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In vivo loss of tumorigenicity in a patient-derived orthotopic xenograft mouse model of ependymoma.
Whitehouse, Jacqueline P; Hii, Hilary; Mayoh, Chelsea; Wong, Marie; Ajuyah, Pamela; Barahona, Paulette; Cui, Louise; Dholaria, Hetal; White, Christine L; Buntine, Molly K; Byrne, Jacob; Rodrigues da Silva, Keteryne; Howlett, Meegan; Girard, Emily J; Tsoli, Maria; Ziegler, David S; Dyke, Jason M; Lee, Sharon; Ekert, Paul G; Cowley, Mark J; Gottardo, Nicholas G; Endersby, Raelene.
Afiliação
  • Whitehouse JP; Brain Tumour Research Program, Telethon Kids Institute, Nedlands, WA, Australia.
  • Hii H; Centre for Child Health Research, University of Western Australia, Nedlands, WA, Australia.
  • Mayoh C; Brain Tumour Research Program, Telethon Kids Institute, Nedlands, WA, Australia.
  • Wong M; Children's Cancer Institute, Lowy Cancer Research Centre, UNSW Sydney, Kensington, NSW, Australia.
  • Ajuyah P; School of Clinical Medicine, University of New South Wales (UNSW) Sydney, Kensington, NSW, Australia.
  • Barahona P; Children's Cancer Institute, Lowy Cancer Research Centre, UNSW Sydney, Kensington, NSW, Australia.
  • Cui L; School of Clinical Medicine, University of New South Wales (UNSW) Sydney, Kensington, NSW, Australia.
  • Dholaria H; Children's Cancer Institute, Lowy Cancer Research Centre, UNSW Sydney, Kensington, NSW, Australia.
  • White CL; Children's Cancer Institute, Lowy Cancer Research Centre, UNSW Sydney, Kensington, NSW, Australia.
  • Buntine MK; Children's Cancer Institute, Lowy Cancer Research Centre, UNSW Sydney, Kensington, NSW, Australia.
  • Byrne J; Brain Tumour Research Program, Telethon Kids Institute, Nedlands, WA, Australia.
  • Rodrigues da Silva K; Department of Paediatric and Adolescent Oncology/Haematology, Perth Children's Hospital, Nedlands, WA, Australia.
  • Howlett M; Division of Paediatrics, University of Western Australia Medical School, Nedlands, WA, Australia.
  • Girard EJ; Genetics and Molecular Pathology Laboratory, Hudson Institute of Medical Research, Clayton, VIC, Australia.
  • Tsoli M; Department of Molecular and Translational Science, Monash University, Clayton, VIC, Australia.
  • Ziegler DS; Division of Genetics and Genomics, Victorian Clinical Genetics Services, Parkville, VIC, Australia.
  • Dyke JM; Genetics and Molecular Pathology Laboratory, Hudson Institute of Medical Research, Clayton, VIC, Australia.
  • Lee S; Department of Molecular and Translational Science, Monash University, Clayton, VIC, Australia.
  • Ekert PG; Brain Tumour Research Program, Telethon Kids Institute, Nedlands, WA, Australia.
  • Cowley MJ; Brain Tumour Research Program, Telethon Kids Institute, Nedlands, WA, Australia.
  • Gottardo NG; Medical School of Rbeirão Preto (FMRP-USP), University of São Paulo, São Paulo, Brazil.
  • Endersby R; Brain Tumour Research Program, Telethon Kids Institute, Nedlands, WA, Australia.
Front Oncol ; 13: 1123492, 2023.
Article em En | MEDLINE | ID: mdl-36937401
ABSTRACT

Introduction:

Ependymomas (EPN) are the third most common malignant brain cancer in children. Treatment strategies for pediatric EPN have remained unchanged over recent decades, with 10-year survival rates stagnating at just 67% for children aged 0-14 years. Moreover, a proportion of patients who survive treatment often suffer long-term neurological side effects as a result of therapy. It is evident that there is a need for safer, more effective treatments for pediatric EPN patients. There are ten distinct subgroups of EPN, each with their own molecular and prognostic features. To identify and facilitate the testing of new treatments for EPN, in vivo laboratory models representative of the diverse molecular subtypes are required. Here, we describe the establishment of a patient-derived orthotopic xenograft (PDOX) model of posterior fossa A (PFA) EPN, derived from a metastatic cranial lesion.

Methods:

Patient and PDOX tumors were analyzed using immunohistochemistry, DNA methylation profiling, whole genome sequencing (WGS) and RNA sequencing.

Results:

Both patient and PDOX tumors classified as PFA EPN by methylation profiling, and shared similar histological features consistent with this molecular subgroup. RNA sequencing revealed that gene expression patterns were maintained across the primary and metastatic tumors, as well as the PDOX. Copy number profiling revealed gains of chromosomes 7, 8 and 19, and loss of chromosomes 2q and 6q in the PDOX and matched patient tumor. No clinically significant single nucleotide variants were identified, consistent with the low mutation rates observed in PFA EPN. Overexpression of EZHIP RNA and protein, a common feature of PFA EPN, was also observed. Despite the aggressive nature of the tumor in the patient, this PDOX was unable to be maintained past two passages in vivo.

Discussion:

Others who have successfully developed PDOX models report some of the lowest success rates for EPN compared to other pediatric brain cancer types attempted, with loss of tumorigenicity not uncommon, highlighting the challenges of propagating these tumors in the laboratory. Here, we discuss our collective experiences with PFA EPN PDOX model generation and propose potential approaches to improve future success in establishing preclinical EPN models.
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Texto completo: 1 Base de dados: MEDLINE Idioma: En Ano de publicação: 2023 Tipo de documento: Article País de afiliação: Austrália
Texto completo
Imprimir
XML
PubMed Links
Buscar no Google

Texto completo: 1 Base de dados: MEDLINE Idioma: En Ano de publicação: 2023 Tipo de documento: Article País de afiliação: Austrália