Mutation Assessor - Lung Adenocarcinoma (Primary solid tumor)

Mutation Assessor

Lung Adenocarcinoma (Primary solid tumor)

17 April 2019 | None

Maintainer Information

Maintained by David Heiman (Broad Institute)

Overview

Introduction

This report serves to summarize the functional impact of missense mutations in each gene as determined by Mutation Assessor[1].

Summary

High Functional Impact Missense Mutations: 1770
Medium Functional Impact Missense Mutations: 7766
Low Functional Impact Missense Mutations: 6100
Neutral Functional Impact Mutations: 3811

Results

Functional Impact by Gene

Table 1. Get Full Table A gene-level breakdown of missense mutation functional impact, ordered by MutSig rank. Includes missense mutation counts broken down by level of functional impact (high, medium, low, neutral), median functional impact score and level, and most common level(s) of functional impact (mode) per gene.

MutSig Rank	Gene	High Functional Impact Count	Medium Functional Impact Count	Low Functional Impact Count	Neutral Functional Impact Count	Median Functional Impact Score	Median Functional Impact Level	Mode Functional Impact Level
1	TP53	0	45	0	0	3.2150	medium	medium
2	KRAS	0	26	6	2	2.5600	medium	medium
3	STK11	2	4	2	0	2.6575	medium	medium
4	EGFR	17	8	8	2	3.2450	medium	high
5	KEAP1	1	7	3	0	2.4100	medium	medium
6	RB1	0	1	0	1	1.7475	low	medium/neutral
7	IL21R	0	1	1	2	0.9225	low	neutral
9	LMO2	1	1	0	2	1.4275	low	neutral
10	C10orf62	0	0	1	1	0.7500	neutral	low/neutral
11	DKK3	0	1	0	0	2.1750	medium	medium

Methods & Data

Input

CPTAC3-LUAD-TP.ma.maf
sig_genes.txt
Mutation Assessor Scores Release 3:

hg38

A lookup is done against the relevant Mutation Assessor Scores table for each missense mutation in a given MAF file, and available functional impact score and level are appended as two new columns to generate CPTAC3-LUAD-TP.ma.maf. These are summarized in Table 1, sorted by MutSig rank.

References

[1] Boris Reva, Yevgeniy Antipin, and Chris Sander, Predicting the functional impact of protein mutations: application to cancer genomics, Nucl. Acids Res. 39(17):e118 (2011)

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