Immunophenotypic Heterogeneity of Primary Sinonasal Melanoma With Aberrant Expression of Neuroendocrine Markers and Calponin

Lee, Hwajeong; Torres, Frank X.; McLean, Scott A.; Chen, Ruey; Lee, Min Won

doi:10.1097/pai.0b013e3181ee8dcb

Cited by 31 publications

(33 citation statements)

References 24 publications

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“…Similarly, Shah et al 33 found only a single neurofilamentpositive melanoma out of 64 examined melanomas. Neurofilament expression has, however, been reported in a higher percentage of melanomas in some small series, including those of Eyden et al, 11 Lee et al, 9 and the previously mentioned abstract published by Azam et al 23 Neurofilament expression has also been reported in very rare melanomas showing overt ganglioneuromatous differentiation. 34 With the exception of the abstract published by Azam et al, 23 we are aware of only a single study that has systematically evaluated glial fibrillary acidic protein expression in melanoma, by Iwamoto et al, 35 showing expression in 9/17 (53%) spindled and 2/10 (20%) melanomas.…”

Section: Modern Pathology (2015) 28 1033-1042mentioning

confidence: 79%

“…49 On the other hand, round cell melanomas, particularly in the sinonasal region, often show patchy or no S100 protein expression, showing instead uniform expression of more specific melanocytic markers. 9,50 In summary, we have identified aberrant expression of various intermediate filaments, including keratins, desmin, neurofilament protein and glial fibrillary acidic protein, and of the neuroendocrine marker synaptophysin in significant subsets of both epithelioid and spindle melanomas. These findings have obvious implications with regard to the use of ancillary immunohistochemical studies in the diagnosis of melanoma, and emphasize the need to employ a broad panel of markers in the differential diagnosis of poorly differentiated cutaneous tumors and in the setting of metastasis.…”

Section: Modern Pathology (2015) 28 1033-1042mentioning

confidence: 99%

“…5 It is less widely appreciated that melanomas too may show aberrant expression of various immunohistochemical markers, with a relatively small number of reports, of melanomas showing expression of intermediate filaments other than vimentin (e.g., keratins, desmin, neurofilament protein, and glial fibrillary acidic protein) [6][7][8] and/or neuroendocrine markers. [9][10][11] Over the past several years, we have seen in consultation a significant number of melanomas in which aberrant expression of intermediate filaments and/or neuroendocrine markers obscured the correct diagnosis, and prompted consideration of various non-melanocytic neoplasms, including carcinoma, rhabdomyosarcoma, neural neoplasms, and various neuroendocrine tumors. As no study to date appears to have comprehensively examined this issue, we evaluated a large number of well-characterized melanomas, using contemporary immunohistochemical techniques, to better determine the actual frequency of aberrant expression of these markers.…”

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confidence: 99%

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Aberrant intermediate filament and synaptophysin expression is a frequent event in malignant melanoma: an immunohistochemical study of 73 cases

2015

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Malignant melanomas are known to express vimentin, among other intermediate filaments. Though anomalous keratin expression by malignant melanoma has been reported, its frequency is not well-established and this phenomenon is not well-known. We have seen in consultation a number of malignant melanomas with anomalous expression of keratin, other intermediate filaments, or synaptophysin, and therefore studied a large group of primary and metastatic melanomas to determine the frequency of these events. About 73 cases of malignant melanoma (22 primaries and 51 metastases) from 71 patients (51 male, 20 female; mean 59 years, range 17-87 years) were retrieved from our archives. Prior diagnoses were confirmed by re-review of hematoxylin and eosin sections and relevant (e.g., S100 protein, HMB45, Melan-A, and tyrosinase) immunohistochemical studies. Available sections were immunostained for keratin (OSCAR and AE1/AE3 antibodies), desmin, neurofilament protein, glial fibrillary acidic protein, synaptophysin, and chromogranin A. Not all cases could be tested for all markers. Cases were predominantly epithelioid (48/73, 66%) or spindle cell/desmoplastic (25/73, 34%). S100 protein, Melan-A, HMB45, and tyrosinase were positive in 60/65 (92%), 34/64 (53%), 30/60 (50%), 25/48 (52%) of cases, respectively. All five S100-protein-negative cases expressed at least one of the other melanocytic markers: Melan-A (two of four, 50%), HMB45 (two of three, 67%), and tyrosinase (one of two, 50%). All cases expressed at least one melanocytic marker. Cases were positive for keratin (OSCAR, 17/61, 28%; AE1/AE3, 16/40, 40%), desmin (11/47, 24%), neurofilament protein (5/31, 16%), glial fibrillary acidic protein (3/32, 9%), and synaptophysin (10/34, 29%), typically only in a minority of cells. Chromogranin was negative (0/32, 0%).

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Section: Modern Pathology (2015) 28 1033-1042mentioning

confidence: 79%

Section: Modern Pathology (2015) 28 1033-1042mentioning

confidence: 99%

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confidence: 99%

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Aberrant intermediate filament and synaptophysin expression is a frequent event in malignant melanoma: an immunohistochemical study of 73 cases

2015

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“…When pigmentation is absent, immunohistochemistry becomes helpful, with S100 protein and SOX10 usually strongly and diffusely reactive, whereas other melanocytic markers (HMB45, tyrosinase, melan A, MITF) are expressed to a variable degree, often based on tumor morphology; 6,7,11,12 in undifferentiated tumors, scant cytoplasm may result in focal or negative reactions, requiring careful high-power examination. Crossreactivity with neuroendocrine markers is rare.…”

Section: Melanomamentioning

confidence: 99%

“…Crossreactivity with neuroendocrine markers is rare. 12 In general, RAS and then KIT mutations (mutually exclusive) are detected at a distinctly higher rate than cutaneous melanomas, with BRAF mutations rarely detected. [13][14][15] Outcome and management.…”

Section: Melanomamentioning

confidence: 99%

Small round blue cell tumors of the sinonasal tract: a differential diagnosis approach

Thompson

2017

Modern Pathology

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One of the most challenging diagnostic categories within tumors of the sinonasal tract is the small round blue cell tumors. Biopsies are usually small and limited, resulting in considerable diagnostic difficulty for practicing surgical pathologists. These tumors share several overlapping histologic and immunophenotypic findings while also showing considerable variation within and between cases. Specific tumor site of origin, imaging findings, and clinical findings must be combined with the histology and pertinent ancillary studies if the correct diagnosis is to be reached. Discrimination between neoplasms is critical as there are significant differences in therapy and overall outcome. It is important to have a well developed differential diagnosis for this category of tumors, where each of the diagnoses is considered, evaluated, and either confirmed or excluded from further consideration. In an undifferentiated tumor, showing a small round blue cell morphology, using the mnemonic 'MR SLEEP' helps to highlight tumors to consider: melanoma, mesenchymal chondrosarcoma, rhabdomyosarcoma, sinonasal undifferentiated carcinoma, squamous cell carcinoma (including NUT carcinoma), small cell osteosarcoma, lymphoma, esthesioneuroblastoma (olfactory neuroblastoma), Ewing sarcoma/primitive neuroectodermal tumor, pituitary adenoma, and plasmacytoma. A panel of pertinent immunohistochemistry studies, histochemistries and/or molecular tests should aid in reaching a diagnosis, especially when taking the pattern and intensity of reactions into consideration.

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Sinonasal melanoma: survival and prognostic implications based on site of involvement

Khan

Kanumuri

Raikundalia

et al. 2013

Int Forum Allergy Rhinol

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Immunophenotypic Heterogeneity of Primary Sinonasal Melanoma With Aberrant Expression of Neuroendocrine Markers and Calponin

Cited by 31 publications

References 24 publications

Aberrant intermediate filament and synaptophysin expression is a frequent event in malignant melanoma: an immunohistochemical study of 73 cases

Aberrant intermediate filament and synaptophysin expression is a frequent event in malignant melanoma: an immunohistochemical study of 73 cases

Small round blue cell tumors of the sinonasal tract: a differential diagnosis approach

Sinonasal melanoma: survival and prognostic implications based on site of involvement

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