the effect of Matrine Injection Combined with Scatheter Arterrial Chemoembolization on 36 Hepatocellular Carcinoma patients. Journal of China Coal Industry Medicine. 2011; 14:1625–1627.

39. Xiang GH, Zhou JX, Luo JH. Marin injection in treatment of post-TACE syndrome. Contemporary Medicine. 2011; 17:26–28.

40. Zhang LY, Tian YZ. Efficacy and Safety of Composite Matrine injection combined with TACE in the treatment of Patients with Liver Carcinoma. Chinese Journal of New Drugs. 2011; 20:2003–2009.

41. Tong HZ. The Observation of the Clinical Effects of Transcatheter Arterial Chemoembolization and Complex Prescrption Kushen Injection on the Advanced Period of Liver Cancer. Jiangxi Province, Chinese medicine, Chinese and Western medicine combined with tumor academic exchange. 2010; 8–10.

42. Tong HZ. The Observation of the Clinical Effects of Transcatheter Arterial Chemoembolization and Complex Prescrption Kuseng Injection on the Advanced Period of Liver Cancer. Jiangxi Medical Journal. 2011; 45:637–639.

43. Xu P, Wang WD, Lu J, Fan C. Efficacy of Compound Kushen Injection in the Prevention and Treatment of the Advance Reactions Following Transcatheter Hepatic Arterial Chemoembolization in the Patients with Liver Cancer. Evaluation and analysis of drug-use in hospitals of China. 2010; 10:457–458.

44. Yu ML, Kang XH. Clinical Study on Treatment of Primary Liver Cancer with Compound Kushen Injection Combined with Transcatheter Arterial Chemoembolization. Guide of China Medicine. 2010; 8:123–125.

45. Zhang ZH, Ni BQ, Chen RX. Effect of Matrine Injection on Liver Function of Patients with Primary Liver Cancer due to HB virus infection after Transaterial Chemoembolization. Acta Academiae Medicine Militars Tertice. 2010; 32:2552–2555.

46. Zhao Y. Clinical Observation on the Quality of Life of Patients with Liver Cancer Chemotherapy Treated by Compound Kushen Injection. Inner Mongolian Medicine. 2010; 29:130–131.

47. Cao J, Wang ZL, Fang J, Liu HQ, He Y. Clinical Study of Compound Kushen Injection Combined with TACE in the Treatment of Advanced Liver Cancer. Shandong Medicine. 2009; 49:74–76.

48. Deng L, Li ZW, Wu YT, Lu QH, Chen LZ, Wu JY, Wu XY, Chen QQ. Treatment of advanced primary hepatocellular carcinoma with continuous infusion of compound Kushen injection combined with transcatheter arterial chemoembolization: a report of 20 cases. Journal of New Chinese Medicine. 2009; 41:28–29.

49. Chen YH. Efficacy of Transcatheter Arterial Chemoembolization Combined with Complex Prescription Kushen Injection in the treatment of Primary Advanced Liver Cancer. Chin J Integr Trad West Med Dig. 2009; 16:5–6.

50. Wang HM. Composite Kushen Injection Combined with Hepatic Artery Embolism on Unresectable Primary Liver Cancer. Modern Journal of Integrated Traditional Chinese and Western Medicine. 2009; 18:1334–1335.

51. Yu LP, Jiang DY, Li GY. Compound Martrine Injection Combined with Transcatheter Arterial Chemoembolization in the Treatment of 30 Cases with Primary Hepatocellular Carcinoma. Journal of Oncology. 2009; 15:777–778.

52. Yu LP, Jiang DY, Li GY. Clinical Observation of Compound Kushen Injection Combined with TACE in the Treatment of Primary Liver Cancer. China Prac Med. 2009; 14:74–75.

53. Chen GH, Li SR, Yang L. Therapeutic effects of complex kushen injection combined with double interventional therapy on treating primary hepato carcinoma. Chin J Integr Trad West Med Dig. 2007; 15:239–241.

54. Lao YQ. The clinical observation of the treatment of patients with primary hepatic hepatic artery embolization after chemotherapy. Chinese Herbal Medicine. 2005; 28:637–638.

55. Liang JX, Zeng WT, Zhu KL, Ma PQ. Clinical observation of matrine combined with chemoembolization in the treatment of advanced liver cancer. Guangzhou Medicine. 2005; 36:45–47.

56. Zhao ZH, Li H, Li CY, Zhang H. Application of Compound Kushen Injection in Interventional Therapy of Hepatocellular Carcinoma. Chinese Medicine Emergency. 2005; 14:1053–1075.

57. Liu QR, Li YH. Clinical Observation on 75 Cases of Hepatocellular Carcinoma Treated by Oxymatrine Combined with Hepatic Artery. China Journal of Modern Medicine. 2004; 14:33–35.

58. Wan XY, Chen Z. Clinical observation of matrine injection combined with TACE in the treatment of primary hepatocellular carcinoma. Journal of Zhejiang College Traditional Chinese Medicine. 2002; 26:22–25.

59. Zhou BG, Sun JZ, Jing SH, Fan YZ, Huang YN. Clinical Observation on 26 Cases of Advanced Hepatocellular Carcinoma Treated by Integrated Traditional Chinese and Western Medicine. New Chinese Medicine. 2002; 34:37–38.

60. Yao X, Yan D, Zeng H, Liu D, Li H. Concurrent sorafenib therapy extends the interval to subsequent TACE for patients with unresectable hepatocellular carcinoma. J Surg Oncol. 2016; 113:672–7. https://doi.org/10.1002/jso.24215.

61. Bai W, Wang YJ, Zhao Y, Qi XS, Yin ZX, He CY, Li RJ, Wu KC, Xia JL, Fan DM, Han GH. Sorafenib in combination with transarterial chemoembolization improves the survival of patients with unresectable hepatocellular carcinoma: a propensity score matching study. J Dig Dis. 2013; 14:181–90. https://doi.org/10.1111/1751-2980.

62. Kudo M, Imanaka K, Chida N, Nakachi K, Tak WY, Takayama T, Yoon JH, Hori T, Kumada H, Hayashi N, Kaneko S, Tsubouchi H, Suh DJ, et al. Phase III study of sorafenib after transarterial chemoembolisation in Japanese and Korean patients with unresectable hepatocellular carcinoma. Eur J Cancer. 2011; 47:2117–27. https://doi.org/10.1016/j.ejca.2011.05.007.

63. Kudo M, Han G, Finn RS, Poon RT, Blanc JF, Yan L, Yang J, Lu L, Tak WY, Yu X, Lee JH, Lin SM, Wu C, et al. Brivanib as adjuvant therapy to transarterial chemoembolization in patients with hepatocellular carcinoma: A randomized phase III trial. Hepatology. 2014; 60:1697–707. https://doi.org/10.1002/hep.27290.

64. Ma J, Wang JH. 131I-Labeled-Metuximab Plus Transarterial Chemoembolization in Combination Therapy for Unresectable Hepatocellular Carcinoma: Results from a Multicenter Phase IV Clinical Study. Asian Pac J Cancer Prev. 2015; 16:7441–7.

65. Zhang X, Wang K, Wang M, Yang G, Ye X, Wu M, Cheng S. Transarterial chemoembolization (TACE) combined with sorafenib versus TACE for hepatocellular carcinoma with portal vein tumor thrombus: a systematic review and meta-analysis. Oncotarget. 2017; 8:29416–29427. https://doi.org/10.18632/oncotarget.15075.

66. Yang M, Yuan JQ, Bai M, Han GH. Transarterial chemoembolization combined with sorafenib for unresectable hepatocellular carcinoma: a systematic review and meta-analysis. Mol Biol Rep. 2014; 41:6575–82. https://doi.org/10.1007/s11033-014-3541-7.

67. Spano D, Heck C, De Antonellis P, Christofori G, Zollo M. Molecular networks that regulate cancer metastasis. Semin Cancer Biol. 2012; 22:234–49. https://doi.org/10.1016/j.semcancer.2012.03.006.

68. Wang QC, Chen W, Chen DQ, Xu YP, Yan RH, Wu YY. Influence of toad venom, salvia miltiorrhiza and matrine combined with transcatheter arterialchemoembolization on the immune function of the patients with hepatocellular carcinoma. Chin J Gastroenterol Hepatol. 2013; 22.

69. Gu XB, Yang XJ, Wang D, Zhu YF, Ding H, Zhang B, Xu YQ, Wu HY. Influence of Kurarinol on cell immunity in patients with chronic hepatitis B. Pharmacol Clin Chin Mater Med. 2010; 26:75–77.

70. Tian Y, Wu ZY, Ma XM, Dong J, Li ZH. Efficacy of Transcatheter Arterial Chemoembolization Combined with Complex Prescription Kushen Injection in the Treatment of Primary Advanced Liver Cancer. Liaoning Journal of Traditional Chinese Medicine. 2015; 42:1270–1271.

71. Li B, Liu ZW, Li L, Ma LB, Zhou ZX, Hu WN. Therapeutic effect of hepatic artery embolization combined with compound Kushen injection on 98 cases of primary liver cancer. JGCTCM. 2013; 35:90–92.

72. Moher D, Liberati A, Tetzlaff J, Altman DG; PRISMA Group. Preferred reporting items for systematic reviews and meta-analyses: the PRISMA statement. BMJ. 2009; 339:b2535. https://doi.org/10.1136/bmj.b2535.

73. Hutton B, Salanti G, Caldwell DM, Chaimani A, Schmid CH, Cameron C, Ioannidis JP, Straus S, Thorlund K, Jansen JP, Mulrow C, Catalá-López F, Gøtzsche PC, et al. The PRISMA extension statement for reporting ofsystematic reviews incorporating network meta-analyses of health care interventions: checklist and explanations. Ann Intern Med. 2015; 162:777–784. https://doi.org/10.7326/M14-2385.

74. Higgins JPT. Cochrane handbook for systematic reviews of interventions. John Wiley & Sons. 2011.

75. Zhang Y, Hou J, Feng F, Li D, Jiang Q, Li X, Zhao Q, Li BA. Genetic polymorphisms in human UDP-glucuronosyltransferases 1A7 and the risk of gastrointestinal carcinomas: A systematic review and network meta-analysis. Oncotarget. 2017; 8:66371–66381. https://doi.org/10.18632/oncotarget.18675.

76. PROSPERO, Centre for Reviews and Dissemination. Systematic Reviews: CRD’s Guidance for Undertaking Reviews in Health Care (Internet). York, England: University of York. http://www.cdr.york.ac.uk/prospero). 2009.

77. Higgins JP, Altman DG, Gotzsche PC, Jüni P, Moher D, Oxman AD, Savovic J, Schulz KF, Weeks L, Sterne JA; Cochrane Bias Methods Group; Cochrane Statistical Methods Group. The Cochrane Collaboration’s tool for assessing risk of bias in randomised trials. BMJ. 2011; 343:d5928. https://doi.org/10.1136/bmj.d5928.

78. Lencioni R, Llovet JM. Modified RECIST (mRECIST) assessment for hepatocellular carcinoma. Semin Liver Dis. 2010; 30:52–60. https://doi.org/10.1055/s-0030-1247132.

79. Terret C, Albrand G, Droz JP. Geriatric assessment in elderly patients with prostate cancer. Clin Prostate Cancer. 2004; 2:236–40.

80. Johnson MJ, Bland JM, Davidson PM, Newton PJ, Oxberry SG, Abernethy AP, Currow DC. The relationship between two performance scales: New York Heart Association classification and Karnofsky performance status scale. Journal of pain and symptom management. 2014; 47:652–658. https://doi.org/10.1016/j.jpainsymman.2013.05.006.

81. Dias S, Welton NJ, Sutton AJ, Caldwell DM, Lu G, Ades AE. Evidence synthesis for decision making 4: Inconsistency in networks of evidence based on randomized controlled trials. Med Decis Making. 2013; 33:641–56. https://doi.org/10.1177/0272989X12455847.

82. Mills EJ, Thorlund K, Ioannidis JP. Demystifying trial networks and network meta-analysis. BMJ. 2013; 346:f2914. https://doi.org/10.1136/bmj.f2914.

83. Higgins JP, Thompson SG, Deeks JJ, Altman DG. Measuring inconsistency in meta-analyses. BMJ. 2013; 327:557–60.

84. The Cochrane Collaboration. Cochrane handbook for systematic reviews of interventions (Version 5.1.0). March, 2011. http://handbook.cochrane.org (accessed Oct 20, 2015).

85. Salanti G, Higgins JP, Ades AE, Ioannidis JP. Evaluation of networks of Randomized trials. Stat Methods Med Res. 2008; 17:279–301.

86. Chaimani A, Higgins JP, Mavridis D, Spyridonos P, Salanti G. Graphical tools for network meta-analysis in STATA. PLoS One. 2013; 8:e76654. https://doi.org/10.1371/journal.pone.0076654.

87. Salanti G, Ades AE, Ioannidis JP. Graphical methods and numerical summaries for presenting results from multiple-treatment meta-analysis: an overview and tutorial. J Clin Epidemiol. 2011; 64:163–71. https://doi.org/10.1016/j.jclinepi.2010.03.016.

88. Balshem H, Helfand M, Schünemann HJ, Oxman AD, Kunz R, Brozek J, Vist GE, Falck-Ytter Y, Meerpohl J, Norris S, Guyatt GH. GRADE guidelines: 3. Rating the quality of evidence. Journal of clinical epidemiology. 2011; 64:401–406. https://doi.org/10.1016/j.jclinepi.2010.07.015.

89. Guyatt GH, Oxman AD, Vist GE, Kunz R, Falck-Ytter Y, Alonso-Coello P, Schünemann HJ; GRADE Working Group. GRADE: an emerging consensus on rating quality of evidence and strength of recommendations. British Medical Journal. 2008; 336:924. https://doi.org/10.1136/bmj.39489.470347.AD.