Background
Colon cancer is one of the leading forms of malignancy in the developed countries. Epidemiologic and animal studies have suggested that risk factors for coronary artery disease like insulin resistance and dyslipidemia are probably related to the development of colon cancer
While dietary administration of pan-PPAR ligand bezafibrate has been demonstrated to suppress the development of colonic tumors in rodents
Methods
The major inclusion and exclusion criteria for the BIP study, as well as the ethical guidelines, have been previously reported
There were 3090 patients who were included in the BIP study after screening. Patients in whom a diagnosis of cancer had been made after screening but before the launch of the study medication as well as patients with unknown vital status were excluded from this analysis. Thus, the final study sample for our study comprised 3011 patients.
The patients received either 400 mg of bezafibrate retard or placebo once a day. Patients continued their prescribed medications for cardiac and other conditions except lipid lowering drugs. The primary endpoint of the BIP study was fatal or non-fatal MI or sudden death (combined major cardiovascular events).
Cancer incidence data were obtained by matching a subject's personal identification number (PID) with the Israel National Cancer Registry (INCR). Each matched record was checked for correct identification.
The detailed description of INCR has been published previously
The mean follow-up period of the BIP study was 6.2 ± 0.8, range 4.7 to 7.6 years. The trial was conducted independently of the sponsor (Boehringer Mannheim GmbH, which is now part of F. Hoffmann-La Roche, Ltd), and it was approved by the Helsinki Committees of each center and the central national Helsinki Committee.
Data were analyzed using the SAS software, version 8.2 (SAS Institute Inc., Cary, NC, USA). Continuous variables at baseline were presented as mean values ± standard deviation (SD). Comparisons between groups were made using chi-square tests for discrete variables and Student t-test or Wilcoxon rank sum test for continuous variables. A
Kaplan-Meier curves were produced using the LIFETEST procedure. The log-rank test was used for comparing the curves.
Multivariable analysis of the incidence of colon cancer was performed using the Cox proportional hazard model (PHREG procedure) to account for differing lengths of follow-up and correlation with covariates. Hazard ratio (HR) and 95% confidence interval (CI) for new colon cancer was calculated. Variables included in the models were age, gender, total cholesterol, ln transformed triglycerides, smoking status, study medication and body mass index (BMI).
Results
Baseline data
Our population included 2 groups: 1) Bezafibrate group – 1506 patients; 2) Placebo group – 1505 patients.
Patients in the placebo and bezafibrate groups were well balanced in terms of clinical and laboratory baseline characteristics (Table
Baseline characteristics of the study population.
Bezafibrate (n = 1506)
Placebo (n = 1505)
p value
Age (years)
60.0 ± 6.8
60.0 ± 6.7
0.9
Body mass index (kg/m2)
26.7 ± 3.3
26.7 ± 3.3
0.7
Men (%)
1374(91)
1382 (92)
0.6
Past myocardial infarction (%)
1184 (79)
1163 (77)
0.3
Angina (%)
848 (56)
876 (58)
0.3
NYHA Class ≥2 (%)
45 (27)
47 (26)
0.9
Hypertension (%)
462 (31)
507 (34)
0.1
Current smokers
177 (12)
184 (12)
0.7
Systolic blood pressure (mmHg)
134 ± 18
133 ± 18
0.3
Diastolic blood pressure (mmHg)
81.1 ± 9.0
80.8 ± 9.1
0.4
Heart rate (beats/min)
70.1 ± 9.3
70.0 ± 9.3
0.8
Total cholesterol (mg/dl)
211 ± 17
213 ± 18
0.2
HDL-cholesterol (mg/dl)
34.5 ± 5.5
34.6 ± 5.5
0.7
LDL-cholesterol (mg/dl)
148 ± 16
149 ± 16
0.2
Triglycerides (mg/dl)
145 ± 51
145 ± 51
0.9
Fibrinogen (mg/dl)
350 ± 72
351 ± 74
0.7
Clinical outcomes
During the follow-up period, development of new cancer (all types) was recorded in 177 patients: in 79 (5.25%) patients from the bezafibrate group vs. 98 (6.51%) from the placebo group (p = 0.14). Development of new colon cancer was recorded in 25 patients (Figure
New colon cancers (%) during follow-up; bezafibrate vs. placebo (Fisher's exact test: one side p = 0.05; two side p = 0.07)
New colon cancers (%) during follow-up; bezafibrate vs. placebo (Fisher's exact test: one side p = 0.05; two side p = 0.07).
Kaplan-Meier curves of colon cancer incidence (in accordance with the time of diagnosis) for the two study groups are presented in Figure
Kaplan-Meier curves of colon cancer incidence (in accordance with the time of diagnosis) for the study groups (bezafibrate vs. placebo; 6.2 years mean follow-up, p log-rank = 0.07)
Kaplan-Meier curves of colon cancer incidence (in accordance with the time of diagnosis) for the study groups (bezafibrate vs. placebo; 6.2 years mean follow-up, p log-rank = 0.07).
On multivariable analysis the colon cancer risk in patients received bezafibrate tended to be lower with a hazard ratio of 0.47 and 95% confidence interval 0.2–1.1.
Discussion
The main novel finding in this
Accumulating animal experimental, human laboratory and epidemiologic data
The fact that the incidence of insulin resistance has been increasing in the Western world where colon cancer is the second leading cause of cancer death makes the exploration of the interrelationship of these conditions a subject of high priority for public health.
The biological role of the peroxisome proliferator-activated receptors (PPARs) in various diseases, including inflammation and cancer, has been highlighted recently
The fibric acid derivative bezafibrate is the pan – (alpha, beta/delta, gamma) PPAR activator with predominantly PPAR alpha (as all fibrates) and beta/delta effects but also with perceptible PPAR gamma properties
Limitations of the study
Although development of new colon cancer in patients randomized to bezafibrate was more than half as frequent as in those randomized to placebo, the difference reached only borderline statistical significance. The BIP study was designed (both in terms of sample size and time of follow-up) to detect the effect of the lipid-modifying agent bezafibrate on major cardiovascular events in coronary patients at high risk, but had not an appropriate statistical power to explore development of such a relatively low-incidence disease as colon cancer. In addition, caution should be used in interpreting our findings, as they were identified in post-hoc analysis.
However, the detected pattern of the time course in the differences between groups, suggesting a biologically meaningful effect, is encouraging and supports the initiation of a large prospective controlled trial in light of its importance for public health.
Conclusion
The use of bezafibrate as lipid-modifying agent in patients with coronary artery disease appears to be associated with a reduced risk of colon cancer.
Competing interests
The authors declare that they have no competing interests.
Authors' contributions
AT conceived the study and drafted the manuscript, EZF, YA and SB were involved in the study design, coordination and data acquisition, AT, VB and SB studied and matched the records from the Cancer Registry, EZF, IG, ES, JS and MSF interpreted the results and VB performed the statistical analysis of the data presented, EZF, DT, SB, ES, MSF and MM critically reviewed the study for important intellectual content. All authors approved the final version of the manuscript.