| Literature DB >> 23554906 |
Kristin R Delfino1, Sandra L Rodriguez-Zas.
Abstract
The identification of reliable transcriptome biomarkers requires the simultaneous consideration of regulatory and target elements including microRNAs (miRNAs), transcription factors (TFs), and target genes. A novel approach that integrates multivariate survival analysis, feature selection, and regulatory network visualization was used to identify reliable biomarkers of ovarian cancer survival and recurrence. Expression profiles of 799 miRNAs, 17,814 TFs and target genes and cohort clinical records on 272 patients diagnosed with ovarian cancer were simultaneously considered and results were validated on an independent group of 146 patients. Three miRNAs (hsa-miR-16, hsa-miR-22*, and ebv-miR-BHRF1-2*) were associated with both ovarian cancer survival and recurrence and 27 miRNAs were associated with either one hazard. Two miRNAs (hsa-miR-521 and hsa-miR-497) were cohort-dependent, while 28 were cohort-independent. This study confirmed 19 miRNAs previously associated with ovarian cancer and identified two miRNAs that have previously been associated with other cancer types. In total, the expression of 838 and 734 target genes and 12 and eight TFs were associated (FDR-adjusted P-value <0.05) with ovarian cancer survival and recurrence, respectively. Functional analysis highlighted the association between cellular and nucleotide metabolic processes and ovarian cancer. The more direct connections and higher centrality of the miRNAs, TFs and target genes in the survival network studied suggest that network-based approaches to prognosticate or predict ovarian cancer survival may be more effective than those for ovarian cancer recurrence. This study demonstrated the feasibility to infer reliable miRNA-TF-target gene networks associated with survival and recurrence of ovarian cancer based on the simultaneous analysis of co-expression profiles and consideration of the clinical characteristics of the patients.Entities:
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Year: 2013 PMID: 23554906 PMCID: PMC3595291 DOI: 10.1371/journal.pone.0058608
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Number and distribution of individuals analyzed for post-diagnostic survival and post-diagnostic recurrence and levels of the cohort factors considered.
| Survival | Recurrence | ||||||||
| Training Set | Validation Set | Training Set | Validation Set | ||||||
| Number | Percent | Number | Percent | Number | Percent | Number | Percent | ||
|
| 272 | 146 | 157 | 92 | |||||
|
| 107 | 39% | 75 | 51% | 31 | 20% | 38 | 41% | |
|
|
| 253 | 93% | 101 | 69% | 150 | 96% | 67 | 72% |
|
| 14 | 5% | 25 | 17% | 5 | 3% | 18 | 20% | |
|
| 5 | 2% | 20 | 14% | 2 | 1% | 7 | 8% | |
|
|
| 21 | 8% | 36 | 25% | 7 | 4% | 25 | 27% |
|
| 251 | 92% | 110 | 75% | 150 | 96% | 67 | 73% | |
|
|
| 113 | 41% | 49 | 34% | 106 | 67% | 45 | 49% |
|
| 37 | 14% | 35 | 24% | 34 | 22% | 35 | 38% | |
|
| 122 | 45% | 62 | 42% | 17 | 11% | 12 | 13% | |
|
|
| 12 | 4% | 17 | 12% | 5 | 3% | 9 | 10% |
|
| 239 | 88% | 89 | 61% | 143 | 91% | 59 | 64% | |
|
| 21 | 8% | 40 | 27% | 9 | 6% | 24 | 26% | |
|
|
| 12 | 4% | 45 | 31% | 6 | 4% | 35 | 38% |
|
| 260 | 96% | 101 | 69% | 151 | 96% | 57 | 62% | |
|
|
| 71 | 26% | 52 | 36% | 34 | 22% | 30 | 33% |
|
| 167 | 61% | 60 | 41% | 102 | 65% | 40 | 43% | |
|
| 34 | 13% | 34 | 23% | 21 | 13% | 22 | 24% | |
|
|
| 157 | 58% | 92 | 63% | 157 | 100% | 92 | 100% |
|
| 115 | 42% | 54 | 37% | 0 | 0% | 0 | 0% | |
N: Number of patients;
Treatment: Type of treatment received;
Chemo: Only chemotherapy;
Chemo_Other: Chemotherapy plus another treatment;
Other: Any treatment other than chemotherapy;
Preadjuvant Therapy: Any treatment that the patient received prior to surgery and sample collection;
Additional Treatment: Treatment given after initial first round treatment;
Tumor Stage: pathological stage of the tumor in AJCC format (Primary Tumor: T; Stage I: IA; IB; IC; Stage II: IIA; IIB; IIC; Stage III: IIIA; IIIB; IIIC; Stage IV: IV);
I_II: Stage I or II ovarian cancer;
III: Stage III ovarian cancer;
IV: Stage IV ovarian cancer;
Tumor Grade: Numeric value used to express the degree of abnormality of cancer cells;
I or II: Grade I or II tumor;
Rest: Any tumor grades other than I or II;
Tumor Residual Disease: Measure of the largest remaining nodule;
0: No macroscopic disease;
1_20∶1–20 mm;
>20: Greater than 20 mm;
Recurrence: Return of cancer.
MicroRNAs associated with post-diagnostic survival and supporting independent studies.
| MicroRNA |
| Estimate | Hazard Ratio (95% C.I. | Relevant Literature References |
| hsa-miR-22* | <.0001 | −1.4007 | 0.25 (0.14 to 0.44) |
|
| hsa-miR-770-5p | <.0001 | −1.2946 | 0.27 (0.16 to 0.47) | NA |
| hsa-miR-485-3p | <.0001 | −0.8158 | 0.44 (0.30 to 0.66) |
|
| hsa-miR-16 | <.0001 | 0.7249 | 2.07 (1.53 to 2.79) |
|
| hsa-miR-144 | <.0001 | 0.2644 | 1.3 (1.14 to 1.49) |
|
| ebv-miR-BHRF1-2* | 0.0001 | 1.4787 | 4.39 (2.06 to 9.33) | NA |
| hsa-miR-182* | 0.0001 | 0.8547 | 2.35 (1.51 to 3.65) |
|
| hsa-miR-381 | 0.0001 | 0.6801 | 1.97 (1.40 to 2.79) |
|
| hsa-miR-509-3-5p | 0.0001 | −0.3725 | 0.69 (0.57 to 0.83) |
|
| hsa-miR-19a* | 0.0002 | 0.5574 | 1.75 (1.31 to 2.33) |
|
| hsa-miR-573 | 0.0007 | 0.6298 | 1.88 (1.31 to 2.70) | NA |
| hsa-miR-329 | 0.0031 | −1.4082 | 0.25 (0.10 to 0.62) |
|
| hsa-miR-106b | 0.0024 | 0.4525 | 1.57 (1.17 to 2.11) |
|
| hsa-miR-18b* | 0.0042 | 0.6678 | 1.95 (1.24 to 3.08) |
|
| hsa-miR-521 | 0.0051 | 1.3416 | I_II |
|
| Rest | ||||
| hsa-miR-148a | 0.0063 | −0.2493 | 0.78 (0.65 to 0.93) |
|
C.I.: Confidence Interval;
NA: No information found; OAssociated with Ovarian Cancer; ZAssociated with other cancer type;
I_II: Grade I or II tumor;
Rest: Any tumor grades other than I or II.
MicroRNAs associated with post-diagnostic recurrence on a cohort-independent or -dependent manner and supporting independent studies.
| MicroRNA |
| Estimate | Hazard Ratio (95% C.I. | Relevant Literature References |
| hsa-miR-550* | <.0001 | −2.1165 | 0.12 (0.05 to 0.29) | NA |
| hsa-miR-22* | <.0001 | −1.4397 | 0.24 (0.12 to 0.46) |
|
| hsa-miR-223 | <.0001 | 0.5267 | 1.69 (1.36 to 2.12) |
|
| hsa-miR-146a | <.0001 | −0.4869 | 0.62 (0.49 to 0.77) |
|
| hsa-miR-497 | 0.0001 | 1.5869 | Chemo |
|
| 1.125 | C_O | |||
| Other | ||||
| hsa-miR-214* | 0.0001 | 0.7059 | 2.03 (1.41 to 2.91) |
|
| ebv-miR-BHRF1-2* | 0.0028 | 1.092 | 2.98 (1.46 to 6.10) | NA |
| hsa-miR-96 | 0.0065 | 0.1984 | 1.22 (1.06 to 1.41) |
|
| hsa-miR-924 | 0.0102 | 1.3019 | 3.68 (1.36 to 9.92) | NA |
| hsa-miR-28-3p | 0.0109 | 1.1811 | 3.26 (1.31 to 8.09) | NA |
| hsa-miR-369-3p | 0.0130 | 0.4208 | 1.52 (1.09 to 2.12) |
|
C.I.: Confidence Interval;
NA: No information found;
Associated with Ovarian Cancer;
Associated with other cancer type;
Chemo: Only chemotherapy;
C_O: Chemotherapy plus another therapy;
Other: Any therapy other than chemotherapy.
Figure 1Probability of ovarian cancer survival for patients that have lower grade (I and II) tumors (black lines) or higher (Rest) grade tumors (gray lines) and high (dashed lines) or low (solid line) levels of hsa-miR-521.
Figure 2Probability of ovarian cancer non-recurrence for patients receiving the treatment chemotherapy only, chemotherapy along with another treatment, or some other treatment or combination of treatments except chemotherapy that have high or low levels of hsa-miR-497.
Transcription factors associated with ovarian cancer survival.
| Transcription Factor | Estimate | Hazard Ratio (95% C.I. | Relevant Literature References |
|
| 0.0097 | 0.81 (0.58 to 1.11) |
|
|
| 0.0065 | 1.15 (1.03 to 1.28) |
|
|
| 0.0038 | 1.17 (1.06 to 1.30) |
|
|
| 0.0065 | 0.66 (0.49 to 0.88) |
|
|
| 0.0098 | 1.32 (0.99 to 1.76) |
|
|
| 0.0056 | 1.15 (1.03 to 1.28) |
|
|
| 0.0093 | 1.63 (1.13 to 2.37) |
|
|
| 0.0096 | 0.71 (0.53 to 0.97) |
|
|
| 0.009 | 1.27 (1.05 to 1.54) |
|
|
| 0.0086 | 0.53 (0.34 to 0.82) |
|
|
| 0.008 | 0.64 (0.45 to 0.93) |
|
|
| 0.0054 | 0.46 (0.32 to 0.66) |
|
C.I.: Confidence Interval;
NA: No information found;
Associated with Ovarian Cancer;
Associated with other cancer type.
Transcription factors associated with ovarian cancer recurrence.
| Transcription Factor | Estimate | Hazard Ratio (95% C.I. | Relevant Literature References |
|
| 0.0063 | 1.71 (1.11 to 2.64) |
|
|
| 0.0076 | 1.15 (1.03 to 1.28) |
|
|
| 0.0054 | 1.17 (1.05 to 1.31) |
|
|
| 0.0092 | 1.13 (1.01 to 1.27) |
|
|
| 0.0075 | 0.77 (0.63 to 0.95) |
|
|
| 0.0082 | 0.77 (0.62 to 0.95) |
|
|
| 0.0088 | 1.63 (1.19 to 2.24) |
|
|
| 0.0088 | 0.56 (0.39 to 0.80) |
|
C.I.: Confidence Interval;
Associated with Ovarian Cancer;
Associated with other cancer type.
Differentially enriched Gene Ontology biological processes among all target genes segmented by low and high hazard of ovarian cancer death or recurrence identified by set enrichment analyses.
| − hazard genes | + hazard genes | Loge
| FDR- | ||||
| Trait and GO Category | GO identifier | In GO | Not in GO | In GO | Not in GO | (odds ratio) | adjusted P-value |
|
| |||||||
| regulation of cellular metabolic process | GO:0031323 | 218 | 502 | 198 | 766 | 0.52 | 1.46E−02 |
| regulation of metabolic process | GO:0019222 | 229 | 491 | 214 | 750 | 0.49 | 1.47E−02 |
|
| |||||||
| nucleobase, nucleoside, nucleotide and nucleic acid metabolic process | GO:0006139 | 117 | 175 | 321 | 1034 | 0.77 | 3.91E−05 |
| RNA processing | GO:0006396 | 29 | 263 | 49 | 1306 | 1.08 | 5.96E−03 |
| nitrogen compound metabolic process | GO:0006807 | 122 | 170 | 354 | 1001 | 0.71 | 1.94E−04 |
| regulation of gene expression | GO:0010468 | 84 | 208 | 237 | 1118 | 0.64 | 5.48E−03 |
| gene expression | GO:0010467 | 109 | 183 | 291 | 1064 | 0.78 | 3.91E−05 |
| regulation of transcription | GO:0045449 | 78 | 214 | 213 | 1142 | 0.67 | 5.48E−03 |
| cellular metabolic process | GO:0044237 | 264 | 223 | 492 | 668 | 0.47 | 8.33E−03 |
| cellular biosynthetic process | GO:0044249 | 106 | 186 | 342 | 1013 | 0.52 | 3.13E−02 |
| RNA metabolic process | GO:0016070 | 80 | 212 | 219 | 1136 | 0.67 | 5.48E−03 |
| transcription | GO:0006350 | 82 | 210 | 219 | 1136 | 0.71 | 3.22E−03 |
| regulation of nitrogen compound metabolic process | GO:0051171 | 84 | 208 | 237 | 1118 | 0.64 | 5.48E−03 |
| macromolecule biosynthetic process | GO:0009059 | 97 | 195 | 283 | 1072 | 0.63 | 5.42E−03 |
− hazard genes: number of genes that have a negative association between the hazard of ovarian cancer death (higher survival) or recurrence and expression.
+ hazard genes: number of genes that have a positive association between the hazard of ovarian cancer death (lower survival) or recurrence and expression.
Loge(Odds Ratio): values >1 indicate that the category was more enriched among the genes that have a negative association with hazard than among the genes that have a positive association with hazard; values <1 indicate that the category was more enriched among the genes that have a positive association with hazard than among the genes that have a negative association with hazard; Extreme values indicate higher difference in the enrichment percentages between the negative and positive association groups. Values close to zero indicate similar enrichment percentages between positive and negative association groups.
FDR-adjusted P-value: False discovery rate adjusted P-value of the log odds ratio test. Enrichment at FDR-adjusted Pvalue <0.05) and ≥75 genes in the category.
Figure 3Network of microRNAs, transcription factors, and target genes associated with survival in ovarian cancer.
(Node Shape: microRNA = diamond, target gene = circle, transcription factor = square; Node Color: Red indicates increased hazard with high expression, Green indicates decreased hazard with high expression; Node Size: larger indicates a more extreme association (P-value <0.006), smaller indicates a less extreme association.).
Figure 4Network of microRNA, transcription factors, and target genes associated with ovarian cancer recurrence.
(Node Shape: microRNA = diamond, target gene = circle, transcription factor = square; Node Color: Red indicates increased hazard with high expression, Green indicates decreased hazard with high expression; Node Size: larger indicates a more extreme association (P-value <0.006), smaller indicates a less extreme association.).