Hepatocellular carcinoma (HCC) is the most common primary liver malignancy and is the third leading cause of cancer death worldwide.1 Transcatheter arterial chemoembolization (TACE) has been widely used to treat unresectable HCC.2, 3, 4, 5 According to the Barcelona Clinic Liver Cancer staging system, TACE is the first-line treatment for patients with intermediate-stage HCC6, underlining the importance of TACE in the treatment of HCC.
HCC often has satellite lesions that cannot be diagnosed by imaging modalities, and the local tumor recurrences may occur because of untreated satellite lesion.7, 8 Therefore, it is necessary to treat not only the tumor itself but also the area around the tumor in the treatment of HCC. Previous studies reported that the adequate safety margin of iodized oil in TACE also affects microsatellite lesions around the tumor, which resulted in a lower rate of local tumor recurrence.9, 10, 11
Corona enhancement is one of the characteristic findings of hypervascular HCC, and it results in perinodular enhancement with bright branching structures depicted on late-phase computed tomography during hepatic arteriography (CTHA).12, 13, 14, 15, 16 The corona enhancement area has been proposed as the blood drainage area of HCC and a previous study reported that satellite lesions of HCC existed in the blood drainage area.17 The corona enhancement area is expected to be an accurate safety margin in the treatment of HCC. However, there have been no studies that have evaluated the association between embolization of corona enhancement area and local tumor recurrence following TACE.
The aim of this retrospective study was to investigate the relationship between local recurrence following TACE and embolization of corona enhancement area.
This study was conducted in accordance with the guidelines of the Declaration of Helsinki and was approved by our institutional ethics committee (protocol number 20200502). Informed consent was waived by the committee because this study was a retrospective study.
Between April 2016 and October 2019, TACE procedures were performed on 345 patients with HCC at our hospital. TACE was done because patients were ineligible for surgery or they refused to undergo surgical resection. Radiofrequency ablation (RFA) procedures were not performed due to the location of the tumor, where ablation may cause insufficient therapeutic effects and/or adverse effects on adjacent organs. The diagnosis of HCC was confirmed by at least 2 of the following modalities: contrast-enhanced computed tomography (CECT), contrast-enhanced ultrasonography, and/or gadolinium-ethoxybenzyl-diethylenetriamine pentaacetic acid (Gd-EOB-DTPA)-enhanced magnetic resonance imaging (MRI). Eligibility criteria for this study were as follows: (a) the presence of fewer than five nodules; (b) nodules treated with balloon-occluded TACE (B-TACE); (c) nodules that showed corona enhancement on late-phase CTHA; and (d) nodules showing dense accumulation of iodized oil throughout the tumor on non-contrast-enhanced CT performed immediately after TACE. The exclusion criteria were as follows: (a) the nodules with prior treatment; (b) impaired renal function, a contraindication for CECT; and (c) extrahepatic metastases. Fifty-three patients with a total of 60 nodules were enrolled in this study. A flow diagram of patient and nodule selection is shown in Figure 1.
The nodules were retrospectively divided into two groups based on the degree of iodized oil accumulation identified on non-contrast-enhanced CT performed immediately after TACE. In group A, a dense accumulation of iodized oil covered the whole tumor and the entire corona enhancement area. In group B, a dense accumulation of iodized oil covered the whole tumor but did not cover the entire corona enhancement area.
Double-phase CTHA was performed in all patients prior to TACE. After left brachial artery puncture, A 4-Fr catheter (FNSAC IV, Angiomaster; Terumo, Tokyo, Japan) was selectively inserted into the proper, common, or replaced hepatic artery and CTHA was performed to identify tumor staining, corona enhancement, and the feeding arteries of the tumor. Examinations were performed using a 64 multidetector-row CT scanner (Aquilion CX; Canon, Tokyo, Japan). The imaging CT parameters were rotation time 0.5 s, beam collimation 64 × 0.5 mm, 0.5 mm slice thickness at 0.4 mm intervals, a tube voltage 120 kV, and volume EC. Helical scanning was initiated 6 or 7 s after the infusion of 13 ml iomeprol (iodine concentration 350 mg/mL; Iomeron, Eisai, Tokyo, Japan) diluted with 26 ml of saline into the common, proper, or replaced hepatic artery at a rate of 3 or 3.5 ml/s. The late-phase scanning was performed 40 s after the initiation of the infusion.
All patients had a B-TACE using a 1.8-Fr microb-alloon catheter (Attendant Delta, Terumo, Tokyo, Japan) through a 4-Fr catheter. The microballoon catheter was placed as close to the tumor feeding artery as possible, and miriplatin (MIRIPLA; Dainippon-Sumitomo Pharmaceutical, Tokyo, Japan) suspended in iodized oil (Ultra-Fluid; Dainippon-Sumitomo Pharmaceutical) was injected into the tumor feeding artery under balloon occlusion. The doses of miriplatin were determined on the basis of tumor size, however. injections of miriplatin were stopped immediately before the flow ceased completely. The total amount of miriplatin per session was limited to 120 mg. This stage was followed by embolization with 1-mm gelatin sponge particles (Gerpart; Nippon Kayaku, Tokyo, Japan) crushed by pumping ten times with two 2.5-mL syringes and a three-way stopcock. If several tumor feeding arteries were confirmed, B-TACE was also performed through each artery.
Double-phase CTHA images were evaluated to determine whether corona enhancement was depicted around the hypervascular tumor. When intranodular enhancement was observed on the early-phase CTHA and subsequently perinodular enhancement appeared on the late phase of CTHA, we determined that corona enhancement was positive in this study. we also measured the thickness of corona enhancement. Based on previous report16, perinodular enhancement with or without irregular protrusions that was greater than 2 mm thickness was classified as thick corona enhancement, and flat perinodular enhancement that was less than or equal to 2 mm thick was classified as thin corona enhancement. In all patients, an unenhanced CT was performed immediately after TACE to check for iodized oil accumulation in the target nodules and the nodules were divided into group A or B based on the degree of iodized oil accumulation. Contrast-enhanced CT was performed 4 weeks after TACE for evaluation of the treatment effect. If no local tumor recurrence was identified, then contrast-enhanced CT or Gd-EOB-DTPA-enhanced MRI was performed every 3–4 months thereafter. Local tumor recurrence was judged when identifiable nodular enhancement in the arterial phase was seen in or adjacent to the treated tumor. In this study, two board-certified hepatologists (> 10 years of experience in abdominal CT) independently assessed the images of unenhanced CT, contrast-enhanced CT, Gd-EOB-DTPA enhanced MRI, and CTHA. If two hepatologists had different assessments, the final result of that particular investigation was obtained by consensus through discussion of them.
Data analyses were performed using EZR (Saitama Medical Center, Jichi Medical University, Saitama, Japan), a graphical user interface for R (The R Foundation for Statistical Computing, Vienna, Austria).
The significance of differences in background parameters was evaluated by the Mann-Whitney U test and Fisher exact test. Univariate and multivariate logistic regression analyses were performed to identify the factors correlated with local tumor recurrence. The main objective of this study was to investigate the relationship between embolization including corona enhancement area and local tumor recurrence in TACE, and thus, tumor recurrence rates were compared between group A and group B. The cumulative local recurrence rate was calculated using the Kaplan-Meier method and evaluated using the log-rank test.
Group A had 36 cases and group B had 24 cases. The clinical characteristics of nodules are summarized in Table 1. Except for des-gamma-carboxy prothrombin, the baseline characteristics did not differ significantly between groups A and B.
Clinical characteristics of nodules in group A and B
Clinical characteristics | Group A (n = 36) | Group B (n = 24) | |
---|---|---|---|
Age, years* | 74 (70–79) | 71 (64–79) | 0.149 |
Gender, male/female | 8/28 | 6/18 | 0.999 |
Etiology (HCV/HBV/Alcohol/Unknown) | 16/8/8/4 | 9/5/6/4 | 0.912 |
Child-Pugh classification (A/B) | 31/5 | 19/5 | 0.569 |
BCLC stage(0/A/B) | 11/20/5 | 5/17/2 | 0.545 |
Size of tumor, mm* | 14.5 (12–21.3) | 15.5 (11–22) | 0.757 |
Thickness of corona enhancement(≤ 2mm/>2mm) | 17/19 | 10/14 | 0.793 |
AFP, ng/ml* | 4.9 (2.6–10.6) | 5.9 (2.7–14.1) | 0.419 |
DCP, mAU/mL* | 26.4 (17.0–49.2) | 48.8 (25.3–153.9) | 0.021 |
Usage of miriplatin, mg* | 28 (20–38.5) | 30 (22.4–51.5) | 0.310 |
AFP = alpha-fetoprotein; BCLC = The Barcelona Clinic Liver Cancer Classification; DCP = des-gamma-carboxy prothrombin; HBV = hepatitis B virus; HCV = hepatitis C virus;
* = data are the median (interquartile range)
In the total sample, local tumor recurrence was observed in 22 out of 60 cases (36.7%) and the cumulative 3-, 6-, 12-month tumor local recurrence rates for all cases were 10%, 20%, and 35% respectively. The median time to local recurrence was 167 days (range, 32–375 days). In group B, local tumor recurrence was observed in 18 out of 24 cases (75%) (Figure 2). Meanwhile, in group A, local tumor recurrence was observed in only 4 out of 36 cases (11.1%), and most nodules had no local tumor recurrence (Figure 3). The cumulative 3-, 6-, 12-month tumor local recurrence rates were 2.8%, 2.8%, 8.3%, respectively for group A, and 20.8%, 45.8%, 75%, respectively for group B. The cumulative local tumor recurrence rates in group A were significantly lower than those in group B (hazard ratio [HR], 0.079; 95% confidence interval [CI], 0.026–0.24;
Univariate logistic regression analysis for prognostic factors affecting local tumor recurrence was performed for the following factors: the size of tumors, serum alpha-fetoprotein level, serum des-gamma-carboxy prothrombin level, usage of miriplatin, thickness of corona enhancement, and the degree of iodized oil accumulation (Group A or B). The degree of iodized oil accumulation only showed
Univariate and multivariate logistic regression analysis for factor affecting local tumor recurrence
Factor | Univariate analysis |
Multivariate analysis |
||
---|---|---|---|---|
Odds ratio (95% CI) | Odds ratio (95% CI) | |||
Size of tumor (< 20 |
0.67 (0.20–2.32) | 0.577 | ||
AFP (< 10 |
0.45 (0.13–1.61) | 0.242 | ||
DCP (< 40 |
0.59 (0.18–1.92) | 0.417 | ||
Usage of miriplatin (< 30 |
0.70 (0.17–1.89) | 0.420 | ||
Thickness of corona enhancement (≤ 2mm/ > 2mm) | 0.97 (0.30–3.20) | 0.999 | ||
Degree of iodized oil accumulation (Group A |
0.045 (0.0080–0.20) | < 0.001 | 0.042 (0.010–0.17) | < 0.001 |
AFP = alpha-fetoprotein; CI = confidence interval; DCP = des-gamma-carboxy prothrombin
In this study, we investigated whether the embolization of not only the tumor but also the corona enhancement area could provide a better therapeutic effect for TACE. Our findings showed that the group with a dense embolization of HCC including the corona enhancement area had a significantly lower local tumor recurrence rate and a higher therapeutic effect than the group with a dense embolization of HCC itself but not including the corona enhancement area. Our study demonstrated a relationship between local recurrence following TACE and embolization of corona enhancement area.
HCC often has satellite lesions that cannot be diagnosed by imaging modalities.7, 8 Previous histopathological research reported that microsatellite lesions found in 46% of HCCs were smaller than 5 cm, and in 29% of HCCs, the lesions were smaller than 2.5 cm.18 Another study reported that 28 of 149 resected specimens exhibited microsatellite lesions.7 These reports indicate that it is important to embolize the tumor and the surrounding tissues by TACE. Miyayama
The usefulness of CTHA, including cone-beam CTHA during the TACE procedure, has been reported because of its ability to offer relevant information for tumor identification, assessment of tumor feeding artery, and navigation guidance.22, 23, 24 Moreover, it has become possible for the accurate identification of tumor feeding arteries in combination with guidance software19, suggesting that CTHA will be performed more frequently during TACE. By performing not only the early phase of CTHA but also the late phase of CTHA and depicting the corona-like deep stain, CTHA can be used not only for tumor vessel identification and navigation guidance but also for determination of safety margin. As it requires two CT scans, in the early phase and in the delayed phase, it has the disadvantage of increasing the radiation exposure. However, since the therapeutic effect of TACE can be expected to increase, we consider that the benefits outweigh the risks for the patient. If conventional CT or cone-beam CT is performed before the end of the TACE procedure and accumulation of iodized oil to the corona enhancement area is insufficient, we believe that additional embolization should be performed considering the possibility of inadequate drug administration or the presence of the feeding artery. Whether the additional embolization will improve the treatment effect is an issue for further study.
Our study had several limitations. First, our study population was small and the study was retrospective. This limitation could have led to some patient selection bias. Moreover, as many tumors with relatively small diameters have been enrolled and only four tumors were larger than 30 mm in diameter in this study, it is unclear whether the same results as this study apply to large diameter tumors. Therefore, confirmation of our findings would require additional studies on large numbers of patients, including patients with large diameter tumors. Second, the observation period after TACE was relatively short. Longer-term observations may increase local recurrence rates. However, there was a large difference in local recurrence rates between the two groups, and it is considered that there is a significant difference between the two groups even after long-term observation. Third, as late-phase CTHA was not performed at a single-slice level, assessment of corona enhancement area may be slightly incorrect. In the nodules in which local tumor recurrence was recognized despite the assessment that the embolization was obtained throughout the corona enhancement area, the corona enhancement area may have been underestimated.
In conclusion, local tumor recurrence was significantly lower when embolizing not only the tumor itself but also the corona enhancement area, and corona enhancement area may be an accurate safety margin in TACE. Our results suggested that TACE should be continued until the embolic area covers the entire corona enhancement area.