| Literature DB >> 19672256 |
A F Lomholt1, G Høyer-Hansen, H J Nielsen, I J Christensen.
Abstract
BACKGROUND: Colorectal cancer (CRC) is a leading cause of cancer-related morbidity and mortality in developed countries. It is known that early detection results in improved survival, and consequently there is a need for improved diagnostic tools in CRC. The plasma level of soluble urokinase plasminogen activator receptor (suPAR) was proposed as a marker in CRC patients. This study was undertaken to evaluate the individual molecular forms of suPAR as discriminators in a group of patients undergoing endoscopical examination following symptoms related to colorectal cancer.Entities:
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Year: 2009 PMID: 19672256 PMCID: PMC2743369 DOI: 10.1038/sj.bjc.6605228
Source DB: PubMed Journal: Br J Cancer ISSN: 0007-0920 Impact factor: 7.640
Subject characteristics for each case/controls with 77 individuals in each group
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|---|---|
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| Female | 37 (48) |
| Male | 40 (52) |
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| 40+ | 3 (4) |
| 50+ | 10 (13) |
| 60+ | 17 (22) |
| 70+ | 26 (34) |
| 80+ | 21 (27) |
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| Right colon | 23 (30) |
| Left colon | 34 (44) |
| Rectum | 20 (26) |
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| I | 9 (12) |
| II | 32 (42) |
| III | 16 (21) |
| IV | 15 (19) |
| not specified | 5 (6) |
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| Tubular | 45 (58) |
| Tubulovillous | 16 (21) |
| Villous | 1 (1) |
| Serrat | 1 (1) |
| Not specified | 14 (18) |
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| <1 cm | 41 (53) |
| >1 cm | 33 (43) |
| Not specified | 3 (4) |
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| Diverticulosis | 72 (94) |
| Haemorrhoids | 4 (5) |
| Inflammatory bowel disease | 1 (1) |
Figure 1Box plot showing the distribution of the different plasma uPAR forms in the four different diagnostic groups.
uPAR(I) treated as a binary variable with cut-point at the limit of quantification or the 3rd quartile
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|---|---|---|
| CRC | 46 (59.7) | 25 (32.5) |
| Adenoma | 36 (46.8) | 18 (23.4) |
| Other non-malignant finding | 28 (36.4) | 12 (15.6) |
| No finding | 38 (49.4) | 22 (28.6) |
The table shows the proportion of subjects with detectable uPAR(I) in each diagnosis group (n=77).
The odds ratios (OR) for elevated uPAR(I) comparing diagnostic groups.(ONM=other non-malignant)
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|---|---|---|
| ONM finding | 0.50 (0.25–0.99) | 0.047 |
| Adenoma | 1.18 (0.62–2.23) | 0.611 |
| Adenoma | 2.38 (1.27–4.47) | 0.007 |
| CRC | 1.45 (0.79–2.63) | 0.235 |
| CRC | 1.71 (0.91–3.18) | 0.093 |
| CRC | 3.44 (1.86–6.37) | <0.0001 |
Relative mean difference (%) between the diagnostic groups for intact suPAR and intact+cleaved suPAR
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|---|---|---|---|
| suPAR(I–III) | Non-malignant | −3.3 (−13.3–5.8) | 0.488 |
| Adenoma | 6.4 (−3.4–17.2) | 0.208 | |
| Adenoma | 9.9 (−0.1–21.0) | 0.052 | |
| CRC | 9.0 (−1.5–18.5) | 0.089 | |
| CRC | 17.0 (5.5–29.7) | 0.003 | |
| CRC | 20.9 (10.2–32.6) | <0.0001 | |
| suPAR(I–III)+(II–III) | Non-malignant | −6.5 (−17.0–3.1) | 0.190 |
| Adenoma | 2.3 (−7.2–12.7) | 0.653 | |
| Adenoma | 8.9 (−0.8–19.5) | 0.072 | |
| CRC | 8.1 (−1.9–17.2) | 0.110 | |
| CRC | 11.3 (−0.1–24.0) | 0.052 | |
| CRC | 18.5 (9.0–28.8) | <0.0001 |
Results of type III hypothesis tests (ONM=other non-malignant).
Showing the proportion of cancer patients with uPAR levels exceeding the level found in the corresponding adenoma, ONM and no finding was estimated with 95% CI
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|---|---|---|---|---|
| suPAR( I–III)+(II–III) | All | 64 (53–74) | 70 (60–80) | 66 (56–77) |
| M0 | 59 (44–73) | 67 (54–80) | 61 (48–75) | |
| suPAR(I–III) | All | 55 (43–66) | 70 (60–80) | 64 (53–74) |
| M0 | 51 (37–65) | 67 (54–80) | 61 (48–75) | |
| uPAR(I) | All | 61 (49–73) | 67 (55–80) | 60 (48–72) |
| M0 | 54 (38–70) | 68 (49–83) | 59 (44–75) |
M0=analyses restricted to the group of patients presenting no distant metastases (n=49).
Ties excluded.