| Literature DB >> 21989116 |
Patricia P Reis1, Levi Waldron, Bayardo Perez-Ordonez, Melania Pintilie, Natalie Naranjo Galloni, Yali Xuan, Nilva K Cervigne, Giles C Warner, Antti A Makitie, Colleen Simpson, David Goldstein, Dale Brown, Ralph Gilbert, Patrick Gullane, Jonathan Irish, Igor Jurisica, Suzanne Kamel-Reid.
Abstract
BACKGROUND: Oral Squamous Cell Carcinoma (OSCC) is a major cause of cancer death worldwide, which is mainly due to recurrence leading to treatment failure and patient death. Histological status of surgical margins is a currently available assessment for recurrence risk in OSCC; however histological status does not predict recurrence, even in patients with histologically negative margins. Therefore, molecular analysis of histologically normal resection margins and the corresponding OSCC may aid in identifying a gene signature predictive of recurrence.Entities:
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Year: 2011 PMID: 21989116 PMCID: PMC3198722 DOI: 10.1186/1471-2407-11-437
Source DB: PubMed Journal: BMC Cancer ISSN: 1471-2407 Impact factor: 4.430
Clinicopathological data, recurrence and outcome data from 24 OSCC patients (N = 96 samples, training set)
| Variables | N (%) |
|---|---|
| Median (range) | 58.5 (37-83) |
| Male | 15 (62.5) |
| Female | 9 (37.5) |
| Yes | 16 (67) |
| No | 8 (33) |
| Yes | 17 (71) |
| No | 7 (29) |
| Tongue | 16 (67) |
| Floor of mouth | 4 (17) |
| Buccal mucosa | 2 (8) |
| Alveolar | 2 (8) |
| T1-T2 | 12 (50) |
| T3-T4 | 12 (50) |
| Negative (N0) | 12 (50) |
| Positive (N1, N2b, N2c) | 12 (50) |
| I, II | 7 (29) |
| III, IV | 17 (71) |
| Moderately differentiated | 18 (75) |
| Poorly differentiated | 6 (25) |
| Yes | 9 (37.5) |
| No | 15 (62.5) |
| Median (range) | 32 (1.8-34) |
| Median (range) | 13 (1.7-58.8) |
| Alive with no evidence of disease | 13 (55) |
| Alive with disease | 2 (8) |
| Dead of disease | 7 (29) |
| Dead of other causes | 2 (8) |
Clinicopathological data, recurrence data and outcome data from 30 OSCC patients (N = 136 samples, validation set)
| Variables | N (%) |
|---|---|
| Median (range) | 67 (48-81) |
| Male | 21 (70) |
| Female | 9 (30) |
| Yes | 25 (83) |
| No | 5 (17) |
| Yes | 21 (70) |
| No | 9 (30) |
| Tongue | 18 (50) |
| Floor of mouth | 8 (27) |
| Tongue + Floor of mouth | 3 (10) |
| Buccal mucosa | 2 (7) |
| Alveolar | 1 (3) |
| Retromolar | 1 (3) |
| T1-T2 | 14 (47) |
| T3-T4 | 16 (53) |
| Negative (N0) | 24 (80) |
| Positive (N1, N2b, N2c) | 6 (20) |
| I, II | 13 (43) |
| III, IV | 17 (57) |
| Moderately differentiated | 23 (77) |
| Poorly differentiated | 7 (23) |
| Yes | 7 (23) |
| No | 23 (77) |
| Median (range) | 8 (2-36) |
| Median (range) | 21 (1-81) |
| Alive with no evidence of disease | 23 (77) |
| Alive with disease | 4 (13) |
| Dead of disease | 2 (7) |
| Dead of other causes | 1 (3) |
Description of the five publicly available data sets used for meta-analysis
| Public Data Set Reference and Accession ID | Sample Size | Array Platform |
|---|---|---|
| 16 oral carcinoma and 4 adjacent normal tissues from 16 patients | Human Genome U133A Plus 2.0 (Affymetrix) | |
| 26 oral carcinoma samples and 12 adjacent normal tissues from 26 patients | Human Genome U133A Plus 2.0 (Affymetrix) | |
| 22 head and neck carcinomas and 22 adjacent normal tissues from 22 patients | Human Genome U95A (Affymetrix) | |
| 35 oral carcinoma samples from 35 patients and 6 normal oral tissues from healthy individuals | Human Oligo Set 4.0 (Operon) | |
| 42 head and neck carcinoma samples from 42 patients and 14 normal oral tissues from healthy individuals | Human Genome U133A Plus 2.0 (Affymetrix) | |
Figure 1Heatmap of 138 genes up-regulated in OSCC. Expression values for each row (gene) are scaled to z-scores for visualization. Margins and tumors annotated with darker colors above the heatmap are from patients who experienced recurrence.
Figure 2Protein-protein interaction network of 138 genes. I2D version 1.72 was used to identify protein interactions for the 138 genes shown in the heatmap. The resulting network was visualized using NAViGaTOR 2.1.14 http://ophid.utoronto.ca/navigator. Color of nodes corresponds to Gene Ontology biological function, as described in the legend. Red-highlighted squares represent the four genes in the signature of OSCC recurrence.
Figure 3Heatmap of validation data and Kaplan-Meier plot of disease recurrence. (A) Unsupervised hierarchical clustering of the quantitative real-time PCR (validation data) showing the maximum expression levels of MMP1, P4HA2, THBS2 and COL4A1 in margins from patients with and without recurrence and with a follow-up time ≥ 12 months. Margins annotated with darker green above the heatmap are from patients who experienced recurrence. Margins from patients with locally recurrent tumors show increased expression levels of the four-gene signature compared to patients who did not recur. (B) Kaplan-Meier plot of quantitative real-time PCR data for patients in the validation set. Patients are assigned to high or low risk based on their four-gene signature risk score. As seen in the Kaplan-Meier plot, patients with over-expression of the 4-gene signature are at high risk for disease recurrence; all patients who experienced recurrence in the validation set are in the high risk group, suggesting that over-expression of this signature was highly predictive of recurrence in the validation set.
Coefficients of the linear risk score for z-score normalized log2-expression values.
| Gene | Coefficient | FC (microarray) | FC (RQ-PCR) | |
|---|---|---|---|---|
| 0.63 | 405 | 798 | 9E-16 | |
| 0.25 | 3.7 | 4.3 | 7E-09 | |
| 0.45 | 2.7 | 2.8 | 1E-06 | |
| 0.34 | 3 | 1.9 | 6E-03 | |
Fold-change (FC) is the geometric-average expression in tumors relative to surgical resection margins. P-values are for tumor/margin differential expression in the qPCR (independent validation set) (Wilcoxon Rank Sum test)