<i>POU5F1</i>, encoding a key regulator of stem cell pluripotency, is fused to <i>EWSR1</i> in hidradenoma of the skin and mucoepidermoid carcinoma of the salivary glands

Möller, Emely; Stenman, Göran; Mandahl, Nils; Hamberg, Hans; Mölne, Lena; Oord, JJ van den; Brosjö, Otte; Mertens, Fredrik; Panagopoulos, Ioannis

doi:10.1002/path.2327

Cited by 107 publications

(97 citation statements)

References 40 publications

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“…7,12,[19][20][21] The remaining 10 fusion-negative, high-grade tumors were also negative for the EWSR1-POU5F1 fusion previously identified in high-grade mucoepidermoid carcinomas. 22 These findings support the notion that low-grade mucoepidermoid carcinomas are fusion-positive and genetically stable tumors with few genomic imbalances. The fact that CRTC1-MAML2 is a potent oncogene with effects on critical signaling pathways (Enlund et al, unpublished data) 17,29 might at least partly explain why these tumors contain relatively few copy number alterations.…”

Section: Discussionsupporting

confidence: 76%

“…16,19 Fluorescence In Situ Hybridization (FISH) Analysis FISH analyses for detection of the CRTC1-MAML2 and EWSR1-POU5F1 gene fusions were performed on 3 mm formalin-fixed paraffin-embedded sections using dual-color break-apart rearrangement probes for the MAML2 (ZytoVision GmbH, Bremerhaven, Germany) and EWSR1 genes (Vysis, Downer's Grove, IL) as previously described. 22,28 To validate recurrent copy number alterations detected by arrayCGH we performed FISH analyses using locus-specific probes for MALT1 located at 18q21.32 (MALT1 Break-apart probe; Cytocell, Cambridge, UK) and MECOM located at 3q26.2 (MECOM/ RUNX1 t(3;21) Fusion-probe; Kreatech Diagnostics, Amsterdam, The Netherlands). Locus-specific probes for CCND1 (IGH/ CCND1 Translocation Probe; Cytocell) and HER2 (Vysis) were used to confirm amplifications involving 11q and 17q sequences.…”

Section: Rt-pcr Analysismentioning

confidence: 99%

“…12,13,20,21 A second gene fusion involving the sarcoma-associated EWSR1 gene and the stem cell regulator POU5F1 was recently identified in mucoepidermoid carcinomas with a more immature morphology compared with MAML2 positive tumors. 22 Except for the CRTC1-MAML2 fusion, little is known about other genomic rearrangements of importance for the genesis and progression of mucoepidermoid carcinoma. 23,24 To identify such alterations, we performed a genome-wide, array-based comparative genomic hybridization (arrayCGH) study of a series of 28 mucoepidermoid carcinomas.…”

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confidence: 99%

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Genomic profiles and CRTC1–MAML2 fusion distinguish different subtypes of mucoepidermoid carcinoma

et al. 2013

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Mucoepidermoid carcinoma is the most common salivary gland malignancy, and includes a spectrum of lesions ranging from non-aggressive low-grade tumors to aggressive high-grade tumors. To further characterize this heterogeneous group of tumors we have performed a comprehensive analysis of copy number alterations and CRTC1-MAML2 fusion status in a series of 28 mucoepidermoid carcinomas. The CRTC1-MAML2 fusion was detected by RT-PCR or fluorescence in situ hybridization in 18 of 28 mucoepidermoid carcinomas (64%). All 15 low-grade tumors were fusion-positive whereas only 3 of 13 high-grade tumors were fusion-positive. Highresolution array-based comparative genomic hybridization revealed that fusion-positive tumors had significantly fewer copy number alterations/tumor compared with fusion-negative tumors (1.5 vs 9.5; P ¼ 0.002). Twelve of 18 fusion-positive tumors had normal genomic profiles whereas only 1 out of 10 fusionnegative tumors lacked copy number alterations. The profiles of fusion-positive and fusion-negative tumors were very similar to those of low-and high-grade tumors. Thus, low-grade mucoepidermoid carcinomas had significantly fewer copy number alterations/tumor compared with high-grade mucoepidermoid carcinomas (0.7 vs 8.6; Po0.0001). The most frequent copy number alterations detected were losses of 18q12.2-qter (including the tumor suppressor genes DCC, SMAD4, and GALR1), 9p21.3 (including the tumor suppressor genes CDKN2A/B), 6q22.1-q23.1, and 8pter-p12.1, and gains of 8q24.3 (including the oncogene MAFA), 11q12.3-q13.2, 3q26.1-q28, 19p13.2-p13.11, and 8q11.1-q12.2 (including the oncogenes LYN, MOS, and PLAG1). On the basis of these results we propose that mucoepidermoid carcinoma may be subdivided in (i) low-grade, fusion-positive mucoepidermoid carcinomas with no or few genomic imbalances and favorable prognosis, (ii) high-grade, fusion-positive mucoepidermoid carcinomas with multiple genomic imbalances and unfavorable prognosis, and (iii) a heterogeneous group of high-grade, fusion-negative adenocarcinomas with multiple genomic imbalances and unfavorable outcome. Taken together, our studies indicate that molecular genetic analysis can be a useful adjunct to histologic scoring of mucoepidermoid carcinoma and may lead to development of new clinical guidelines for management of these patients.

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Section: Discussionsupporting

confidence: 76%

Section: Rt-pcr Analysismentioning

confidence: 99%

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confidence: 99%

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Genomic profiles and CRTC1–MAML2 fusion distinguish different subtypes of mucoepidermoid carcinoma

et al. 2013

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“…10 Hidradenoma, a biphasic epithelial skin appendage tumor with occurrence of ductal/glandular and cystic structures, earlier thought to be a clear cell myoepithelioma, 13,14 possess in a subset of cases the specific fusion CRTC1-MAML2, which has been also described in mucoepidermoid carcinomas and Warthin's tumors of salivary glands. 15,16 One study demonstrated the occurrence of EWSR1-POUF5F1 fusion in hidradenomas, 17 whereas Antonescu et al 10 did not find an EWSR1 rearrangement in five eccrine hidradenomas. 10 Therefore, one could speculate whether these described lesions by Mö ller et al 17 are more related to myoepithelial tumors.…”

Section: Ewsr1 In Cutaneous Myoepitheliomamentioning

confidence: 99%

“…10 Therefore, one could speculate whether these described lesions by Mö ller et al 17 are more related to myoepithelial tumors. 17 The much more common occurring and investigated myoepithelial tumors of the salivary glands are known for a different genetic background, which contains rearrangements of PLAG1 and HMGA2. 18 A differential diagnosis of cutaneous myoepithelial tumors in our opinion represents epithelioid sarcoma, especially the very rarely occurring myxoid variant.…”

Section: Ewsr1 In Cutaneous Myoepitheliomamentioning

confidence: 99%

EWSR1 gene rearrangement occurs in a subset of cutaneous myoepithelial tumors: a study of 18 cases

et al. 2011

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Cutaneous myoepithelial tumors form a clinicopathological spectrum ranging from mixed tumor to myoepithelioma and myoepithelial carcinoma. Recently, EWSR1 rearrangement has been described in a subset of soft tissue myoepithelial tumors, whereas the cutaneous counterparts showed this aberration in a minority of cases. This raises the question whether cutaneous myoepithelial tumors have comparable genetic alterations. We examined 18 cases of cutaneous myoepithelial tumors arising in 7 female and 11 male patients (age range, 34-86 years; mean, 58 years). Eight mixed tumors occurred at the head, and one at the scrotum. Six myoepitheliomas arose at the extremities, and one case each at the back and head. One myoepithelial carcinoma occurred at the cheek. The tumor size ranged from 0.3 to 1.7 cm (mean, 1.0 cm). All mixed tumors and three myoepitheliomas were limited to the dermis. Four myoepitheliomas and the myoepithelial carcinoma involved the subcutis. Mixed tumors and myoepitheliomas were composed of myoepithelial cells with a variable cytomorphology, architecture and stromal background. Ductal structures were seen by definition in mixed tumors. The myoepithelial carcinoma represented an infiltrative dermal neoplasm consisting of atypical spindle cells. Immunohistochemically, all cases tested were positive for EMA and calponin, whereas S100, CK, ASMA and GFAP were expressed in 90%, 80%, 78% and 50% of the cases tested, respectively. By fluorescent in situ hybridization analysis, 7 out of 16 cases (44%) exhibited EWSR1 rearrangement. Four of them were mixed tumors, two were myoepitheliomas and one was a myoepithelial carcinoma, confirming that these lesions represent a spectrum of dermal myoepithelial tumors. Follow-up information, available for five patients (including the patient with a myoepithelial carcinoma), revealed no evidence of disease in all cases (range, 6-72 months). Our study provides a genetic relationship of myoepithelial tumors of the skin with their counterparts in soft tissue, bone and visceral localization by sharing EWSR1 rearrangement.

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Molecular Genetics of Salivary Gland Cancer

Clair

2017

Encyclopedia of Life Sciences

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Malignant salivary gland tumours are rare cancers of the head and neck with varied histopathology and clinical behaviour. The most common forms of salivary gland malignancies include mucoepidermoid carcinoma (MEC), adenoid cystic carcinoma (AdCC), acinic cell carcinoma (ACC) and a number of rare disease entities. Novel sequencing techniques and chromosomal analysis have led to an increased understanding of the genetics of these tumours. A characteristic molecular profile of many of these tumours is emerging and involves balanced chromosomal translocations that result in the expression of unique fusion proteins, as well as mutations in a limited subset of genes. Further elucidation of the molecular mechanisms of this heterogeneous group of tumours will be essential to design effective targeted therapies for salivary gland malignancies. Key Concepts Malignant salivary gland tumors are rare tumors with varied clinical behavior and histopathology. Advances in genetic sequencings has enabled improved insight into the genetics of salivary gland tumors. The majority of salivary gland malignancies result from well-defined chromosomal translocations. The chromosomal translocations found in salivary gland malignancies result in the expression of fusion genes that are important in the etiology of these tumors. Salivary gland tumors result from the deregulation of a limited number of pathways and genes – which may be enable the development of targeted therapeutics for these rare tumors.

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POU5F1, encoding a key regulator of stem cell pluripotency, is fused to EWSR1 in hidradenoma of the skin and mucoepidermoid carcinoma of the salivary glands

Cited by 107 publications

References 40 publications

Genomic profiles and CRTC1–MAML2 fusion distinguish different subtypes of mucoepidermoid carcinoma

Genomic profiles and CRTC1–MAML2 fusion distinguish different subtypes of mucoepidermoid carcinoma

EWSR1 gene rearrangement occurs in a subset of cutaneous myoepithelial tumors: a study of 18 cases

Molecular Genetics of Salivary Gland Cancer

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