| Literature DB >> 28888050 |
Yukihiro Shiraki1, Shinji Mii1, Atsushi Enomoto1, Hiroyuki Momota2, Yi-Peng Han1, Takuya Kato1, Kaori Ushida1, Akira Kato3, Naoya Asai1, Yoshiki Murakumo4, Kosuke Aoki3,5, Hiromichi Suzuki3,5, Fumiharu Ohka3, Toshihiko Wakabayashi3, Tomoki Todo2, Seishi Ogawa5, Atsushi Natsume3, Masahide Takahashi1.
Abstract
In the progression of glioma, tumour cells often exploit the perivascular microenvironment to promote their survival and resistance to conventional therapies. Some of these cells are considered to be brain tumour stem cells (BTSCs); however, the molecular nature of perivascular tumour cells has not been specifically clarified because of the complexity of glioma. Here, we identified CD109, a glycosylphosphatidylinositol-anchored protein and regulator of multiple signalling pathways, as a critical regulator of the progression of lower-grade glioma (World Health Organization grade II/III) by clinicopathological and whole-genome sequencing analysis of tissues from human glioma. The importance of CD109-positive perivascular tumour cells was confirmed not only in human lower-grade glioma tissues but also in a mouse model that recapitulated human glioma. Intriguingly, BTSCs isolated from mouse glioma expressed high levels of CD109. CD109-positive BTSCs exerted a proliferative effect on differentiated glioma cells treated with temozolomide. These data reveal the significance of tumour cells that populate perivascular regions during glioma progression, and indicate that CD109 is a potential therapeutic target for the disease.Entities:
Keywords: CD109; brain tumour stem cells; glioma; tumour microenvironment
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Year: 2017 PMID: 28888050 DOI: 10.1002/path.4981
Source DB: PubMed Journal: J Pathol ISSN: 0022-3417 Impact factor: 7.996