Comprehensive assessment of cancer missense mutation clustering in protein structures

Kamburov, Atanas; Lawrence, Michael S.; Polak, Paz; Leshchiner, Ignaty; Lage, Kasper; Golub, Todd R.; Lander, Eric S.; Getz, Gad

Author(s)

Kamburov, Atanas; Polak, Paz; Lage, Kasper; Lawrence, Michael; Leshchiner, Ignaty; ... Show more

DownloadE5486.full.pdf (1.470Mb)

PUBLISHER_POLICY

Terms of use

Article is made available in accordance with the publisher's policy and may be subject to US copyright law. Please refer to the publisher's site for terms of use.

Metadata

Show full item record

Abstract

Large-scale tumor sequencing projects enabled the identification of many new cancer gene candidates through computational approaches. Here, we describe a general method to detect cancer genes based on significant 3D clustering of mutations relative to the structure of the encoded protein products. The approach can also be used to search for proteins with an enrichment of mutations at binding interfaces with a protein, nucleic acid, or small molecule partner. We applied this approach to systematically analyze the PanCancer compendium of somatic mutations from 4,742 tumors relative to all known 3D structures of human proteins in the Protein Data Bank. We detected significant 3D clustering of missense mutations in several previously known oncoproteins including HRAS, EGFR, and PIK3CA. Although clustering of missense mutations is often regarded as a hallmark of oncoproteins, we observed that a number of tumor suppressors, including FBXW7, VHL, and STK11, also showed such clustering. Beside these known cases, we also identified significant 3D clustering of missense mutations in NUF2, which encodes a component of the kinetochore, that could affect chromosome segregation and lead to aneuploidy. Analysis of interaction interfaces revealed enrichment of mutations in the interfaces between FBXW7-CCNE1, HRAS-RASA1, CUL4B-CAND1, OGT-HCFC1, PPP2R1A-PPP2R5C/PPP2R2A, DICER1-Mg 2+ , MAX-DNA, SRSF2-RNA, and others. Together, our results indicate that systematic consideration of 3D structure can assist in the identification of cancer genes and in the understanding of the functional role of their mutations. Keywords: cancer; cancer genetics; mutation clustering; protein structures; interaction interfaces

Date issued

2015-09

URI

http://hdl.handle.net/1721.1/115276

Department

Broad Institute of MIT and Harvard; Massachusetts Institute of Technology. Department of Biology; Massachusetts Institute of Technology. Department of Chemical Engineering

Journal

Proceedings of the National Academy of Sciences

Publisher

National Academy of Sciences (U.S.)

Citation

Kamburov, Atanas et al. “Comprehensive Assessment of Cancer Missense Mutation Clustering in Protein Structures.” Proceedings of the National Academy of Sciences 112, 40 (September 2015): E5486–E5495

Version: Final published version

ISSN

0027-8424

1091-6490

Collections

MIT Open Access Articles

DSpace@MIT