Pancreatic neuroendocrine tumors (NETs)

In the case of F-PanNET, special laboratory tests can detect a hormone produced in excess in the blood (insulin, gastrin, VIP...).

Insulinoma can be diagnosed by measuring blood glucose and insulin levels. A fasting test (prolonged fasting for 72 hours in the absence of symptoms of hypoglycemia) can be useful for diagnosis.

A diagnosis of gastrinoma can be made by measuring blood gastrin levels; if gastrin levels are borderline or undiagnostic, a secretin stimulation test, which causes a rapid increase in blood gastrin levels in patients with gastrinoma, can be used.

RADIOLOGIC EXAMINATIONS

The following instrumental examinations are used to confirm the presumptive diagnosis, determine the location of the tumor, assess its relationship to the surrounding structures, and make a judgment about surgical removal:

• computed tomography (CT) with contrast agent: it allows to localize even small lesions, study the relationship with adjacent structures (especially vascular structures) and assess the presence of metastases (in lymph nodes and liver);
• magnetic resonance imaging (MRI) with contrast agent: the information obtained with this technique is similar to that obtained with CT to characterize a primary pancreatic tumor; thanks to the introduction of a hepatospecific contrast agent, it also allows the assessment of liver lesions with suspected metastases with greater precision than a CT examination;
• ecoendoscopy: this examination is similar to gastroscopy, in which an instrument called an endoscope is inserted through the mouth into the stomach and duodenum with a small ultrasound probe attached, allowing accurate visualization of the pancreas through the walls of the stomach and duodenum. It can be particularly useful for detecting very small tumors; it is also a technique that allows a small sample of the tumor (needle aspiration) to be taken for analysis and pathological diagnosis;
• PET gallium 68-DOTA-peptide: it involves the use of a radiopharmaceutical that can bind to somatostatin receptors, which are usually abundantly expressed in neuroendocrine tumors. This type of receptor study allows not only to confirm the diagnosis but also to select patients who may respond to therapy with analogue somatostatin drugs.
• 18F-FDG PET: 18FDG accumulates in neoplastic lesions with high glucose metabolism. The higher the absorption of this tracer, the more aggressive the tumor.

Treatment of pancreatic neuroendocrine tumors is multidisciplinary and should be appropriate for the type of tumor, the extent of the lesion, and the associated symptoms.

All patients with PanNET who come to us are discussed collegially within the San Raffaele NET Multidisciplinary Group, which meets every two weeks to improve the diagnosis and therapy of these tumors. The multidisciplinary team includes: surgeons, endocrinologists, oncologists, radiologists, pathologists, nuclear physicians, and endoscopists.

• Active surveillance: it is offered to patients with non-functioning, asymptomatic, incidentally discovered neuroendocrine tumors less than 2 cm in size, which usually do not exhibit aggressive characteristics and tend to remain stable in size. Active surveillance includes radiologic examination (ultrasound/magnetic resonance imaging) every 6 months for the first 2 years after diagnosis and every 12 months thereafter.
• Surgery: surgical removal is the method of first choice and can permanently cure the tumor in most cases. Possible interventions are duodenocephalopancreasectomy (DCP), distal pancreasectomy, enucleation or, in rare cases, intermediate pancreasectomy and total pancreasectomy. Some of these operations (distal pancreasectomy, intermediate pancreasectomy and enucleation) can be performed using a minimally invasive laparoscopic access.
• Somatostatin analogues (octreotide/lanreotide): these drugs can be given as monthly injections to patients with neuroendocrine neoplasms that cannot be removed surgically, provided they express somatostatin receptors. These drugs can both slow tumor growth and control symptoms in the case of functioning tumors.
• Radiotherapy: this therapy is usually given to patients with metastatic or inoperable locally spread tumors. It involves the use of a somatostatin analog drug appropriately radioactively labeled (yttrium or lutetium). The radiopharmaceutical administered intravenously recognizes its target by binding the somatostatin analog to its receptors and allows selective irradiation of tumor cells.
• Other antitumor therapies are usually reserved for patients with tumors that cannot be removed surgically or are metastatic, biologically aggressive and/or unresponsive to somatostatin analog therapy. Both conventional chemotherapy and “biological” drugs selectively affecting the mechanisms responsible for growth and metastasis of these tumors (everolimus and sunitinib) are used.

In resectable pancreatic cancer, postoperative adjuvant radiotherapy may be considered for positive lymph node metastases or resection margins. Radical radiotherapy is indicated in patients with unresectable disease. The available technologies, capable of obtaining a high dose conformation with consequent saving of the surrounding risk organs, have made it possible to develop hypofractionation protocols in 15 fractions. Currently, disease control even in advanced cases with combined treatment is around 27 months. In selected cases it is possible to use a hypofractionation with stereotaxic technique in 5 sessions for curative or even symptomatic purposes.