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. 2021 Nov 3;13:8273–8279. doi: 10.2147/CMAR.S334171

Efficacy and Safety of Interferon-Alpha 2b for Patients with Hepatic Epithelioid Hemangioendothelioma: Outcomes of a Case-Series Analysis

Xiaolei Liu 1, Zihuan Zhang 1, Jia Huang 1, Haidong Tan 1, Zhiying Yang 1,
PMCID: PMC8572744  PMID: 34764690

Abstract

Background

Hepatic epithelioid hemangioendothelioma (HEH) is a rare tumor type. No effective medicine or standard treatment for HEH has been established.

Patients and Methods

From March 2014 to April 2021, 62 patients with pathologically diagnosed HEH were observed regularly, and interferon-alpha 2b (IFN-a 2b) was administered to patients with progressive disease or reoccurrence. Adverse events (AEs) were assessed and recorded, and a tumor assessment scan was performed every 3 months.

Results

A total of 42 patients with HEH received IFN-a 2b treatment in this study. No severe (grade ≥3) AEs were reported in the group overall. The most common treatment-related AEs in patients receiving IFN-a 2b were fever (50.0%) and fatigue (21.4%). Partial response and complete response were achieved in 20 patients (47.6%) and 2 patients (4.8%), respectively, and the objective response rate was 52.4%. Stable disease was observed in 12 patients (28.6%), and the disease control rate was 81.0%. Progressive disease was observed in 8 patients (19.0%). The 1-, 3-, and 5-year progression-free survival rates were 81.0%, 69.2%, and 62.3%, respectively. Only 1 patient died as a result of disease progression during the study. The 1-, 3-, and 5-year overall survival rates were 100%, 97.2%, and 97.2%, respectively.

Conclusion

IFN-a 2b is a safe and effective treatment for patients with HEH. The encouraging results with IFN-a 2b use make it a promising option for patients who have other types of epithelioid hemangioendothelioma; additional clinical trials are needed.

Keywords: liver, epithelioid hemangioendothelioma, interferon, sarcoma, chemotherapy

Introduction

Epithelioid hemangioendothelioma (EH) was initially described in 1982 by Weiss and Enzinger;1 it can involve both soft tissues and visceral organs, including the liver, lung, spleen, and heart. Hepatic EH (HEH) is an extremely rare tumor type (estimated incidence of less than 1 in 1,000,000 worldwide) with a clinical course intermediately between benign hemangioma and angiosarcoma.2 Surgical resection, liver transplantation, chemotherapy, and immunotherapy have all been implemented in patients with HEH. However, because of the scarcity of the disease and the difficulty of including patients, prospective clinical trials are very hard to conduct. Liver transplantation has reportedly achieved satisfying long-term survival for patients with HEH.3–7 However, organ donation shortages limit the accessibility of liver transplantation for most patients with HEH unless they are in critical condition. Clinical studies of surgical resection, anti-angiogenesis drugs, chemotherapy, or transarterial embolization (TAE) have reported indeterminate results.8–11 At present, no effective medicine or standard treatment has been established yet for patients with HEH.

Interferon-alpha 2b (IFN-a 2b) as an immunotherapy has been used to treat hematological malignancies.12 IFN-a therapy for EH has also been proposed for tumor reduction and metastasis prevention.9,13,14 Since 2014, our team has been investigating patients with HEH, and 62 patients are under regular follow-up now. According to our previous retrospective study, IFN-a 2b showed effective responses in patients with HEH.15 After we observed a clinically responsive outcome, we suggested IFN-a 2b treatment to patients with HEH progression or reoccurrence. This study aimed to report the clinical outcomes after IFN-a 2b treatment in patients with HEH.

Patients and Methods

From March 2014 to April 2021, 62 patients with histologically diagnosed HEH (53 patients diagnosed by liver biopsy and 9 patients, by surgery) were involved in the study and were observed regularly. Our previous retrospective study showed a responsive effect of IFN-a 2b in patients with HEH.15 IFN-a 2b was suggested to patients who experienced disease progressive disease (PD) or reoccurrence after previous treatment, for whom no other effective medicine was eligible. Patients who accepted the suggestion received 3 million units of IFN-a 2b by subcutaneous injection once every other day. Tolerability and safety were assessed each month by interviewing patients and monitoring the blood cell counts as well as the liver, thyroid, and renal functions until month 6 and then every 3 months. A tumor assessment scan, including computed tomography (CT) and magnetic resonance imaging (MRI), was performed every 3 months, and the tumor status was assessed according to the Response Evaluation Criteria in Solid Tumors Committee (RECIST).16 Treatment was continued until disease progression occurred, unacceptable toxicity developed, or patients decided to terminate the medication. For patients who had HEH with extrahepatic metastases, the tumor assessment was based on the intrahepatic lesions. Safety assessments consisted of the monitoring and recording of adverse events (AEs) according to Common Terminology Criteria for Adverse Events version 4.03, laboratory evaluations, and vital signs. Patients with HEH who did not receive IFN-a 2b treatment were observed regularly to record disease management and outcomes.

Informed consent forms were signed by all the patients who accepted the IFN-a 2b treatment. The study protocol was approved by the ethics committee of the China-Japan Friendship Hospital, and the study was conducted in accordance with the principles of the Declaration of Helsinki and Good Clinical Practice Guidelines.

Statistical Analysis

Descriptive statistics were used to summarize patient characteristics. Progression-free survival (PFS) and overall survival (OS) were estimated using the Kaplan-Meier method. PFS was calculated from the start of IFN-a 2b treatment to the first evidence of PD. OS was calculated from the start of IFN-a 2b treatment to the time of death from any cause or last follow-up. Patients who remained alive or who were lost to follow-up had their data censored at the last contact. All statistical analyses were performed using SAS version 9.4 (SAS Institute, Cary, NC).

Results

Patients

Overall, a total of 62 patients with HEH were regularly observed in our clinic. Ten patients chose to maintain observation without treatment, and 6 patients without reoccurrence after surgery were observed regularly. Four patients chose targeted therapy (2 received apatinib; 1, sorafenib; and 1, sunitinib). Forty-two patients with HEH that progressed or recurred received IFN-a 2b treatment, including 25 patients with tumor progression during observation, 11 patients with recurrence after curatively intended surgery or radiofrequency ablation, and 6 patients with tumor progression after chemotherapy or TAE (Table S1). The median age of patients who received IFN-a 2b was 36 years (range, 18–65 years), and genders were almost equally distributed (52.4% were men and 47.6% were women). The median time between diagnosis and initiation of IFN-a 2b treatment was 9 months (range, 2–57 months).

At baseline, all 42 patients had an Eastern Cooperative Oncology Group performance status (ECOG PS) of 0 and no severe liver injury. Mild abdominal pain occurred in 9 patients, but no other symptom was recorded. Extrahepatic metastases were detected in 23 patients, and 50% patients had lung metastases (Table 1).

Table 1.

Baseline Demographic and Clinical Characteristics of Patients with IFN-a 2b (N=42)

Characteristics No. (%)
Age, years
 Median 36
 Range 18–65
Gender
 Male 22 (52.4)
 Female 20 (47.6)
Symptoms
 Abdominal pain 9 (21.4%)
 None 33 (78.6%)
Number of intrahepatic lesions
 Multiple 40 (95.2)
 Solitary 2 (4.8)
Involved disease sites
 Lung 21 (50.0)
 Bone 2 (4.8)
 Spleen 1 (2.4)
 Abdomen 1 (2.4)
 None 19 (45.2)
Inclusion reasons
 Progression with no treatment 25 (59.5)
 Reoccurrence after surgery or RF 11 (26.2)
 Failure of previous treatment 6 (14.3)
ECOG PS
 0 42 (100)
 1 0 (0)
Range (median) serum liver function
 (ALT), U/L 16–79 (24)
 (AST), U/L 8–83 (25)
 (ALP), U/L 25–226 (93)
 (GGT), U/L 7–177 (41)
 (Range of TB), μmol/L 9.4–44.8 (12.7)
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Abbreviations: ALP, alkaline phosphatase; ALT, alanine aminotransferase; AST, aspartate aminotransferase; ECOG PS, Eastern Cooperative Oncology Group performance status; GGT, gamma-glutamyl transpeptidase; IFN-a 2b, interferon-alpha 2b; RF, radiofrequency ablation; TB, total bilirubin.

Safety of IFN-a 2b

No severe (grade ≥3) AEs from IFN-a 2b were recorded in the group. The most common treatment-related AEs were fever (50.0%) and fatigue (21.4%). Fever occurred most often after the first several shots and disappeared within 1 month. Lasting fever was not recorded. Other AEs included leukopenia, thrombocytopenia, alopecia, rash, decreased appetite, anemia, and hypothyroidism (Table 2). Two patients had grade 2 hypothyroidism, and one patient had grade 2 leukopenia and thrombocytopenia. Thirteen patients (31.0%) had no treatment-related AEs. No patients had treatment-related AEs that led to the interruption of IFN-a 2b therapy.

Table 2.

Treatment-Related Adverse Events with IFN-a 2b (N=42)

Adverse Events No. (%)
Any Grade Grade 1 Grade 2
Fever 21 (50.0) 21 (50) 0
Fatigue 9 (21.4) 9 (21.4) 0
Leukopenia 2 (4.8) 1 (2.4) 1 (2.4)
Thrombopenia 2 (4.8) 1 (2.4) 1 (2.4)
Rash 2 (4.8) 2 (4.8) 0
Alopecia 2 (4.8) 2 (4.8) 0
Hypothyroidism 2 (4.8) 0 2 (4.8)
Decreased appetite 1 (2.4) 1 (2.4) 0
Anemia 1 (2.4) 1 (2.4) 0
None 13 (31.0) / /
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Abbreviation: IFN-a 2b, interferon-alpha 2b.

Efficacy of IFN-a 2b

The median follow-up time after IFN-a 2b initiation was 33 months (range, 3–76 months). The median duration of IFN-a 2b treatment was 19 months (range, 3–48 months). In the 42 IFN-treated patients, partial response (PR) and complete response (CR) were achieved in 20 patients (47.6%) and 2 patients (4.8%), respectively, and the objective response rate (ORR) was 52.4% (Figures 1 and 2). The median time from the start of IFN-a 2b to observation of tumor regression was 10 months (range, 3–22 months). Stable disease (SD) was observed in 12 patients (28.6%), and the disease control rate (DCR) was 81.0%. PD was observed in 8 patients (19.0%) (Figure S1).

Figure 1.

Figure 1

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The complete response to interferon-alpha 2b (IFN-a 2b) is illustrated in a female patient who had progressive disease after treatment with transarterial embolization (TAE). (A) Contrast-enhanced computed tomography (CT) scan reveals multiple intrahepatic lesions. (B) After TAE, intrahepatic tumors progressed (marked with white arrows), and new lesions occurred (marked with red arrows). Then, IFN-a 2b treatment started. (C) Ten months after initiation of IFN-a 2b treatment, the size of tumors had decreased significantly (marked with black arrows). (D) Eighteen months after initiation of IFN-a 2b treatment, the intrahepatic tumors disappeared.

Figure 2.

Figure 2

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The partial response to interferon-alpha 2b (IFN-a 2b) is illustrated in a male patient who experienced disease reoccurrence after surgery. (A) Small lesions were found 18 months after surgery. (B) Intrahepatic lesions (marked with white arrows) progressed after 12 months of observation. (C) Intrahepatic lesions (marked with white arrows) continued to progress after 24 months of observation, and IFN-a 2b was treatment started. (D) Fifteen months after initiation of IFN-a 2b treatment, the size of tumors decreased (marked with black arrows).

Of the 34 patients with disease control, treatment of IFN-a 2b was terminated in 21 patients (PR, n=14; CR, n=2; SD, n=5), and all terminations except those in the 2 patients with CR were conducted in accordance with patient decisions. IFN-a 2b treatment was continued in 13 patients (PR, n=6; SD, n=7). Of the 8 patients with PD, targeted therapy was used in 4 patients, and the other patients chose observation only.

PD was detected in 4 of the 21 patients who stopped IFN-a 2b treatment; PD occurred 10, 12, 12, and 36 months after the termination of IFN-a 2b for each patient, respectively. The 1-, 3-, and 5-year PFS rates were 81.0%, 69.2%, and 62.3%, respectively. Only one patient died as a result of disease progression during the study. The 1-, 3-, and 5-year OS rates were 100%, 97.2%, and 97.2%, respectively. The flowchart and brief results of this study were depicted in Figure 3. Detailed outcomes information and radiological changes are provided in the Table S1 and Figure S1.

Figure 3.

Figure 3

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The flowchart and brief results of this study.

Abbreviations: HEH, hepatic epithelioid hemangioendothelioma; CR, complete response; PR, partial response; SD, stable disease; PD, progressive disease.

Discussion

HEH is an extremely rare hepatic tumor with varying biological behavior. Currently, there is no effective indicator to predict the malignancy. For most patients with HEH, the tumor progresses slowly and no severe clinical symptoms manifest. Because of the rarity of the disease, patients with HEH are commonly misdiagnosed as having metastatic carcinoma. Although several studies have reported the radiological characteristics of HEH,17–20 a confirmed diagnosis still relies on histological examination.

No standard treatment has been established for HEH yet. Liver transplantation was reportedly effective, with acceptable long-term outcomes.4,7,21,22 However, the scarcity of organ donation limits the accessibility of liver transplantation for patients with HEH. Surgical resection is another treatment option, but the long-term results have been poor.23–25 Moreover, curative surgery is implausible for most patients with HEH because of the multicentricity of the tumor. Studies of chemotherapy, targeted therapy, or immunotherapy have reported indeterminate results.10,26–33 Thalidomide as anti-angiogenic therapy has reportedly controlled tumor progression, but a tumor response has seldom been achieved.8,34–37 Recently, a retrospective study of 38 patients with EH showed that sirolimus was an effective treatment, and PD was achieved in 75.7% of patients.38 Similar results have been reported using sirolimus in pediatric patients with EH.39 However, the molecular mechanism remains unclear.

IFN-a 2b as an immunotherapy has been used to treat hematological malignancies.12 IFN-a therapy for EH has also been proposed for tumor reduction and metastasis prevention.9,13,14 Kayler et al40 reported that IFN-α was used to treat a metastatic HEH after liver transplantation. Antiproliferative activity of IFN-A, resulting from cancer cell growth inhibition, activation of immune cells, inhibition of vascularization, and induction of cytokines, has also been reported.12,41 Moreover, in our previous retrospective study, IFN-a 2b achieved an effective response in 6 patients with HEH (PR, n=4; CR, n=1; SD, n=1), which suggests that it is a promising treatment option.15 However, all the previous studies were case reports, and no long-term results of IFN-a 2b treatment for a large group of patients with HEH have been reported.

Since 2014, 42 patients with progressive HEH have received IFN-a 2b treatment in this study. PR and CR were observed in 22 patients, and the ORR was 52.4%. SD was observed in 12 patients, and the DCR was 81.0%. To our knowledge, this study indicates that IFN-a 2b is the most effective medicine reported so far for patients with HEH. Moreover, compared with previous studies of liver transplantation that reported a 5-year survival rate of 70–83%,4,7 this study achieved a 5-year survival rate of 97.2% in patients with HEH. Although the median follow-up time in this study was only 33 months, a tendency toward better long-term survival could be speculated. Moreover, the safety of long-term treatment with IFN-a 2b was fully verified. The median duration of IFN-a 2b therapy was 19 months, and no severe (grade ≥3) AEs were recorded. Given the risk of hypothyroidism, the serum level of thyroxin should be monitored regularly in IFN-treated patients. The anti-tumor mechanism of IFN-a 2b is not fully investigated or understood, but the encouraging results of this study provide evidence-based support for its use in HEH. Because EH also develops in other organs, such as lung and bone, additional clinical studies could be designed to verify the effect of IFN-a 2b in other types of EH. Moreover, the combination of IFN-a 2b and sirolimus may be a promising treatment option for patients with HEH, and additional clinical studies to explore this option are needed.

In conclusion, IFN-a 2b is a safe and effective treatment for patients with HEH. Because of the extreme scarcity of the disease, a randomized clinical trial would be unrealistic. Although this was a single-arm study, the results still provided valuable clinical evidence for the treatment of HEH. The encouraging results observed with IFN-a 2b treatment makes it a promising option for other types of EH as well and warrants additional clinical trial investigations.

Acknowledgments

The authors thank all the associated staff of Radiology Department for assisting with the implementation of this study.

Funding Statement

This study has no funding.

Data Sharing Statement

All the detailed information and radiological images are provided in the Table S1 and Figure S1.

Disclosure

The authors declare that they have no conflicts of interest.

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