Correlation between gene methylation status and clinical features

Thymoma (Primary solid tumor)

21 August 2015 | analyses__2015_08_21

Maintainer Information

Citation Information

Maintained by Juok Cho (Broad Institute)

Cite as Broad Institute TCGA Genome Data Analysis Center (2015): Correlation between gene methylation status and clinical features. Broad Institute of MIT and Harvard. doi:10.7908/C1154GBW

Overview

Introduction

This pipeline uses various statistical tests to identify genes whose promoter methylation levels correlated to selected clinical features.

Summary

Testing the association between 20084 genes and 8 clinical features across 124 samples, statistically thresholded by P value < 0.05 and Q value < 0.3, 5 clinical features related to at least one genes.

30 genes correlated to 'YEARS_TO_BIRTH'.

VRK2 , TMEM62 , ABCC4 , CCDC82 , JRKL , ...

30 genes correlated to 'GENDER'.

TFDP1 , KIF4B , ZBTB20 , RAD21 , WBP11P1 , ...

30 genes correlated to 'RADIATION_THERAPY'.

MLC1 , FRMPD2 , IFI30 , SOCS1 , KRT80 , ...

30 genes correlated to 'HISTOLOGICAL_TYPE'.

PI16 , ZNF721__1 , C17ORF58 , MS4A2 , KCNMB2 , ...

3 genes correlated to 'RACE'.

LOC401010 , GRAPL , PM20D1

No genes correlated to 'DAYS_TO_DEATH_OR_LAST_FUP', 'TUMOR_TISSUE_SITE', and 'ETHNICITY'.

Results

Overview of the results

Complete statistical result table is provided in Supplement Table 1

Table 1. Get Full Table This table shows the clinical features, statistical methods used, and the number of genes that are significantly associated with each clinical feature at P value < 0.05 and Q value < 0.3.

Clinical feature	Statistical test	Significant genes	Associated with		Associated with
DAYS_TO_DEATH_OR_LAST_FUP	Cox regression test	N=0
YEARS_TO_BIRTH	Spearman correlation test	N=30	older	N=0	younger	N=30
TUMOR_TISSUE_SITE	Wilcoxon test	N=0
GENDER	Wilcoxon test	N=30	male	N=30	female	N=0
RADIATION_THERAPY	Wilcoxon test	N=30	yes	N=30	no	N=0
HISTOLOGICAL_TYPE	Kruskal-Wallis test	N=30
RACE	Kruskal-Wallis test	N=3
ETHNICITY	Wilcoxon test	N=0

Clinical variable #1: 'DAYS_TO_DEATH_OR_LAST_FUP'

No gene related to 'DAYS_TO_DEATH_OR_LAST_FUP'.

Table S1. Basic characteristics of clinical feature: 'DAYS_TO_DEATH_OR_LAST_FUP'


DAYS_TO_DEATH_OR_LAST_FUP	Duration (Months)	0.5-150 (median=40.6)
	censored	N = 114
	death	N = 9

	Significant markers	N = 0

Clinical variable #2: 'YEARS_TO_BIRTH'

30 genes related to 'YEARS_TO_BIRTH'.

Table S2. Basic characteristics of clinical feature: 'YEARS_TO_BIRTH'


YEARS_TO_BIRTH	Mean (SD)	58.15 (13)
	Significant markers	N = 30
	pos. correlated	0
	neg. correlated	30

List of top 10 genes differentially expressed by 'YEARS_TO_BIRTH'

Table S3. Get Full Table List of top 10 genes significantly correlated to 'YEARS_TO_BIRTH' by Spearman correlation test

	SpearmanCorr	corrP	Q
VRK2	-0.4898	8.945e-09	0.000109
TMEM62	-0.4853	1.281e-08	0.000109
ABCC4	-0.4822	1.635e-08	0.000109
CCDC82	-0.4677	4.913e-08	0.000197
JRKL	-0.4677	4.913e-08	0.000197
FAM3C	-0.4556	1.189e-07	0.000254
ARL9	-0.4548	1.261e-07	0.000254
ADAM11	-0.4544	1.296e-07	0.000254
GHDC	-0.4536	1.368e-07	0.000254
UTP23	-0.4536	1.374e-07	0.000254

Clinical variable #3: 'TUMOR_TISSUE_SITE'

No gene related to 'TUMOR_TISSUE_SITE'.

Table S4. Basic characteristics of clinical feature: 'TUMOR_TISSUE_SITE'


TUMOR_TISSUE_SITE	Labels	N
	ANTERIOR MEDIASTINUM	27
	THYMUS	97

	Significant markers	N = 0

Clinical variable #4: 'GENDER'

30 genes related to 'GENDER'.

Table S5. Basic characteristics of clinical feature: 'GENDER'


GENDER	Labels	N
	FEMALE	60
	MALE	64

	Significant markers	N = 30
	Higher in MALE	30
	Higher in FEMALE	0

List of top 10 genes differentially expressed by 'GENDER'

Table S6. Get Full Table List of top 10 genes differentially expressed by 'GENDER'. 0 significant gene(s) located in sex chromosomes is(are) filtered out.

	W(pos if higher in 'MALE')	wilcoxontestP	Q	AUC
TFDP1	79	3.497e-20	7.02e-16	0.9794
KIF4B	102	1.013e-19	1.02e-15	0.9734
ZBTB20	3701	5.46e-19	3.66e-15	0.9638
RAD21	3568	1.758e-16	8.83e-13	0.9292
WBP11P1	3494	3.618e-15	1.45e-11	0.9099
TUBB8	568	1.404e-11	4.7e-08	0.8521
FRG1B	701	1.112e-09	3.19e-06	0.8174
YARS2	710	1.471e-09	3.69e-06	0.8151
FAM35A__1	830	5.108e-08	0.000103	0.7839
GLUD1__1	830	5.108e-08	0.000103	0.7839

Clinical variable #5: 'RADIATION_THERAPY'

30 genes related to 'RADIATION_THERAPY'.

Table S7. Basic characteristics of clinical feature: 'RADIATION_THERAPY'


RADIATION_THERAPY	Labels	N
	NO	81
	YES	43

	Significant markers	N = 30
	Higher in YES	30
	Higher in NO	0

List of top 10 genes differentially expressed by 'RADIATION_THERAPY'

Table S8. Get Full Table List of top 10 genes differentially expressed by 'RADIATION_THERAPY'

	W(pos if higher in 'YES')	wilcoxontestP	Q	AUC
MLC1	2583	1.009e-05	0.0785	0.7416
FRMPD2	922	1.71e-05	0.0785	0.7353
IFI30	932	2.164e-05	0.0785	0.7324
SOCS1	946	2.996e-05	0.0785	0.7284
KRT80	957	3.855e-05	0.0785	0.7252
EP400	2516	4.834e-05	0.0785	0.7224
NETO1	2516	4.834e-05	0.0785	0.7224
GP1BB	2515	4.944e-05	0.0785	0.7221
SEPT5	2515	4.944e-05	0.0785	0.7221
PALMD	972	5.408e-05	0.0785	0.7209

Clinical variable #6: 'HISTOLOGICAL_TYPE'

30 genes related to 'HISTOLOGICAL_TYPE'.

Table S9. Basic characteristics of clinical feature: 'HISTOLOGICAL_TYPE'


HISTOLOGICAL_TYPE	Labels	N
	THYMOMA; TYPE A	17
	THYMOMA; TYPE AB	38
	THYMOMA; TYPE B1	15
	THYMOMA; TYPE B2	31
	THYMOMA; TYPE B3	12
	THYMOMA; TYPE C	11

	Significant markers	N = 30

List of top 10 genes differentially expressed by 'HISTOLOGICAL_TYPE'

Table S10. Get Full Table List of top 10 genes differentially expressed by 'HISTOLOGICAL_TYPE'

	kruskal_wallis_P	Q
PI16	4.251e-15	1.94e-11
ZNF721__1	7.283e-15	1.94e-11
C17ORF58	7.395e-15	1.94e-11
MS4A2	1.026e-14	1.94e-11
KCNMB2	1.271e-14	1.94e-11
MFHAS1	1.287e-14	1.94e-11
BIRC2	1.31e-14	1.94e-11
C17ORF63	1.412e-14	1.94e-11
CCDC50	1.618e-14	1.94e-11
UTS2D	1.618e-14	1.94e-11

Clinical variable #7: 'RACE'

3 genes related to 'RACE'.

Table S11. Basic characteristics of clinical feature: 'RACE'


RACE	Labels	N
	ASIAN	13
	BLACK OR AFRICAN AMERICAN	6
	WHITE	103

	Significant markers	N = 3

List of 3 genes differentially expressed by 'RACE'

Table S12. Get Full Table List of 3 genes differentially expressed by 'RACE'

	kruskal_wallis_P	Q
LOC401010	3.301e-06	0.0663
GRAPL	1.097e-05	0.102
PM20D1	1.522e-05	0.102

Clinical variable #8: 'ETHNICITY'

No gene related to 'ETHNICITY'.

Table S13. Basic characteristics of clinical feature: 'ETHNICITY'


ETHNICITY	Labels	N
	HISPANIC OR LATINO	10
	NOT HISPANIC OR LATINO	100

	Significant markers	N = 0

Methods & Data

Input

Expresson data file = THYM-TP.meth.by_min_clin_corr.data.txt
Clinical data file = THYM-TP.merged_data.txt
Number of patients = 124
Number of genes = 20084
Number of clinical features = 8

Selected clinical features

Further details on clinical features selected for this analysis, please find a documentation on selected CDEs (Clinical Data Elements). The first column of the file is a formula to convert values and the second column is a clinical parameter name.

There are also useful links about clinical features.

CDE Browser

Data dictionary for clinical data

NCI wiki - Biospecimen and Clinical XSD Files Specification

Survival time data

Survival time data is a combined value of days_to_death and days_to_last_followup. For each patient, it creates a combined value 'days_to_death_or_last_fup' using conversion process below.

if 'vital_status'==1(dead), 'days_to_last_followup' is always NA. Thus, uses 'days_to_death' value for 'days_to_death_or_fup'

if 'vital_status'==0(alive),

if 'days_to_death'==NA & 'days_to_last_followup'!=NA, uses 'days_to_last_followup' value for 'days_to_death_or_fup'

if 'days_to_death'!=NA, excludes this case in survival analysis and report the case.

if 'vital_status'==NA,excludes this case in survival analysis and report the case.

cf. In certain diesase types such as SKCM, days_to_death parameter is replaced with time_from_specimen_dx or time_from_specimen_procurement_to_death .

This analysis excluded clinical variables that has only NA values.

Survival analysis

For survival clinical features, Wald's test in univariate Cox regression analysis with proportional hazards model (Andersen and Gill 1982) was used to estimate the P values using the 'coxph' function in R. Kaplan-Meier survival curves were plot using the four quartile subgroups of patients based on expression levels

Correlation analysis

For continuous numerical clinical features, Spearman's rank correlation coefficients (Spearman 1904) and two-tailed P values were estimated using 'cor.test' function in R

Wilcoxon rank sum test (Mann-Whitney U test)

For two groups (mutant or wild-type) of continuous type of clinical data, wilcoxon rank sum test (Mann and Whitney, 1947) was applied to compare their mean difference using 'wilcox.test(continuous.clinical ~ as.factor(group), exact=FALSE)' function in R. This test is equivalent to the Mann-Whitney test.

Q value calculation

For multiple hypothesis correction, Q value is the False Discovery Rate (FDR) analogue of the P value (Benjamini and Hochberg 1995), defined as the minimum FDR at which the test may be called significant. We used the 'Benjamini and Hochberg' method of 'p.adjust' function in R to convert P values into Q values.

Download Results

In addition to the links below, the full results of the analysis summarized in this report can also be downloaded programmatically using firehose_get, or interactively from either the Broad GDAC website or TCGA Data Coordination Center Portal.

References

[1] Andersen and Gill, Cox's regression model for counting processes, a large sample study, Annals of Statistics 10(4):1100-1120 (1982)

[2] Spearman, C, The proof and measurement of association between two things, Amer. J. Psychol 15:72-101 (1904)

[3] Mann and Whitney, On a Test of Whether one of Two Random Variables is Stochastically Larger than the Other, Annals of Mathematical Statistics 18 (1), 50-60 (1947)

[4] Benjamini and Hochberg, Controlling the false discovery rate: a practical and powerful approach to multiple testing, Journal of the Royal Statistical Society Series B 59:289-300 (1995)

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