IDEAS home Printed from https://ideas.repec.org/a/nat/nature/v560y2018i7717d10.1038_s41586-018-0389-3.html
   My bibliography  Save this article

Human glioblastoma arises from subventricular zone cells with low-level driver mutations

Author

Listed:
  • Joo Ho Lee

    (Korea Advanced Institute of Science and Technology (KAIST))

  • Jeong Eun Lee

    (Korea Advanced Institute of Science and Technology (KAIST)
    College of Medicine, Chungnam National University)

  • Jee Ye Kahng

    (Korea Advanced Institute of Science and Technology (KAIST)
    KAIST)

  • Se Hoon Kim

    (Brain Korea 21 Project for Medical Science, Yonsei University College of Medicine)

  • Jun Sung Park

    (Korea Advanced Institute of Science and Technology (KAIST))

  • Seon Jin Yoon

    (Brain Tumor Center, Severance Hospital, Yonsei University College of Medicine)

  • Ji-Yong Um

    (KAIST)

  • Woo Kyeong Kim

    (Korea Advanced Institute of Science and Technology (KAIST))

  • June-Koo Lee

    (Korea Advanced Institute of Science and Technology (KAIST))

  • Junseong Park

    (Brain Tumor Center, Severance Hospital, Yonsei University College of Medicine)

  • Eui Hyun Kim

    (Brain Tumor Center, Severance Hospital, Yonsei University College of Medicine)

  • Ji-Hyun Lee

    (Brain Tumor Center, Severance Hospital, Yonsei University College of Medicine)

  • Joon-Hyuk Lee

    (KAIST)

  • Won-Suk Chung

    (KAIST)

  • Young Seok Ju

    (Korea Advanced Institute of Science and Technology (KAIST))

  • Sung-Hong Park

    (Korea Advanced Institute of Science and Technology (KAIST)
    KAIST)

  • Jong Hee Chang

    (Brain Tumor Center, Severance Hospital, Yonsei University College of Medicine)

  • Seok-Gu Kang

    (Brain Tumor Center, Severance Hospital, Yonsei University College of Medicine)

  • Jeong Ho Lee

    (Korea Advanced Institute of Science and Technology (KAIST)
    Center for Synaptic Brain Dysfunctions, Institute for Basic Science)

Abstract

Glioblastoma (GBM) is a devastating and incurable brain tumour, with a median overall survival of fifteen months1,2. Identifying the cell of origin that harbours mutations that drive GBM could provide a fundamental basis for understanding disease progression and developing new treatments. Given that the accumulation of somatic mutations has been implicated in gliomagenesis, studies have suggested that neural stem cells (NSCs), with their self-renewal and proliferative capacities, in the subventricular zone (SVZ) of the adult human brain may be the cells from which GBM originates3–5. However, there is a lack of direct genetic evidence from human patients with GBM4,6–10. Here we describe direct molecular genetic evidence from patient brain tissue and genome-edited mouse models that show astrocyte-like NSCs in the SVZ to be the cell of origin that contains the driver mutations of human GBM. First, we performed deep sequencing of triple-matched tissues, consisting of (i) normal SVZ tissue away from the tumour mass, (ii) tumour tissue, and (iii) normal cortical tissue (or blood), from 28 patients with isocitrate dehydrogenase (IDH) wild-type GBM or other types of brain tumour. We found that normal SVZ tissue away from the tumour in 56.3% of patients with wild-type IDH GBM contained low-level GBM driver mutations (down to approximately 1% of the mutational burden) that were observed at high levels in their matching tumours. Moreover, by single-cell sequencing and laser microdissection analysis of patient brain tissue and genome editing of a mouse model, we found that astrocyte-like NSCs that carry driver mutations migrate from the SVZ and lead to the development of high-grade malignant gliomas in distant brain regions. Together, our results show that NSCs in human SVZ tissue are the cells of origin that contain the driver mutations of GBM.

Suggested Citation

  • Joo Ho Lee & Jeong Eun Lee & Jee Ye Kahng & Se Hoon Kim & Jun Sung Park & Seon Jin Yoon & Ji-Yong Um & Woo Kyeong Kim & June-Koo Lee & Junseong Park & Eui Hyun Kim & Ji-Hyun Lee & Joon-Hyuk Lee & Won-, 2018. "Human glioblastoma arises from subventricular zone cells with low-level driver mutations," Nature, Nature, vol. 560(7717), pages 243-247, August.
    • Handle: RePEc:nat:nature:v:560:y:2018:i:7717:d:10.1038_s41586-018-0389-3
    DOI: 10.1038/s41586-018-0389-3
    as

    Download full text from publisher

    File URL: https://www.nature.com/articles/s41586-018-0389-3
    File Function: Abstract
    Download Restriction: Access to the full text of the articles in this series is restricted.
    File URL: https://libkey.io/10.1038/s41586-018-0389-3?utm_source=ideas
    LibKey link: if access is restricted and if your library uses this service, LibKey will redirect you to where you can use your library subscription to access this item
    ---><---

    As the access to this document is restricted, you may want to search for a different version of it.

    Citations

    Citations are extracted by the CitEc Project, subscribe to its RSS feed for this item.
    as


    Cited by:

    1. Catarina Rebelo & Tiago Reis & Joana Guedes & Cláudia Saraiva & Artur Filipe Rodrigues & Susana Simões & Liliana Bernardino & João Peça & Sónia L. C. Pinho & Lino Ferreira, 2022. "Efficient spatially targeted gene editing using a near-infrared activatable protein-conjugated nanoparticle for brain applications," Nature Communications, Nature, vol. 13(1), pages 1-16, December.
    2. Claire Vinel & Gabriel Rosser & Loredana Guglielmi & Myrianni Constantinou & Nicola Pomella & Xinyu Zhang & James R. Boot & Tania A. Jones & Thomas O. Millner & Anaelle A. Dumas & Vardhman Rakyan & Je, 2021. "Comparative epigenetic analysis of tumour initiating cells and syngeneic EPSC-derived neural stem cells in glioblastoma," Nature Communications, Nature, vol. 12(1), pages 1-20, December.
    3. Norman L. Lehman & Nathalie Spassky & Müge Sak & Amy Webb & Cory T. Zumbar & Aisulu Usubalieva & Khaled J. Alkhateeb & Joseph P. McElroy & Kirsteen H. Maclean & Paolo Fadda & Tom Liu & Vineela Gangala, 2022. "Astroblastomas exhibit radial glia stem cell lineages and differential expression of imprinted and X-inactivation escape genes," Nature Communications, Nature, vol. 13(1), pages 1-20, December.

    More about this item

    Statistics

    Access and download statistics

    Corrections

    All material on this site has been provided by the respective publishers and authors. You can help correct errors and omissions. When requesting a correction, please mention this item's handle: RePEc:nat:nature:v:560:y:2018:i:7717:d:10.1038_s41586-018-0389-3. See general information about how to correct material in RePEc.

    If you have authored this item and are not yet registered with RePEc, we encourage you to do it here. This allows to link your profile to this item. It also allows you to accept potential citations to this item that we are uncertain about.

    We have no bibliographic references for this item. You can help adding them by using this form .

    If you know of missing items citing this one, you can help us creating those links by adding the relevant references in the same way as above, for each refering item. If you are a registered author of this item, you may also want to check the "citations" tab in your RePEc Author Service profile, as there may be some citations waiting for confirmation.

    For technical questions regarding this item, or to correct its authors, title, abstract, bibliographic or download information, contact: Sonal Shukla or Springer Nature Abstracting and Indexing (email available below). General contact details of provider: http://www.nature.com .

    Please note that corrections may take a couple of weeks to filter through the various RePEc services.

    IDEAS is a RePEc service. RePEc uses bibliographic data supplied by the respective publishers.