Abstract

Beta-carotene (BC), which is present in many fruits and vegetables, and is relatively non-toxic, has been identified as an important chemotherapeutic agent to reduce the risk of epithelial cancer, including cancer of the colon. The hypothesis of the present study is that BC, at appropriate tissue levels, affects the rate of colonic cell proliferation (CCP), as evaluated by specific biochemical and/or histological markers. Our preliminary data have shown that chronic BC intake significantly reduces ornithine decarboxylase (ODC) activity in colonic epithelium of patients with colon cancer. We have also observed a decrease in serum lipid peroxide levels in normal young subjects upon supplementation with 15 mg BC per day. In the present study we will determine whether BC supplementation affects biochemical and histological indices of CCP such as urinary polyamines, cell cycle kinetics (measured by monoclonal antibody Ki-67) and the sialic acid free dissacharide residue, beta-D-Gal(1-3)-D-GalNAc. A total of 100 subjects (45-75 years old) will participate in the first phase of this study. They will include 20 normal subjects and two groups of 40 patients, including one group with colon cancer and another group with adenomatous colonic polyps, a precancerous condition. Initially we will determine the nutritional status and BC nutriture of all the groups and will assay indices of CCP. Subsequently, patients will be randomized into BC (30 mg/day) or placebo treatment groups and will be followed monthly. At 3 months the subjects will be evaluated again for BC status and indices of CCP. Patients on BC in whom ODC activity will be normalized will be asked to stop taking the supplement and will be followed for 3 more months. The patients in whom colonic ODC activity has not responded to BC supplementation will be entered into the second phase of the study and receive a maximal dose of 180 mg BC per day for 3 months. By providing detailed information on BC serum and tissue levels along with biochemical indices of CCP in 3 different groups, these studies will enable us to assess the appropriateness of certain intermediate endpoints in chemopreventive trials and may help establish target tissue levels for a potential therapeutic agent (BC).

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project--Cooperative Agreements (U01)
Project #
5U01CA053799-03
Application #
3549719
Study Section
Special Emphasis Panel (SRC (42))
Project Start
1991-03-01
Project End
1995-01-31
Budget Start
1993-02-01
Budget End
1994-01-31
Support Year
3
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
Loyola University Chicago
Department
Type
Schools of Medicine
DUNS #
791277940
City
Maywood
State
IL
Country
United States
Zip Code
60153

  Publications

Kazi, N; Radvany, R; Oldham, T et al. (1997) Immunomodulatory effect of beta-carotene on T lymphocyte subsets in patients with resected colonic polyps and cancer. Nutr Cancer 28:140-5
Iftikhar, S; Lietz, H; Mobarhan, S et al. (1996) In vitro beta-carotene toxicity for human colon cancer cells. Nutr Cancer 25:221-30
Maiani, G; Pappalardo, G; Ferro-Luzzi, A et al. (1995) Accumulation of beta-carotene in normal colorectal mucosa and colonic neoplastic lesions in humans. Nutr Cancer 24:23-31
Frommel, T O; Mobarhan, S; Doria, M et al. (1995) Effect of beta-carotene supplementation on indices of colonic cell proliferation. J Natl Cancer Inst 87:1781-7
Tang, G; Shiau, A; Russell, R M et al. (1995) Serum retinoic acid levels in patients with resected benign and malignant colonic neoplasias on beta-carotene supplementation. Nutr Cancer 23:291-8
Frommel, T O; Lietz, H; Mobarhan, S (1994) Expression of mRNA for the gap-junctional protein connexin43 in human colonic tissue is variable in response to beta-carotene supplementation. Nutr Cancer 22:257-65
Mobarhan, S; Shiau, A; Grande, A et al. (1994) beta-Carotene supplementation results in an increased serum and colonic mucosal concentration of beta-carotene and a decrease in alpha-tocopherol concentration in patients with colonic neoplasia. Cancer Epidemiol Biomarkers Prev 3:501-5
Keshavarzian, A; Olyaee, M; Sontag, S et al. (1993) Increased levels of luminol-enhanced chemiluminescence by rectal mucosa of patients with colonic neoplasia: a possible marker for colonic neoplasia. Nutr Cancer 19:201-6
Keshavarzian, A; Zapeda, D; List, T et al. (1992) High levels of reactive oxygen metabolites in colon cancer tissue: analysis by chemiluminescence probe. Nutr Cancer 17:243-9