Ignite Creation Date:
2024-05-05 @ 12:04 PM
Last Modification Date:
2024-10-26 @ 9:20 AM
Study NCT ID:
NCT00234182
Status:
COMPLETED
Last Update Posted:
2005-12-01
First Post:
2005-10-05
Brief Title:
Postoperative Adjuvant Therapy With Recombinant Interferon-Alpha Following Curative Resection of HCC
Sponsor:
The University of Hong Kong
Organization:
The University of Hong Kong
Study Overview
Official Title:
Postoperative Adjuvant Therapy With Recombinant Interferon-Alpha Following Curative Resection of Hepatocellular Carcinoma a Randomized Controlled Trial
Status:
COMPLETED
Status Verified Date:
2005-10
Last Known Status:
None
Delayed Posting:
No
If Stopped, Why?:
Not Stopped
Has Expanded Access:
False
If Expanded Access, NCT#:
N/A
Has Expanded Access, NCT# Status:
N/A
Acronym:
None
Brief Summary:
We conducted a randomized controlled trial of adjuvant interferon therapy in patients with predominantly hepatitis B-related hepatocellular carcinoma HCC to investigate whether the prognosis after hepatic resection could be improved Since February 1999 patients with no residual disease after hepatic resection for HCC were randomly assigned with stratification by pTNM stage to receive no treatment control group interferon alpha-2b 10 MIUm2 IFN-I group or 30 MIUm2 IFN-II group thrice weekly for 16 weeks Enrollment to the IFN-II group was terminated from January 2000 because adverse effects resulted in treatment discontinuation in the first 6 patients By June 2002 40 patients each had been enrolled into the control group and IFN-I group The baseline clinical laboratory and tumor characteristics of both groups were comparable The 1- and 5-year survival rates were 85 and 61 respectively for the control group and 97 and 79 respectively for the IFN-I group P0137 After adjusting for the confounding prognostic factors in a Cox model the relative risk of death for interferon treatment was 042 95 CI 017 - 105 P0063 Exploratory subset analysis showed that adjuvant interferon had no survival benefit for pTNM stage III tumor 5-year survival 90 in both groups P0917 but prevented early recurrence and improved the 5-year survival of patients with stage IIIIVA tumor from 24 to 68 P0038 In conclusion in a group of patients with predominantly hepatitis B-related HCC adjuvant interferon therapy prevented early recurrence and improved survival in those with pTNM stage IIIIVA tumors
Detailed Description:
1 Background
Hepatocellular carcinoma HCC is the second commonest cause of cancer death in Hong Kong and the majority are hepatitis B related Hepatic resection has remained the only therapeutic option that can offer these patients a chance of long-term survival Although the safety of hepatectomy has improved postoperative recurrences are frequent Depending on the size of the primary tumors recent reports from Japan France and Hong Kong1 showed that the postoperative recurrence rate was 20 to 64 at one year and 57 to 81 at 3 years
While the hepatic remnant is the predominant site of recurrence involvement of extrahepatic organs was not infrequent There are three possible mechanisms for the development of recurrent disease
i residual tumor cells due to an inadequate resection margin ii subclinical metastasis that occurs before or during hepatic resection iii metachronous multicentric hepatocarcinogenesis which may be related to the underlying necroinflammation of chronic active hepatitis and oncogenic activities of hepatitis viruses
The surgeons attempt to prevent recurrence by more extensive resection is prohibited by the need to preserve hepatic function Futhermore even a major hepatic resection cannot guarantee freedom from recurrence since metachronous multicentric tumors can develop in the entire liver Theorectically total hepatectomy and liver transplantation removes both the subclinical metastases in the liver and prevent metachronous lesions Unfortunately with immunosuppressive therapy recurrences are frequent and tumors grow more rapidly thus illustrating the importance of the host immune surveillance in preventing the development of recurrence
The use of postoperative regional and systemic chemotherapy has been reported Although retrospective studies have shown encouraging results there are only limited number of prospective trials The favourable result of the use of oral 1-hexylcarbomyl-5-fluorouracil in a multi-center trial as reported by Yamamoto and colleagues was questionable since treatment was suspended due to side-effects in 44 of the patients Our single-center prospective randomised study performed at Queen Mary Hospital QMH using a combination of transarterial chemoembolisation and systemic epirubicin showed a higher extrahepatic recurrence rate and worse outcome with the use of adjuvant chemotherapy The reasons for the failure of adjuvant chemotherapy include
i HCC is slow-growing and hence cytotoxic drug resistant ii the associated liver cirrhosis limits the maximum tolerated intensity of chemotherapy iii the anticancer agents may adversely affect the host immunity
2 Interferon alpha-2b
Interferon alpha-2b is a recombinant form of human interferon Interferons are cytokines possessing anti-viral anti-proliferative and immunodulatory effects Interferon may halt the replication of both hepatitis B and hepatitis C virus thus reducing the severity of the chronic active hepatitis The histologic activity of chronic active hepatitis is an important risk factor for recurrence related to metachronous multicentric hepatocarcinogenesis and the use of interferon has been shown to reduce the incidence of HCC in patients with cirrhosis due to hepatitis C and possibly hepatitis B
Interferon has a powerful anti-proliferative effect on hepatoma cell-line PLCPRF5 in a dose-dependent manner both in-vitro and in-vivo The use of interferon has been applied to patients with inoperable HCC with a tumour regression rate and survival rate superior to that of placebo-control or chemotherapeutic agents such as doxorubicin
Peripheral blood mononuclear cells from patients with HCC have considerably reduced cytotoxicity against hepatoma cell lines Interferon has been shown to normalise the T-lymphocyte subpopullation and enhance the cytotoxic activity against an HBsAg-producing hepatoma cell line in-vitro
3 Interferon adverse effects
Interferon alpha-2b is registered for treatment of HCC and chronic hepatitis B in Hong Kong In patients with unresectable HCC interferon has a much lower incidence of fatal side-effects when compared to doxorubicin Most patients experience flu-like symptoms including fever headache fatigue and myalgia which usually subside spontaneously with continuation of treatment Less common but more serious adverse effects include alopecia leukopenia thrombocytopenia depression irritability and mental deterioration The adverse effects are dose-dependent and the majority are reversible with a reduction in dosage The use of high-dose interferon has been well-tolerated in clinical trials involving patients with unresectable HCC
4 Rationale
Interferon has anti-viral anti-proliferative and immunodulatory activities It has been used clinically in the treatment of unresectable HCC as well as viral hepatitis B and C It can potentially reduce the incidence of recurrence due to residual tumour cells or metachronous multicentric disease in patients after resection for HCC
Hepatocellular carcinoma HCC is the second commonest cause of cancer death in Hong Kong and the majority are hepatitis B related Hepatic resection has remained the only therapeutic option that can offer these patients a chance of long-term survival Although the safety of hepatectomy has improved postoperative recurrences are frequent Depending on the size of the primary tumors recent reports from Japan France and Hong Kong1 showed that the postoperative recurrence rate was 20 to 64 at one year and 57 to 81 at 3 years
While the hepatic remnant is the predominant site of recurrence involvement of extrahepatic organs was not infrequent There are three possible mechanisms for the development of recurrent disease
i residual tumor cells due to an inadequate resection margin ii subclinical metastasis that occurs before or during hepatic resection iii metachronous multicentric hepatocarcinogenesis which may be related to the underlying necroinflammation of chronic active hepatitis and oncogenic activities of hepatitis viruses
The surgeons attempt to prevent recurrence by more extensive resection is prohibited by the need to preserve hepatic function Futhermore even a major hepatic resection cannot guarantee freedom from recurrence since metachronous multicentric tumors can develop in the entire liver Theorectically total hepatectomy and liver transplantation removes both the subclinical metastases in the liver and prevent metachronous lesions Unfortunately with immunosuppressive therapy recurrences are frequent and tumors grow more rapidly thus illustrating the importance of the host immune surveillance in preventing the development of recurrence
The use of postoperative regional and systemic chemotherapy has been reported Although retrospective studies have shown encouraging results there are only limited number of prospective trials The favourable result of the use of oral 1-hexylcarbomyl-5-fluorouracil in a multi-center trial as reported by Yamamoto and colleagues was questionable since treatment was suspended due to side-effects in 44 of the patients Our single-center prospective randomised study performed at Queen Mary Hospital QMH using a combination of transarterial chemoembolisation and systemic epirubicin showed a higher extrahepatic recurrence rate and worse outcome with the use of adjuvant chemotherapy The reasons for the failure of adjuvant chemotherapy include
i HCC is slow-growing and hence cytotoxic drug resistant ii the associated liver cirrhosis limits the maximum tolerated intensity of chemotherapy iii the anticancer agents may adversely affect the host immunity
2 Interferon alpha-2b
Interferon alpha-2b is a recombinant form of human interferon Interferons are cytokines possessing anti-viral anti-proliferative and immunodulatory effects Interferon may halt the replication of both hepatitis B and hepatitis C virus thus reducing the severity of the chronic active hepatitis The histologic activity of chronic active hepatitis is an important risk factor for recurrence related to metachronous multicentric hepatocarcinogenesis and the use of interferon has been shown to reduce the incidence of HCC in patients with cirrhosis due to hepatitis C and possibly hepatitis B
Interferon has a powerful anti-proliferative effect on hepatoma cell-line PLCPRF5 in a dose-dependent manner both in-vitro and in-vivo The use of interferon has been applied to patients with inoperable HCC with a tumour regression rate and survival rate superior to that of placebo-control or chemotherapeutic agents such as doxorubicin
Peripheral blood mononuclear cells from patients with HCC have considerably reduced cytotoxicity against hepatoma cell lines Interferon has been shown to normalise the T-lymphocyte subpopullation and enhance the cytotoxic activity against an HBsAg-producing hepatoma cell line in-vitro
3 Interferon adverse effects
Interferon alpha-2b is registered for treatment of HCC and chronic hepatitis B in Hong Kong In patients with unresectable HCC interferon has a much lower incidence of fatal side-effects when compared to doxorubicin Most patients experience flu-like symptoms including fever headache fatigue and myalgia which usually subside spontaneously with continuation of treatment Less common but more serious adverse effects include alopecia leukopenia thrombocytopenia depression irritability and mental deterioration The adverse effects are dose-dependent and the majority are reversible with a reduction in dosage The use of high-dose interferon has been well-tolerated in clinical trials involving patients with unresectable HCC
4 Rationale
Interferon has anti-viral anti-proliferative and immunodulatory activities It has been used clinically in the treatment of unresectable HCC as well as viral hepatitis B and C It can potentially reduce the incidence of recurrence due to residual tumour cells or metachronous multicentric disease in patients after resection for HCC
Study Oversight
Has Oversight DMC:
None
Is a FDA Regulated Drug?:
None
Is a FDA Regulated Device?:
None
Is an Unapproved Device?:
None
Is a PPSD?:
None
Is a US Export?:
None
Is an FDA AA801 Violation?:
None