Molecular variants and mutations in medulloblastoma.

dc.contributor.author

Schroeder, Kristin

dc.contributor.author

Gururangan, Sri

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New Zealand

dc.date.accessioned

2017-08-01T05:53:59Z

dc.date.available

2017-08-01T05:53:59Z

dc.date.issued

2014

dc.description.abstract

Medulloblastoma is the commonest malignant brain tumor in children. Treatment with surgery, irradiation, and chemotherapy has improved outcomes in recent years, but patients are frequently left with devastating neurocognitive and other sequelae following such therapy. While the prognosis has traditionally been based on conventional histopathology and clinical staging (based on age, extent of resection, and presence or absence of metastasis), it has become apparent in recent years that the inherent biology of the tumor plays a significant part in predicting survival and sometimes supersedes clinical or pathologic risk factors. The advent of deep sequencing gene technology has provided invaluable clues to the molecular makeup of this tumor and allowed neuro-oncologists to understand that medulloblastoma is an amalgamation of several distinct disease entities with unique clinical associations and behavior. This review is a concise summary of the pathology, genetic syndromes, recent advances in molecular subgrouping, and the associated gene mutations and copy number variations in medulloblastoma. The association of molecular alterations with patient prognosis is also discussed, but it should be remembered that further validation is required in prospective clinical trials utilizing uniform treatment approaches.

dc.identifier

https://www.ncbi.nlm.nih.gov/pubmed/24523595

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pgpm-7-043

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1178-7066

dc.identifier.uri

https://hdl.handle.net/10161/15103

dc.language

eng

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Informa UK Limited

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Pharmgenomics Pers Med

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10.2147/PGPM.S38698

dc.subject

adults

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children

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medulloblastoma

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molecular subgroups

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mutations

dc.title

Molecular variants and mutations in medulloblastoma.

dc.type

Journal article

duke.contributor.orcid

Schroeder, Kristin|0000-0002-6433-6174

pubs.author-url

https://www.ncbi.nlm.nih.gov/pubmed/24523595

pubs.begin-page

43

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51

pubs.organisational-group

Clinical Science Departments

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Duke

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Faculty

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Pediatrics

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Pediatrics, Hematology-Oncology

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School of Medicine

pubs.publication-status

Published online

pubs.volume

7

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