Variable methylation of the imprinted gene, SNRPN, supports a relationship between intracranial germ cell tumours and neural stem cells

被引:0
作者
Shih-Han Lee
Vanessa Appleby
Jennie N. Jeyapalan
Roger D. Palmer
James C. Nicholson
Virginie Sottile
Erning Gao
Nicholas Coleman
Paul J. Scotting
机构
[1] University of Nottingham,Children’s Brain Tumour Research Centre, Institute of Genetics
[2] Queen’s Medical Centre,Wolfson Centre for Stem Cells, Tissue, Engineering and Modelling (STEM), School of Clinical Sciences
[3] The University of Nottingham,MRC Cancer Cell Unit
[4] Hutchison/MRC Research Centre,Department of Paediatric Oncology
[5] Box 197,undefined
[6] Addenbrooke’s Hospital,undefined
[7] Box 181,undefined
来源
Journal of Neuro-Oncology | 2011年 / 101卷
关键词
Intracranial; Germ cell tumour; Germinoma; SNRPN; Imprinting;
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摘要
Germ cell tumours (GCTs) are a diverse group of neoplasms all of which are generally believed to arise from germ cell progenitors (PGCs). Even those that form in the nervous system are likewise believed to be PGC-derived, despite being found a great distance from the normal location of germ cells. The primary evidence in favour of this model for the origins of intracranial GCTs is that they share molecular features with other GCTs. Those features include shared gene expression and a lack of methylation of imprinted genes, including SNRPN. Contrary to this model, we have proposed that endogenous neural stem cells of the brain are a more likely origin for these tumours. We show here that the lack of methylation of SNRPN that has previously been taken to indicate an origin for GCTs from PGCs is also seen in neural stem cells of mice and humans. We believe that, in the light of these and other recent observations, endogenous neural precursors of the brain are a more plausible origin for intracranial GCTs than are misplaced PGCs.
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页码:419 / 428
页数:9
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