hand out pancreatic cytology Sarajevo 2016-06-18 out pancreatic... · PANCREATIC CYTOLOGY ... •...

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2016-06-16 1 PANCREATIC CYTOLOGY Mehmet Akif Demir, MD Clinical Pathologyand Genetics Sahlgrenska University Hospital Gothenburg-Sweden Papanicolau Society of Cytopathology 5 Commities and their publications in 2014 Adler D, Schmidt CM, Al-Haddad M, et al. Clinical evaluation, imaging studies, indications for cytologic study, and preprocedural requirements for duct brushing studies and pancreatic FNA: The Papanicolau Society of Cytopathology recommendations for pancreatic and biliary cytology. Diagnostic Cytopathology, 2014;42(4):325-332 Brugge W, DeWitt J, KlapmanJB. Techniques for cytologic sampling of pancreatic and bile duct lesions. Diagnostic Cytopathology, 2014; 42(4):333-337 Pitman MB, Centeno BA, Ali SZ, et al. Standardized terminology and nomenclature for pancreatobiliary cytology: The Papanicolau Society of Cytopathology Guidelines. Diagnostic Cytopathology 2014;42(4):338-350. Layfield LJ, Ehya H, Fille AC et al. Utilisation of ancillary studies in the cytologic diagnosis of biliary tract and pancreatic lesions: The Papanicolau Society of Cytopathology Guidelines for Pancreatobiliary Cytology. 2014 Diagnostic Cytopathology, 42(4):351-362 Kurtycz DFI, Field A, TabatabaiL, et al. Post-brushing and fine needle-aspiration biopsy follow-up and treatment options for patients with pancreatobiliary lesions: The papanicolau Society of Cytopathology Guidelines. Cytojournal 2014; 11(Suppl 1):5. Published online 2014 Jun 2. doi: 10.4103/1742-6413.133356 Otherreferences Pitman MB, Layfield LJ. Guidelines for pancreaticobiliary cytology from the Papanicolau Society of Cytopathology: a review. Cancer Cytopathol 2014;122:399-411. Layfield LJ, Dodd L, Factor R, Schmidt RL. Malignancy risk associated with diagnostic categories defined by the Papanicolau Society of Cytopathology Pancreatobiliary Guidelines. Cancer Cytopathology 2014;122:420-427. Benefits of a common nomenclature Standardization of nomenclature Unifies reporting of disease categories Contributes to evaluation of interobserver variability Improves intraobserver reproducibility Better alignspatient management options with interpretations Improves patient care Universally understanding by clinicians and pathologists ”Statistics” (economical aspects) Categories General tiered System in Cytology PSC suggestion for PB cytology Nondiagnostic I. Nondiagnostic Negative (Benign) II. Negative Atypical III. Atypical Suspicious IV. Neoplastic -Benign -Other V. Suspicious Positive VI. Positive/Malignant Management Malignant ………………………..surgery Premalignant Low-intermediate grade………observation with repeat sampling Hig grade …………………………….surgery Neoplasm…………………………..surgery or observation Benign………………………………..medical management Endocrine tumors………………. surgery, chemotherapy, observation Clinical information Patient age, gender Symptoms Anamnesis (important details that may effect diagnosis)

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Page 1: hand out pancreatic cytology Sarajevo 2016-06-18 out pancreatic... · PANCREATIC CYTOLOGY ... • GIST WHO 2010 classification ... between biopsy & FNAC Hot-spots and nucleolar ”hot-spots”.

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PANCREATIC CYTOLOGY

Mehmet Akif Demir, MD

Clinical Pathology and Genetics

Sahlgrenska University Hospital Gothenburg-Sweden

Papanicolau Society of Cytopathology5 Commities and their publications in 2014

• Adler D, Schmidt CM, Al-Haddad M, et al. Clinical evaluation, imaging studies, indications for cytologic study, and preprocedural requirements for duct brushing studies and pancreatic FNA: The Papanicolau Society of Cytopathology recommendations for pancreatic and biliary cytology. Diagnostic Cytopathology, 2014;42(4):325-332

• Brugge W, DeWitt J, Klapman JB. Techniques for cytologic sampling of pancreatic and bile duct lesions. Diagnostic Cytopathology, 2014; 42(4):333-337

• Pitman MB, Centeno BA, Ali SZ, et al. Standardized terminology and nomenclature for pancreatobiliary cytology: The Papanicolau Society of Cytopathology Guidelines. Diagnostic Cytopathology 2014;42(4):338-350.

• Layfield LJ, Ehya H, Fille AC et al. Utilisation of ancillary studies in the cytologic diagnosis of biliary tract and pancreatic lesions: The Papanicolau Society of Cytopathology Guidelines for Pancreatobiliary Cytology. 2014 Diagnostic Cytopathology, 42(4):351-362

• Kurtycz DFI, Field A, Tabatabai L, et al. Post-brushing and fine needle-aspiration biopsy follow-up and treatment options for patients with pancreatobiliary lesions: The papanicolau Society of Cytopathology Guidelines. Cytojournal 2014; 11(Suppl 1):5. Published online 2014 Jun 2. doi: 10.4103/1742-6413.133356

Other references

• Pitman MB, Layfield LJ. Guidelines for pancreaticobiliary cytology from the Papanicolau Society of Cytopathology: a review. Cancer Cytopathol 2014;122:399-411.

• Layfield LJ, Dodd L, Factor R, Schmidt RL. Malignancy risk associated with diagnostic categories defined by the Papanicolau Society of Cytopathology Pancreatobiliary Guidelines. Cancer Cytopathology 2014;122:420-427.

Benefits of a common nomenclature

• Standardization of nomenclature

• Unifies reporting of disease categories

• Contributes to evaluation of interobserver variability

• Improves intraobserver reproducibility

• Better aligns patient management options with interpretations

• Improves patient care

• Universally understanding by clinicians and pathologists

• ”Statistics” (economical aspects)

Categories

General tiered System in Cytology PSC suggestion for PB cytology

Nondiagnostic I. Nondiagnostic

Negative (Benign) II. Negative

Atypical III. Atypical

Suspicious IV. Neoplastic

-Benign

-Other

V. Suspicious

Positive VI. Positive/Malignant

Management

• Malignant ………………………..surgery

• Premalignant

• Low-intermediate grade………observation with repeat sampling

• Hig grade …………………………….surgery

• Neoplasm…………………………..surgery or observation

• Benign………………………………..medical management

• Endocrine tumors………………. surgery, chemotherapy, observation

Clinical information

• Patient age, gender

• Symptoms

• Anamnesis (important details that may effect diagnosis)

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Radiological information

• Localisation of the lesion in the pancreas

• Characteristics of the lesion• Size, growth pattern (rounded, infiltrative)

• Solid or cystic (unilocular, multilocular, solid with cystic component, thickness of the wall, calcifications)

• Vascularisation

• Cyst contents: thin, thick, mucinous, viscous, water-clear, brown,…

• NEEDLE TRACT!!! EUS Via?• Esophagus?

• Gastric wall?

• Duodenum?

Ancillary tests

• CEA

• AMYLASE

• Molecular analyses: KRAS, GNAS

• Immunocytochemistry & Immunohistochemistry (cell-block)

Differential Diagnostic Approach

SOLID

• Chronic pancreatitis

• Ductal adenocarcinoma

• Acinar cell carcinoma

• Pancreatic endocrine neoplasm

• Solid pseudopapillary tumor

• Pancreatoblastoma

• Metastasis

CYSTIC

• Pseudocyst

• Serous cyst

• Mucinous cyst (MCN, IPMN)

• Cystic degeneration of typicallysolid tumors

• Rare cystic lesions• Simple cysts

• Lymphoepthelial cyst

• Peripancreatic cysts

Important!

• DO NOT DIAGNOSE AS ”TUMOR” IF THERE IS NO RADIOLOGIC MASS LESION!!!

• NO MASS LESION: MOST PROBABLY NORMAL ACINAR CELLS/FRAGMENT, NOT ACINAR CELL CARCINOMA OR NEUROENDOCRINE TUMOR!!!

NormalNormal

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Contamination !!!

• Gastric

• Intestinal

• Contamination or a component of the tumor?

Gastric contamination, cell-block

Duodenal contamination

Cystic lesions

• Direct smears

• Other analyses on fresh undiluted cyst fluid

• CEA

• Molecular

• Cytomorphologic

• Cytospin

• Cellblock

http://www.radiologyassistant.nl/en/p4ec7bb77267de/pancreas-cystic-lesions.html

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Amylase & CEA

• Amylase levels

• High levels associated with pseudocysts

• May be increased in IPMN and LEC

• Not increased in serous cysts and MCN

• Elevated CEA: in favour of mucinous cyst

• Cannot distinguish IPMN from MCN

• No correlation with malignancy

• May be increased in duplication cysts, lymphoepithelial cysts

Molecular tests

• KRAS• supports a neoplastic mucinous cyst

• Cannot distinguish IPMN and MCN

• Does not contribute grading

• GNAS• supports IPMN over MCN

• No correlation with grade

• RNF43• Supports a mucinous cyst

• Does not distinguish IPMN and MCN

• 3p deletions• 3p25, VHL gene, and other 3p deletions supports Serous Cystic Adenoma (SCA)

• CTNNB1 (Beta-catenin) deletion• Support Solid Pseudopapillary Neoplasm (SPN)

Suggested Categories (Papanicolau Society ofCytopathologists)

• I. NONDIAGNOSTIC

• II. NEGATIVE

• III. ATYPIA

• IV. NEOPLASTIC

• BENIGN

• OTHER

• SUSPICIOUS FOR MALIGNANCY

• POSITIVE/MALIGNANT

I. Nondiagnostic

• A specimen that provides no diagnostic or useful information aboutthe lesion sampled.

• Criteria• Preparation artifact

• Obscuring artifact

• Gastrointestinal epithelium only

• Normal pancreatic tissue elements in the setting of a clearly defined mass by imaging

• Acellular aspirates of a solid mass or pancreatobiliary brushing

• Acellular aspirate of a cyst without evidence of a mucinous etiology (thickmucin, elevated CEA or KRAS mutation)

II: Negative

• Definition: A sample that contains adequate cellular and/or extracellular tissue to evaluate or define a non-neoplastic lesion thatis identified on imaging.

• Includes the presence of normal pancreatic tissue in the appropriateclinical setting such a vague fullness on imaging and no distict masslesion.

(Benign pancreas, Chronic pancreatitis, Autoimmune pancreatitis, pseudocyst, lymphoepithelial cyst, accessory spleen)

III. Atypical

• Definition: Cells with cytoplasmic, nuclear, or architectural features not consistent with normal or reactive cellular components of the pancreas or bile ducts, and insufficient features to classify them as a neoplasm or suspicious for a high grade malignancy.

• The findings do not explain a lesion identified on imaging studies

• Follow-up evaluation is warranted.

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Atypical

• Mild-moderate cellular atypia, NOS

• Mucinous/ductal epithelium with mild-moderate nuclear atypia (from a solid lesion or not clearly from a mucinous cyst)

• PanIN

• GI contamination with atypia

• Ductal atypia in bile duct samples

IV. Neoplastic

• Benign

• Other

IV. Neoplastic: Benign

• Definition: Cytological specimen sufficientlycellular and representative, with or without the context of clinical, imaging, and ancillary studies, to be diagnostic of a benign neoplasm.

• SCA (Serous cystadenoma)• Sparse cellularity

• Clean or bloody background

• Flat sheets and loose clusters

• Bland cuboidal cells

• Clear, finely vacuolated or granular cytoplasm with indistinct borders

• Associated hemosiderin-laden macrophages

• Low CEA; low amylase

• No KRAS mutation

IV. Neoplastic: Other

• Definition: A neoplasm that is either premalignant such as IPMN or MCN with low, intermediate or high grade dysplasia, or a solid-cellular neoplasmsuch as well-differentiated PanNET or SPN

• PanNET

• SPN

• Mucinous cyst (IPMN or MCN), not otherwise specified

• Mucinous cyst (IPMN or MCN), with low-grade atypia

• Mucinous cyst (IPMN or MCN) with high-grade atypia

• GIST

WHO 2010 classification of the primary neuroendocrine tumors of the gastrointestinal system

• NET G1 (carcinoid) (Neuroendocrine Tumor Gr-1)

• NET G2 (Neuroendocrine Tumor Gr-2)

• NEC (Neuroendocrine Carcinoma, large cell or small cell type)

• MANEC (Mixed Adenoneuroendocrine Carcinoma)

• Hyperplastic and preneoplastic lesions.

• NETs usually show local metastases but NECs are usually much more aggressive tumors and can show widespread metastases

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PanNET

• Almost the same classification and grading system as in gastrointestinal system

• “Pancreatic small cell NECs may not express neuroendocrine markersand this does not preclude the diagnosis so long as alternative diagnostic considerations are excluded”.

• NET usually p53(-), NEC usually p53(+)

• NET can be positive for CD99. t(11;22) translocation can be helpful in differential diagnosis of PNET.

ENETS (European Neuroendocrine Tumor Society) grading*

• G1

• mitotic count <2/10HPF and/or

• Ki 67 index 2≤ %

• G2

• mitotic count 2-20/10HPF and/or

• Ki67 index 3-20

• G3

• mitotic count >20/10HPF and/or

• Ki67 index >20

• Mitotic count in at least 50HPFs

• Ki 67 index as a percentage of 500-2000 cells counted in areas of strongest nuclear labelling (hot spots)

ENETS (European Neuroendocrine Tumor Society) gradinG

High Ki67 in FNA but about 1% in

surgical biopsy ??? 5 months interval

between biopsy & FNAC

Hot-spots and nucleolar ”hot-

spots”. How can we standardize

Ki-67 counting in cytology?

Cyto Ki67 Cyto Ki67

CASE: Scull base neuroendocrine tumour /lymph node FNAC…

IHC-panel for PanNET/NEC

• Chromogranin-A

• CK8/18

• Gastrin

• Glukagon

• Insulin

• Ki67

• Pancreatic Polypeptid

• Somatostatin

• Synaptophysin

• (Trypsin)

• (Beta-cathenin)

Case: Pancreas EUSPanNET

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GASTRIN

SYNAPTOPHYSIN

CK 8/18

CHROMOGRANIN AZES

Case-pancreas tumor: SCPPN

Onlymucin: Category?

Category?

Case:pancreas MCN?

CEA

Whipple: PanIN-I-II, IPMN borderline, kr pancreatit, squa metap

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Case: Cytologically lowgrade MCN/IPMN?Whipple: PanIn-II

V: Suspicious for malignancy

• Definition:

• A specimen is suspicious for malignancy when some but not all of the criteria of a specific malignant neoplasm are present, mainly pancreatic adenocarcinoma.

• The cytological features raise strong suspicion for malignancy, but the findings are qualitatively and/or quantitatively insufficient for a conclusive diagnosis.

VI: Positive/Malignant

• Definition: Unequivocal display of malignant cytologiccharacteristics

• Adenocarcinoma of the pancreatobiliary ducts, and variants

• Acinar cell carcinoma

• High-grade neuroendocrine carcinoma (small and large cell type)

• Pancreatoblastoma

• Lymphoma

• Metastases

Acinar cell carcinoma

Acinar cell carcinoma

TrypsinTrypsinTrypsinTrypsin (!!!positive in normal cells also)

Cell-block

Cytospin

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IHCC-panel for GIST

• ASMA

• CD34

• C-KIT

• DESMIN

• DOG-1

• Ki-67

• S100

C-kit

CD34

DOG-1

Ki-67

CASEOld man with a3 cm tumorin the pacreaticcorpus

Renal Cell Carcinoma metastasis

CD10

VIMENTIN

CARBA

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