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Copyright ©The Author(s) 2021.
World J Gastrointest Oncol. Nov 15, 2021; 13(11): 1680-1695
Published online Nov 15, 2021. doi: 10.4251/wjgo.v13.i11.1680
Table 1 Predisposing factors in developing hepatic tumors in chronic liver diseases
Predisposing factors
Oxidative stress
Dysregulation of protumorigenic growth factors and cytokines
Genetic factors: p53 mutation, telomere shortening, homozygous PiZZ mutation, tumor suppressor kinase-1 expression
Hepatocarcinogenesis: HBV, HCV, HIV
Toxic substances: Tyrosinemia type I (maleyl acetoacetate, fumaryl acetoacetate and succinyl acetone), PFIC type 2 and 3 (bile salt)
Metabolic disturbance: Glycogen storage disease type 1 and 4, obesity and NAFLD
Vascular disruption: Congenital absence of portal vein, noncirrhotic portal hypertension, Budd-Chiari syndrome
Table 2 Liver tumors identified in chronic liver diseases
Liver disease and main pathogenesis
Tumor type
Genetic or metabolic syndromes
Hereditary tyrosinemia type 1[80-83]HCC
GSD type 1, 3, 4HA, HCC, HB
Alagille syndromeHCC, regenerative nodule
Other familial cholestatic syndromesHCC
NAFLDHCC
α-1 antitrypsin deficiencyHCC
Infections
HBVHCC
HCVHCC
Vascular
AbernethyFNH, HCC, HA
Noncirrhotic portal hypertensionNRH
Congenital portosystemic shuntHCC, HB
Cirrhosis and cholestatic conditions
Biliary atresiaHCC, FNH, pseudotumor
Autoimmune hepatitisHCC
Wilson diseaseHCC
Congenital hepatic fibrosisHCC
Cryptogenic cirrhosisHCC
Table 3 Typical imaging appearances of liver tumors
Tumors
US with doppler
CT
MRI
HBWell circumscribed hyperechoic or heterogenous echogenic lesionHypoattenuating lesion in non-contrast image with heterogeneous arterial and venous enhancementT1W; hypointense
T2W; hyperintense
Heterogeneous arterial and venous enhancement
HCCVariable from hypo-, iso-, or hyperechoic from internal fat, necrosis or hemorrhageWell- or poorly defined, hypoattenuating lesion with arterial hyperenhancement and venous “wash-out” with/without delayed capsular enhancementT1W; hypointense
T2W; hyperintense
Early arterial enhancement and wash-out with relative low signal intensity on venous and delayed phases
Tumor thrombus enhancement in portal veinDelayed capsular enhancement
FNHHomogenous, well-circumscribed Homogeneous, well-circumscribed iso- to slightly hypoechoic lesionT1W; iso- to slightly hypointense with hypointense scar
T2W; iso- to slightly hyperintense with hyperintense scar
Hypoattenuating scarEnhancement pattern same as CT
Internal color flow in the central scar extending to the periphery in a spoke-wheel patternArterial and early portal venous enhancement and becomes isoattenuating to liver in the late portal venous and delayed phasesNormal or increased uptake on delayed hepatobiliary phases of the hepatocyte specific contrast agent
AdenomaHyperechoic lesion in the normal liverWell-circumscribed hypoattenuating lesion with hyperattenuation if hemorrhagingT1W; hyperintense
T2W; hyperintense
Fat component; Signal dropout on opposed-phase or fat suppression images
Hypoechoic lesion in the background of diffuse fatty infiltration or glycogen storageIntense arterial enhancement and isoattenuating in venous and delayed phasesPeripheral pseudocapsular enhancement
Enhancement pattern same as CT
NRHMultiple tiny and typically isoechoic lesions, difficult to detect.Slightly hypo- or isoattenuating lesion to liverT1W; homogenous and slightly hyperintense.
T2W; variable
Isoattenuation to liver in both arterial and portal venous phasesEnhancement in portal phase like normal liver parenchyma