TCam-2 Cells Deficient for SOX2 and FOXA2 Are Blocked in Differentiation and Maintain a Seminoma-Like Cell Fate In Vivo

Daniel Nettersheim; Saskia Vadder; Sina Jostes; Alena Heimsoeth; Hubert Schorle

doi:10.3390/cancers11050728

Cancers (May 2019)

TCam-2 Cells Deficient for SOX2 and FOXA2 Are Blocked in Differentiation and Maintain a Seminoma-Like Cell Fate In Vivo

Daniel Nettersheim,
Saskia Vadder,
Sina Jostes,
Alena Heimsoeth,
Hubert Schorle

Affiliations

Daniel Nettersheim: Department of Urology, Urological Research Lab, Translational Urooncology, University Hospital Düsseldorf, 40225 Düsseldorf, Germany
Saskia Vadder: Department of Developmental Pathology, Institute of Pathology, Bonn University Medical School, 53127 Bonn, Germany
Sina Jostes: Department of Developmental Pathology, Institute of Pathology, Bonn University Medical School, 53127 Bonn, Germany
Alena Heimsoeth: Department of Developmental Pathology, Institute of Pathology, Bonn University Medical School, 53127 Bonn, Germany
Hubert Schorle: Department of Developmental Pathology, Institute of Pathology, Bonn University Medical School, 53127 Bonn, Germany

DOI: https://doi.org/10.3390/cancers11050728
Journal volume & issue: Vol. 11, no. 5
p. 728

Abstract

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Testicular germ cell tumors (GCTs) are very common in young men and can be stratified into seminomas and non-seminomas. While seminomas share a similar gene expression and epigenetic profile with primordial germ cells, the stem cell population of the non-seminomas, the embryonal carcinoma (EC), resembles malignant embryonic stem cells. Thus, ECs are able to differentiate into cells of all three germ layers (teratomas) and even extra-embryonic-tissue-like cells (yolk-sac tumor, choriocarcinoma). In the last years, we demonstrated that the cellular microenvironment considerably influences the plasticity of seminomas (TCam-2 cells). Upon a microenvironment-triggered inhibition of the BMP signaling pathway in vivo (murine flank or brain), seminomatous TCam-2 cells reprogram to an EC-like cell fate. We identified SOX2 as a key factor activated upon BMP inhibition mediating the reprogramming process by regulating pluripotency, reprogramming and epigenetic factors. Indeed, CRISPR/Cas9 SOX2-deleted TCam-2 cells were able to maintain a seminoma-cell fate in vivo for about six weeks, but after six weeks in vivo still small sub-populations initiated differentiation. Closer analyses of these differentiated clusters suggested that the pioneer factor FOXA2 might be the driving force behind this induction of differentiation, since many FOXA2 interacting genes and differentiation factors like AFP, EOMES, CDX1, ALB, HAND1, DKK, DLK1, MSX1 and PITX2 were upregulated. In this study, we generated TCam-2 cells double-deficient for SOX2 and FOXA2 using the CRISPR/Cas9 technique and xenografted those cells into the flank of nude mice. Upon loss of SOX2 and FOXA2, TCam-2 maintained a seminoma cell fate for at least twelve weeks, demonstrating that both factors are key players in the reprogramming to an EC-like cell fate. Therefore, our study adds an important piece to the puzzle of GCT development and plasticity, providing interesting insights in what can be expected in a patient, when GCT cells are confronted with different microenvironments.

Published in Cancers

ISSN: 2072-6694 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://www.mdpi.com/journal/cancers/

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