review and updates of immunohistochemistry inselected salivary gland and head and neck tumors
TRANSCRIPT
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Thanks to my resident Dr. Babar Yasin for making this presentation.
JOURNEL CLUB PRESENTATION
Review and Updates of Immunohistochemistry inSelected Salivary Gland and Head and Neck Tumors.
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Review and Updates of Immunohistochemistry inSelected Salivary Gland and Head and Neck Tumors
Shaobo Zhu, MD; Conrad Schuerch, MD; Jennifer Hunt, MD
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Background:34 benign and malignant salivary
gland epithelial tumors according to the 2005 classification of the World Health Organization.
Diverse morphology and overlapping histologic features.
Immunohistochemistry is an adjunct tool to identify the cellular differentiation and assign correct classifications.
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3 major pairs of salivary glands and many minor salivary glands.
The glands are composed of acini (serous, mucinous, and mixed) and ducts (intercalated, striated, and excretory).
The acini and intercalated duct are surrounded by myoepithelial cells.
The striated duct and excretory duct are surrounded by basal cells.
Most salivary gland tumors originate from acinar/ductal epithelial cells (luminal cells) and/or myoepithelial/basal cells (abluminal cells).
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Monophasic tumors : myoepithelioma, acinic cell carcinoma, and salivary duct carcinoma.
Biphasic tumors includes tumors pleomorphic adenoma, epithelial myoepithelial carcinoma, and adenoid cystic carcinoma.
Some tumors demonstrate other unique cellular differentiation, such as sebaceous adenoma/carcinoma, lymphadenoma, and mucoepidermoid carcinoma.
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The acinar/ductal epithelial cells are:
Positive for keratins (CK7 and CAM 5.2) and epithelial membrane antigen (EMA).
They are focally positive or negative for high molecular-weight keratins (HMWKs; CK5/6 and 34bE12)
Negative for p63, myoid markers (smooth muscle myosin heavy chain, smooth muscle actin, calponin), and CK20
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A-Keratin B- CAM 5.23.SOX10
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Myoepithelial cells:
Positive for p63, myoid markers, vimentin, S100, and HMWKs (CK5/6, 34bE12),
Weak expression for CK7 and CAM 5.2
No expression for EMA.
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Basal cells:Positive for p63 and HMWKs (CK5/6,
34bE12)Weakly positive or negative for CK7, CAM
5.2 and myoid markers (SMMHC, SMA, calponin)
Negative for CK20, vimentin, S100, and EMA.
(p63 also stains squamous epithelium)
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A, Calponin. B, SMA. C, SMHC. D, Cytokeratin 5/6. E, p63. F, S100
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SOX10 expression
SOX10-positive tumors1) Acinic cell carcinomas2) Adenoid cystic carcinomas3) Epithelial-myoepithelial carcinomas4) Myoepithelial carcinomas5) Pleomorphic adenomas
SOX10-negative tumors1) Salivary duct carcinomas2) Mucoepidermoid carcinomas3) Squamous cell carcinomas4) Oncocytic carcinomas/oncocytomas5) Warthin tumors
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Acinic Cell Carcinoma
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Demonstrates both serous acinar and intercalated ductal epithelial differentiation.
Express CK7 and CAM 5.2
Negative for p63 and CK20, myoid markers.
Positive for DOG1.(DOG1 with PAS can be used to distinguish it from mammary analogue secretory carcinoma)
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Mammary Analogue Secretory CarcinomaHistologically, immunohistochemically, and
genetically similar to secretory carcinoma of the breast.
The tumor has a t(12;15)(p13;q25) ETV6-NTRK3 translocation that is also present in breast secretory carcinoma.
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Positive for S100, mammaglobin, CK7, CK8, CK18, CK19, 34bE12, EMA, GCDFP-15, GATA3, STAT5a, MUC1, MUC4, and vimentin.
Basal cell/myoepithelial cell markers usually do not show expression in the tumor.
Negative for androgen receptor, ER, PR, HER2/neu.
The MIB-1 indices range between 5% and 28%.46
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Acinic cell carcinoma
Mammary analogue secretory carcinoma
CK8, CK 19 NEGATIVE POSITIVE
GCDFP-15, Mammoglonin
RARELY POSITIVE POSITIVE
MUC4, S100 NEGATIVE POSITIVE
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mammaglobin and S100 expression can be seen in polymorphous low-grade adenocarcinomas (60%) and adenoid cystic carcinomas (13.3%).
However both these tumors are positive for p63 and negative for GCDFP-15.
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Mucoepidermoid carcinoma
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Positive for CK5, CK6, CK7, CK8, CK14, CK18, CK19, EMA, CEA, and p63
CK20, SMA, muscle specific actin (MSA), and S100.
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Strong staining for p63 helps differentiating Mucoepidermoid carcinoma from acinic cell carcinoma, oncocytoma and oncocytic carcinoma and mammary analogue secretory carcinoma.mmary analogue secretory carcinoma
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Myoepithelial Carcinoma
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Immunoreactivity for both keratins and at least 1 myoepithelial marker is required for the diagnosis.
vimentin, calponin, S100, CK AE1/3, 34bE12, CAM 5.2, EMA caldesmon, SMA, MSA, GAFP
Calponin is the most sensitive and specific marker to identify myoepithelial differentiation.
A panel including CK AE1/3, CAM 5.2, CK5/6, calponin, SMA, S100, and vimentin, can be helpful to make an accurate diagnosis.
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Markers for Salivary Gland Tumors With Clear Cell Differentiation
ACC MEC MC EMC OC/OCA CCC
p63 _ + + + outer layer
Scant peripheral
+
Calponin/SMA/SMMHC
_ _ + + outer layer
_ _
CK7/CAM 5.2
+ _ +/- + inner layer
+ +
SOX10 + _ + + _
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Salivary Duct Carcinoma
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AR, GCDFP-15, GATA3, CK AE1/3, CK7, 34bE12, CEA, and EMA.
Ki-67 expression markedly increased.
The immunophenotype AR+/ER-/PR-/GCDFP+ is characteristic of salivary duct carcinoma, but it does not completely exclude metastasis from the breast, which might also be AR+, ER/PR –
80% of salivary duct carcinomas show HER2/ neu and p53 overexpression, which correlates to poor prognosis.
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Prostatic acid phosphatase and prostate-specific antigen expression can be detected.
In men with unknown prostatic acid phosphatase–positive and prostate-specific antigen positive metastatic carcinoma, salivary duct carcinoma should be included in the differential diagnosis in addition to prostatic adenocarcinoma.
CK7 and HMWKs are helpful.
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Markers for Salivary Gland Tumors With Oncocytic Differentiation
MEC EMC ACC OC/OCA SDCp63 + +outer
layer_ +
peripheral_
Calponin/SMA/SMMHC
_ +outer layer
_ _ _
CK7/CAM 5.2
_ + inner layer
+ + +
AR _ _ _ _ +SOX10 _ + + _ _
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Adenoid Cystic Carcinoma
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Malignant biphasic epithelial tumor composed of modified myoepithelial and ductal cells.
Both ductal and myoepithelial/basal cell markers, such as CK7, CAM 5.2, calponin, SMA, SMMHC, p63, SOX10, and S100.
Most adenoid cystic carcinomas showed strong and diffuse expression of c-KIT
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Overexpression of Ki-67 and p5 associated with poor prognosis.
A recurrent t(6;9)(q22-23;p23-24) translocation identified in adenoid cystic carcinoma. This leads to the fusion of MYB and NFIB.
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Polymorphous Low-Grade Adenocarcinoma
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Expresses CK AE1/3, CAM 5.2, 34bE12, EMA, p53, p63, vimentin, bcl-2, S100.
Overlapping histologic features with pleomorphic adenoma/canalicular adenoma and adenoid cystic carcinoma (especially in small biopsies).
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Differentiation of Adenoid Cystic Carcinoma, Polymorphous Low-Grade Adenocarcinoma,and Pleomorphic Adenoma
c-KIT Calponin/SMA
CK7 MIB-1 PLGA1 GFAP
PA -/+ + + luminal
<5% + +
PLGA -/+ - + all cells
<5% - -
AdCC + + + luminal cells
> 10% - -