Rui Li1, Ping Cai2, Kuan-Sheng Ma1, Shi-Yi Ding2, De-Yu Guo3, Xiao-Chu Yan3. 1. Dept. Hepato-biliary-Pancreatic Surgery, Southwest Hospital Affiliated to Third Military Medical University, P. R. China. 2. Dept. Radiology, Southwest Hospital Affiliated to Third Military Medical University, P. R. China. 3. Dept. Pathology, Southwest Hospital Affiliated to Third Military Medical University, P. R. China.
Abstract
This study aimed to assess the features of intrahepatic cholangiocarcinoma (ICC) at computerized tomography (CT) and verify the risk of misdiagnosis of ICC as hepatocellular carcinoma (HCC) in cirrhosis. CT appearances of 98 histologically confirmed ICC nodules from 84 cirrhotic patients were retrospectively reviewed, taking into consideration the pattern and dynamic contrast uptake during the arterial, portal venous and delayed phases. During the arterial phase, 53 nodules (54.1%) showed peripheral rim-like enhancement, 35 (35.7%) hyperenhancement, 9 (9.2%) hypoenhancement and 1 (1.0%) isoenhancement. The ICC nodules showed heterogeneous dynamic contrast patterns, being progressive enhancement in 35 nodules (35.7%), stable enhancement in 28 nodules (28.6%), wash-in and wash-out pattern in 15 nodules (15.3%) and all other enhancement patterns in 20 nodules (20.4%). There were no significant differences in the dynamic vascular patterns of ICC according to nodule size (p > 0.05). ICC in cirrhosis has varied enhancement patterns at contrast-enhanced multiphase multidetector CT. Though the majority of ICC did not display typical radiological hallmarks of HCC, if dynamic CT scan was used as the sole modality for the non-invasive diagnosis of nodules in cirrhosis, the risk of misdiagnosis of ICC for HCC is not negligible.
This study aimed to assess the features of intrahepatic cholangiocarcinoma (ICC) at computerized tomography (CT) and verify the risk of misdiagnosis of ICC as hepatocellular carcinoma (HCC) in cirrhosis. CT appearances of 98 histologically confirmed ICC nodules from 84 cirrhotic patients were retrospectively reviewed, taking into consideration the pattern and dynamic contrast uptake during the arterial, portal venous and delayed phases. During the arterial phase, 53 nodules (54.1%) showed peripheral rim-like enhancement, 35 (35.7%) hyperenhancement, 9 (9.2%) hypoenhancement and 1 (1.0%) isoenhancement. The ICC nodules showed heterogeneous dynamic contrast patterns, being progressive enhancement in 35 nodules (35.7%), stable enhancement in 28 nodules (28.6%), wash-in and wash-out pattern in 15 nodules (15.3%) and all other enhancement patterns in 20 nodules (20.4%). There were no significant differences in the dynamic vascular patterns of ICC according to nodule size (p > 0.05). ICC in cirrhosis has varied enhancement patterns at contrast-enhanced multiphase multidetector CT. Though the majority of ICC did not display typical radiological hallmarks of HCC, if dynamic CT scan was used as the sole modality for the non-invasive diagnosis of nodules in cirrhosis, the risk of misdiagnosis of ICC for HCC is not negligible.
Intrahepatic cholangiocarcinoma (ICC) originating from biliary epithelial cells is the
second most common primary cancer of the liver after hepatocellular carcinoma (HCC) in
patients with cirrhosis. The incidence and mortality of ICC have been rising
internationally1234 and some studies have shown an association
of ICC with cirrhosis567. The prognosis of ICC is dismal with respect
to HCC and the treatment modalities of ICC and HCC are of much difference8. In this context, differential diagnosis between ICC and HCC in cirrhotic patients is
very important for clinical management. According to practice guidelines of the American
Association for the Study of Liver Diseases (AASLD) and the European Association for the
Study of the Liver (EASL), radiological diagnosis of HCC in patients with cirrhosis
relies on either magnetic resonance imaging (MRI) or contrast enhanced computerized
tomography (CT) in the context of a sequential algorithm910,
demonstrating the hallmark of intense arterial uptake followed by venous or delayed
phase washout. Contrast-enhanced computed tomography is now considered a standard of
care for the radiological diagnosis of HCC, this modality, however, is not validated to
exclude ICC in cirrhosis, robust studies on diagnostic accuracy of contrast-enhanced CT
for ICC in cirrhotic liver are not available. Up to now, there were only few reports on
CT appearances of ICC in cirrhosis with limited number of patients,, and more
importantly, the results of these previous studies are contradictory111213. Therefore, the aim of this study was to assess of the
enhancement features of ICC on contrast-enhanced multidetector CT in cirrhotic patients
in relation to size and dynamic enhancement pattern of ICC nodules, and with special
emphasis on differential diagnosis between ICC and HCC in a relatively larger number of
patients.
Materials and Methods
Patients
This retrospective study was approved by the ethics committee of Southwest
hospital and the requirement for informed consent waived. The study protocol
conforms to the ethical guidelines of the 1975 Declaration of Helsinki. Through
the review of our institute database between January 2005 and July 2015. We
enrolled patients with: (1) the diagnosis of ICC had to be pathologically proven
through assessment of biopsy or surgical specimen, excluding mixed
hepatocellular-cholangiocarcinoma; (2) histologically confirmed cirrhosis; (3)
abdominal contrast-enhanced CT performed before biopsy or resection; (4) No
systemic chemotherapy or targeted therapy prior to CT scan.
Liver histology
Histological diagnosis was performed on surgically resected specimens and/or by
biopsy. Ultrasound guided biopsy was performed using a 18 gauge needle (Bard
Peripherals Vascular Inc, Tempe, Arizona 85281, USA) within the nodule and the
surrounding liver parenchyma. Specimens were routinely processed, stained with
hematoxylin and eosin and immunohistochemically for biliary differentiation
markers if necessary. Liver sections were examined by experienced liver
pathologists who were unaware of clinical and radiological exams. Final
pathological diagnosis was made in consensus by experienced pathologists with
over 25 year of liver pathology (XCY and DYG).
Serum tests
Routine exams included blood cell count and serum chemistries were measured by
standard laboratory procedures. Serum alpha-fetoprotein (AFP, Elecsys, Roche
Diagnostics GmbH Sandhofer Strasse, Mannfeim, Germany; normal,
≤20 ng/ml) was tested in all patients. Carbohydrate
antigen 19-9 (Ca 19-9) was also tested in all cases. Serum hepatitis B surface
antigen, antibody to hepatitis surface antigen, antibody to hepatitis delta
virus and antibody to hepatitis C virus were also tested in all patients. To
categorize patients in terms of etiology, a complete medical history, including
alcohol intake, smoking habits and other risk factors for liver disease like
hemochromatosis, non-alcoholic steatohepatitis, autoimmunity, and diabetes were
also recorded.
CT scan
CT-scans were performed with a multidetector-row helical quadruplephase (i.e.,
unenhanced, hepatic arterial, portal, and delayed phases) CT scanner (MDCT;
Definition, Siemens Medical Systems, Erlangen, Germany). First, an unenhanced
scan was obtained through the liver. Next, after intravenous infusion of
80–100 ml of a nonionic iodine-containing contrast agent
(ultravist 370, Scherning AG, Berlin, Germany) using a power injector (Stellant
CT Injection System, Medrad, Indianola, Pennsylvania) at a rate of
4 ml/sec, contrast-enhanced scans were obtained in arterial phase
with bolus test trigger for optimal characterization of focal hepatic lesions.
Data acquisitions were obtained through the whole liver in a craniocaudal
direction during a single breath-hold helical acquisition for 4–6
sec with 5 mm slice thickness and 0.5 s rotation time. The
acquisition of the arterial phase was automatically started 4 s after the
arrival of contrast agent in the aorta. The start of acquisition sequences was
60 s for the portal venous phase and 180 s for the delayed phase from the
beginning of contrast agent injection.CT findings were evaluated blindly by 2 radiologists with over 20 year experience
of liver radiology (PC and SYD) who were blinded to the clinical and
histological results. All imaging films were independently evaluated by both
radiologists whereas discrepant diagnoses were jointly re-evaluated to reach a
final consensus.
Categorization of enhancement patterns at CT
After intravenous contrast administration, the enhancement through each of the
different phases was registered as follows: (1) hyperdense: increased density
involving predominant parts (>50%) of the lesion cross-section area
compared to the surrounding liver parenchyma13; (2) peripherally
hyperdense: increased density limited to the periphery of the lesion, resembling
a rim-like pattern; (3) isodense: same density as the surrounding liver
parenchyma; (4) hypodense: lower density compared to the liver parenchyma
involving predominant parts (>50%) of the cross-sectional area of the
tumor excluding peripheral rim-like enhancement. Dynamic pattern of enhancement
was defined according to the combination of contrast enhancement in the
different phases of the study (arterial, portal venous, delayed-venous), as
follows: (1) stable enhancement: the nodule enhancement is unmodified from the
arterial to the portal venous and delayed phases; (2) progressive contrast
enhancement: the nodule enhances progressively over time, reaching maximal
intensity in delayed phases; (3) “wash-in and wash-out”
enhancement pattern: intense hyperdense during the arterial phase followed by
hypodense in the portal and/or delayed venous phases; (4) all other patterns.
This classification was modified from Iavarone et al.14.
Statistical analysis
Quantitative variables, such as tumor size, age, serum levels of AFP, and Ca19-9,
were expressed as median and range. Qualitative variables like etiology of liver
disease, Child-Pugh score, and number of nodules, were expressed as count and
proportions. Differences in signal intensity in baseline and post-contrast
sequences and in dynamic enhancement pattern according to nodule size were
evaluated by the Chi-squared test/Fisher’s exact test for
categorical variables. A P value of less than 0.05 was considered
statistically significant. Statistical analysis was performed using the SPSS
12.0 software package (SPSS Inc, Chicago, IL).
Results
Characteristics of patients
This search yielded a total of 98 histologically proven ICC in 84 patients with
cirrhosis (66 men; mean 50.6 ± 10.9 years).
Characteristics of patients are summarized in Table 1.
Etiology of cirrhosis was HBV infection in most patients (85.7%). Near half of
the patients were cigarette smokers. Mean AFP level was
148.49 ± 732.88 ng/ml and
elevated in 19 patients (22.6%). Mean CA19-9 was
104.59 ± 166.19 U/ml and
elevated in 43 patients (51.2%). Most patients (89.3%) had a single ICC at
diagnosis. In patients with multiple nodules, each nodule was located in a
different segment thereby excluding the diagnosis of peripheral satellite.
Thirty–eight patients (33.3%) were under semi-annual surveillance at
the time of first diagnosis.
Table 1
Demography of 84 patients with ICC in cirrhosis.
Age median[range] (years)
50 [24 ~ 75]
Gender, male/female, No (%)
66 (78.6)/18 (21.4)
Etiology of cirrhosis, No
(%)
HBV
52 (61.9)
HBV + alcohol
20 (23.8
HCV
0
Alcohol
3 (3.6)
Biliary
1 (1.1)
unknown
8 (9.5)
Diabetes, No (%)
7 (8.3)
Cigarette smokers, No (%)
39 (46.4)
Child-Pugh class A, No (%)
75 (89.3)
AFP (ng/ml) median[range] (ng/ml)
6.3[0.2 ~ 5940.0]
≤20 ng/ml, No (%)
65 (77.4%)
>20 ng/ml, No (%)
19 (22.6)
CA19-9 (U/ml) median[range] (U/ml)
33.5[2.0 ~ 745.7]
≤37 U/ml, No (%)
41 (48.8%)
>37 U/ml, No (%)
43 (51.2%)
Number of nodules
Single nodule, No (%)
75 (89.3)
Multiple nodule, No (%)
9 (10.7)
Nodule size median[range] (cm)
5.3[1.0 ~ 13.6]
≤3 cm, No (%)
21 (20.4)
3.1–5.0 cm, No (%)
27 (27.6)
>5 cm, No (%)
50 (51.0)
No: number; HBV: hepatitis B virus; HCV: hepatitis C virus;
AFP: alpha-fetoprotein.
CA 19-9: carbohydrate antigen 19-9.
CT scan features
The size of ICC detected by CT at diagnosis was
5.6 ± 2.7 cm. Twenty one nodules
(20.4%) were ≤ 3.0 cm while 77 (78.6%)
nodules >3.0 cm. Hepatic capsular retraction was revealed in
11cases (13.1%). Intrahepatic biliary dilatation was observed in 17 patients
(20.2%). Nine patients had malignant portal veins thrombus (10.7%) and 12
patients had regional lymphadenopathy (14.3%). Hepatic heamangioma was observed
in 1 patient (1.2%) and hepatic cyst noted in 5 patients (6.0%). Intrahepatic
lithiasis was seen in 1 patient (1.2%).The contrast appearance of ICC during different vascular phases is summarized in
Table 2.
Table 2
Contrast-enhanced CT findings of 98 ICC nodules according to the different
vascular enhancement phases.
Arterial phase
Portal phase
Delayed phase
Hyperdense No. (%)
35 (35.7)
13 (13.3)
15 (15.3)
Peripherally hyperdense No. (%)
53 (54.1)
53 (54.1)
51 (52.0)
Isodense No. (%)
1 (1.0)
1 (1.0)
1 (1.0)
Hypodense No. (%)
9 (9.2)
31 (31.6)
31 (31.6)
Dynamic enhancement patterns at CT
The analysis of the vascular dynamic enhancement pattern throughout the different
phases of the 98 ICC nodules is shown in Table 3. Twenty
eight nodules (28.6%) showed a stable contrast enhancement pattern during the
dynamic study including 20 peripherally hyperdens (Fig.
1),6 hypodense and 2 hyperdense during all the three vascular phases.
Thirty five nodules (35.7%) demonstrated a progressive enhancement pattern:
peripherally hyperdense in the arterial phase followed by centripetal
progressive enhancement in the portal and the late phase in 27 nodules (Fig. 2), inhomogeneous hyperdense in the arterial phase
followed by progressive enhancement in the portal and the late phase and reached
maximal intensity in the delayed phase in 4 nodules, hypodense during the
arterial and the portal phase followed by inhomogeneous hyperdense during the
late phase in 2 nodules, globally hypodense during the arterial phase followed
by peripherally hyperdense during the portal phase and the late phase in 2
nodules. Fifteen nodules (15.3%) displayed a “wash-in and
washout” enhancement pattern: intense hyperdense during the arterial
phase followed by hypodense during the portal and the late phase in 13 nodules
(Fig. 3), intense hyperdense during the arterial phase
and the portal phase followed by hypodense during the late phase in 2 nodules.
Twenty nodules (20.4%) showed other enhancement patterns: peripherally
hyperdense during the arterial phase and the portal phase followed by hypodense
during the late phase in 5 nodules, peripherally hyperdense during the arterial
phase followed by hypodense during the portal phase and the late phase in 3
nodules, inhomogeneous hyperdense during the arterial phase followed by
peripherally hyperdense during the portal phase and inhomogeneous hyperdense
during the late phase in 2 nodules, slightly inhomogeneous hyperdense during the
arterial phase followed by hypodense during the portal phase and the late phase
in 6 nodules, hyperdense during the arterial phase and the portal phase followed
by isodense during the late phase in 1nodule, isodense during the arterial phase
followed by peripherally hyperdense during portal phase and hypodense during the
late phase in 1 nodule, slightly inhomogeneous hyperdense during the arterial
phase followed by peripherally hyperdense during the portal phase and the late
phase in 1 nodule, peripherally hyperdense during the arterial phase followed by
isodense during the portal phase and hypodense during the late phase in 1
nodule.
Table 3
Dynamic enhancement patterns of 98 ICC nodules at CT according to tumor
size.
Enhancement pattern
≤3c
(n = 21)
3.1–5.0
(n = 27)
>5 cm
(n = 50)
Stable enhancement
4
10
14
Progressive enhancement
6
9
20
Wash-in and wash-out
4
3
8
Other patterns
7
5
8
Figure 1
tif CT images of a 32-year-old man with a 4.2-cm –diameter ICC
displaying stable contrast enhancement pattern.
(a) unenhanced, (b) Arterial, (c) portal, and (d)
delayed phases. After intravenous contrast administration, the nodule shows
stable peripheral rim-like enhancement (arrow).
Figure 2
tif CT images of a 75-year-old man with a 3.8-cm –diameter ICC
displaying progressive contrast enhancement pattern.
(a) unenhanced, (b) Arterial, (c) portal, and (d)
delayed phases. After intravenous contrast administration, the nodule shows
progressive centripetal enhancement (arrow).
Figure 3
tif CT images of a 69-year-old woman with a 2.7-cm –diameter ICC
displaying wash-in and wash-out enhancement pattern.
The nodule was hypodense at unenhanced CT (a). After intravenous
contrast administration, the nodule shows marked hyper-enhancement during
the arterial phase (b) followed by wash-out during the portal phase
(c) and the late phase (d) (arrow).
Enhancement patterns of ICC nodules during dynamic contrast CT scan according to
nodule size. There were no significant differences in the dynamic vascular
patterns of ICC previously defined according to nodule size
(≤3 cm, 3.1–5.0 cm,
>5 cm), including stable enhancement
(p = 0.174,
p = 0.429,
p = 0.414, respectively), progressive enhancement
(p = 0.724,
p = 0.362
p = 0.565, respectively), wash-out enhancement
(p = 0.718,
p = 1.000,
p = 0.807, respectively) and other enhancement
patterns (p = 0.240,
p = 0.189,
p = 1.000, respectively).
Characterization of nodules according to enhancement pattern at
CT
Thirty five nodules demonstrating a progressive enhancement pattern and 28
nodules showing a stable contrast enhancement pattern were characterized as ICC
(64.3%). Fifteen nodules displaying a “wash-in and
washout” enhancement pattern were characterized as HCC ((15.3%)).
Twenty nodules showing other enhancement patterns were indeterminate
(20.4%).
Discussion
Ninety eight ICC consecutively identified in cirrhotic patients between January 2005
and July 2015 in our hospital exhibited varied enhancement patterns at
contrast-enhanced multiphase multidetector CT. Over half of the ICC nodules (54.1%)
had a peripheral rim-like enhancement during the arterial phase, whereas during the
portal and delayed phase, 26 nodules (49.1%) showed a centripetal progressive
enhancement,20 nodules (37.7%) a stable enhancement and 7 nodules (13.2%) other
enhancement pattern. The proportion of ICC nodules showing peripheral rim-like
enhancement during the arterial phase in our patients was similar to previous
studies by Kim et al.11 and Lavarone et al. (42.8%, 50%
respectively). We consider that the presence of a central necrosis and fibrosis may
account for the rim-like arterial contrast uptake at the periphery of the
nodules13. The rate of ICC nodules showing a progressive
enhancement pattern in our study (35.7%) is similar to that reported by Kim et
al. (32.1%)11 but slightly lower than that by Lavarone et
al. (42%)14. We favor to interpret these slight variances in
the light of the difference of sample size.Twenty two ICC nodules (15.3%) displayed a “wash-in and
wash-out” enhancement pattern in our study, resembling the radiological
hallmarks of HCC, namely, arterial hypervascularity followed by venous or delayed
phase washout10, and in fact, these nodules were independently
characterized as HCC by radiologists with over 20 year experience of liver radiology
in our hospital (PC and SYD). The rate of ICC nodules showing “wash-in
and wash-out” enhancement pattern in our study is lower than that
reported by Kim et al. (21.4%)11 but higher than that by
Galassi et al. (4.2%)12 and Lavarone et al. (0%)14. We favor to interpret the difference from that of Kim et al.
in the light of two reasons: (1) the difference of sample size (28 nodules in the
study of Kim et al., 98 nodules in the present study); (2) the difference of
scanning protocol. All the 26 patients in the study of Kim et al. underwent
dual-phase helical CT (arterial phase and portal venous phase imaging), without
providing any account on their contrast appearance during the delayed phase,
reflecting the lack of an internationally accepted, standardized protocol for
contrast CT scan in the diagnosis of ICC. An explanation of the difference from that
of Galassi et al. may be the sample size and etiology of cirrhosis (25 ICC
nodules ≤5 cm enrolled and 62.5% of cirrhosis related to
hepatitis C virus infection in the study of Galassi et al., 48 ICC nodules
≤5 cm enrolled and 85.7% of cirrhosis related to hepatitis B
virus infection in our study). The difference from that of Lavarone et al.
may be attributed to the following three factors: (1) different definition of
“wash-in and wash-out” enhancement pattern; (2) the
difference in tumor size; (3) the difference of sample size and etiology of
cirrhosis. The definition of “wash-in and wash-out” by
lavarone et al. was global intense contrast enhancement during the arterial
phase followed by contrast wash-out in the portal and/or delayed phase14. However, this definition may not be suitable for characterizing
nodules that show predominantly hyperdense (i.e., involving 60∼90% of
the nodule cross section area) during the arterial phase followed by hypodense in
the portal and/or delayed phase. The majority of HCC in cirrhosis displayed
inhomogeneous enhancement during the arterial phase111516,
therefore, it is not reasonable to correspond arterial hypervascularity to only
global intense contrast enhancement during the arterial phase. In our opinion, to
define predominantly hyperdense of a nodule during arterial phase as arterial
hypervascularity, regardless of global or predominantly partial1315
is more reasonable. The median tumor size was 3.0 cm in the study of
lavarone et al.14, while 5.3 cm in our study.
However, after stratification, the ICC nodules ≤3 cm
enrolled in our study (21 nodules) is comparable to that of lavarone et al.
(23 nodules) because much more ICC nodules were included in our series. More
importantly, 4 ICC nodules ≤3 cm (19.0%) showed
“wash-in and wash-out” enhancement pattern and there were no
significant differences in the dynamic vascular patterns of ICC according to nodule
size (≤3 cm, 3.1–5.0 cm,
>5 cm) in our study. Patients with cirrhosis who undergo
surveillance may have an earlier stage of HCC at diagnosis17.
Unfortunately, surveillance for HCC in patients with cirrhosis is recommended but
may not be successfully performed. Less than 20% of patients with cirrhosis who
developed HCC received regular surveillance in the United States18.
HCCs were detected during surveillance in the minority of patients even at major
referral center19. Surveillance for HCC is still not a consolidated
practice as it should be20. Therefore, differentiation of ICC from
HCC in large nodules is still a common clinical situation worldwide for most liver
tumors in cirrhosis are found not at very early stage. (3) Forty ICC nodules were
enrolled and 18.8% of cirrhosis related to hepatitis B virus infection in the study
of lavarone et al., while 98 ICC nodules enrolled and 85.7% of cirrhosis
related to hepatitis B virus infection in our study. Additionally, in the paper of
lavarone et al., one ICC nodule showed hyperdense during both the arterial
and portal phases, followed by hypodense in the delayed venous phase (patient No.
33, Table 3), should be judged as “wash-in and
wash-out” pattern according to the definition, though wash-out occurred
in the delayed phase and be subsequently characterized as HCC. Because radiological
diagnosis of HCC should be based on imaging techniques (4-phase MDCT/dynamic
contrast enhanced MRI) showing arterial hypervascularity and venous or delayed phase
washout according to the practice guidelines of AASLD and EASL910.
This discrepancy reflects the lack of internationally agreed standard for the review
of radiological films aimed at optimizing the diagnosis of ICC in cirrhosis. Our
results indicate if dynamic contrast CT scan was used as the sole modality for the
non-invasive diagnosis of HCC in cirrhosis, about 15% of ICC would be misdiagnosed
for HCC, however, this estimate needs to be clarified prospectively in the
future.There were some limitations to our study. First, it was limited by its retrospective
nature and thus by our limited control regarding patient selection. Therefore, we
are unable to calculate the sensitivity and specificity of dynamic contrast CT in
differentiation between ICC and HCC in cirrhosis. Second, though we provided a
largest series of pathologically proven ICC in cirrhosis seen on contrast-enhanced
multiphasic multidetector CT up to now, the sample size of ICC nodules
≤3 cm is still limited and just comparable to that of the
previous study14. This reflects the low incidence of ICC in patients
with cirrhosis, accounting for about 1–2% of all new nodules in
cirrhosis2122 and surveillance for hepatic tumor in patients
with cirrhosis is not widely performed in our country. Prospective multiple center
study including more small ICCs in cirrhosis is expected Third, it is impossible for
us to compare the enhancement patterns of CT and MRI because only 11 out of 84
patients of ICC underwent both MRI and CT scan in our series, though the enhancement
appearance of ICC at MRI was reported much different from that of HCC23 and this reflects the fact that in many countries worldwide, with a high
incidence of HCC, MRI is still not as readily available as CT. The usefulness of our
present results is restricted to centers which use CT for characterization of
hepatic nodules in cirrhosis.In conclusion, ICC in cirrhosis has varied enhancement patterns at contrast-enhanced
multiphase multidetector CT. Though the majority of ICC did not display typical
radiological hallmarks of HCC, if dynamic CT scan was used as the sole diagnostic
modality for the non-invasive diagnosis of nodules in cirrhosis, the risk of
misdiagnosis of ICC for HCC is not negligible.
Additional Information
How to cite this article: Li, R. et al. Dynamic enhancement patterns of
intrahepatic cholangiocarcinoma in cirrhosis on contrast-enhanced computed
tomography: risk of misdiagnosis as hepatocellular carcinoma. Sci. Rep.
6, 26772; doi: 10.1038/srep26772 (2016).
Authors: Jessica A Davila; Robert O Morgan; Peter A Richardson; Xianglin L Du; Katherine A McGlynn; Hashem B El-Serag Journal: Hepatology Date: 2010-07 Impact factor: 17.425
Authors: Jordi Rimola; Alejandro Forner; Maria Reig; Ramon Vilana; Carlos Rodríguez de Lope; Carmen Ayuso; Jordi Bruix Journal: Hepatology Date: 2009-09 Impact factor: 17.425
Authors: Su Jin Kim; Jeong Min Lee; Joon Koo Han; Ki Hyun Kim; Jae Young Lee; Byung Ihn Choi Journal: AJR Am J Roentgenol Date: 2007-12 Impact factor: 3.959
Authors: Shahid A Khan; Simon D Taylor-Robinson; Mireille B Toledano; Angus Beck; Paul Elliott; Howard C Thomas Journal: J Hepatol Date: 2002-12 Impact factor: 25.083
Authors: Lang Chen; Furong Zeng; Lei Yao; Tongdi Fang; Mengting Liao; Jing Long; Liang Xiao; Guangtong Deng Journal: Cancer Med Date: 2020-01-05 Impact factor: 4.452
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