| Literature DB >> 18268491 |
J H Gibcus1, M F Mastik, L Menkema, G H de Bock, Ph M Kluin, Ed Schuuring, J E van der Wal.
Abstract
Amplification of the 11q13 region is one of the most frequent aberrations in squamous cell carcinomas of the head and neck region (HNSCC). Amplification of 11q13 has been shown to correlate with the presence of lymph node metastases and decreased survival. The 11q13.3 amplicon carries numerous genes including cyclin D1 and cortactin. Recently, we reported that FADD becomes overexpressed upon amplification and that FADD protein expression predicts for lymph node positivity and disease-specific mortality. However, the gene within the 11q13.3 amplicon responsible for this correlation is yet to be identified. In this paper, we compared, using immunohistochemical analysis for cyclin D1, FADD and cortactin in a series of 106 laryngeal carcinomas which gene correlates best with lymph node metastases and increased disease-specific mortality. Univariate Cox regression analysis revealed that high expression of cyclin D1 (P=0.016), FADD (P=0.003) and cortactin (P=0.0006) predict for increased risk to disease-specific mortality. Multivariate Cox analysis revealed that only high cortactin expression correlates with disease-specific mortality independent of cyclin D1 and/or FADD. Of genes located in the 11q13 amplicon, cortactin expression is the best predictor for shorter disease-specific survival in late stage laryngeal carcinomas.Entities:
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Year: 2008 PMID: 18268491 PMCID: PMC2266851 DOI: 10.1038/sj.bjc.6604246
Source DB: PubMed Journal: Br J Cancer ISSN: 0007-0920 Impact factor: 7.640
Patient characteristics as determined for the entire series of 167 patients (series) and the overlapping group of 106 patients (overlap)
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|---|---|---|
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| 155 | 106 |
| Median | 61 | 61 |
| Range | 34–89 | 34–89 |
| <61 | 75 (48) | 53 (50) |
| >=61 | 80 (52) | 53 (50) |
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| 156 | 106 |
| Male | 136 (87) | 91 (86) |
| Female | 20 (13) | 15 (14) |
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| 167 | 106 |
| T1 | 22 (13) | 8 (8) |
| T2 | 29 (17) | 22 (21) |
| T3 | 40 (24) | 31 (29) |
| T4 | 76 (46) | 45 (42) |
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| 166 | 106 |
| N0 | 102 (61) | 67 (63) |
| N1 | 24 (15) | 16 (15) |
| N2 | 35 (21) | 21 (20) |
| N3 | 5 (3) | 2 (2) |
| Negative (N−) | 102 (61) | 67 (63) |
| Positive (N+) | 64 (39) | 39 (37) |
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| 156 | 106 |
| Well | 37 (24) | 25 (24) |
| Moderate | 79 (51) | 51 (48) |
| Poor | 40 (26) | 30 (27) |
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| 143 | 106 |
| Surgery | 55 (38) | 42 (40) |
| RT | 24 (17) | 16 (15) |
| Surgery + RT | 64 (45) | 48 (45) |
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| 138 | 106 |
| Median percentage | 20% | 23% |
| <23% | 71 (51) | 52 (49) |
| >23% | 67 (49) | 54 (51) |
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| 136 | 106 |
| Median percentage | 10% | 13% |
| <13% | 71 (52) | 55 (52) |
| >13% | 65 (48) | 51 (48) |
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| 140 | 106 |
| −/+ | 78 (56) | 60 (57) |
| ++/+++ | 62 (44) | 46 (43) |
Abbreviation: RT=radiotherapy.
Figure 1Immunohistochemical staining for cyclin D1, cortactin and FADD. A case without amplification and low cyclin D1 (A), FADD (B) and cortactin (C) expression and a case with amplification and high expression of cyclin D1 (E), FADD (F) and cortactin (G). Expression of ki-67 was unrelated to expression of the 11q13.3 genes (D, H).
Cross table showing the relation between amplification and immunohistochemical staining for cyclin D1, FADD and cortactin
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| Negative | 3 | 5 | 8 |
| Positive | 0 | 8 | 8 |
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| Negative | 6 | 1 | 7 |
| Positive | 1 | 8 | 9 |
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| Negative | 4 | 3 | 7 |
| Positive | 1 | 8 | 9 |
Pearson χ2 P-values for cyclin D1, FADD and cortactin were 0.055, 0.003 and 0.049 respectively.
Univariate Cox regression for FADD, CCND1and CTTN to DSM
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|---|---|---|---|
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| 106 | ||
| Low (<23%) | 52 (49) | 1 | |
| High (>23%) | 54 (51) | 3.51 | 1.27–9.70 ( |
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| 106 | ||
| Low (−/+) | 60 (57) | 1 | |
| High (++/+++) | 46 (43) | 4.73 | 1.71–13.08 ( |
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| 106 | ||
| Low (<13%) | 55 (52) | 1 | |
| High (>13%) | 51 (48) | 13.14 | 3.04–56.87 ( |
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| 106 | ||
| Negative (cN−) | 67 (63) | 1 | |
| Positive (cN+) | 39 (37) | 3.16 | 1.29–7.75 ( |
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| 106 | ||
| Surgery | 42 (40) | 1 | |
| Radiotherapy | 16 (15) | 4.49 | 1.51–13.41 ( |
| Both | 48 (45) | 1.32 | 0.44–3.94 ( |
Abbreviations: CI=confidence interval; DSM=disease specific mortality; HR=hazard ratio; N pos.=number of positive cases.
Age, gender, T-status and grade were not significant and not included in this table.
Multivariate Cox regression for CCND1, CTTN, FADD and lymph node metastasis to DSM
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| 106 | ||
| Low (<23%) | 52 (49) | 1 | |
| High (>23%) | 54 (51) | 1.28 | 0.38–4.24 ( |
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| 106 | ||
| Low (−/+) | 60 (57) | 1 | |
| High (++/+++) | 46 (43) | 1.96 | 0.57–6.68 ( |
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| 106 | ||
| Low (<13%) | 55 (52) | 1 | |
| High (>13%) | 51 (48) | 8.46 | 1.63–43.88 ( |
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| 106 | ||
| Negative (cN−) | 67 (63) | 1 | |
| Positive (cN+) | 39 (37) | 3.96 | 1.30–12.06 ( |
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| 106 | ||
| Surgery | 42 (40) | 1 | |
| Radiotherapy | 16 (15) | 2.72 | 0.75–9.86 ( |
| Both | 48 (45) | 0.75 | 1.50–13.31 ( |
Abbreviations: CI=confidence interval; DSM=disease specific mortality; HR=hazard ratio; N pos.=number of positive cases.
Multivariate Cox regression for CTTN and lymph node metastasis to DSM
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| 106 | ||
| Low (<13%) | 55 (52) | 1 | |
| High (>13%) | 51 (48) | 15.96 | 3.55–71.73 ( |
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| 106 | ||
| Negative (cN−) | 67 (63) | 1 | |
| Positive (cN+) | 39 (37) | 4.03 | 1.57–10.35 ( |
Abbreviations: CI=confidence interval; DSM=disease specific mortality; HR=hazard ratio; N pos.=number of positive cases.
Figure 2Kaplan–Meier analysis on disease-specific mortality for cortactin (A), lymph node positivity (B) and cortactin positivity within lymph node-positive cases (C). Remaining cases are shown below the plots.