Introduction
Hepatitis B virus (HBV) infection is a serious and
common global public health problem (1). It is conservatively estimated that >2
billion individuals have been infected with HBV worldwide and 350
million have suffered from chronic HBV infection. In Asia and the
majority of Africa, the disease is particularly prevalent and
usually acquired perinatally or in childhood (1). In total, 15–40% of the infected patients
will develop cirrhosis, liver failure or hepatocellular carcinoma
(HCC), which is currently the fifth most frequent cancer and
accounts for between 300,000 and 500,000 mortalities per year
(2).
Curative surgery is currently available for only 10%
of patients. Due to the low tolerance of the liver for irradiation,
radiotherapy is limited and is therefore not optimal for the
treatment of HCC (3). Therefore,
chemotherapy has become a main palliative treatment for certain
inoperable patients. However, there is a considerable probability
for the reactivation of HBV in HCC patients that receive
chemotherapeutic drugs, which may be a fatal complication and may
lead to disruption in treatment schedules (4). With the development of novel
radiotherapy as 3-dimensional conformal therapy or stereotactic
radiation therapy, the role of radiotherapy has become of
increasing importance in the treatment of HCC, particularly for HCC
patients with portal vein tumor thrombus (PVTT) or a tumor diameter
<10 cm (3–5).
To the best of our knowledge, previous studies have
reported the occurrence of chemotherapy-associated reactivation of
HBV in the literature (6,7). However, the occurrence of
radiotherapy-associated HBV reactivation is rare. Therefore, the
present study reports the case of a patient that experienced fatal
HBV reactivation during radiotherapy for HCC with portal vein tumor
thrombosis (PVTT) formation.
Case report
A 46-year-old male patient with a long history as a
HBV carrier presented with fatigue, yellow sclera and abdominal
distension that had lasted for >10 days was referred to the
First Affiliated Hospital of Anhui Medical University (Hefei,
Anhui, China) on June 26, 2012. The patient possessed a family
history of chronic HBV infection and a history of alcohol abuse.
The patient had been diagnosed with HBV-associated HCC at the First
Affiliated Hospital of Zhengzhou University (Zhengzhou, Henan,
China) in April 2012.
Abdominal computed tomography with contrast medium
revealed a left frontal tumor, 8.7 cm in diameter, in the liver
with PVTT. The total liver volume of the patient was 1617.4
cm3 and the gross tumor volume was 352.7 cm3.
The patient was identified to possess the following pattern of HBV
markers: Hepatitis B surface antigen (HBsAg)-positive;
anti-hepatitis B surface antibody (HBsAb)-negative; hepatitis B
envelope antigen (HBeAg)-negative; anti hepatitis B envelope
antibody (HBeAb)-positive; and anti hepatitis B core antibody
(HBcAb)-positive. The quantitative polymerase chain reaction (qPCR)
level of HBV-DNA remained undetectable. The biochemical analyses of
liver function tests revealed normal function, as follows: Alanine
aminotransferase (ALT), 26 U/l (normal, 7–40 U/l); aspartate
aminotransferase (AST), 20 U/l (normal, 13–35 U/l); total bilirubin
(TB), 17.34 µmol/l (normal, 5–19 µmol/l); and prothrombin time
(PT), 15.6 sec (normal, 11–16 sec). The patient received
prophylactic antiviral therapy with oral administration of the
nucleoside analog entecavir (0.5 mg/day over 8 weeks) in addition
to undergoing radiotherapy, commencing on May 1, 2012. The patient
was administered with a daily fraction of 2 Gy, up to a total
radiation dose of ~50 Gy over 5 weeks.
On June 26, 2012, ~8 weeks subsequent to the first
dose of radiotherapy, the patient was admitted to the Department of
Infectious Diseases at the First Affiliated Hospital of Anhui
Medical University due to fatigue, yellow sclera and abdominal
distension that had lasted >10 days. The liver function tests
revealed severe liver dysfunction, as follows: Albumin, 29.3 g/l
(normal, 40–50 g/l); ALT, 741 U/l (normal, 7–40 U/l); AST, 405 U/l
(normal, 13–35 U/l); TB, 356.15 µmol/l (normal, 5–19 µmol/l); and
PT, 57.5 sec (normal, 11–16 sec). The HBV serology status continued
to indicate that the patient was HBsAg-positive, HBeAb-positive,
HBcAb-positive, HBsAb-negative and HBeAg-negative. However, the
detectable qPCR level of HBV-DNA was 7.2×104 copies/ml.
The laboratory characteristics for infection with the hepatitis A,
C, D or E viruses were absent. As entecavir demonstrates few
side-effects on liver function, the nucleoside analogue was not
considered to be the cause of the changes in liver function.
On the basis of the symptoms, physical signs and
laboratory examination, the patient was diagnosed with
acute-on-chronic liver failure resulting from the reactivation of
HBV. The patient received prompt symptomatic and supportive
treatment for liver dysfunction in addition to active antiviral
therapy. The duration of antiviral therapy was ~8 weeks from May
2012. However, the liver failure was further aggravated by the HBV
reactivation. The breathing and circulation of the patient
gradually weakened; on June 27, the second day subsequent to
admission, the patient demonstrated acute thoracodynia, dyspnea and
mania. The blood gas analysis revealed a PaO2 level of
55 mmHg, PaCO2 level of 30 mmHg and
PA-aO2 level of 0.86 kPa. The patient
succumbed to HBV reactivation at 3 weeks after the end of
radiotherapy.
Discussion
HBV reactivation is a common problem that clinicians
often encounter following chemotherapy or immunosuppressive therapy
for disorders including hematological or solid malignancies,
rheumatism and systemic lupus erythematosus.
Chemotherapy-associated reactivation has been well described in the
literature. Induced immunosuppression facilitates an increased
viral load and antigen expression. Upon recovery of the immunity of
the patient subsequent to treatment withdrawal or reduction, there
is an intense immune-mediated response that eradicates HBV-infected
hepatocytes and manifests clinically as asymptomatic anicteric
hepatitis, severe hepatitis or even fatal liver failure (8). The aforementioned hypothesis may not
apply to the pathogenesis of radiation-induced HBV reactivation due
to the differences between radiotherapy and chemotherapy, and since
radiotherapy usually exerts an increased effect on local tissue
rather than the whole immune system.
HBV reactivation is a severe complication that
occurs in patients with HCC that undergo radiotherapy, and it may
occasionally be fatal. Although the present patient with HCC was
treatment with entecavir in addition to radiotherapy,
radiation-induced HBV reactivation occurred and led to the
development of liver failure. The mortality rate directly due to
HBV reactivation has been reported as ~60% in previous studies
(7,9–11).
Therefore, awareness of this potentially life-threatening
complication and regular monitoring of the clinical parameters
associated with HBV reactivation during thermotherapy or
radiotherapy are of considerable importance (12). To the best of our knowledge, HBV
reactivation during chemotherapy is associated with baseline
HBV-DNA levels and HBeAg positivity. Few studies have investigated
the risk factors and incidence of HBV reactivation in patients with
HBV-associated HCC undergoing radiotherapy (13). However, a recent study reports that
the serum HBV-DNA level and certain dosimetric parameters, such as
normal liver volume, gross tumor volume and mean radiological dose,
acted as prognosis factors for HBV reactivation and should be
considered carefully prior to radiotherapy (14).
The present study indicated that preemptively
prophylactic administration of entecavir prior to the performance
of radiotherapy may be proposed as a first-line preventive therapy
in patients with HCC that are inactive carriers of HBV, rather than
as a preventive therapy once radiotherapy has commenced or as a
rescue therapy when HBV reactivation has occurred. The optimal
duration of entecavir administration for the prevention of
radiotherapy-induced HBV reactivation has yet to be clarified. In
the future, large prospective and case-controlled studies should be
performed to determine the optimal duration. A previous study
reported that an increased and persistent interleukin (IL)-6
density in the liver was evident following radiotherapy. IL-6 was
released from irradiated endothelial cells and induce HBV
reactivation in vitro and in vivo through the
bystander effect. The signal transducer and activator of
transcription 3 signaling pathway mainly plays an important role in
this phenomenon reported from the literature (13). As a result, the additional studies are
also required to delineate the precise mechanism on HBV
reactivation subsequent to radiotherapy.
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