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Treatment of Large Hepatocellular Carcinoma using Transarterial Chemoembolisation Combined with Sorafenib |
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SD Madhu, Fanai Lalsawmpuii, B Harish, Nilesh Suryavamshi, KN Lokesh, LK Rajeev, Amritham Usha 1. Associate Professor, Department of Radiodiagnosis, Kidwai Memorial Institute of Oncology, Bangalore, Karnataka, India. 2. Postgraduate, Department of Radiodiagnosis, Kidwai Memorial Institute of Oncology, Bangalore, Karnataka, India. 3. Associate Professor, Department of Nuclear Medicine, Kidwai Memorial Institute of Oncology, Bangalore, Karnataka, India. 4. Postgraduate, Department of Radiodiagnosis, Kidwai Memorial Institute of Oncology, Bangalore, Karnataka, India. 5. Associate Professor, Department of Medical Oncology, Kidwai Memorial Institute of Oncology, Bangalore, Karnataka, India. 6. Associate Professor, Department of Medical Oncology, Kidwai Memorial Institute of Oncology, Bangalore, Karnataka, India. 7. Associate Professor, Department of Pathology, Kidwai Memorial Institute of Oncology, Bangalore, Karnataka, India. |
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Correspondence Address : Dr. SD Madhu, No. 51044, Building 5, Prestige Falcon City, Near Konanakunte Cross, Kanakapura Road, Bangalore-560062, Karnataka, India. E-mail: sdmadhudoc@gmail.com |
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ABSTRACT | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
: Introduction: Hepatocellular Carcinoma (HCC) is the most common primary malignant tumour of liver, accounts for 90% of all primary hepatic tumours, with second most common cause for cancer-related deaths worldwide. Majority of HCC presents in Barcelona Clinic Liver Cancer (BCLC) intermediate stage (B), for which Transarterial Chemoembolisation (TACE) is the most commonly available treatment . Even though overall prognosis of these locally advanced tumours is poor, significant improvement can still be made in overall survival and recurrence free survival with locoregional therapy like TACE. Aim: To assess the efficiency, safety and limitations of TACE in large HCC with specific focus on importance of appropriate patient selection. Materials and Methods: The study was conducted on 30 histopathologically proven cases of HCC with BCLC intermediate stage. All cases underwent TACE followed by repeat TACE or treated with sorafenib depending on their response and clinical status. Treatment-related complications, treatment response, recurrence free survival was assessed. Results: Of the 30 cases, six cases had lesion size less than 5 cm, six cases with lesion size 5-10 cm and remaining 18 cases had lesion size more than 10 cm, with the largest lesion being 16 cm. Twenty-one cases had elevated Alfa Fetoprotein (AFP), chronic liver disease was seen in 10 cases, with five cases having at least two lesions. Total 50% of cases with lesion less than 5 cm showed complete response at 15 months, four of six cases with lesion size of 5-10 cm showed partial response at 15 months, other two cases were lost for follow-up. Cases with lesion size more than 10 cm showed mixed response, at 15 months follow-up, 10 cases showed stable response, six cases showed progressive disease and two patients died due to liver dysfunction. Conclusion: Transarterial Chemoembolisation combined with sorafenib prolonged the overall survival in selected large tumours with high disease burden status. | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Keywords : Child-pugh criteria, Liver, Malignancy | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
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DOI and Others :
DOI: 10.7860/IJARS/2021/45348:2587
Date of Submission: Jun 09, 2020 Date of Peer Review: Jun 25, 2020 Date of Acceptance: Sep 10, 2020 Date of Publishing: Jan 01, 2021 b#bAuthor Declaration:b?b • Financial or Other Competing Interests: None • Was Ethics Committee Approval obtained for this study? Yes • Was informed consent obtained from the subjects involved in the study? Yes • For any images presented appropriate consent has been obtained from the subjects. Yes |
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INTRODUCTION | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
The HCC is the fifth most common tumour and second most common cause for cancer-related deaths worldwide (1). The frequency of HCC has increased as a result of rising cases of cirrhosis and chronic hepatitis [2-4]. Though there is a major progress in the cancer screening protocols, diagnosis and treatment, the prognosis of HCC remains poor with a five-year survival rate of less than 5% (5). The incidence-to-mortality ratio of liver cancer was assessed to be as high as 95% according to World Health Organisation (WHO) in 2012 (6). Heterogenicity and complexity are one of the major challenges in treating HCC. The prognosis of HCC depends on remaining liver reserve, underlying liver disease and tumour load which includes tumour size, number of lesions and presence of portal vein invasion. Application of these anatomical factors is imperative in culling the relevant treatment modalities (7),(8),(9). Currently, BCLC system is proposed and validated in the management of HCC. It is used for tumour characterisation and for assessment of the factors influencing long-term prognostication, thus assisting the clinicians to adopt the right treatment for specific patients (1),(10),(11),(12). In case of early HCC, potential curative management strategies like surgical resection, hepatic transplant or ablation therapies can be employed with a good five-year survival of 60-70%. Despite the advancement in screening, detection of early HCC is rare. Majority of the HCC is diagnosed in intermediate or advance stage of the disease with compromised liver function (13), thereby only eligible for palliative care. TACE (14),(15),(16) is the most common bridge therapy offered (>70%), for patients with HCC waiting for liver transplant (17),(18). It is a locoregional therapy widely recommended as first line treatment option for a patient with intermediate stage HCC (BCLC stage B) (1),(11). For patients with BCLC stage A, curative treatment like surgical resection, ablation or liver transplantation is used. In case of advanced HCC with BCLC stage C, only systemic therapy with oral sorafenib tablet and supportive care is used (1),(11). The present study aimed at assessing the efficiency, safety, limitations and consequence of TACE on liver function in large HCC with specific focus on importance of appropriate patient selection. | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Material and Methods | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
A prospective, cross-sectional observational study was performed in the Department of Radiodiagnosis and Interventional Radiology at Kidwai Memorial Institute of Oncology, Bangalore from January 2017 to December 2018 for over two years with follow-up to February 2020. Approval (KCI/MEC/015/JAN.2017) was taken from the Institutional Scientific Review Committee and Ethical Committee. Written consent was procured from the patient for considering their data for the study. All the cases were discussed in a multidisciplinary meeting which involved medical oncologist, surgical oncologist and pathologist along with interventional radiologist. Inclusion Criteria Patients only aged between 18-75 years were considered for the study. Patients with child-pugh class A or B, Eastern Cooperative Oncology Group (ECOG) performance status of 0-1, number of lesions less than three, (with a size of the lesion 3-15 cm), no obvious main portal vein or opposite portal vein invasion or hepatic vein invasion on imaging and no extrahepatic disease were included in the study. Exclusion Criteria Patients with a previous history of any treatment for HCC including TACE, systemic therapy and ablation, serious medical comorbidities, deranged Renal Function Test (RFT), deranged coagulation profile, other malignancies, ECOG score of more than two or child-pugh class C or BCLC advanced disease were excluded from the study. Patient’s details including age, sex, clinical presentation, associated co-morbidities, laboratory information including AFP levels and imaging details were collected. TACE Procedure Transarterial chemoembolisation was conducted by an interventional radiologist with more than five years of experience. Proper assessment of triphasic CT scan was performed in all the cases to identify the celiac artery, SMA anatomy, anatomical variations if any, and to look for any extrahepatic feeders particularly from phrenic artery, internal mammary artery, intercoastal artery, and from Superior Mesenteric Artery (SMA) branches, as their assessment will help the interventional radiologist to plan to embolise these vessels. After puncturing the femoral artery with Seldinger’s technique, 5F sheath was introduced. A 4F cobra diagnostic glide catheter was used to cannulate celiac axis and celiac artery angiogram was performed followed by SMA angiogram to look for any additional feeders. In difficult cannulation of the celiac axis, 4F Simmons 1 or 4 French Yashiro glide catheter was used. A 2.8F microcatheter was used further to superselectively cannulate the feeding arteries. Emulsion of lipiodol and doxorubicin in 3:1 ratio was prepared and injected into feeding arteries. Total of 5-20 mL of lipiodol was used and a maximum of 50 mg of doxorubicin was used in powder form which was diluted depending on the amount of lipiodol used. Finally, the feeding vessels were embolised using gel foam slurry mixed with contrast, with the endpoint being stasis of contrast. After the embolisation, an angiogram was performed to look for occlusion of feeding artery and to look for any additional feeding vessels. All patients were monitored with Liver Function Test (LFT), RFT and Complete Blood Count (CBC) on day one, three, and seven after the procedure to assess the post-embolisation syndrome and for derangement of liver functions. Patients with refractory disease, or progressive disease, or not tolerating TACE were referred to medical oncologist for systemic therapy with sorafenib. These patients were treated with sorafenib 400 mg BD, one hour before or two hours after food. Dose titration was done based on the adverse effects like diarrhoea, hand-foot syndrome, fatigue, nausea vomiting, hypertension and rarely pancytopenia. All patients were followed-up after one month with detailed clinical history, physical examinations, laboratory data including AFP and triphasic CT or Magnetic Resonance Imaging (MRI) to assess the treatment response. Tumour responses of patients to the procedure was classified according to the Modified Response Evaluation Criteria in Solid Tumours for HCC (mRECIST) as either complete response, partial response, stable disease or progressive disease. In case of complete response achieved after 1st TACE, patients were started with sorafenib 400 mg BD and were followed-up after three months and six months with the same investigation. In case of stable disease or partial response, repeat TACE was done and further started with sorafenib. Several repeat TACE were performed depending on the tumour response and patient’s acceptability, and upto three repeat TACE were done in this study. Sorafenib was continued if the patient tolerated the medication. In the case of liver dysfunction or any other adverse effects, the chemotherapy was discontinued. Most of our cases tolerated sorafenib well with tolerable adverse effects. STATISTICAL ANALYSIS Normally distributed data were expressed as mean±standard deviation (SD), while non-normally distributed data were expressed as median (range), and enumeration data were expressed as n (%). 6Differences in tumour responses and post-treatment complications between the patients with different tumour sizes were assessed for significance using independent-samples ?2 tests. The p-value <0.05 was considered as statistically significant. Patients lost to follow-up were excluded from the final analysis. | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Results | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Overall, 50 patients of HCC were considered for TACE in this study. Of these patients, 20 patients were excluded, as they did not meet the inclusion criteria. Detailed patient baseline characteristics are depicted in (Table/Fig 1). In this study group, 25 (83.33%) were males and 5 (16.67%) were females with a mean age of 56.28±10.69 years. Of the total, majority {10 (33.3%)} had alcoholic liver disease, and at least 5 cases with AFP levels more than 50,000 ng/mL among 21 elevated AFP levels. Total 17 (81%) out of 21 patients with increased AFP levels had lesion size more than 10 cm. Most of the cases in this study belonged to child-pugh’s class B (20,66.7%) with 80% of patients did not had any ascites. Majority of the patients (83%, 25) had single lesion. Among 18 patients with lesion size more than 10 cm, at least two cases had multiple lesions and 5 cases had vascular invasion with tumour thrombus in segmental portal vein branches. In this study, six patients had vascular invasion in which five had segmental portal vein thrombus and one had partial thrombus extending into the main portal vein. All these patients underwent TACE with feeding artery embolisation. Among 30 cases, selective catheterisation was performed using microcatheter in 23 cases, out of which in seven cases 4F glide diagnostic catheter was enough to cannulate the feeding artery, as the right hepatic artery was supplying the entire tumour. AFP was used for follow-up of cases after TACE, as elevated AFP indicates presence of active disease (Table/Fig 2). Of 21 cases with elevated AFP, after 1st TACE, 10 cases showed significant reduction in AFP values (<400 ng/mL), rest showed elevated AFP with average value of 5000 ng/mL with all these cases at one month follow-up showing residual disease. Among the cases with size larger than 10 cm, after 1st TACE, five cases were in stable disease, eleven cases showed partial response and remaining two cases showed progressive disease with appearance of new small lesions. The cases with progressive disease had elevated AFP more than 50,000 ng/mL, cirrhotic background, low albumin, and high child-pugh score of 8. In this study, four well-defined capsulated lesions at CT scan showed complete response at one and three months follow-up (Table/Fig 3). Two lesions which were ill-defined at CT scan showed partial response at 1st month follow-up, which underwent second TACE at the 2nd month. At the end of 3rd TACE and follow-up at 6th month, two cases with lesion size of 6 cm showed complete response, two cases were lost for follow-up and another two cases had partial response (Table/Fig 4). Rest of the cases underwent 2nd TACE after one month and on further follow-up after a month, of the five cases with stable disease, one patient showed progressive disease and rest of the cases showed partial response (Table/Fig 5),(Table/Fig 6). In (Table/Fig 7) overall tumour responses of patients at 1, 3, 12 and 15-month follow-up were listed and at the end of six months, four patients were lost to follow-up. Tumour responses of patients at 15-month follow-up were compared based on the initial size of the tumours (<5 cm, 5-10 cm and >10 cm) and shown in (Table/Fig 8). It was observed that tumour response among the patients with different sizes of tumour differed significantly (p-value=0.018). Post-embolisation syndrome was the most common complication encountered in this study with n-12 is not 60% developing symptoms within a week after the procedure. In all cases the symptoms were self-limiting and were treated with antiemetics and anti inflammatory drugs. Of the 30 patients treated with TACE, none of the patient developed any major complication after the 1st TACE. After 2nd TACE procedure, two patients died within eight months due to chronic liver dysfunction who had larger tumour diameter (>10 cm diameter) with cirrhosis. One patient with large tumour size and with child-pugh score eight developed acute liver failure signs after 1st TACE however responded well to medical management. Rest of the patients were on follow-up for 15 months from the date of 1st TACE. Ten patients who had signs of cirrhosis at the time of diagnosis developed worsening child-pugh score with increasing ascites. Three of the six Hepatitis B virus (HBV) positive cases that had high viral load at the time of 1st TACE showed worsening of liver function; however they were managed conservatively and were shifted to systemic therapy after stabilising the liver functions. All the patients tolerated the sorafenib well with tolerable side effects. One of the patients had lesion in segment V developed cholecystitis, however he responded well to medical treatment. Treatment-related complications in the patients at 15 months follow-up were compared based on the initial size of the tumours (<5 cm, 5-10 cm and >10 cm) and shown in (Table/Fig 9). Comparison of complications between all the patients with different tumour sizes did not show any statistically significant differences (p-value=0.764). | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Discussion | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
As the treatment of sorafenib in combination with TACE in advanced HCC has proven to be more effective (19), the present study was carried out to evaluate the efficiency, safety and limitations of TACE in large HCC and to identify the consequence of TACE on liver function in case of very large tumours. Overall, 50 patients received combined therapy. Of these patients, 20 patients were excluded from the study. Out of 20 excluded cases, eight patients already underwent repeat TACE elsewhere, seven patients had significant main portal vein thrombus and five patients had the extrahepatic disease at the time of presentation. In total, 30 patients met the inclusion criteria and considered for the evaluation in the present study. In this study, it was observed in the baseline characteristics 18 out of 30 cases TACE was performed for patients with tumour size more than 10 cm. Since there is a dearth of information in literature on TACE in HCC larger than 10 cm, the current study remains unique. Tumour size is an important factor in deciding the outcome of TACE. Even though there is no cut-off above which TACE cannot be done, large lesions will leave small normal residual liver, which makes prognosis poor (20). Patients with large tumours carry worst prognosis compared to patients with tumour size less than 5 cm (19),(20). The same was observed in the current study where it was seen that smaller the tumour size then the complete response was highest (50% for <5 cm diameter) and as the tumour size increased there was a reduction in response (16.67% for 5-10 cm diameter and 0% for >10 cm diameter). For larger tumour (>10 cm diameter),11% patient each had disease progression and death which was completely absent in tumour <5 cm in diameter. In a different study Peng ZW et al., reported use of TACE with RFA for lesion around 7 cm with a good outcome, compared to TACE alone (21). However due to non-availability of RFA in this institute, this method was not employed, however, all of the cases received sorafenib after TACE. Even if the TACE achieves good local necrosis, high recurrence rates in these large tumours inhibit overall survival rates. Tumour revascularisation with blood supply from extrahepatic circulation after TACE along with HCC cell proliferation may accelerate tumour recurrence or progression (22),(23),(24),(25),(26),(27). Additionally, sorafenib may block HCC proliferation by inducing tumour cell apoptosis in malignant cells that remain after TACE, which may increase recurrence-free survival (28). In the present study though 28% Patient had segmental portal vein thrombus; it did not affect the tumour responses after the treatment. Similar results reported by Chan LL et al., who determined that segmental portal vein thrombus in HCC did not affect the overall outcome (20). The AFP is an important prognostication factor and its level is associated with tumour activity in HCC and its increasing level after TACE is associated with recurrence or residual disease (29). In this study, 70% (21 of the 30 cases) of cases had elevated AFP (>400 ng/mL). Of these, 14% cases with size less than 5 cm and 10% cases with size 5-10 cm showed recurrence at six months, rest of the 76% cases with size more than 10 cm, showed partial response in 9% cases, progressive disease in 29% cases, stable disease in 29% cases and death in 9% cases at the end of 15 months. These results confirmed that higher AFP levels are associated with poor prognosis. Current conclusion is in the same line with the outcome of a study carried out by Zhu K et al., where they have observed that cases with elevated AFP >400 ng/mL, carried worse overall median survival compared to those with normal AFP (19). The hypoxia induced by TACE may activate Hypoxia Inducible Factor-1alfa (HIF-1afla)/Vascular Endothelial Growth Factor A (VEGFA) pathway (22),(24). However, sorafenib has been reported to suppress HIF-1afla/VEGFA expression (28), and thus suppresses the rapid progression of residual HCC cells (23),(25), increasing the overall recurrence free survival in patients taking sorafenib. The present study showed that combination of sorafenib with TACE in patients with large tumour was safe with minimal tolerable side effects and is comparable with previous studies (30),(31),(32). None of the cases in this study developed on the table or immediate postprocedure complications. Even though the majority of the case were having tumour more than 10 cm, none of the cases developed hepatic dysfunction due to the procedure. This is attributed to selective infusion of chemotherapy emulsion into feeding vessels only, sparing the vessels supplying the normal liver. Limitation(s) The option of using Radiofrequency Ablation (RFA) for larger cases was not available. There was no adequate information supporting the utilisation of TACE alone or TACE with sorafenib in tumours bigger than 10 cm. There is no standard treatment protocol to be used for follow-up cases, the decision on the treatment option was according to the patient condition, ECOG status, child-pugh score and tumour response on imaging. Finally, for the study patients were followed-up for only 15 months. | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
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Original article / research
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