DICER1 hot‐spot mutations in ovarian gynandroblastoma

Wang, Yemin; Karnezis, Anthony N.; Magrill, Jamie; Tessier‐Cloutier, Basile; Lum, Amy; Senz, Janine; Gilks, C Blake; McCluggage, W. Glenn; Huntsman, David G.; Kommoss, Friedrich

doi:10.1111/his.13630

Cited by 31 publications

(40 citation statements)

References 25 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Among ovarian sex cord–stromal tumours, no FOXL2 C134W mutations have been identified in cellular fibromas, sclerosing stromal tumours, MCSTs, steroid cell tumours, Sertoli cell tumours, sex cord tumours with annular tubules (SCTATs), or gynandroblastomas . The C134W FOXL2 mutation has been identified in 1.6% (1/62) of conventional fibromas, 20% (7/35) of thecomas, 3% (2/59) of juvenile granulosa cell tumours (JGCTs), 13% (12/90) of SLCTs, 50% (6/12) of granulosa theca cell tumours, and 8% (2/24) of gynandroblastomas . These observations raise a nosological dilemma regarding the gold standard for tumour classification: morphology, immunophenotype, molecular phenotype, or some combination thereof.…”

Section: Agct and Foxl2mentioning

confidence: 99%

“…DICER1 mutations have been reported in 50% (5/10) of Sertoli cell tumours, 36% (9/25) of gynandroblastomas, 11% (3/26) of JGCTs, 10% (2/20) of yolk sac tumours, 5% (1/20) of teratomas, 14% (2/14) of mixed germ cell tumours, and 20% (1/5) of gonadoblastomas with dysgerminoma …”

Section: Slct and Dicer1mentioning

confidence: 99%

“…18 The C134W FOXL2 mutation has been identified in 1.6% (1/62) of conventional fibromas, 1,6,8,9,11,18 20% (7/35) of thecomas, 1,6,11 3% (2/59) of juvenile granulosa cell tumours (JGCTs), 1,6,[9][10][11][12]16,17 13% (12/90) of SLCTs, 1,6,8,9,11,18,23 50% (6/12) of granulosa theca cell tumours, 24 and 8% (2/24) of gynandroblastomas. 18,25,26 These observations raise a nosological dilemma regarding the gold standard for tumour classification: morphology, immunophenotype, molecular phenotype, or some combination thereof. In the absence of evidence on outcome or response to treatment, the approach to the answer is subjective, and may lead to observer variation in tumour classification and management.…”

Section: S P E C I F I C I T Y O F F O X L 2 M U T a T I O N F O R A mentioning

confidence: 99%

“…Among ovarian tumours, no DICER1 mutations have been reported in AGCTs, 9,37 fibromas, 9 SCTATs, 9,26,39 sclerosing stromal tumours, 9 steroid cell tumours, 9 dysgerminomas, 37,39 or small-cell carcinomas, hypercalcaemic type. 39 DICER1 mutations have been reported in 50% (5/ 10) of Sertoli cell tumours, 9,26 36% (9/25) of gynandroblastomas, 25,26,50 11% (3/26) of JGCTs, 9,37,39 10% (2/20) of yolk sac tumours, 37,39 5% (1/20) of teratomas, 37,39 14% (2/14) of mixed germ cell tumours, 39 and 20% (1/5) of gonadoblastomas with dysgerminoma. 39…”

Section: S P E C I F I C I T Y O F D I C E R 1 M U T a T I O N F O R mentioning

confidence: 99%

See 3 more Smart Citations

Practical roles for molecular diagnostic testing in ovarian adult granulosa cell tumour, Sertoli–Leydig cell tumour, microcystic stromal tumour and their mimics

2019

Self Cite

View full text Add to dashboard Cite

Within the last decade, molecular advances have provided insights into the genetics of several ovarian sex cord–stromal tumours that have otherwise been enigmatic. Chief among these advances are the identification of FOXL2, DICER1 and CTNNB1 mutations in adult granulosa cell tumours, Sertoli–Leydig cell tumours (SLCTs), and microcystic stromal tumours (MCSTs), respectively. As access to molecular diagnostic laboratories continues to become more widely available, the potential roles for tumour mutation testing in the pathological diagnosis of these tumours merit discussion. Furthermore, links to inherited cancer susceptibility syndromes may exist for some women with SLCT (DICER1 syndrome) and MCST [familial adenomatous polyposis (FAP)]. This review will address practical issues in deciding when and how to apply mutation testing in the diagnosis of these three sex cord–stromal tumours. The pathologist's role in recommending referral for formal risk assessment for DICER1 syndrome and FAP will also be discussed.

show abstract

Section: Agct and Foxl2mentioning

confidence: 99%

Section: Slct and Dicer1mentioning

confidence: 99%

Section: S P E C I F I C I T Y O F F O X L 2 M U T a T I O N F O R A mentioning

confidence: 99%

Section: S P E C I F I C I T Y O F D I C E R 1 M U T a T I O N F O R mentioning

confidence: 99%

See 2 more Smart Citations

Practical roles for molecular diagnostic testing in ovarian adult granulosa cell tumour, Sertoli–Leydig cell tumour, microcystic stromal tumour and their mimics

2019

Self Cite

View full text Add to dashboard Cite

show abstract

“…ATK1, FOXL2, and DICER1 gene mutations have been associated with SCSTs ( Rosario et al, 2014 , Auguste et al, 2015 ). DICER1 mutations have been associated with Sertoli-Leydig cell tumors (SLCTs) and gynandroblastomas ( Heravi-Moussavi et al, 2012 Jan 19 , Wang et al, 2018 Aug ). In addition to ovarian SCSTs, DICER1 pathogenic variants are also associated with an increased risk of benign and malignant lung, kidney, thyroid, and CNS tumors ( Schultz et al, 2018 ).…”

Section: Introductionmentioning

confidence: 99%

Recurrent gynandroblastoma of the ovary with germline DICER1 mutation: A case report and review of the literature

Mercier

Zorn

Quick

et al. 2021

Gynecologic Oncology Reports

View full text Add to dashboard Cite

Highlights Sertoli-Leydig cell tumor and gynandroblastoma are rare ovarian sex cord-stromal tumors that warrant germline DICER1 testing. DICER1 mutations are associated with an increased risk of various benign and malignant tumors especially during childhood. Childhood genetic testing is controversial but provides earlier screening and diagnosis in DICER1 mutation patients.

show abstract