Diagnostic imaging of gastrointestinal neuroendocrine neoplasms (NEN) is of fundamental importance for determining the location of the primary lesion, disease staging, selection of treatment and monitoring its effects. Currently, more than half of gastrointestinal NEN are detected incidentally, usually during surgery, diagnostic imaging studies or endoscopic procedures performed for other indications(1,2). Sometimes metastatic lesions in the liver are the first sign of the disease when the primary lesion is not yet known(1). Focal lesions, both primary and metastatic may be small and often have an atypical location, which makes NEN imaging and diagnosis difficult.
Gastroenteropancreatic neuroendocrine neoplasms (GEP-NEN) account for approximately 70% of neuroendocrine neoplasms and approximately 1.5–2% of all gastrointestinal and pancreatic neoplasms(1,2). GEP-NEN arise from diffuse endocrine system (DES) cells present in the pancreas and the gastrointestinal system(1,3). Neuroendocrine tumours of the pancreas account for 7% of all GEP-NEN and approximately 10% of all pancreatic neoplasms(4). In recent years an increase in the prevalence of gastric and rectal NEN versus intestinal NEN has been observed(1,5–10). The NEN detection rate has significantly increased over the last few decades(1,3). Currently, it is estimated that NEN incidence is 3–5.2/100,000 new cases per year. The general prevalence rate for these neoplasms is 35/100,000 cases on average, i.e. 5.86/100,000 individuals per year(1,3). The prevalence of NEN in men is higher than that in women (52%; 5.35/100,000/year vs 48%; 4.76/100,000/year)(1,3). A higher risk of the disease has been noted in African Americans, Latinos and Asians and the mean age upon diagnosis is 63 years(5,6). The majority of NEN are sporadic in nature and develop approximately 15 years later than the rarer NEN associated with genetic syndromes (25%)(4,7). Pancreatic neuroendocrine neoplasms (mainly hormonally inactive ones) and gastrinoma occur in 25–75% patients with MEN1 syndrome(7). In patients with a mutation in the VHL gene, neuroendocrine tumours are usually benign, while other neoplasms occurring in this syndrome (e.g. clear cell renal cell carcinoma) are malignant(7,8). Pancreatic neuroendocrine neoplasms in NF1 syndrome and tuberous sclerosis complex are rare (1%); the diagnosis is made in late-stage disease(9).
In the majority of GEP-NEN cases no risk factor for the development of a tumour was identified. It was observed that hypergastrinaemia, diabetes and ulcerative colitis may be associated with the development of NEN, but no cause-and-effect relationship was confirmed(4).
A special feature of NEN is the production of hormones or biogenic amines which can produce numerous clinical symptoms. In the case of disease spread symptoms of carcinoid syndrome may occur such as diarrhoea, tachycardia, hot flushes and reddening of the skin(3). The majority of NEN are hormonally inactive with uncharacteristic symptoms associated mainly with the local development of a tumour (abdominal pain, compression, ileus) or spread to the liver(4).
Currently, more than half of GEP-NEN are detected incidentally, usually during surgery of the small intestine and appendix and in imaging studies or endoscopic procedures performed for other indications(1,4). Sometimes the first symptom of the disease is metastatic lesions in the liver(1,4). The proportion of small intestinal NEN in which the primary lesion was not found is approximately 70%. The 5-year survival rate for these patients is estimated to be 50%(10).
A neuroendocrine tumour is diagnosed based on clinical presentation, assessment of specific and non-specific NEN markers, imaging studies and histopathological examination(4). As for laboratory testing, assay of chromogranin A (CgA), which is a characteristic, but non-specific marker, may be helpful. The monitoring of changes in the levels of this marker may be very helpful for excluding recurrence or spread of the neoplastic process, particularly for NEN arising from the small intestine(1). Other markers assessed depending on the symptoms presented by the patient and the suspected type of NEN include: chromogranin B, pancreatic polypeptide, gastrin, 5-hydroxyindoleacetic acid (5-HIAA), glucose, insulin, C-peptide, glucagon and vasoactive intestinal peptide (VIP). If MEN1 is suspected, the assessment of pituitary function, evaluation of calcium and phosphate balance and genetic testing are necessary. A diagnostic novelty is NETest with the assessment of expression of selected gene transcripts characteristic for NEN. The evaluation of circulating microRNA, which are stable in body fluids and characteristic for a given neoplasm, is a promising method(1,11).
Many different classifications have been proposed in the history of neuroendocrine neoplasms. The most recent one, adopted by the World Health Organisation (WHO) in 2017, introduced a division according to the histological grade of the neoplasm (the G feature) and the proliferation index (Ki-67) into four groups: NEN G1, G2 and G3 and NEC (neuroendocrine carcinoma(1).
The primary method of GEP-NEN management is surgery, whose scope depends on the location of the tumour, the stage of the neoplasm and the patient’s condition. In selected cases endoscopic treatment is an alternative method(1). The gold standard of pharmacotherapy in patients with NEN is somatostatin analogue treatment for hormonally active and inactive tumours, both during stable disease and progression(1). Another NEN treatment method is chemotherapy, which is selected depending on the stage and grade of the disease. For NEN G3 a less aggressive capecitabine and temozolomide (CAPTEM) regimen can be used, while for NEC cisplatin and etoposide are used(1). Molecularly targeted therapies (everolimus and sunitinib) are offered particularly for pancreatic NEN(1). In patients with metastatic or inoperable NEN with high somatostatin receptor expression on somatostatin receptor scintigraphy (SRS), treatment with radiolabelled somatostatin analogues (DOTA-Tyr3-octreotide and DOTA-Tyr3-octreotate labelled with radioisotopes 177Lu, 90Y) is recommended, which is called peptide receptor radionuclide therapy (PRRT)(1).
Diagnostic imaging of neuroendocrine tumours plays a fundamental role in diagnosis, staging, selection of treatment method, assessment for radioisotope therapy and monitoring response to treatment(1,2). Diagnostic imaging methods make it possible not only to detect tumours, but also to perform therapeutic procedures based on the result. Diagnostic imaging of NEN is difficult since the tumours have a various, often non-specific clinical presentation or are diagnosed incidentally in asymptomatic patients. Focal lesions, both primary and metastatic may be small and often have an atypical location. It is important to use various diagnostic methods, both morphological and functional. Morphological imaging (transabdominal ultrasound, contrast-enhanced ultrasound, [CEUS]; elastography; endoscopic ultrasound [EUS]; computed tomography [CT]; magnetic resonance imaging [MRI]; endoscopy, including video capsule endoscopy [VCE]) is usually used to detect a tumour and assess the stage of the disease. Functional imaging techniques (scintigraphy with 99mTc-labelled somatostatin analogues [99mTc-SPECT]; positron emission tomography with 68Ga-labelled peptides [68Ga-PET/CT] and with other tracers: 18F-FDG, 18F-DOPA and 11C-HTP) are useful for tumour detection, prognostic assessment and treatment planning(4) (Tab. 1).
Method | Advantages | Disadvantages |
---|---|---|
Ultrasound |
No exposure to ionising radiation Repeatability Transabdominal ultrasound – wide availability EUS – primary method for pancreatic tumour assessment (EUS + CEUS, elastography) EUS-FNA – possibility of cytological verification EUS-RFA – possibility to treat focal lesions of the pancreas CEUS, elastography – improved sensitivity for focal lesion assessment, evaluation of unclear lesions on CT/MRI IOUS – possibility of intraoperative lesion assessment IDUS – thorough assessment of intraductal lesions |
Assessment dependent on the skills and experience of the examiner and the class of the device Poorer sensitivity of the classic method EUS, IOUS, IDUS, CEUS – access only at specialised centres, invasive procedures |
Computed tomography |
High spatial resolution (min. 2–4 mm) Thorough anatomical assessment of abdominal organs Multiplanar imaging, 3D reconstruction Disease staging Assessment of intestinal focal lesions (enteroclysis, enterography, CT colonoscopy) Aid in surgery planning Availability, quick results, repeatability |
Exposure to ionising radiation Exposure to iodine contrast agent and the associated complications (renal failure, allergic reactions, hyperthyroidism) Vasculature assessment dependent on the phase and dose of contrast Difficult reassessment of both small and too large lesions in terms of volume Difficult assessment of response to treatment if necrosis, haemorrhage or fibrosis are present with no reduction in lesion size Difficult assessment in slowly growing lesions |
Magnetic resonance imaging |
High spatial resolution (min. 2–4 mm) Best differentiation between soft tissues Multiplanar imaging, 3D reconstruction Disease staging The best method for the assessment of hepatic and pancreatic focal lesions Assessment of bile duct and pancreatic duct – MRI cholangiopancreatography No exposure to ionising radiation Gadolinium contrast – fewer allergic reactions, no kidney damage Repeatability |
High costs Limited availability Long duration of procedure Patient cooperation required Contraindication: metal parts in the body Difficult reassessment of both small and too large lesions in terms of volume Difficult assessment of response to treatment if necrosis, haemorrhage or fibrosis are present with no reduction in lesion size Difficult assessment in slowly growing lesions |
99mTc-SPECT |
Functional examination Full-body scan CT imaging possible Assessment of primary lesion location, stage of the disease Evaluation for appropriate forms of treatment, assessment of treatment response, evaluation for PRRT Monitoring, reassessment 1-day procedure, SPECT 4 hours after tracer administration |
Exposure to ionising radiation Low resolution, poor assessment of lesions <1 cm High background hinders midgut NEN assessment on gastrointestinal examination Low sensitivity in insulinoma detection Possible interference with cold somatostatin analogues |
68Ga-DOTA-PET |
Functional examination Full-body scan Multiplanar imaging, high resolution 4–6 mm, imaging together with CT Possibility to calculate the level of uptake – standardised uptake value (SUV) Good anatomical assessment Assessment of primary lesion location, stage of disease, evaluation for appropriate forms of treatment, assessment of treatment response, monitoring, reassessment Assessment for PRRT 1-day procedure, images obtained quickly, after 2 hours |
Uptake in normal tissues (pituitary gland, spleen, kidneys, adrenal glands) or in inflammatory foci may be mistaken for a tumour Possible interference with cold somatostatin analogues Lack of complete validation |
18FDG-PET |
Functional examination Full-body scan Multiplanar imaging, high resolution 4–6 mm, imaging together with CT Good anatomical assessment Disease staging, assessment of treatment response, prognostic factor, monitoring For the assessment of poorly differentiated NEN Prognostic value in highly and medium differentiated NEN |
Exposure to radiation Poor uptake in NEN G1 and G2 Procedure available in specialised centres |
131I-MIBG-SPECT |
Functional examination Full-body scan High specificity for phaeochromocytoma, paraganglioma, neuroblastomas Assessment for treatment with 131I-MIBG |
High background Poor anatomical assessment Interference from many pharmaceuticals Need for preparation with organic iodine in order to block the thyroid gland before the procedure Procedure 24–72 hours after tracer administration |
EUS – endoscopy ultrasound; EUS-FNA – EUS fine-needle aspiration; EUS-RFA – EUS-guided radiofrequency ablation; CEUS – contrast-enhanced ultrasonography, IDUS – intraductal ultrasonography; IOUS – intraoperative ultrasonography; SRS – somatostatin receptor scintigraphy; SSA – somatostatin analog; PRRT – peptide-receptor radionuclide therapy; 99mTc-SPECT – 99mTc-single-photon emission computed tomography; 68Ga-DOTA-PET – 68Ga-DOTA-positron emission tomography; 18FDG-PET – 18FDG-positron emission tomography; 131I-MIBG – 131I-MIBG – single-photon emission computed tomography
Transabdominal ultrasound is usually a first-line diagnostic imaging procedure for GEP-NEN. The use of various ultrasound techniques: harmonic and Doppler imaging, computer processing and compound imaging (CI) makes ultrasound a commonly used method for the diagnosis and monitoring of NEN. It is also possible to perform ultrasound-guided biopsy of tumours located in the liver, pancreas and retroperitoneal space.
The sensitivity of this method depends on the location of abnormalities, anatomical conditions, experience of the physician performing the procedure and technical aspects of the ultrasound device(1). The sonographic image of NEN, both the primary lesion and liver metastases is non-characteristic; it depends on the type of NEN, proliferation index, tumour size and location and on the presence of regressive changes(1).
A pancreatic neuroendocrine neoplasm is often well-defined, hypoechoic (less commonly hyper- or normoechoic), sometimes with a hyperechoic halo, areas of necrosis and calcifications(1,4).
Transabdominal ultrasound has limited utility for detecting a primary lesion in the small intestine. It is rarely possible to detect a lesion in the intestinal wall using high-frequency probes(12). A case of small intestinal tumour diagnosis with abdominal ultrasound despite negative results of other imaging studies has been reported in the literature(10). Secondary lesions in the mesentery (enlarged, hypoechoic lymph nodes, mesenteric fibrosis) may be an indirect indication of a tumour in the intestinal wall(12).
Hepatic metastases of a primary NEN tumour located in the lungs, stomach or colon are usually hypo- or isoechoic compared to the hepatic parenchyma. In tumours arising from the small intestine and pancreas the echogenicity of secondary lesions is various and non-characteristic (hypo-, iso-, hyperechoic or sometimes mixed lesions). In insulinoma tumours, liver metastases usually have decreased echogenicity(13–15). Areas of necrosis are usually found in large tumours (>3 cm) with a Ki-67 proliferation index of >2% and in individuals who have undergone treatment (interferon, embolisation, chemotherapy, radiofrequency ablation). No necrotic changes were observed in patients treated with cold or hot somatostatin analogues(13–15).
On Doppler ultrasound, primary NEN foci and liver and lymph node metastases have a rich network of blood vessels. In tumours with Ki-67 >2% the vascular network may be irregular(13–15).
The sensitivity of transabdominal ultrasound in the diagnosis of metastatic lesions in the liver is 82–88% and its specificity is 92–95%. The sensitivity for pancreatic tumours is lower: 39%(1).
In recent years new ultrasound imaging techniques have been developed that improve the efficacy of NEN diagnosis(15): ultrasound elastography, CEUS, EUS, intraductal ultrasound (IDUS) and intraoperative ultrasound (IOUS).
Endoscopic ultrasound is an invasive imaging method which involves the insertion of a flexible endoscope with a high-frequency ultrasound probe (7.5–12 MHz), which is positioned near the pancreas, stomach, duodenum or rectum. The minimisation of the distance between the probe and the abnormality to be evaluated makes it possible to thoroughly assess anatomical relationships, depth of tumour invasion through the gastrointestinal wall and the presence of metastases in local lymph nodes(1).
Endoscopic ultrasound is a fundamental diagnostic tool for the detection of NEN in the pancreas and the distal part of the colon. Combined with simultaneous fine-needle biopsy, it is the most sensitive method of pancreatic NEN diagnosis. It is a method of choice for the detection of small lesions (even 1–2 mm), particularly those hormonally active and a screening method for patients with genetic abnormalities (e.g. with MEN1 syndrome)(4). In a multi-centre retrospective study investigating the size of pancreatic NEN in patients with MEN1 syndrome using EUS more than 90% of small lesions of less than 7 mm were visualised(16). In other studies the sensitivity of EUS depended on the location of the focal lesion and was 77–100% for tumours located in the head and body of the pancreas and 75–80% for tumours located in the distal part of the pancreas(1,17). Recent studies report that the sensitivity of EUS may be higher than that of computed tomography (91.7% vs 63.3%), particularly for insulinoma (84.2% vs 31.6%)(1,2,4). The sensitivity of EUS in the detection of doudenal lesions is 45–60%(1,2). Comparative studies on conventional examination methods (transabdominal ultrasound, CT and MRI) demonstrated their lower sensitivity compared to EUS(16).
Hormonally active pancreatic neuroendocrine tumours present as single homogeneous, hypoechoic solid tumours (less often normo- and hyperechoic ones) which are characterised by intensive enhancement following contrast administration(16). A cystoid form of the tumour may occur in approximately 10–20% of patients(18). Calcifications in hormonally active and inactive NEN of the pancreas may be found in approximately 25% of cases, while being rarely observed in adenocarcinomas. In larger tumours, the pancreatic duct may become dilated and the pancreatic parenchyma may undergo atrophy(1,18). EUS plays an important role in disease staging, assessment of blood vessel invasion and differential diagnosis of pancreatic tumours of unclear nature (distinguishing between NEN and adenocarcinomas, cystoid lesions and tumours with atypical, poor vasculature). It may be stated that EUS combined with Doppler ultrasound, contrast, elastography and EUS-guided biopsy makes it possible to detect all pancreatic NEN(1,18).
In diagnostic imaging of rectal tumours endoscopic ultrasound is also the most sensitive method for preoperative local staging. A neuroendocrine neoplasm in the form of a polyp presents as a well-defined, iso- or hypoechoic, homogeneous lesion on EUS(19). The sensitivity of this method in the assessment of the tumour and the depth of its invasion in the rectal wall is 76–93%. For the assessment of metastases in the nearby lymph nodes the sensitivity is 61–88%(1,2,4,19).
The assessment of lesions located in the distal part of the ileum is possible on EUS using high-frequency miniprobes inserted through the biopsy channel of a colonoscope(4,19).
An advantage of EUS is also the fact that it is possible to insert a radiofrequency ablation (RFA) probe in the echoendoscope channel, which causes thermal coagulation necrosis of the tumour. It has been demonstrated that this technique is safe and effective in patients with hormonally active NEN of the pancreas who were denied surgery due to comorbidities(13). The disadvantages of EUS include the fact that the result depends on the skills and experience of the examiner and that the field of vision is limited, which may reduce its efficacy in detecting lesions beyond the area of interest(4).
It is possible to achieve an even better visualisation of pancreatic NEN in the immediate vicinity of the pancreatic duct and abnormalities in its lumen by inserting a miniprobe to the pancreatic or bile duct through the biopsy channel of an endoscope (IDUS)(1). The sensitivity of the procedure is around 94% and approximates 100% if the abnormalities in the pancreatic duct are larger than 3 mm(20).
Third-generation contrast agents used for ultrasound diagnosis are gas-filled microvesicles coated with phospholipids with a long half-life and perfusion-dependent greyscale image enhancement(1). On CEUS, focal lesions are assessed based on characteristic vasculature patterns indicating benign or malignant abnormality(15). Primary pancreatic NEN, even small ones, have a good network of blood vessels. Following contrast administration, pancreatic NEN show intensive enhancement in the arterial phase(16). The majority of NEN metastases in the liver (78–86%) show enhancement in the arterial phase following contrast administration with a quick contrast clearance in the venous phase(1,16,17). Wen-Tao
Ultrasound imaging using elastography is an increasingly available technique allowing one to assess tumour hardness. This method may be used to assess focal lesions in the pancreas on EUS and focal lesions of the liver on transabdominal ultrasound. In a study by Iglesias-Garcia
Intraoperative ultrasound (IOUS) is used mainly to diagnose focal lesions in the liver and pancreas, particularly in patients with multiple endocrine neoplasia (MEN) syndromes. The procedure also makes it possible to detect multifocal tumours and metastatic lesions in the liver and assess the distance of a pancreatic tumour, particularly a small one, from the pancreatic duct(1). The sensitivity of IOUS in the detection of tumours is 90%(1).
Transabdominal ultrasound is usually the first diagnostic imaging procedure for NEN. However, the possibility of precise staging of the disease using transabdominal ultrasound is limited due to a number of factors (technical aspects of the procedure, small tumour dimensions and often unfavourable location inaccessible to transabdominal ultrasound). New ultrasound techniques improve the precision of the diagnosis and constitute an important part of a NEN diagnostic process.
Patients with NEN may show a large discrepancy between the clinical presentation and actual stage of the disease. Due to their rare occurrence, atypical symptoms and slow growth, the majority of NEN are diagnosed with a few years’ delay, usually at an advanced stage. Only some neuroendocrine tumours present with characteristic signs of hormonal activity, suggesting the diagnosis(1,12,18,19).
Sometimes in asymptomatic patients or patients undergoing ultrasound examination for non-specific abdominal pain a primary lesion is found in the pancreas, less often in the stomach, duodenum or the retroperitoneal space. Metastatic foci in the liver or lymph nodes may also be found. The search for the primary lesion in a patient with metastatic NEN of an unknown point of origin may be particularly difficult since primary lesions are often small. Depending on the type of visualised changes the examiner should propose a further diagnostic algorithm.
In a reverse situation when NEN is diagnosed based on clinical symptoms and/or biochemical testing, the key steps are to search for the primary lesions and make a baseline assessment of the stage of the neoplastic process. Depending on the symptoms and the type of the suspected NEN one should identify the possible sites of the tumour focusing on the pancreas, intestines, appendix, mesentery and retroperitoneal space (Tab. 2).
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Abdominal
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Abdominal and pelvic
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EUS – endoscopy ultrasound; EUS-FNA – EUS fine-needle aspiration; EUS-RFA – EUS-guided radiofrequency ablation; CEUS – contrast-enhanced ultra-sonography; IDUS – intraductal ultrasonography; IOUS – intraoperative ultrasonography; SRS – somatostatin receptor scintigraphy; SSA – somatostatin analog; PRRT – peptide-receptor radionuclide therapy; 99mTc-SPECT – 99mTc-single-photon emission computed tomography; 68Ga-DOTA-PET – 68Ga--DOTA-positron emission tomography; 18FDG-PET – 18FDG-positron emission tomography; 131I-MIBG – 131I-MIBG – single-photon emission computed tomography