PT  - JOURNAL ARTICLE
AU  - Navid Ahmadinejad
AU  - Shayna Troftgruben
AU  - Carlo Maley
AU  - Junwen Wang
AU  - Li Liu
TI  - MAGOS: Discovering Subclones in Tumors Sequenced at Standard Depths
AID  - 10.1101/790386
DP  - 2019 Jan 01
TA  - bioRxiv
PG  - 790386
4099  - http://biorxiv.org/content/early/2019/10/02/790386.short
4100  - http://biorxiv.org/content/early/2019/10/02/790386.full
AB  - Understanding intratumor heterogeneity is critical to designing personalized treatments and improving clinical outcomes of cancers. Such investigations require accurate delineation of the subclonal composition of a tumor, which to date can only be reliably inferred from deep-sequencing data (>300x depth). To enable accurate subclonal discovery in tumors sequenced at standard depths (30-50x), we develop a novel computational method that incorporates an adaptive error model into statistical decomposition of mixed populations, which corrects the mean-variance dependency of sequencing data at the subclonal level. Tested on extensive computer simulations and real-world data, this new method, named model-based adaptive grouping of subclones (MAGOS), consistently outperforms existing methods on minimum sequencing depth, decomposition accuracy and computation efficiency. MAGOS supports subclone analysis using single nucleotide variants and copy number variants from one or more samples of an individual tumor. Applications of MAGOS to whole-exome sequencing data of 331 liver cancer samples discovered a significant association between subclonal diversity and patient overall survival. MAGOS is freely available as an R package at github (https://github.com/liliulab/magos).