This pipeline uses various statistical tests to identify genes whose promoter methylation levels correlated to selected clinical features.
Testing the association between 17131 genes and 3 clinical features across 134 samples, statistically thresholded by Q value < 0.05, 1 clinical feature related to at least one genes.
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1 gene correlated to 'GENDER'.
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C2ORF7
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No genes correlated to 'Time to Death', and 'AGE'.
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 Q value < 0.05.
| Clinical feature | Statistical test | Significant genes | Associated with | Associated with | ||
|---|---|---|---|---|---|---|
| Time to Death | Cox regression test | N=0 | ||||
| AGE | Spearman correlation test | N=0 | ||||
| GENDER | t test | N=1 | male | N=1 | female | N=0 |
Table S1. Basic characteristics of clinical feature: 'Time to Death'
| Time to Death | Duration (Months) | 0.2-346 (median=47.5) |
| censored | N = 64 | |
| death | N = 67 | |
| Significant markers | N = 0 |
Table S2. Basic characteristics of clinical feature: 'AGE'
| AGE | Mean (SD) | 56.28 (16) |
| Significant markers | N = 0 |
Table S3. Basic characteristics of clinical feature: 'GENDER'
| GENDER | Labels | N |
| FEMALE | 49 | |
| MALE | 85 | |
| Significant markers | N = 1 | |
| Higher in MALE | 1 | |
| Higher in FEMALE | 0 |
Table S4. Get Full Table List of one gene differentially expressed by 'GENDER'
| T(pos if higher in 'MALE') | ttestP | Q | AUC | |
|---|---|---|---|---|
| C2ORF7 | 6.73 | 1.567e-09 | 2.69e-05 | 0.8703 |
Figure S1. Get High-res Image As an example, this figure shows the association of C2ORF7 to 'GENDER'. P value = 1.57e-09 with T-test analysis.
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Expresson data file = SKCM-TM.meth.for_correlation.filtered_data.txt
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Clinical data file = SKCM-TM.clin.merged.picked.txt
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Number of patients = 134
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Number of genes = 17131
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Number of clinical features = 3
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
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
For two-class clinical features, two-tailed Student's t test with unequal variance (Lehmann and Romano 2005) was applied to compare the log2-expression levels between the two clinical classes using 't.test' function in R
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.
This is an experimental feature. The full results of the analysis summarized in this report can be downloaded from the TCGA Data Coordination Center.