Pancreatic lesions
Pancreatic cystic lesion differential
[edit | edit source]- Unilocular
- Pseudocyst
- IPMN
- Serous cystadenoma
- Simple pancreatic cyst
- Cystic neuroendocrine tumour of the pancreas
- Diffuse pancreatic cysts
- In association with VHL, ADPKD, isolated poycystic disease of the pancreas, or pancreatic cystosis (in CF)
- Macrocystic: multilocular
- Mucinous cystic neoplasm of the pancreas
- IPMN
- Serous cystadenoma
- Acinar cell cystadenocarcinoma
- Hydatid cyst
- Microcystic
- Serous cystadenoma
- Cystic with a solid component
- Walled off necrosis
- Macrocystic tumours
- Solid pseudopapillary tumour of the pancreas
- Primary ductal pancreatic tumour with cystic degeneration
- Cystic degeneration of islet cell tumours (insulinoma or glucagonoma)
- Cystic teratoma
- Metastases to pancreas
Pancreatic solid lesions differential
[edit | edit source]- Neoplastic
- Pancreatic ductal adenocarcinoma
- Acinar cell carcinoma
- Endocrine tumours - PNETs - functional and non-functional
- Non-neoplastic
- Focal pancreatitis, including autoimmune
- Fatty infiltration-replacement
- Intra-pancreatic accessory spleen
- Peri-pancreatic lymph node
- Congenital abnormalities - prominent lobulations, bifid pancreatic tail
- Sarcoidosis
- Castleman disease
Key demographic and clinical features of patients with pancreatic cystic neoplasms[1-4]
| Serous cystadenoma | Mucinous cystic neoplasm | Main-duct intraductal papillary mucinous neoplasm | Branch-duct intraductal papillary mucinous neoplasm | Solid pseudopapillary neoplasm | |
| Age of presentation | Variable, usually 5th to 7th decade | Variable, usually 5th to 7th decade | Variable, usually 5th to 7th decade | Variable, usually 5th to 7th decade | Usually 2nd to 3rd decade |
| Gender distribution | Females >males | Exclusively females | Females = males | Females = males | Females >males |
| Typical clinical presentation | Incidental, less commonly abdominal pain or mass effect | Incidental, less commonly abdominal pain or malignancy related | Incidental or pancreatitis or pancreatic insufficiency or malignancy related | Incidental, less commonly pancreatitis or malignancy related | Incidental or abdominal pain or mass effect |
| Typical imaging characteristics | Microcystic/honeycomb appearance
Oligocystic appearance less common May have central scar or calcification |
Unilocular or septated cyst ± wall calcifications
Solid component, if present, may suggest malignancy |
Dilated main pancreatic duct ± parenchymal atrophy
Solid component, if present, may suggest malignancy |
Dilated pancreatic duct branch or branches
Solid component, if present, may suggest malignancy |
Solid and cystic mass ± calcifications |
| Typical aspirate characteristic | Thin, often bloody | Viscous | Viscous | Viscous or thin | Bloody |
| Typical cytology findings | Cuboidal cells that stain positive for glycogen; yield <50% | Columnar cells with variable atypia
Stains positive for mucin; yield <50% High yield from solid component for malignancy |
Columnar cells with variable atypia
Stains positive for mucin; yield <50% High yield from solid component for malignancy |
Columnar cells with variable atypia
Stains positive for mucin; yield <50% High yield from solid component for malignancy |
Characteristic branching papillae with myxoid stroma
High yield from solid component |
| Typical carcinoembryonic antigen (CEA) level | <5 to 20 ng/mL in majority of lesions | >200 ng/mL in approximately 75% of lesions | Typically elevated (limited data) | >200 ng/mL in approximately 75% of lesions | Insufficient data |
| Typical glucose level | >50 mg/dL in majority | <50 mg/dL in majority | <50 mg/dL (limited data) | <50 mg/dL in majority | Insufficient data |
| Typical DNA analysis | VHL mutation specific | K-ras mutation specific (>90%), not sensitive (<50%)
TP53, PTEN, PIK3CA mutations seen in malignancy |
K-ras and GNAS mutation specific (>90%), not sensitive (<50%)
TP53, PTEN, PIK3CA mutationsseen in malignancy |
K-ras and GNAS mutation specific (>90%), not sensitive (<50%)
TP53, PTEN, PIK3CA mutationsseen in malignancy |
CTNNB1 mutation specific |
| Relative malignant potential | Negligible | Moderate | High | Low to moderate | Moderate to high |
| Treatment | Resect if symptomatic | Resection | Resection and post-resection surveillance | Monitor or resect
Post-resection surveillance required |
Resection |
Cystic neoplasms (classified according to WHO histologic criteria)
[edit | edit source]- Mucinous
Intraductal papillary mucinous neoplasms (IPMN)
[edit | edit source]- Mucinous epithelial neoplasms which arise from pancreatic ducts
- Pathophysiology
- Composed of mucin-producing columnar cells
- Classified as low-grade, moderate, and high-grade dysplasia; and presence or absence of invasive malignancy
- Four subtypes:
- Gastric
- Primarily BD-IPMN
- Typically low-grade
- Intestinal
- Most common type of MD-IPMN
- Found in pancreatic head
- Pancreaticobiliary
- Typically involves main duct, in pancreatic head
- Greatest likelihood of malignancy
- Poor prognosis
- Oncocytic
- Gastric
- Classification
- Main duct
- Diffuse or segmental involvement of the main PD, with radiographic findings of main duct >5mm without any other cause of obstruction
- Risk of high-grade dysplasia or invasive carcinoma (30-50% risk of invasive cancer at time of presentation)
- Branch duct
- Involve smaller side branches but not main duct
- Typically occur in younger patients
- More common than main duct (10:1)
- Can occur anywhere in pancreas
- Often multifocal (multiplicity of cysts favours BD-IPMN)
- Lower risk of malignant transformation
- Overall risk of invasive malignant disease is 10-15% (2-3% per year)
- Mixed
- Side branch IPMNs that extend into the main duct, and often lead to upstream dilation
- Behave clinically like main duct lesions - 30-50% risk of invasive malignancy at presentation
- Main duct
- Clinical presentation
- Most commonly 50-70yo
- Mostly found incidentally
- If symptoms are present, they are non-specific
- Can develop pancreatitis-like symptoms, especially with MD-IPMN
- Diagnosis
- Imaging
- CT and MRI are equivalent for tumour type, location, development of additional lesions, lymph node and organ mets, invasion
- MRI better for ?septae and ?mural nodules and ?solid components and more accurately defines involvement of main PD
- Endoscopy
- Fish-mouth sign - pathognomic
- Other features below on EUS
- Imaging
- Management
- MD-IPMN or mixed-type IPMN: Resect if medically fit
- BD-IPMN: Risk stratification with Fukuoka guidelines
- High-risk stigmata (surgery recommended if any one of these)
- Enhancing mural nodule >5mm
- Main duct size >=10mm
- Obstructive jaundice
- Worrisome features (needs EUS if any of these)
- Size >3cm
- Main PD size 5-9mm
- Abrupt change in calibre of PD with distal pancreatic atrophy
- Symptoms other than jaundice
- Thickened, enhancing cyst walls
- Enhancing mural nodule <5mm
- Extra worrisome features according to Sabiston: clinical pancreatitis, elevated CA 19-9, cyst growth of >5mm over two years
- EUS/histo features: (operate if any of these)
- Definite mural nodule/s >=5mm
- Main duct features suspicious for involvement
- Cytology suspicious or positive for malignancy
- Other factors
- FHx pancreatic cancer (two or more first-degree relatives)
- Inability to tolerate surgery
- Patient preference
- High-risk stigmata (surgery recommended if any one of these)
- Operations
- Extent of resection depends on location and pathologic features
- BD-IPMN - target the lesion of concern with partial pancreatectomy
- MD-IPMN - harder to determine the extent of microscopic abnormality within the duct. Generally right-sided pancreatectomy with frozen section, with total pancreatectomy for those with HGD/cancer at margin.
- Prognosis
- Survival 77% 5 years for non-invasive IPMNs
- 43% for invasive IPMNs
- Surveillance
- See below
- Extra-pancreatic malignancy
- High-risk for cancer in other places
- Frequent locations include breast, colon and prostate
Mucinous cystic neoplasms (MCN)
[edit | edit source]- Mucin-producing cystic tumours which do not communicate with the pancreatic duct (therefore different from IPMN)
- Pathophysiology
- Dysplastic neoplasms with clear-cut malignant potential
- Felt to follow adenoma-to-carcinoma sequence - malignancy risk 5-15%
- When invasive type, not as aggressive as ductal adenocarcinoma
- 5 year survival 50-60% expected after resection
- Mostly offer adjuvant chemotherapy, especially with positive nodes
- Singular, large, thick-walled cysts, lined with mucin-secreting columnar epithelium, almost never communicating with ductal system
- Pathology shows 'ovarian-type' stroma within the cyst capsule, typically seen histologically after resection
- Stain positive for oestrogen and progesterone in most cases
- Dysplastic neoplasms with clear-cut malignant potential
- Presentation
- Strong female predilection, most commonly seen in body and tail of pancreas
- Mean age at presentation 45yo
- 20% have had pancreatitis
- Often initially misdiagnosed as pseudocyst - to differentiate, may need FNA with aspirate showing a fluid high in mucin and CEA (pseudocyst is higher in amylase)
- Typically asymptomatic - 50% can have vague abdominal pain
- Imaging
- Solitary cyst with fine septations and a rim of calcification
- Eggshell calcification, larger tumour size, or a mural nodule on cross-sectional imaging are suggestive of malignancy
- Aspirate
- Mucin-rich
- CEA > 192mg/ml
- Low amylase
- Management
- Recommend resection in ALL suitable operative candidates - usually distal pancreatectomy. Curative if no invasive malignant disease.
- Observation may be considered in medically unfit patients
- Nondysplastic mucinous cysts (NDMC)
- Unclear whether these cysts are entirely benign or represent the earliest stage of MCNs
- Solid pseudopapillary neoplasm
- Lymphoepithelial cysts
Serous cystic neoplasm
[edit | edit source]- Serous cystadenoma
- Epidemiology
- Tend to occur in older patients
- Pathology
- Benign
- True epithelium lined with glycogen-rich, clear, cuboidal cells that stain positive for periodic acid-Schiff
- Don't communicate with ductal system
- Mostly found HOP, but can be anywhere in gland, variable size and morphology
- FNA of cyst fluid yields clear serous fluid low in CEA and mucin
- Sometimes see cellular atypia leading to diagnostic uncertainty
- Presentation
- Often completely asymptomatic
- Commonly present with vague pain
- Can cause mass symptoms (uncommon)
- Bile duct obstruction
- Pancreatic duct obstruction
- Gastric outlet obstruction
- Imaging
- Thin-walled capsule with microcystic pattern with thin-walled septae
- 'Sun-burst' pattern due to central calcification and radiating septa (seen in 10-20%)
- Management
- Given they are overwhelmingly benign, observation is the rule
- Some will increase in size, up to about 0.5cm/year
- Larger cysts can increase more quickly
- Intervention indications
- Symptomatic lesions (generally need to be >4cm)
- Consider intervention for larger cysts or rapidly-enlarging ones
- Epidemiology
- Serous cystadenocarcinoma (very rare)
- Thought to represent malignant degeneration of SCA
- There are only about 50 cases in the literature
- Serous cystadenoma
Solid pseudopapillary neoplasms (SPN)
[edit | edit source]- Usually occur 10-30yo
- F>M (90%)
- Usually incidental, or abdominal mass effect causing pain
- Typically seen as a solid and cystic mass +/- calcifications
- Bloody aspirate
- Cytology - characteristic branching papillae with myxoid stroma
- Resect when found
- Generally considered a low-grade malignancy, although prognosis is good if resected
Autoimmune pancreatitis
[edit | edit source]- See section under pancreatitis
Acinar cell carcinoma
[edit | edit source]- Rare, with unique features
- Arise from acinar cells - site of synthesis of exocrine enzymes
- Risk factors
- Mid-50s
- Males
- Presentation
- Non--specific symptoms
- Often >5cm at diagnosis
- Sometimes generate lipase - can cause paraneoplastic syndromes in some patients
- Polyarthralgia
- Eosinophilia
- Subcutaneous fat necrosis and rashes ('pancreatic panniculitis')
- Mostly malignant - should be resected
- Better prognosis than PDAC
Primary pancreatic lymphoma
[edit | edit source]- Exceedingly rare - once in a career type diagnosis
- Vague symptoms including B symptoms
- Diagnosed on FNA
- Treatment
- Chemotherapy is first-line (CHOP)
- Resection is very difficult and fraught with complications
Metastatic lesions
[edit | edit source]- Rare
- RCC can do it
- Also melanoma, breast, lung, colon, gynae
- Mostly seen as hypervascular tumours, which is unusual in the pancreas