| Literature DB >> 22907422 |
Jason A Zell1, Bruce S Lin, Nikki Madson, Christine E McLaren, Eugene W Gerner, Frank L Meyskens.
Abstract
BACKGROUND: Chemoprevention with the polyamine-inhibitory regimen difluoromethylornithine (DFMO) + sulindac markedly reduces risk of recurrent adenoma in colorectal adenoma patients. Obesity is associated with risk of colorectal adenoma and colorectal cancer. This study investigates how obesity influences risk of recurrent adenoma after prolonged treatment with DFMO + sulindac versus placebo.Entities:
Mesh:
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Year: 2012 PMID: 22907422 PMCID: PMC3443348 DOI: 10.1007/s10552-012-0051-6
Source DB: PubMed Journal: Cancer Causes Control ISSN: 0957-5243 Impact factor: 2.506
Clinicopathologic baseline characteristics of the final analytic cohort
| All ( | BMI < 30 ( | BMI ≥ 30 ( |
| |
|---|---|---|---|---|
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| ||||
| Median | 60.8 | 61.9 | 59.0 | 0.004a |
| Range | 41.4–78.8 | 41.4–78.8 | 42.4–73.8 | |
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| Male | 202 (75.7 %) | 138 (76.2 %) | 64 (74.4 %) | 0.74 |
| Female | 65 (24.3 %) | 43 (23.8 %) | 22 (25.6 %) | |
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| Asian/Pacific Islander | 12 (4.5 %) | 11 (6.1 %) | 1 (1.1 %) | 0.14 |
| Black | 8 (3.0 %) | 5 (2.8 %) | 3 (3.5 %) | |
| Hispanic | 19 (7.1 %) | 9 (5.0 %) | 10 (11.6 %) | |
| White | 224 (83.9 %) | 153 (84.5 %) | 71 (82.6 %) | |
| Other | 4 (1.5 %) | 3 (1.7 %) | 1 (1.1 %) | |
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| Yes | 103 (38.6 %) | 74 (40.9 %) | 29 (33.7 %) | 0.26 |
| No | 164 (61.4 %) | 107 (59.1 %) | 57 (66.3 %) | |
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| Median | 28.8 | – | – | – |
| Range | 17.0–52.4 | – | – | |
| 95 % CI | 21.9–39.3 | – | – | |
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| DFMO/sulindac | 138 (51.7 %) | 95 (52.5 %) | 43 (50.0 %) | 0.70 |
| Placebo | 129 (49.3 %) | 86 (47.5 %) | 43 (50.0 %) | |
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| Putrescine | ||||
| Median | 0.49 | 0.5 | 0.49 | 0.58a |
| Range | 0.01–5.29 | 0.01–5.29 | 0.01–3.27 | |
| Spermidine | ||||
| Median | 2.06 | 2.07 | 2.05 | 0.93a |
| Range | 0.76–11.45 | 0.76–9.18 | 1.05–11.45 | |
| Spermine | ||||
| Median | 7.07 | 7.07 | 7.12 | 0.43a |
| Range | 2.29–34.10 | 2.29–28.31 | 3.88–34.10 | |
| Spermidine:spermine Ratio | ||||
| Median | 0.3 | 0.3 | 0.29 | 0.33a |
| Range | 0.19–0.98 | 0.19–0.98 | 0.20–0.76 | |
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| Mean | 2.4 (± 2.0 SD) | 2.2 (± 1.6 SD) | 3.0 (± 2.6 SD) | 0.006 |
| Median | 2 | 2 | 2 | |
| 95 % CI | 1–6 | 1–6 | 1–8 | |
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| <10 | 183 (68.5 %) | 136 (75.1 %) | 47 (54.6 %) | 0.0008 |
| ≥10 | 84 (31.5 %) | 45 (24.9 %) | 39 (45.4 %) | |
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| <3 | 182 (68.9 %) | 132 (73.7 %) | 50 (58.8 %) | 0.01 |
| ≥3 | 82 (31.1 %) | 47 (26.3 %) | 35 (41.2 %) | |
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| Yes | 46 (17.2 %) | 24 (13.3 %) | 22 (25.6 %) | 0.013 |
| No | 221 (82.8 %) | 157 (86.7 %) | 64 (74.4 %) | |
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| Proximalf | 99 (37.2 %) | 78 (43.3 %) | 21 (24.4 %) | 0.003 |
| Distalg | 167 (62.8 %) | 102 (56.7 %) | 65 (75.6 %) | |
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| Yes | 144 (53.9 %) | 82 (45.3 %) | 62 (72.1 %) | <0.0001 |
| No | 123 (46.1 %) | 99 (54.7 %) | 24 (27.9 %) | |
* p values indicate comparisons between the obese and non-obese groups
aMann–Whitney U test
bData missing from three patients
cnmol polyamine per milligram protein
dIncludes adenomas with villous or tubulovillous features, high-grade dysplasia, or carcinoma-in situ
eData missing from one patient
fIncludes the cecum, right colon, and transverse colon
gIncludes the left colon and rectum
hIncludes adenomas >1 cm in size, multiple adenomas (3 or more at baseline), or those with the following histologic characteristics: villous or tubulovillous features, high-grade dysplasia, or carcinoma-in situ
Colorectal adenoma recurrence risk* after treatment with DFMO + sulindac versus placebo, by obesity status at baseline
| Non-obese patients ( | Obese patients ( | |||||
|---|---|---|---|---|---|---|
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| Risk ratio (95 % confidence interval) |
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| Risk ratio (95 % confidence interval) |
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| Any adenoma | 49 | 0.27 (0.15–0.49) | <0.0001 | 23 | 0.32 (0.15–0.71) | 0.005 |
Risk ratios indicate the effect of DFMO + sulindac compared with placebo (as a referent value) on recurrent colorectal adenomas
* Relative risk estimation by log-binomial regression. Likelihood ratio test p values are reported. Risk ratios indicate risk of metachronous adenoma after treatment with DFMO + sulindac versus placebo (referent group). All risk ratios are adjusted for aspirin intake