Scalable Open Science Approach for Mutation Calling of Tumor Exomes Using Multiple Genomic Pipelines

MC3 Working Group; The Cancer Genome Atlas Research Network

doi:10.1016/j.cels.2018.03.002

Scalable Open Science Approach for Mutation Calling of Tumor Exomes Using Multiple Genomic Pipelines

MC3 Working Group, The Cancer Genome Atlas Research Network

School of Medicine

Research output: Contribution to journal › Article › peer-review

183 Scopus citations

Abstract

The Cancer Genome Atlas (TCGA) cancer genomics dataset includes over 10,000 tumor-normal exome pairs across 33 different cancer types, in total >400 TB of raw data files requiring analysis. Here we describe the Multi-Center Mutation Calling in Multiple Cancers project, our effort to generate a comprehensive encyclopedia of somatic mutation calls for the TCGA data to enable robust cross-tumor-type analyses. Our approach accounts for variance and batch effects introduced by the rapid advancement of DNA extraction, hybridization-capture, sequencing, and analysis methods over time. We present best practices for applying an ensemble of seven mutation-calling algorithms with scoring and artifact filtering. The dataset created by this analysis includes 3.5 million somatic variants and forms the basis for PanCan Atlas papers. The results have been made available to the research community along with the methods used to generate them. This project is the result of collaboration from a number of institutes and demonstrates how team science drives extremely large genomics projects. The MC3 is a variant calling project of over 10,000 cancer exome samples from 33 cancer types. Over three million somatic variants were detected using seven different methods developed from institutions across the United States. These variants formed the basis for the PanCan Atlas papers.

Original language	English (US)
Pages (from-to)	271-281.e7
Journal	Cell Systems
Volume	6
Issue number	3
DOIs	https://doi.org/10.1016/j.cels.2018.03.002
State	Published - Mar 28 2018

Keywords

PanCanAtlas project
TCGA
large-scale
open science
pan-cancer
reproducible computing
somatic mutation calling

ASJC Scopus subject areas

Pathology and Forensic Medicine
Histology
Cell Biology

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10.1016/j.cels.2018.03.002

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@article{4cdb40f285454a308fe76733ab44db3c,

title = "Scalable Open Science Approach for Mutation Calling of Tumor Exomes Using Multiple Genomic Pipelines",

abstract = "The Cancer Genome Atlas (TCGA) cancer genomics dataset includes over 10,000 tumor-normal exome pairs across 33 different cancer types, in total >400 TB of raw data files requiring analysis. Here we describe the Multi-Center Mutation Calling in Multiple Cancers project, our effort to generate a comprehensive encyclopedia of somatic mutation calls for the TCGA data to enable robust cross-tumor-type analyses. Our approach accounts for variance and batch effects introduced by the rapid advancement of DNA extraction, hybridization-capture, sequencing, and analysis methods over time. We present best practices for applying an ensemble of seven mutation-calling algorithms with scoring and artifact filtering. The dataset created by this analysis includes 3.5 million somatic variants and forms the basis for PanCan Atlas papers. The results have been made available to the research community along with the methods used to generate them. This project is the result of collaboration from a number of institutes and demonstrates how team science drives extremely large genomics projects. The MC3 is a variant calling project of over 10,000 cancer exome samples from 33 cancer types. Over three million somatic variants were detected using seven different methods developed from institutions across the United States. These variants formed the basis for the PanCan Atlas papers.",

keywords = "PanCanAtlas project, TCGA, large-scale, open science, pan-cancer, reproducible computing, somatic mutation calling",

author = "{MC3 Working Group} and {The Cancer Genome Atlas Research Network} and Kyle Ellrott and Bailey, {Matthew H.} and Gordon Saksena and Covington, {Kyle R.} and Cyriac Kandoth and Chip Stewart and Julian Hess and Singer Ma and Chiotti, {Kami E.} and McLellan, {Michael D.} and Sofia, {Heidi J.} and Hutter, {Carolyn M.} and Gad Getz and Wheeler, {David A.} and Li Ding and Caesar-Johnson, {Samantha J.} and Demchok, {John A.} and Ina Felau and Melpomeni Kasapi and Ferguson, {Martin L.} and Roy Tarnuzzer and Zhining Wang and Liming Yang and Zenklusen, {Jean C.} and Zhang, {Jiashan (Julia)} and Sudha Chudamani and Jia Liu and Laxmi Lolla and Rashi Naresh and Todd Pihl and Qiang Sun and Yunhu Wan and Ye Wu and Juok Cho and Timothy DeFreitas and Scott Frazer and Nils Gehlenborg and Heiman, {David I.} and Jaegil Kim and Lawrence, {Michael S.} and Pei Lin and Sam Meier and Noble, {Michael S.} and Doug Voet and Hailei Zhang and Brady Bernard and Stephen Baylin and Leslie Cope and Ludmila Danilova and Michael Torbenson",

note = "Publisher Copyright: {\textcopyright} 2018 The Authors",

year = "2018",

month = mar,

day = "28",

doi = "10.1016/j.cels.2018.03.002",

language = "English (US)",

volume = "6",

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journal = "Cell Systems",

issn = "2405-4712",

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T1 - Scalable Open Science Approach for Mutation Calling of Tumor Exomes Using Multiple Genomic Pipelines

AU - MC3 Working Group

AU - The Cancer Genome Atlas Research Network

AU - Ellrott, Kyle

AU - Bailey, Matthew H.

AU - Saksena, Gordon

AU - Covington, Kyle R.

AU - Kandoth, Cyriac

AU - Stewart, Chip

AU - Hess, Julian

AU - Ma, Singer

AU - Chiotti, Kami E.

AU - McLellan, Michael D.

AU - Sofia, Heidi J.

AU - Hutter, Carolyn M.

AU - Getz, Gad

AU - Wheeler, David A.

AU - Ding, Li

AU - Caesar-Johnson, Samantha J.

AU - Demchok, John A.

AU - Felau, Ina

AU - Kasapi, Melpomeni

AU - Ferguson, Martin L.

AU - Tarnuzzer, Roy

AU - Wang, Zhining

AU - Yang, Liming

AU - Zenklusen, Jean C.

AU - Zhang, Jiashan (Julia)

AU - Chudamani, Sudha

AU - Liu, Jia

AU - Lolla, Laxmi

AU - Naresh, Rashi

AU - Pihl, Todd

AU - Sun, Qiang

AU - Wan, Yunhu

AU - Wu, Ye

AU - Cho, Juok

AU - DeFreitas, Timothy

AU - Frazer, Scott

AU - Gehlenborg, Nils

AU - Heiman, David I.

AU - Kim, Jaegil

AU - Lawrence, Michael S.

AU - Lin, Pei

AU - Meier, Sam

AU - Noble, Michael S.

AU - Voet, Doug

AU - Zhang, Hailei

AU - Bernard, Brady

AU - Baylin, Stephen

AU - Cope, Leslie

AU - Danilova, Ludmila

AU - Torbenson, Michael

PY - 2018/3/28

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N2 - The Cancer Genome Atlas (TCGA) cancer genomics dataset includes over 10,000 tumor-normal exome pairs across 33 different cancer types, in total >400 TB of raw data files requiring analysis. Here we describe the Multi-Center Mutation Calling in Multiple Cancers project, our effort to generate a comprehensive encyclopedia of somatic mutation calls for the TCGA data to enable robust cross-tumor-type analyses. Our approach accounts for variance and batch effects introduced by the rapid advancement of DNA extraction, hybridization-capture, sequencing, and analysis methods over time. We present best practices for applying an ensemble of seven mutation-calling algorithms with scoring and artifact filtering. The dataset created by this analysis includes 3.5 million somatic variants and forms the basis for PanCan Atlas papers. The results have been made available to the research community along with the methods used to generate them. This project is the result of collaboration from a number of institutes and demonstrates how team science drives extremely large genomics projects. The MC3 is a variant calling project of over 10,000 cancer exome samples from 33 cancer types. Over three million somatic variants were detected using seven different methods developed from institutions across the United States. These variants formed the basis for the PanCan Atlas papers.

AB - The Cancer Genome Atlas (TCGA) cancer genomics dataset includes over 10,000 tumor-normal exome pairs across 33 different cancer types, in total >400 TB of raw data files requiring analysis. Here we describe the Multi-Center Mutation Calling in Multiple Cancers project, our effort to generate a comprehensive encyclopedia of somatic mutation calls for the TCGA data to enable robust cross-tumor-type analyses. Our approach accounts for variance and batch effects introduced by the rapid advancement of DNA extraction, hybridization-capture, sequencing, and analysis methods over time. We present best practices for applying an ensemble of seven mutation-calling algorithms with scoring and artifact filtering. The dataset created by this analysis includes 3.5 million somatic variants and forms the basis for PanCan Atlas papers. The results have been made available to the research community along with the methods used to generate them. This project is the result of collaboration from a number of institutes and demonstrates how team science drives extremely large genomics projects. The MC3 is a variant calling project of over 10,000 cancer exome samples from 33 cancer types. Over three million somatic variants were detected using seven different methods developed from institutions across the United States. These variants formed the basis for the PanCan Atlas papers.

KW - PanCanAtlas project

KW - TCGA

KW - large-scale

KW - open science

KW - pan-cancer

KW - reproducible computing

KW - somatic mutation calling

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DO - 10.1016/j.cels.2018.03.002

M3 - Article

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AN - SCOPUS:85044569292

SN - 2405-4712

VL - 6

SP - 271-281.e7

JO - Cell Systems

JF - Cell Systems

IS - 3

ER -

Scalable Open Science Approach for Mutation Calling of Tumor Exomes Using Multiple Genomic Pipelines

Abstract

Keywords

ASJC Scopus subject areas

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