Correlation between gene methylation status and clinical features

Uveal Melanoma (Primary solid tumor)

21 August 2015 | analyses__2015_08_21

Maintainer Information

Citation Information

doi:10.7908/C1930SH4

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/C1930SH4

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 19254 genes and 7 clinical features across 80 samples, statistically thresholded by P value < 0.05 and Q value < 0.3, 4 clinical features related to at least one genes.

30 genes correlated to 'DAYS_TO_DEATH_OR_LAST_FUP'.

ITGB3 , C5ORF60 , RIMBP2 , C14ORF138 , CP110 , ...

1 gene correlated to 'YEARS_TO_BIRTH'.

MDGA2

30 genes correlated to 'PATHOLOGY_T_STAGE'.

ACTN4 , LGALS3BP , PSMG3__1 , PPAPDC1B , SRA1 , ...

14 genes correlated to 'GENDER'.

DKFZP434L187 , CROCC , ATP5J__1 , GABPA__1 , FAM35A__1 , ...

No genes correlated to 'PATHOLOGIC_STAGE', 'PATHOLOGY_M_STAGE', and 'RADIATION_THERAPY'.

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=30	shorter survival	N=3	longer survival	N=27
YEARS_TO_BIRTH	Spearman correlation test	N=1	older	N=0	younger	N=1
PATHOLOGIC_STAGE	Kruskal-Wallis test	N=0
PATHOLOGY_T_STAGE	Spearman correlation test	N=30	higher stage	N=0	lower stage	N=30
PATHOLOGY_M_STAGE	Wilcoxon test	N=0
GENDER	Wilcoxon test	N=14	male	N=14	female	N=0
RADIATION_THERAPY	Wilcoxon test	N=0

Clinical variable #1: 'DAYS_TO_DEATH_OR_LAST_FUP'

30 genes 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)	0.1-85.5 (median=19.5)
	censored	N = 66
	death	N = 13

	Significant markers	N = 30
	associated with shorter survival	3
	associated with longer survival	27

List of top 10 genes differentially expressed by 'DAYS_TO_DEATH_OR_LAST_FUP'

Table S2. Get Full Table List of top 10 genes significantly associated with 'Time to Death' by Cox regression test

	HazardRatio	Wald_P	Q	C_index
ITGB3	0	1.437e-06	0.011	0.242
C5ORF60	0	2.269e-06	0.011	0.143
RIMBP2	0	2.966e-06	0.011	0.152
C14ORF138	0	3.053e-06	0.011	0.107
CP110	0	3.544e-06	0.011	0.288
GDE1	0	3.544e-06	0.011	0.288
AQP11	25001	4.702e-06	0.012	0.859
LYG1	0	5.114e-06	0.012	0.241
ADAM20	0	6.102e-06	0.012	0.222
ACAA2	40001	6.429e-06	0.012	0.844

Clinical variable #2: 'YEARS_TO_BIRTH'

One gene related to 'YEARS_TO_BIRTH'.

Table S3. Basic characteristics of clinical feature: 'YEARS_TO_BIRTH'


YEARS_TO_BIRTH	Mean (SD)	61.65 (14)
	Significant markers	N = 1
	pos. correlated	0
	neg. correlated	1

List of one gene differentially expressed by 'YEARS_TO_BIRTH'

Table S4. Get Full Table List of one gene significantly correlated to 'YEARS_TO_BIRTH' by Spearman correlation test

	SpearmanCorr	corrP	Q
MDGA2	-0.4645	1.422e-05	0.274

Clinical variable #3: 'PATHOLOGIC_STAGE'

No gene related to 'PATHOLOGIC_STAGE'.

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


PATHOLOGIC_STAGE	Labels	N
	STAGE IIA	12
	STAGE IIB	27
	STAGE IIIA	25
	STAGE IIIB	10
	STAGE IIIC	1
	STAGE IV	4

	Significant markers	N = 0

Clinical variable #4: 'PATHOLOGY_T_STAGE'

30 genes related to 'PATHOLOGY_T_STAGE'.

Table S6. Basic characteristics of clinical feature: 'PATHOLOGY_T_STAGE'


PATHOLOGY_T_STAGE	Mean (SD)	3.25 (0.74)
		N
	T2	14
	T3	32
	T4	34

	Significant markers	N = 30
	pos. correlated	0
	neg. correlated	30

List of top 10 genes differentially expressed by 'PATHOLOGY_T_STAGE'

Table S7. Get Full Table List of top 10 genes significantly correlated to 'PATHOLOGY_T_STAGE' by Spearman correlation test

	SpearmanCorr	corrP	Q
ACTN4	-0.4844	5.305e-06	0.0912
LGALS3BP	-0.4728	9.47e-06	0.0912
PSMG3__1	-0.463	1.529e-05	0.0981
PPAPDC1B	-0.456	2.128e-05	0.102
SRA1	-0.4389	4.655e-05	0.106
PIM3	-0.4373	4.991e-05	0.106
APBB1IP	-0.4369	5.076e-05	0.106
ZFP36	-0.4352	5.483e-05	0.106
TMEM165	-0.4335	5.893e-05	0.106
NEK6	-0.4327	6.119e-05	0.106

Clinical variable #5: 'PATHOLOGY_M_STAGE'

No gene related to 'PATHOLOGY_M_STAGE'.

Table S8. Basic characteristics of clinical feature: 'PATHOLOGY_M_STAGE'


PATHOLOGY_M_STAGE	Labels	N
	class0	51
	class1	4

	Significant markers	N = 0

Clinical variable #6: 'GENDER'

14 genes related to 'GENDER'.

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


GENDER	Labels	N
	FEMALE	35
	MALE	45

	Significant markers	N = 14
	Higher in MALE	14
	Higher in FEMALE	0

List of top 10 genes differentially expressed by 'GENDER'

Table S10. 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
DKFZP434L187	1451	1.275e-10	2.45e-06	0.9213
CROCC	273	6.194e-07	0.00596	0.8267
ATP5J__1	1279	1.917e-06	0.00923	0.8121
GABPA__1	1279	1.917e-06	0.00923	0.8121
FAM35A__1	337	1.275e-05	0.0409	0.786
GLUD1	337	1.275e-05	0.0409	0.786
SFRS6	354	2.675e-05	0.0736	0.7752
TOR2A	382	8.568e-05	0.172	0.7575
PPHLN1	383	8.92e-05	0.172	0.7568
ZCRB1	383	8.92e-05	0.172	0.7568

Clinical variable #7: 'RADIATION_THERAPY'

No gene related to 'RADIATION_THERAPY'.

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


RADIATION_THERAPY	Labels	N
	NO	76
	YES	3

	Significant markers	N = 0

Methods & Data

Input

Expresson data file = UVM-TP.meth.by_min_clin_corr.data.txt
Clinical data file = UVM-TP.merged_data.txt
Number of patients = 80
Number of genes = 19254
Number of clinical features = 7

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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