High-grade neuroepithelial tumor with BCOR exon 15 internal tandem duplication—a comprehensive clinical, radiographic, pathologic, and genomic analysis

Sean P. Ferris; Jose Velazquez Vega; Mariam Aboian; Julieann C. Lee; Jessica Van Ziffle; Courtney Onodera; James P. Grenert; Tara Saunders; Yunn Yi Chen; Anu Banerjee; Cassie N. Kline; Nalin Gupta; Corey Raffel; David Samuel; Irune Ruiz-Diaz; Shino Magaki; Dianne Wilson; Janna Neltner; Zahra Al-Hajri; Joanna J. Phillips; Melike Pekmezci; Andrew W. Bollen; Tarik Tihan; Matthew Schniederjan; Soonmee Cha; Arie Perry; David A. Solomon

doi:10.1111/bpa.12747

High-grade neuroepithelial tumor with BCOR exon 15 internal tandem duplication—a comprehensive clinical, radiographic, pathologic, and genomic analysis

Sean P. Ferris, Jose Velazquez Vega, Mariam Aboian, Julieann C. Lee, Jessica Van Ziffle, Courtney Onodera, James P. Grenert, Tara Saunders, Yunn Yi Chen, Anu Banerjee, Cassie N. Kline, Nalin Gupta, Corey Raffel, David Samuel, Irune Ruiz-Diaz, Shino Magaki, Dianne Wilson, Janna Neltner, Zahra Al-Hajri, Joanna J. PhillipsMelike Pekmezci, Andrew W. Bollen, Tarik Tihan, Matthew Schniederjan, Soonmee Cha, Arie Perry, David A. Solomon

Producción científica: Article › revisión exhaustiva

84 Citas (Scopus)

Resumen

High-grade neuroepithelial tumor with BCOR exon 15 internal tandem duplication (HGNET BCOR ex15 ITD) is a recently proposed tumor entity of the central nervous system (CNS) with a distinct methylation profile and characteristic genetic alteration. The complete spectrum of histologic features, accompanying genetic alterations, clinical outcomes, and optimal treatment for this new tumor entity are largely unknown. Here, we performed a comprehensive assessment of 10 new cases of HGNET BCOR ex15 ITD. The tumors mostly occurred in young children and were located in the cerebral or cerebellar hemispheres. On imaging all tumors were large, well-circumscribed, heterogeneous masses with variable enhancement and reduced diffusion. They were histologically characterized by predominantly solid growth, glioma-like fibrillarity, perivascular pseudorosettes, and palisading necrosis, but absence of microvascular proliferation. They demonstrated sparse to absent GFAP expression, no synaptophysin expression, variable OLIG2 and NeuN positivity, and diffuse strong BCOR nuclear positivity. While BCOR exon 15 internal tandem duplication was the solitary pathogenic alteration identified in six cases, four cases contained additional alterations including CDKN2A/B homozygous deletion, TERT amplification or promoter hotspot mutation, and damaging mutations in TP53, BCORL1, EP300, SMARCA2 and STAG2. While the limited clinical follow-up in prior reports had indicated a uniformly dismal prognosis for this tumor entity, this cohort includes multiple long-term survivors. Our study further supports inclusion of HGNET BCOR ex15 ITD as a distinct CNS tumor entity and expands the known clinicopathologic, radiographic, and genetic features.

Idioma original	English
Páginas (desde-hasta)	46-62
Número de páginas	17
Publicación	Brain Pathology
Volumen	30
N.º	1
DOI	https://doi.org/10.1111/bpa.12747
Estado	Published - ene 1 2020

Nota bibliográfica

Publisher Copyright:
© 2019 International Society of Neuropathology

Financiación

This study was supported by the NIH Director’s Early Independence Award (DP5 OD021403) to D.A.S. We thank the staff of the UCSF Clinical Cancer Genomics Laboratory for assistance with genetic profiling. We thank the staff of the UCSF Electron Microscopy Core Lab (Cosima Carnahan and Sherry Kamiya) for assistance with ultrastructural analysis. We thank Sarah Bowman and Torrick Taylor for assistance with digital slide scanning. This study was supported by the NIH Director?s Early Independence Award (DP5 OD021403) to D.A.S. We thank the staff of the UCSF Clinical Cancer Genomics Laboratory for assistance with genetic profiling. We thank the staff of the UCSF Electron Microscopy Core Lab (Cosima Carnahan and Sherry Kamiya) for assistance with ultrastructural analysis. We thank Sarah Bowman and Torrick Taylor for assistance with digital slide scanning.

Financiadores	Número del financiador
National Institutes of Health (NIH)	DP5 OD021403
National Childhood Cancer Registry – National Cancer Institute	T32CA128583
University of California San Francisco

ASJC Scopus subject areas

General Neuroscience
Pathology and Forensic Medicine
Clinical Neurology

Acceder al documento

10.1111/bpa.12747

Otros archivos y enlaces

Citar esto

Ferris, S. P., Velazquez Vega, J., Aboian, M., Lee, J. C., Van Ziffle, J., Onodera, C., Grenert, J. P., Saunders, T., Chen, Y. Y., Banerjee, A., Kline, C. N., Gupta, N., Raffel, C., Samuel, D., Ruiz-Diaz, I., Magaki, S., Wilson, D., Neltner, J., Al-Hajri, Z., ... Solomon, D. A. (2020). High-grade neuroepithelial tumor with BCOR exon 15 internal tandem duplication—a comprehensive clinical, radiographic, pathologic, and genomic analysis. Brain Pathology, 30(1), 46-62. https://doi.org/10.1111/bpa.12747

@article{65fa22c1f88142d99bd76eb7db47dd8c,

title = "High-grade neuroepithelial tumor with BCOR exon 15 internal tandem duplication—a comprehensive clinical, radiographic, pathologic, and genomic analysis",

abstract = "High-grade neuroepithelial tumor with BCOR exon 15 internal tandem duplication (HGNET BCOR ex15 ITD) is a recently proposed tumor entity of the central nervous system (CNS) with a distinct methylation profile and characteristic genetic alteration. The complete spectrum of histologic features, accompanying genetic alterations, clinical outcomes, and optimal treatment for this new tumor entity are largely unknown. Here, we performed a comprehensive assessment of 10 new cases of HGNET BCOR ex15 ITD. The tumors mostly occurred in young children and were located in the cerebral or cerebellar hemispheres. On imaging all tumors were large, well-circumscribed, heterogeneous masses with variable enhancement and reduced diffusion. They were histologically characterized by predominantly solid growth, glioma-like fibrillarity, perivascular pseudorosettes, and palisading necrosis, but absence of microvascular proliferation. They demonstrated sparse to absent GFAP expression, no synaptophysin expression, variable OLIG2 and NeuN positivity, and diffuse strong BCOR nuclear positivity. While BCOR exon 15 internal tandem duplication was the solitary pathogenic alteration identified in six cases, four cases contained additional alterations including CDKN2A/B homozygous deletion, TERT amplification or promoter hotspot mutation, and damaging mutations in TP53, BCORL1, EP300, SMARCA2 and STAG2. While the limited clinical follow-up in prior reports had indicated a uniformly dismal prognosis for this tumor entity, this cohort includes multiple long-term survivors. Our study further supports inclusion of HGNET BCOR ex15 ITD as a distinct CNS tumor entity and expands the known clinicopathologic, radiographic, and genetic features.",

keywords = "BCOR exon 15 internal tandem duplication, brain tumor, HGNET, high-grade neuroepithelial tumor, molecular neuro-oncology, molecular neuropathology",

author = "Ferris, \{Sean P.\} and \{Velazquez Vega\}, Jose and Mariam Aboian and Lee, \{Julieann C.\} and \{Van Ziffle\}, Jessica and Courtney Onodera and Grenert, \{James P.\} and Tara Saunders and Chen, \{Yunn Yi\} and Anu Banerjee and Kline, \{Cassie N.\} and Nalin Gupta and Corey Raffel and David Samuel and Irune Ruiz-Diaz and Shino Magaki and Dianne Wilson and Janna Neltner and Zahra Al-Hajri and Phillips, \{Joanna J.\} and Melike Pekmezci and Bollen, \{Andrew W.\} and Tarik Tihan and Matthew Schniederjan and Soonmee Cha and Arie Perry and Solomon, \{David A.\}",

note = "Publisher Copyright: {\textcopyright} 2019 International Society of Neuropathology",

year = "2020",

month = jan,

day = "1",

doi = "10.1111/bpa.12747",

language = "English",

volume = "30",

pages = "46--62",

number = "1",

}

Ferris, SP, Velazquez Vega, J, Aboian, M, Lee, JC, Van Ziffle, J, Onodera, C, Grenert, JP, Saunders, T, Chen, YY, Banerjee, A, Kline, CN, Gupta, N, Raffel, C, Samuel, D, Ruiz-Diaz, I, Magaki, S, Wilson, D, Neltner, J, Al-Hajri, Z, Phillips, JJ, Pekmezci, M, Bollen, AW, Tihan, T, Schniederjan, M, Cha, S, Perry, A & Solomon, DA 2020, 'High-grade neuroepithelial tumor with BCOR exon 15 internal tandem duplication—a comprehensive clinical, radiographic, pathologic, and genomic analysis', Brain Pathology, vol. 30, n.º 1, pp. 46-62. https://doi.org/10.1111/bpa.12747

TY - JOUR

T1 - High-grade neuroepithelial tumor with BCOR exon 15 internal tandem duplication—a comprehensive clinical, radiographic, pathologic, and genomic analysis

AU - Ferris, Sean P.

AU - Velazquez Vega, Jose

AU - Aboian, Mariam

AU - Lee, Julieann C.

AU - Van Ziffle, Jessica

AU - Onodera, Courtney

AU - Grenert, James P.

AU - Saunders, Tara

AU - Chen, Yunn Yi

AU - Banerjee, Anu

AU - Kline, Cassie N.

AU - Gupta, Nalin

AU - Raffel, Corey

AU - Samuel, David

AU - Ruiz-Diaz, Irune

AU - Magaki, Shino

AU - Wilson, Dianne

AU - Neltner, Janna

AU - Al-Hajri, Zahra

AU - Phillips, Joanna J.

AU - Pekmezci, Melike

AU - Bollen, Andrew W.

AU - Tihan, Tarik

AU - Schniederjan, Matthew

AU - Cha, Soonmee

AU - Perry, Arie

AU - Solomon, David A.

PY - 2020/1/1

Y1 - 2020/1/1

N2 - High-grade neuroepithelial tumor with BCOR exon 15 internal tandem duplication (HGNET BCOR ex15 ITD) is a recently proposed tumor entity of the central nervous system (CNS) with a distinct methylation profile and characteristic genetic alteration. The complete spectrum of histologic features, accompanying genetic alterations, clinical outcomes, and optimal treatment for this new tumor entity are largely unknown. Here, we performed a comprehensive assessment of 10 new cases of HGNET BCOR ex15 ITD. The tumors mostly occurred in young children and were located in the cerebral or cerebellar hemispheres. On imaging all tumors were large, well-circumscribed, heterogeneous masses with variable enhancement and reduced diffusion. They were histologically characterized by predominantly solid growth, glioma-like fibrillarity, perivascular pseudorosettes, and palisading necrosis, but absence of microvascular proliferation. They demonstrated sparse to absent GFAP expression, no synaptophysin expression, variable OLIG2 and NeuN positivity, and diffuse strong BCOR nuclear positivity. While BCOR exon 15 internal tandem duplication was the solitary pathogenic alteration identified in six cases, four cases contained additional alterations including CDKN2A/B homozygous deletion, TERT amplification or promoter hotspot mutation, and damaging mutations in TP53, BCORL1, EP300, SMARCA2 and STAG2. While the limited clinical follow-up in prior reports had indicated a uniformly dismal prognosis for this tumor entity, this cohort includes multiple long-term survivors. Our study further supports inclusion of HGNET BCOR ex15 ITD as a distinct CNS tumor entity and expands the known clinicopathologic, radiographic, and genetic features.

AB - High-grade neuroepithelial tumor with BCOR exon 15 internal tandem duplication (HGNET BCOR ex15 ITD) is a recently proposed tumor entity of the central nervous system (CNS) with a distinct methylation profile and characteristic genetic alteration. The complete spectrum of histologic features, accompanying genetic alterations, clinical outcomes, and optimal treatment for this new tumor entity are largely unknown. Here, we performed a comprehensive assessment of 10 new cases of HGNET BCOR ex15 ITD. The tumors mostly occurred in young children and were located in the cerebral or cerebellar hemispheres. On imaging all tumors were large, well-circumscribed, heterogeneous masses with variable enhancement and reduced diffusion. They were histologically characterized by predominantly solid growth, glioma-like fibrillarity, perivascular pseudorosettes, and palisading necrosis, but absence of microvascular proliferation. They demonstrated sparse to absent GFAP expression, no synaptophysin expression, variable OLIG2 and NeuN positivity, and diffuse strong BCOR nuclear positivity. While BCOR exon 15 internal tandem duplication was the solitary pathogenic alteration identified in six cases, four cases contained additional alterations including CDKN2A/B homozygous deletion, TERT amplification or promoter hotspot mutation, and damaging mutations in TP53, BCORL1, EP300, SMARCA2 and STAG2. While the limited clinical follow-up in prior reports had indicated a uniformly dismal prognosis for this tumor entity, this cohort includes multiple long-term survivors. Our study further supports inclusion of HGNET BCOR ex15 ITD as a distinct CNS tumor entity and expands the known clinicopathologic, radiographic, and genetic features.

KW - BCOR exon 15 internal tandem duplication

KW - brain tumor

KW - HGNET

KW - high-grade neuroepithelial tumor

KW - molecular neuro-oncology

KW - molecular neuropathology

UR - https://www.scopus.com/pages/publications/85067418760

UR - https://www.scopus.com/inward/citedby.url?scp=85067418760&partnerID=8YFLogxK

U2 - 10.1111/bpa.12747

DO - 10.1111/bpa.12747

M3 - Article

C2 - 31104347

AN - SCOPUS:85067418760

SN - 1015-6305

VL - 30

SP - 46

EP - 62

JO - Brain Pathology

JF - Brain Pathology

IS - 1

ER -

High-grade neuroepithelial tumor with BCOR exon 15 internal tandem duplication—a comprehensive clinical, radiographic, pathologic, and genomic analysis

Resumen

Nota bibliográfica

Financiación

ASJC Scopus subject areas

Acceder al documento

Otros archivos y enlaces

Huella

Citar esto