作者
Timothy J Ley, Elaine R Mardis, Li Ding, Bob Fulton, Michael D McLellan, Ken Chen, David Dooling, Brian H Dunford-Shore, Sean McGrath, Matthew Hickenbotham, Lisa Cook, Rachel Abbott, David E Larson, Dan C Koboldt, Craig Pohl, Scott Smith, Amy Hawkins, Scott Abbott, Devin Locke, LaDeana W Hillier, Tracie Miner, Lucinda Fulton, Vincent Magrini, Todd Wylie, Jarret Glasscock, Joshua Conyers, Nathan Sander, Xiaoqi Shi, John R Osborne, Patrick Minx, David Gordon, Asif Chinwalla, Yu Zhao, Rhonda E Ries, Jacqueline E Payton, Peter Westervelt, Michael H Tomasson, Mark Watson, Jack Baty, Jennifer Ivanovich, Sharon Heath, William D Shannon, Rakesh Nagarajan, Matthew J Walter, Daniel C Link, Timothy A Graubert, John F DiPersio, Richard K Wilson
发表日期
2008/11/6
期刊
Nature
卷号
456
期号
7218
页码范围
66-72
出版商
Nature Publishing Group UK
简介
Acute myeloid leukaemia is a highly malignant haematopoietic tumour that affects about 13,000 adults in the United States each year. The treatment of this disease has changed little in the past two decades, because most of the genetic events that initiate the disease remain undiscovered. Whole-genome sequencing is now possible at a reasonable cost and timeframe to use this approach for the unbiased discovery of tumour-specific somatic mutations that alter the protein-coding genes. Here we present the results obtained from sequencing a typical acute myeloid leukaemia genome, and its matched normal counterpart obtained from the same patient’s skin. We discovered ten genes with acquired mutations; two were previously described mutations that are thought to contribute to tumour progression, and eight were new mutations present in virtually all tumour cells at presentation and relapse, the function of which …
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TJ Ley, ER Mardis, L Ding, B Fulton, MD McLellan… - Nature, 2008