Recurrent epimutation of SDHC in gastrointestinal stromal tumors.

Authors

J Keith Killian
Markku Miettinen
Robert L Walker
Yonghong Wang
Yuelin Jack Zhu
Joshua J Waterfall
Natalia Noyes
Parvathy Retnakumar
Zhi-Ming Yang MD, PhD, Lehigh Valley Health NetworkFollow
William I Smith
M Scott Killian
C Christopher Lau
Marbin Pineda
Jennifer Walling
Holly Stevenson
Carly Smith
Zengfeng Wang
Jerzy Lasota
Su Young Kim
Sosipatros A Boikos
Lee J Helman
Paul S Meltzer

Publication/Presentation Date

12-24-2014

Abstract

Succinate dehydrogenase (SDH) is a conserved effector of cellular metabolism and energy production, and loss of SDH function is a driver mechanism in several cancers. SDH-deficient gastrointestinal stromal tumors (dSDH GISTs) collectively manifest similar phenotypes, including hypermethylated epigenomic signatures, tendency to occur in pediatric patients, and lack of KIT/PDGFRA mutations. dSDH GISTs often harbor deleterious mutations in SDH subunit genes (SDHA, SDHB, SDHC, and SDHD, termed SDHx), but some are SDHx wild type (WT). To further elucidate mechanisms of SDH deactivation in SDHx-WT GIST, we performed targeted exome sequencing on 59 dSDH GISTs to identify 43 SDHx-mutant and 16 SDHx-WT cases. Genome-wide DNA methylation and expression profiling exposed SDHC promoter-specific CpG island hypermethylation and gene silencing in SDHx-WT dSDH GISTs [15 of 16 cases (94%)]. Six of 15 SDHC-epimutant GISTs occurred in the setting of the multitumor syndrome Carney triad. We observed neither SDHB promoter hypermethylation nor large deletions on chromosome 1q in any SDHx-WT cases. Deep genome sequencing of a 130-kbp (kilo-base pair) window around SDHC revealed no recognizable sequence anomalies in SDHC-epimutant tumors. More than 2000 benign and tumor reference tissues, including stem cells and malignancies with a hypermethylator epigenotype, exhibit solely a non-epimutant SDHC promoter. Mosaic constitutional SDHC promoter hypermethylation in blood and saliva from patients with SDHC-epimutant GIST implicates a postzygotic mechanism in the establishment and maintenance of SDHC epimutation. The discovery of SDHC epimutation provides a unifying explanation for the pathogenesis of dSDH GIST, whereby loss of SDH function stems from either SDHx mutation or SDHC epimutation.

Volume

6

Issue

268

First Page

268

Last Page

268

ISSN

1946-6242

Published In/Presented At

Killian, J. K., Miettinen, M., Walker, R. L., Wang, Y., Zhu, Y. J., Waterfall, J. J., Noyes, N., Retnakumar, P., Yang, Z., Smith, W. I., Jr, Killian, M. S., Lau, C. C., Pineda, M., Walling, J., Stevenson, H., Smith, C., Wang, Z., Lasota, J., Kim, S. Y., Boikos, S. A., … Meltzer, P. S. (2014). Recurrent epimutation of SDHC in gastrointestinal stromal tumors. Science translational medicine, 6(268), 268ra177. https://doi.org/10.1126/scitranslmed.3009961

Disciplines

Medicine and Health Sciences

PubMedID

25540324

Department(s)

Department of Pathology and Laboratory Medicine

Document Type

Article