Somatic intronic microsatellite loci differentiate glioblastoma from lower-grade gliomas

Authors

Enusha Karunasena, Virginia Bioinformatics Institute, Blacksburg, VA
Lauren J. McIver, Virginia Bioinformatics Institute, Blacksburg, VA
Brian R. Rood, George Washington UniversityFollow
Xiaowei Wu, Virginia Polytechnic Institute and State University
Hongxiao Zhu, Virginia Polytechnic Institute and State University
Jasmin H. Bavarva, Virginia Bioinformatics Institute, Blacksburg, VA
Harold R. Garner, Virginia Bioinformatics Institute, Blacksburg, VA

Document Type

Journal Article

Publication Date

8-2014

Journal

Oncotarget

Volume

Volume 5, Issue 15

Inclusive Pages

6003-6014

Abstract

Genomic studies of glioma sub-types have amassed new disease specific mutations, yet these only partially explain how mutations are linked to predisposition or progression. We hypothesized that microsatellite variation could expand the understanding of glioma etiology. Furthermore, germline markers for gliomas are typically undetectable; therefore we also hypothesize that the predictability of cancer-associated microsatellite loci in germline DNA may support the current hypothesis of a glioma cell of origin.

In this study, “normal” germline exome sequenced DNA from the 1000 Genomes Project (n=390) were compared with exome sequences from germlines of subjects with WHO grade II and III lower-grade glioma (LGG, n=136) and WHO grade IV glioblastoma (GBM, n=252) from The Cancer Genome Atlas to identify microsatellite loci non-randomly associated with glioma. From germline data, we identified 48 GBM-specific loci, 42 Lower-grade glioma specific loci and 29 loci that distinguish GBM from LGG (p≤ 0.01). We then attempted to distinguish WHO grade II glioma (n=67) from GBM resulting in 8 informative loci. Significantly, in all glioma grades, comparisons between tumor and matched germline sequences demonstrated no significant differences in these variants (p≥ 0.01). Therefore, these microsatellite loci are considered to be components of grade-specific signatures for glioma which distinguish germline sequences of individuals with cancer from those of individuals that are “normal”. In order to better understand the significance of these loci, we identified biological processes enriched in genes with these variants. Most strikingly, six helicase genes were enriched in the GBM cohort (p≤ 1.0 x10-3). The preservation of these glioma-specific loci could therefore serve as valuable diagnostic and therapeutic markers; especially since the heterogeneity of tumor cell populations can obscure the identification of mutations preceding a metastatic phenotype.

Comments

Reproduced with permission of Impact Journals. Oncotarget.

Creative Commons License

This work is licensed under a Creative Commons Attribution 3.0 License.

APA Citation

Karunasena, E., McIver, L.J., Rood, B., Wu, X., Zhu, H., et al. (2014). Somatic intronic microsatellite loci differentiate glioblastoma from lower-grade gliomas. Oncotarget, 5(15), 6003-6014.

Peer Reviewed

1

Open Access

1