| Literature DB >> 21285972 |
O Oladipo1, S Conlon, A O'Grady, C Purcell, C Wilson, P J Maxwell, P G Johnston, M Stevenson, E W Kay, R H Wilson, D J J Waugh.
Abstract
BACKGROUND: The CXC-chemokine expression is linked with colorectal cancer (CRC) progression but their significance in resected CRC is unclear. We explored the prognostic impact of such expression in stage II and III CRC.Entities:
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Year: 2011 PMID: 21285972 PMCID: PMC3049559 DOI: 10.1038/sj.bjc.6606055
Source DB: PubMed Journal: Br J Cancer ISSN: 0007-0920 Impact factor: 7.640
Clinicopathologic details of patient cohort
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| Median | 64 | |
| Range | 35–80 | |
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| Male | 149 | 58.7 |
| Female | 105 | 41.3 |
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| Colon | 183 | 72.0 |
| Rectum | 71 | 28.0 |
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| Stage II | 163 | 64.2 |
| Stage III | 91 | 35.6 |
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| I | 19 | 6.3 |
| II | 197 | 77.6 |
| III | 30 | 11.8 |
| Not stated | 9 | 3.5 |
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| Yes | 127 | 50.0 |
| No | 127 | 50.0 |
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| Yes | 163 | 64.2 |
| No | 91 | 34.8 |
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| Alive | 148 | 58.2 |
| Dead-all causes | 106 | 41.8 |
| Dead-from CRC | 85 | 33.5 |
Figure 1Immunohistochemical characterisation of CXC-chemokine and its receptor expression in colorectal tissue. (A) Representative high-powered images (magnification × 200) illustrating weak (left panel) and strong (right panel) immunoreactivity to antibodies used to characterize the expression of CXCR1, CXCR2 and CXCL1 in colorectal biopsy tissue. (B) Representative low-powered images showing differential expression of CXCL8 within the inflammatory cells surrounding the colorectal epithelial tissue.
Figure 2Quantitative comparison of CXC-chemokine and its receptor expression in colorectal tissue. (A) Bar graphs presenting the relative immunoreactivity score calculated for CXCR1, CXCR2 and CXCL1 in normal and malignant colorectal epithelial cells. The mean expression in tumor and normal tissues was compared using Student's t-test. Malignant tissue showed significantly higher levels of expression of all three markers in comparison to the surrounding normal tissue; ***P<0.001. (B) Bar graph illustrating the number of positive cases in which CXCL8 immunoreactivity was detected in the inflammatory cells surrounding the normal and malignant epithelial cells in the colorectal tissue. The majority of the cores with normal epithelium are absent for CXCL8 expression within the inflammatory infiltrate. In contrast, a greater number of cores with malignant epithelium show inflammatory cell CXCL8 positivity.
Relationship between clinico-pathological factors and expression of CXC-chemokine biomarkers in the epithelial cells or immune-infiltrate of colorectal tissue
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| <64 | 14 (6.7%) | 78 (37.1%) | 10 (4.8%) | 8 (4.2%) | 55 (29.1%) | 28 (14.8%) | 17 (8.0%) | 74 (34.7%) | 13 (6.1%) | 39 (17.1%) | 72 (31.6%) | ||||
| >64 | 14 (6.7%) | 82 (39.0%) | 12 (5.7%) |
| 10 (5.3%) | 65 (34.4%) | 23 (12.2%) |
| 13 (6.1%) | 88 (41.3%) | 8 (3.8%) |
| 40 (17.5%) | 77 (33.8%) |
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| Male | 20 (9.5%) | 92 (43.8%) | 13 (6.2%) | 12 (6.3%) | 71 (37.6%) | 30 (15.9%) | 17 (8.0%) | 95 (44.6%) | 12 (5.6%) | 43 (18.9%) | 92 (40.4%) | ||||
| Female | 8 (3.8%) | 68 (32.4%) | 9 (4.3%) |
| 6 (3.2%) | 49 (25.9%) | 21 (11.1%) |
| 13 (6.1%) | 67 (31.5%) | 9 (4.2%) |
| 36 (15.8%) | 57 (25.0%) |
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| II | 16 (7.6%) | 103 (49.0%) | 16 (7.6%) | 11 (5.8%) | 72 (38.1%) | 39 (20.6%) | 18 (8.5%) | 105 (49.3%) | 14 (6.6%) | 43 (18.9%) | 103 (45.2%) | ||||
| III | 12 (5.7%) | 57 (27.1%) | 6 (2.9%) |
| 7 (3.7%) | 48 (25.4%) | 12 (6.3%) |
| 12 (5.6%) | 57 (26.8%) | 7 (3.3%) |
| 36 (15.8%) | 46 (20.2%) |
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| Rectum | 5 (2.4%) | 43 (20.5%) | 11 (5.2%) | 6 (3.2%) | 28 (14.8%) | 12 (6.3%) | 8 (3.8%) | 48 (22.5%) | 2 (0.9%) | 16 (7.0%) | 47 (20.6%) | ||||
| Colon | 23 (11.0%) | 117 (55.7%) | 11 (5.2%) |
| 12 (6.3%) | 92 (48.7%) | 39 (20.6%) |
| 22 (10.3%) | 114 (53.5%) | 19 (8.9%) |
| 63 (27.6%) | 102 (44.7%) |
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| No | 15 (7.1%) | 75 (35.7%) | 13 (6.2%) | 8 (4.2%) | 53 (28.0%) | 24 (12.7%) | 15 (7.0%) | 81 (38.0%) | 11 (5.2%) | 46 (20.2%) | 71 (31.1%) | ||||
| Yes | 13 (6.2%) | 85 (40.5%) | 9 (4.3%) |
| 10 (5.3%) | 67 (35.4%) | 27 (14.3%) |
| 15 (7.0%) | 81 (38.0%) | 10 (4.7%) |
| 33 (14.5%) | 78 (34.2%) |
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Values shown in italic are not significant.
Univariate survival analysis for epithelial CXC-chemokine expression
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| II | 40/163 | 51/163 | ||||||||||
| III | 51/91 |
| 55/91 |
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| Absent/weak | 7/28 | 9/28 | 6/19 | 7/19 | 1/9 | 2/9 | ||||||
| Moderate | 63/160 |
| 69/160 |
| 59/103 |
| 65/103 | 0.146 | 4/57 | 0.675 | 4/57 | 0.106 |
| Strong | 10/22 | 11/22 | 10/14 | 11/14 | 0/8 | 0/8 | ||||||
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| Absent/weak | 8/18 | 9/18 | 8/13 | 9/13 | 0/5 | 0/5 | ||||||
| Moderate | 45/120 |
| 47/120 |
| 40/74 |
| 42/74 | 0.880 | 5/46 | 0.314 | 5/46 | 0.698 |
| Strong | 18/51 | 25/51 | 18/36 | 23/36 | 0/15 | 2/15 | ||||||
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| Absent/weak | 9/30 | 9/30 | 8/14 | 9/14 | 1/16 | 0/16 | ||||||
| Moderate | 63/162 |
| 71/162 |
| 61/107 |
| 66/107 | 0.628 | 2/55 | 0.041 | 5/55 | 0.061 |
| Strong | 8/21 | 9/21 | 6/14 | 7/14 | 2/7 | 2/7 | ||||||
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| Negative | 42/79 | 39/79 | 38/50 | 36/50 | 4/29 | 3/29 | ||||||
| Positive | 42/149 |
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| 41/99 | <0.001 | 54/99 | 0.029 | 1/50 | 0.040 | 4/50 | 0.806 |
Values shown in italic are not significant.
Figure 3Relapse-free survival of stage II and III CRC patients, based on CXCL8 expression within the tumour inflammatory infiltrate. Kaplan–Meier curve representing the recurrence-free survival of stage II and stage III colorectal cancer patients. Samples were stratified on the basis of either positive or negative CXCL8 immunoreactivity within the infiltrating immune cells surrounding the tumor epithelium. Patients with a CXCL8 positive infiltrate were shown to have an increased relapse-free survival with the median interval not being reached. In contrast, patients with no CXCL8 immunoreactivity had a median survival of 69 months (P<0.01; log-ranks test).
Multivariate survival analysis for epithelial- and immune infiltrate-localized CXC-chemokine expression
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| Stage II | 1 | 1.92–4.62 | 1 | 1.60–3.92 |
| Stage III | 2.98 | ( | 2.50 | ( |
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| Negative | 1 | 0.36–0.85 | 1 | 0.462–1.147 |
| Positive | 0.55 | ( | 0.728 | ( |