Pediatric Sertoli-Leydig Cell Tumors of the Ovary: An Integrated Study of Clinicopathological Features, Pan-cancer-Targeted Next-generation Sequencing and Chromosomal Microarray Analysis From a Single Institution

Bo Yang; William Chour; Cristo Guardado Salazar; Paul Zamiara; Ryan J Schmidt; Gordana Raca; Nick Shillingford; Shengmei Zhou; Mikako Warren; David M Parham; Bruce Pawel; Larry L Wang

doi:10.1097/PAS.0000000000002149

Pediatric Sertoli-Leydig Cell Tumors of the Ovary: An Integrated Study of Clinicopathological Features, Pan-cancer-Targeted Next-generation Sequencing and Chromosomal Microarray Analysis From a Single Institution

Am J Surg Pathol. 2024 Feb 1;48(2):194-203. doi: 10.1097/PAS.0000000000002149. Epub 2023 Nov 10.

Authors

Bo Yang^{1

2

3}, William Chour¹, Cristo Guardado Salazar^{1

2}, Paul Zamiara^{1

2}, Ryan J Schmidt^{1

2}, Gordana Raca^{1

2}, Nick Shillingford^{1

2}, Shengmei Zhou^{1

2}, Mikako Warren^{1

2}, David M Parham¹, Bruce Pawel^{1

2}, Larry L Wang^{1

2}

Affiliations

¹ Department of Pathology and Laboratory Medicine, Children's Hospital Los Angeles, Los Angeles, CA.
² Keck School of Medicine, University of Southern California, Los Angeles, CA.
³ Department of Pathology, Tianjin Medical University Cancer Institute and Hospital, National Clinical Research Center for Cancer, Key Laboratory of Cancer Prevention and Therapy, Tianjin, Tianjin's Clinical Research Center for Cancer, Tianjin, China.

PMID: 37946548
DOI: 10.1097/PAS.0000000000002149

Abstract

Sertoli-Leydig cell tumors (SLCTs) are currently classified into 3 molecular subtypes: DICER1 -mutant (younger patient age), FOXL2 -mutant, and DICER1/FOXL2 -wildtype. However, it is not clear whether all pediatric SLCTs are DICER1 -mutant molecular subtypes and whether other molecular genetic aberrations besides DICER1 are involved in the pathogenesis and prognosis of these tumors. We studied comprehensive data for 8 cases of pediatric SLCTs, including clinicopathological features, pan-cancer-targeted next-generation sequencing/OncoKids panel, and chromosomal microarray analysis, to further analyze the correlation among clinicopathological features, molecular genetic aberrations, and prognosis. The ages of the patients ranged from 4 to 16 years (median, 14 y). Seven cases were moderately differentiated, and one was poorly differentiated with heterologous mesenchymal elements. Two cases had heterologous epithelium or retiform elements. Follow-up was available for all 8 patients (median, 49.5 mo). Seven patients were alive without evidence of recurrence or metastasis, and only case 5 developed metastases (synchronous bilateral pulmonary tumors with rhabdomyosarcomatous differentiation). All 8 tumors were found to harbor somatic hotspot DICER1 mutations, and 5 patients carried germline DICER1 mutations (2 of them had the phenotype of DICER1 syndrome). Together with recent studies, the DICER1 mutation frequency is 100% in pediatric SLCTs (n=27, age≤16 y). Copy number alterations were detected in 3 tumors; the only recurrent copy number alterations was the gain of whole chromosome 6 in case 5 and case 8. This is the first report describing clinicopathological features and molecular alterations in pediatric SLCTs. Our results demonstrate that all pediatric SLCTs belong to the DICER1 -mutant molecular subtype, highlighting that somatic hotspot DICER1 mutation detection has high sensitivity (100%) for the auxiliary diagnosis of pediatric SLCTs (age ≤16 y). Some pediatric SLCTs harbor molecular genetic aberrations other than DICER1 mutation, and their significance needs further study.

MeSH terms

Adolescent
Child
DEAD-box RNA Helicases / genetics
Female
High-Throughput Nucleotide Sequencing
Humans
Male
Mutation
Ovarian Neoplasms* / pathology
Ribonuclease III / genetics
Sertoli-Leydig Cell Tumor* / genetics
Sertoli-Leydig Cell Tumor* / pathology

Substances

Ribonuclease III
DICER1 protein, human
DEAD-box RNA Helicases