Liver cancer is the sixth most common cancer worldwide and the second leading cause of cancer mortality.1, 2, In the United States, approximately 42220 new cases of liver cancer will be diagnosed and 30200 deaths will occur in 2018.3 The incidence in men is three times higher than in women. Over a third of liver cancer consists of hepatocellular carcinoma (HCC). In recent years, five-year survival rates of HCC have considerably improved due to earlier detection and curative therapies.4 However, the incidence is still rising in women while it has reached a plateau in men since 2010.3
The two most common risk factors of HCC are chronic infection from hepatitis B and/or hepatitis C virus and alcohol abuse.3 Other important risk factors include consumption of aflatoxin (toxin produced by a fungus that can infects grains, soybeans and peanuts) which occurs mainly in less developed countries and nonalcoholic fatty liver disease which occurs mainly in Western countries.2Figure 1 demonstrates the geographical distribution of the main risk factors for HCC worldwide.
Chronic liver disease caused by viral infection, alcohol abuse, or other factors can lead to cirrhosis. Cirrhosis is the most important clinical risk factor for HCC whereby the normal hepatic architecture is replaced by fibrous septa and a spectrum of nodules ranging from benign regenerative nodules to HCC.5 The cirrhotic liver gives way to HCC via hepatocarcinogenesis, an anaplastic complex process characterized by stepwise accumulation of epigenetic and genetic alterations at the molecular and cellular level6, 7, and changes in the hepatic architecture seen at the histologic level. While initially hepatocarcinogenesis involves the replacement of normal hepatic architecture with regenerative nodules, this subsequently progresses to replacement with dysplastic nodules and then HCC. HCC itself progresses from well-differentiated to poorly differentiated HCC.6
The liver has a dual blood supply,
Magnetic resonance imaging (MRI) has rapidly evolved as a superior imaging technique in the oncologic field in the past few decades, having undergone improvements in its acquisition time and imaging quality. Multiple studies have demonstrated that MRI has excellent sensitivity and specificity for the detection and characterization of HCC compared with computed tomography (CT) and ultrasound.8, 9, 10, 11, However, mainly because of its high cost and limited availability especially in underdeveloped countries which bear a disproportionately high risk of HCC, its large-scale use for HCC screening is still restricted. Table 1 summarizes the main indications of MRI for HCC as recommended by the European Association (EASL) and American Association for the Study od Liver Diseases (AASLD) guidelines. 9, 10, 11, 12,
Main indications of MRI for hepatocellular carcinoma (HCC)
Main indications of MRI for HCC evaluation |
---|
Nodules larger than 1.0 cm identified on ultrasound |
For patients on the orthotopic liver transplantation waiting list |
When the imaging features of the nodule on CT are not elucidative |
History of allergy to iodinated contrast agent used on CT scans |
After locoregional therapy |
Standardized MRI protocols for HCC surveillance must be developed to allow clinicians and technologists to perform repeatable and reproducible high-quality examinations.11 The minimum magnetic field strength of 1.5 Tesla (T) provides acceptable temporal, spatial, and contrast resolution that enable adequate assessment of hepatic lesions.12
The following sequences are essential for the diagnosis of HCC: T2-weighted imaging (WI); unenhanced T1WI opposed and in-phase; and multiphase T1WI (pre-contrast, late arterial, portal venous, and delayed or transitional phases). Slice thickness should be 5 mm or less for dynamic series and 8 mm or less for other imaging.13, 14,
Other sequences have been proposed to improve the detection of HCC, especially in cases of well-differentiated HCC or HCC post-treatment. These include diffusion weighted imaging (DWI) with apparent diffusion coefficient mapping, subtraction imaging, multi-planar acquisition, and hepatobiliary phase.14, 15, Table 2 summarizes these MRI sequences.
MRI sequences and hepatocellular carcinoma (HCC) features that can be assessed in each sequence
MRI sequences | HCC imaging features |
---|---|
Usually hyperintense | |
Intralesional microscopic fat (lower signal on opposed-phase) or iron (lower signal on in-phase) | |
Demonstrates the presence of macroscopic fat and blood products After locoregional therapies, hyperintensity indicates coagulative necrosis | |
Hyperenhancement | |
Washout and capsule appearance | |
Washout and capsule appearance | |
Restricted diffusion (helps to identify small lesions) | |
Characterizes contrast enhancement in spontaneously hyperintense nodules on T1WI pre-contrast (especially important for lesions with blood products and after locoregional treatment) | |
Helps to differentiate HCC from mass-like lesions or extra-hepatic lesions | |
Generally hypointense |
T1W1 = T1 weighted image; T2WI = T2 weighted image
DWI improves the characterization of liver nodules without requiring contrast media injection.15, 16, 17, Currently, DWI is used to increase the sensitivity of other sequences for the detection and characterization of HCC. Studies investigating the utility of DWI have demonstrated promising results for assessing prognosis, predicting response, distinguishing tumor from treatment effect, and monitoring response to therapy in patients with HCC.18, 19, 20, 21, 22,
Dynamic contrast-enhanced sequences are routinely performed with gadolinium-based extracellular contrast agents (ECA) or hepatobiliary contrast agents (HBA). They allow the diagnosis of HCC by exploiting the physiologic changes in blood flow that accompany hepatocarcinogenesis. Following administration of the contrast agent, the dual vascular supply of the liver is opacified in the following sequential order: the hepatic arteries, the portal veins, and finally the hepatic veins.7, 8, 9, 10, 11, 12, 13, 14,
Typically, contrast agents are administered at rates of 2 mL/sec followed by saline infusion. The dose is usually based on body weight (ranging from 0.025 to 0.1 mmol gadolinium per kg) as well as on the agent and other factors.7
ECAs include gadoterate meglumine (Gd-DOTA) and gadopentate dimeglumine (Gd-DTPA) which are excreted primarily through glomerular filtration. The pattern of contrast enhancement can be studied in dynamic T1WI in the following phases: late arterial, portal venous, and delayed phases. HBAs include gadoxetate disodium (Gd-EOB-DTPA) and gadobenate dimeglumine (Gd-BOPTA) which are excreted through glomerular filtration but are also taken up by hepatocytes and excreted into the biliary system. As such, HBAs provide additional information regarding the presence of hepatocytes with OATP, which decrease in hepatocarcinogenesis.23 With HBA administration, the pattern of contrast enhancement can be studied in the late arterial, portal venous, transitional, and hepatobiliary phases.
Recently, in Europe, the use of intravenous linear agents such as gadodiamide and intravenous gadopentate dimeglumine have been suspended or restricted in response to the retention of gadolinium in the brain and in other tissues as reported in a scientific review. 24 However, there is still no evidence that this deposition causes any harm to patients. Hepatobiliary linear contrast agents continue to be available as their properties allow the recognition of poorly vascularized hepatic lesions which cannot be studied with other agents. The macrocyclic agents (gadobutrol, gadoteric acid, and gadoteridol) have a lower propensity to release gadolinium than linear agents and can continue to be used in their current indications.24
Liver biopsy is the gold standard for quantifying iron and fat in the liver. However, this method is invasive and susceptible to sampling variability. MRI is a non-invasive, alternative method to quantify iron and fat within the liver. There are several sequences that can be used to quantify iron and fat within the liver. Regarding iron, the following techniques can be employed: signal intensity ratio techniques based on T2WI or T2*WI, quantitative relaxometry (based mainly on T2WI but also on T1WI), and MR susceptometry.25, 26, In regards to fat, post-processing of T1WI in- and opposed-phase provides quantification from a scale of 0–50% while the proton density fat fraction allows quantification of a full fat fraction from 0–100%.27 Iron and fat content may contribute to differential diagnosis and may be a potential prognostic biomarker of HCC.28 However, the evidence is still limited and this method is not used in the daily practice.
Magnetic Resonance Elastography (MRE) is an imaging modality used to stage liver fibrosis.29, 30, Recent studies have demonstrated the use of MRE for the evaluation of HCC with promising results for the prediction of tumor grade31 and assessment of treatment response.32 Well/moderately differentiated tumors demonstrated increased stiffness compared to poorly differentiated ones and there was a correlation between the percentage of tumor necrosis and tumor stiffness, particularly in HCCs treated with radioembolization.31 However, the evidence is still limited and MRE is not yet routinely implemented.
Regenerative nodules correspond to an area of parenchyma surrounded by fibrosis. These nodules are usually similar to background liver parenchyma but some may exhibit a fine area of peripheral late-phase enhancement corresponding to fibrosis. Regenerative nodules may present accumulation of iron which results in low signal intensity on T1-and T2-weighted imaging.6, 7, 8, 9, 10, 11, 12, 13, 14, 15, 16, 17, 18, 19, 20, 21, 22, 23, 24, 25, 26, 27, 28, 29, 30, 31, 32,
Dysplastic nodules contain atypical cells but without malignancy on histological analysis. The radiological pattern of dysplastic nodules is variable and can be similar to regenerative nodules (in those with low-grade dysplasia) or well-differentiated HCC (in those with high-grade dysplasia).33, 34, 35, These lesions often present as iso- or hypointense on T2-weighted imaging and are frequently hypovascular. Occasionally, a mildly elevated signal intensity may occur within a low signal-intensity nodule on T2-weighted imaging. This represents foci of HCC (the foci of high signal intensity) within a dysplastic nodule (the area with low signal intensity). The foci of HCC may also enhance in the arterial phase.35
HCC has a wide spectrum of radiological characteristics depending on its size and degree of histological differentiation. HCC can be classified as early or progressed HCC.
HCC may also be classified according to its growth patterns / macroscopic appearance into: single nodular type, well-defined, encapsulated with better prognosis; or multifocal type (multiple nodules in several hepatic segments), with a diffuse pattern, usually extensive, heterogeneous, with variable enhancement, usually better detected in the delayed phase (hypoenhancement), and often associated with vascular invasion (Figures 4).35, 36, 37, Table 3 summarizes the main imaging features of HCC.
Main imaging features of hepatocellular carcinoma (HCC)
Imaging features | Description |
---|---|
Increased enhancement in the arterial phase. Reflects tumor neoangiogenesis. | |
Hypoenhancement of the lesion compared with background liver tissue. Secondary to HCC extracellular reduced volume, rapid venous drainage and reduced intranodular portal venous supply. | |
Observed in approximately 80% of HCCs, detected on delayed phase, secondary to the lack of portal supply to malignant nodules. Corresponds to a pseudocapsule consisting of compressed adjacent liver parenchyma with occasional nonspecific inflammatory cells on histology. | |
HCC invades and grows within the lumen. The vein appears dilated and with the same pattern of enhancement observed in the nodule. | |
The elevated signal intensity on T2WI can be useful to differentiate HCC from dysplastic nodules. | |
Mildly elevated signal relative to the surrounding liver parenchyma on diffusion weighted imaging (DWI) and low signal intensity on apparent diffusion coefficients (ADC) map. | |
Enhancement of the peritumoral parenchyma after enhancement of the tumor itself, because of the passage of contrast through the draining sinusoids and portal venules into the surrounding sinusoids. | |
Loss of signal on the opposed-phase T1WI compared with the in-phase images. | |
Siderotic nodule is likely to be a dysplastic nodule. Development of an iron-free around the nodule suggests HCC foci. | |
Nodular areas interspersed by areas of fibrosis, hemorrhage, arteriovenous shunting and necrosis. Characteristic of progressed HCCs. | |
Mildly elevated signal intensity on T2WI within nodule with low signal intensity, representing the focus of HCC within the low density dysplastic nodule, that may also enhance in the arterial phase. | |
Hypointensity compared with background liver following administration of a hepatobiliary contrast agent (2–5 minutes after contrast media administration). | |
Hypointensity compared with background liver following administration of a hepatobiliary contrast agent (20 minutes after). |
T1W1 = T1 weighted image; T2WI = T2 weighted image
A minority of HCC presents atypical imaging features and awareness of these is important for early diagnosis and improving patient outcomes. Most of these cases are challenging and biopsy may be needed for confirmatory diagnosis.
Diffuse hepatocellular carcinoma is a rare aggressive form of HCC characterized by poorly defined margins and atypical enhancement patterns (mild heterogeneous enhancement, most commonly hypovascular). Frequently, there is involvement of the portal and hepatic veins with thrombosis (Figures 8).38
Twenty percent of HCCs may occur in a non-cirrhotic liver. The radiological appearance of such HCCs is larger, well-demarcated, solitary lesions with large areas of necrosis; they are usually diagnosed at a later stage.40
Although arterial hyperenhancement is considered the most consistent feature of HCC, it is also present in other non-malignant lesions especially small non-malignant ones, which contributes to the high incidence of false positives.
Transient arterial enhancement due to focal obstruction of a distal parenchymal portal vein or nontumorous arterioportal shunts, for example, is often seen in the cirrhotic liver. Usually, these vascular disorders are peripheral, wedge-shaped lesions, isointense to surrounding parenchyma on pre-contrast images and do not present restricted diffusion or displace internal vasculature.36, 37, 38,
Observed in end-stage liver disease, focal confluent hepatic fibrosis can be mass-like and mistaken for HCC once it presents similar low signal intensity relative to the liver on T1WI and hyperintensity on T2WI. However, unlike HCC, it is usually associated with atrophy and capsular retraction of the affected segment, as well as delayed contrast enhancement. 36, 37, 38,
Other benign lesions such as hemangiomas, focal nodular hyperplasia, and hepatic adenomas are rare in the cirrhotic liver, probably because of the process of cirrhosis, and they can be difficult to distinguish from HCC. 36, 37, 38,
Intrahepatic cholangiocarcinoma usually shows rim enhancement with progressive and concentric filling of contrast material in the later phases, which would be an atypical pattern of enhancement for HCC (Figure 9). Other features more commonly associated with intrahepatic cholangiocarcinoma than HCC are intrahepatic biliary duct dilation distal to the tumor and associated capsular retraction. Association with tumoral thrombosis is rare and when narrowing or obstruction of the portal vein occurs, the latter are usually due to external compression .18
Combined hepatocellular-cholangiocarcinoma (cHCC-CC) is a rare variant of primary hepatic cancer that is clinically and pathologically distinct from pure HCC. Imaging features are variable depending on the predominant histologic component, and although they overlap more frequently with those of cholangiocarcinoma, they can also mimic HCC.18, 19, 20, 21, 22, 23, 24, 25, 26, 27, 28, 29, 30, 31, 32, 33, 34, 35, 36, 37, 38, 39, 40, 41, cHCC-CC may appear hypointense on T1WI and iso to hyperintense on T2WI with or without central hypointense focus, which represents a central cholangiocarcinoma or fibrotic component.19, 20, 21, 22, 23, 24, 25, 26, 27, 28, 29, 30, 31, 32, 33, 34, 35, 36, 37, 38, 39, 40, 41, 42, 43, On dynamic imaging, early ring enhancement with centripetal progression or heterogeneous early enhancement with partial washout are possible presentations.41 On MR imaging with a hepatocellular agent, irregular shape, strong peripheral enhancement, and absence of target sign favor cHCC-CC, particularly the HCC predominant type.42
Hypervascular metastases may also be a diagnostic challenge and typically arise from primary neuroendocrine tumors (pancreatic islet cell tumor, carcinoid tumor, and pheochromocytoma), renal cell carcinoma, thyroid carcinoma, choriocarcinoma, and melanoma.43 They are generally irregular with indistinct margins and hyperintense on T2WI with a central cystic or necrotic component and with a variable sign on T1WI, depending on the presence of blood, melanin, and other substances that present high signal on this sequence. On dynamic imaging, they show perilesional rim enhancement and irregular washout on delayed images.44
Surgical resection or transplantation is the standard treatment of HCC. However, most patients are not eligible for resection and the waiting list for liver transplantation is long. Locoregional therapies can be performed as curative treatment, mainly in small HCC, or as a bridge before transplantation. The goal of locoregional therapy is to achieve tumor necrosis. Overall, treated tumors appear with no internal enhancement on postcontrast phases and viable tumors may have areas of arterial phase hyperenhancement with or without washout appearance (Figures 6).44, 45, Table 4 shows the main systems used to assess tumor response after locoregional treatment.
Main classifications used to assess tumor response after locoregional treatment
Criteria | System | Response | Definition |
---|---|---|---|
Disappearance of all TL | |||
≥ 50% decrease in CP of TL | |||
< 50% decrease to ≤25% increase in CP of TL | |||
> 25% increase from maximum response of TL | |||
Disappearance of all TL | |||
≥ 30% decrease in MD of TL | |||
< 30% decrease to ≤20% increase in MD of TL | |||
> 20% increase from maximum response of TL | |||
Disappearance of any intratumoral enhancement in all TL | |||
≥ 30% decrease in SMD of enhancing tissue in TL | |||
< 30% decrease to ≤20% in SMD of enhancing tissue in TL | |||
> 20% increase in amount of enhancing tissue in TL | |||
Disappearance of any intratumoral enhancement in all TL | |||
≥ 50% decrease in amount of enhancing tissue in TL | |||
< 50% decrease in amount of enhancing tissue in TL | |||
> 25% increase in amount of enhancing tissue in TL and/or new enhancement in previously treated lesions | |||
No suspicious lesion enhancement | |||
Atypical enhancement not meeting criteria to viable tumor | |||
Nodular, mass-like, or thick irregular tissue in or along the treated lesion with any of the following: arterial phase hyperenhancement or washout appearance or enhanced similar to pretreatment 100% of tumor necrosis or reduction | |||
Necrotized area larger than the tumor (enough ablative margin) | |||
Necrotized area similar in size to the tumor (insufficient ablative margin) | |||
50–100% of tumor necrosis or reduction | |||
Other effect than TE3 and TE1 | |||
Tumor enlargement of > 25% regardless of necrosis |
CR = complete response, CP = cross-product, EASL = European Association for the Study of Liver, LI-RADS = Liver Imaging Reporting and Data System, MD = maximum diameter, PD = progressive disease, PR = partial response, RECIST = Response Evaluation Criteria for Solid Tumors, mRECIST = modified RECIST, RECICL = Response Evaluation Criteria in Cancer of the Liver, SD = stable disease, SMD = sum of maximum diameters, TE = treatment effect, TL = target lesion(s), WHO = World Health Organization
The imaging diagnosis of HCC using only the features on dynamic MRI is highly specific. The overall MRI sensitivity for detection of HCC is 81%, against 68% using CT.46 The dynamic contrast enhanced arterial phase is the most sensitive and specific sequence (>95%).47
MRI is especially sensitive for the detection of lesions larger than 2 cm. On the other hand, for the detection of small tumors, although MRI still outperforms CT, the sensitivity remains disappointing.48, 49, 50, 51, 52, 53, This can be explained by the high frequency of atypical enhancement patterns these small lesions present.52 Regarding contrast-enhanced ultrasound (CEUS), it is not recommended as a first-line imaging technique, but improvements have been made in the differential diagnosis of cholangiocarcinoma and hepatocellular carcinoma and some studies have shown it to be more specific than CT and MRI for nodules between 10 and 20 mm.12Table 5 summarizes and compares the sensitivity of MRI, CT, and CEUS for the detection of HCC according to tumor size.51
MRI and CT estimated sensitivity for the detection of hepatocellular carcinoma (HCC)
MRI | CT | CEUS | |
---|---|---|---|
82% | 77% | 73% | |
96% | 94% | 94% | |
66% | 63% | 77% |
CEUS = contrast-enhanced ultrasound
As an attempt to improve the performance of MRI among small HCC, the combined use of DWI with conventional dynamic MRI54 as well as the use of contrast agents other than gadolinium-based contrast media have been proposed.55 The combination of super-paramagnetic iron oxide particles with gadolinium-based contrast media have been shown to increase the sensitivity for the detection of HCC measuring 1–2 cm to 92%.56
After local therapies, MRI has also shown to be specific but not sensitive for the detection of small foci of recurrent or residual tumor.57, 58, In this context, DWI has shown promising results for evaluating response to treatment.
Advances in technology have allowed for quantitative features to be extracted from imaging scans, adding value to clinical decision-making. In oncology, quantitative radiomics features may allow for the assessment of tumor characteristics including cellularity, perfusion, and oxygenation that can help in characterizing tumors characterization, assessing treatment response, and predicting treatment response. Considering that MRI involves different sequences with several physical mechanisms, the use of MRI in radiomics is promising.59
Both quantitative and qualitative data extracted from imaging scans can also be correlated with genetic profiles. It has been demonstrated that imaging phenotypes reflect underlying genomics59 and can guide the treatment of those patients, which is important in the new era of personalized medicine.
Positron Emission Tomography (PET)-MRI combines high contrast and anatomical resolution from MRI with wide metabolic properties from PET. This technique is promising considering several new radiotracers. PET-MRI could be especially beneficial for evaluating tumor characteristics.60, 61, 62,
While conventional imaging modalities (MRI and CT) are preferable for detecting HCC, PET can offer additional information about functional or metabolic characteristics of the tumor. Several radiotracers have been used to achieve this objective, including 18F-fluorodeoxyglucose (18F-FDG) to estimate glucose consumption and choline labelled with either 11C (Cho) or 18F (FCho) to reflect cell-membrane metabolism and tumor proliferation.63, 64, 65,
18F-FDG is the most widely used radiotracer in oncology and has great sensitivity for detecting metastases from most cancers. FDG uptake correlates with the degree of HCC differentiation, with a higher avidity for poorly differentiated HCC.66 On the other hand, choline shows strong avidity for HCC, especially in well and moderately-differentiated tumors.68 Some studies showed that a dual-tracer PET using FDG and choline has the best performance to detect HCC66, 67, 68, as these tracers complement each other in the detection of HCC based on its histological differentiation. This combination may also be a prognostic indicator, with worst outcomes associated with FDG-PET captation.68
Perfusion MRI is a function imaging technique that can provide quantitative data regarding tumor microvasculature. Several studies demonstrated that perfusion MRI can assess tumor response after locoregional therapies, such as transcatheter arterial chemoembolization and radiofrequency ablation.69, 70, Perfusion MRI can detect vasculature changes of HCC before and after therapy. It is a promising tool in the diagnosis of HCC, as it can be used to target lesions for therapy, to evaluate the efficacy of the treatments and to evaluate recurrence.69, 70, 71
In summary, MRI is an essential imaging modality in the diagnostic arsenal of HCC and is especially indicated for the evaluation of small lesions, unclear lesions on CT, and lesions after locoregional therapies. Considering the multiple sequences included on MRI, there is a huge potential to extract several imaging biomarkers that reflect the tumor microenvironment and which, in the future, may add decision-making value in the management of patients with HCC.