A randomized trial of lycopene supplementation in Tobago men with high prostate cancer risk

Clareann H. Bunker; Alicia C. McDonald; Rhobert W. Evans; Noreen De La Rosa; Jocelyne Matar Boumosleh; Alan L. Patrick

doi:10.1080/01635580701274046

A randomized trial of lycopene supplementation in Tobago men with high prostate cancer risk

Clareann H. Bunker, Alicia C. McDonald, Rhobert W. Evans, Noreen De La Rosa, Jocelyne Matar Boumosleh, Alan L. Patrick

Research output: Contribution to journal › Article › peer-review

58 Scopus citations

Abstract

This unblinded, randomized, Phase I clinical trial was conducted to determine whether lycopene supplementation lowered serum prostate specific antigen (PSA), surrogate endpoint for prostate cancer initiation or progression, in men with elevated prostate cancer risk. Afro-Caribbean men (n = 81) with high-grade prostatic intraepithelial neoplasia, atypical foci or repeated non-cancerous biopsies, ascertained in a population-based screening program, were randomized to four months intervention with 30 mg/day lycopene (Lyc-O-Mato®) plus a multivitamin, or to multivitamin, only. Serum PSA and lycopene were compared at randomization, 1, and 4 mo using two-sided χ² and t-tests for independent samples. Treatment groups were similar at baseline. Serum lycopene levels approximately doubled in the lycopene intervention group. Serum PSA declined during the first month of treatment, but returned to randomization level by month 4. The PSA response was nearly identical in both treatment groups. No adverse effects attributed to lycopene supplementation were documented. We conclude that the PSA lowering response to antioxidant supplementation observed in previous 3-wk studies in men awaiting prostatectomy may have been a transient response, perhaps not specific to lycopene. Lowering of serum PSA may not be an appropriate endpoint for the long-term studies needed to evaluate lycopene supplementation for reducing prostate cancer initiation or progression.

Original language	English (US)
Pages (from-to)	130-137
Number of pages	8
Journal	Nutrition and cancer
Volume	57
Issue number	2
DOIs	https://doi.org/10.1080/01635580701274046
State	Published - 2007

All Science Journal Classification (ASJC) codes

Medicine (miscellaneous)
Oncology
Nutrition and Dietetics
Cancer Research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1080/01635580701274046

Cite this

@article{c5ada5aed24d4e378c80ae189bde59c4,

title = "A randomized trial of lycopene supplementation in Tobago men with high prostate cancer risk",

abstract = "This unblinded, randomized, Phase I clinical trial was conducted to determine whether lycopene supplementation lowered serum prostate specific antigen (PSA), surrogate endpoint for prostate cancer initiation or progression, in men with elevated prostate cancer risk. Afro-Caribbean men (n = 81) with high-grade prostatic intraepithelial neoplasia, atypical foci or repeated non-cancerous biopsies, ascertained in a population-based screening program, were randomized to four months intervention with 30 mg/day lycopene (Lyc-O-Mato{\textregistered}) plus a multivitamin, or to multivitamin, only. Serum PSA and lycopene were compared at randomization, 1, and 4 mo using two-sided χ2 and t-tests for independent samples. Treatment groups were similar at baseline. Serum lycopene levels approximately doubled in the lycopene intervention group. Serum PSA declined during the first month of treatment, but returned to randomization level by month 4. The PSA response was nearly identical in both treatment groups. No adverse effects attributed to lycopene supplementation were documented. We conclude that the PSA lowering response to antioxidant supplementation observed in previous 3-wk studies in men awaiting prostatectomy may have been a transient response, perhaps not specific to lycopene. Lowering of serum PSA may not be an appropriate endpoint for the long-term studies needed to evaluate lycopene supplementation for reducing prostate cancer initiation or progression.",

author = "Bunker, {Clareann H.} and McDonald, {Alicia C.} and Evans, {Rhobert W.} and {De La Rosa}, Noreen and Boumosleh, {Jocelyne Matar} and Patrick, {Alan L.}",

note = "Funding Information: This study was supported by funding or in-kind services from the Division of Health and Social Services, Tobago House of Assembly, the University of Pittsburgh Cancer Institute, contract DAMD 17-99-1-9015, U.S. Department of Defense, and grants R01 CA84950, R01 CA84950S1, U.S. National Cancer Institute. The Lyc-O-Mato{\textcopyright}R capsules were donated by Healthy Origins, Pittsburgh, PA. Address correspondence to Clareann H. Bunker, Department of Epidemiology, Graduate School of Public Health, University of Pittsburgh, A542 Crabtree Hall, 130 DeSoto Street, Pittsburgh PA 15261. Phone: 412 624-3467; FAX: 412 624-7397. E-mail: [email protected]",

year = "2007",

doi = "10.1080/01635580701274046",

language = "English (US)",

volume = "57",

pages = "130--137",

journal = "Nutrition and cancer",

issn = "0163-5581",

publisher = "Taylor and Francis Ltd.",

number = "2",

}

TY - JOUR

T1 - A randomized trial of lycopene supplementation in Tobago men with high prostate cancer risk

AU - Bunker, Clareann H.

AU - McDonald, Alicia C.

AU - Evans, Rhobert W.

AU - De La Rosa, Noreen

AU - Boumosleh, Jocelyne Matar

AU - Patrick, Alan L.

N1 - Funding Information: This study was supported by funding or in-kind services from the Division of Health and Social Services, Tobago House of Assembly, the University of Pittsburgh Cancer Institute, contract DAMD 17-99-1-9015, U.S. Department of Defense, and grants R01 CA84950, R01 CA84950S1, U.S. National Cancer Institute. The Lyc-O-Mato©R capsules were donated by Healthy Origins, Pittsburgh, PA. Address correspondence to Clareann H. Bunker, Department of Epidemiology, Graduate School of Public Health, University of Pittsburgh, A542 Crabtree Hall, 130 DeSoto Street, Pittsburgh PA 15261. Phone: 412 624-3467; FAX: 412 624-7397. E-mail: [email protected]

PY - 2007

Y1 - 2007

N2 - This unblinded, randomized, Phase I clinical trial was conducted to determine whether lycopene supplementation lowered serum prostate specific antigen (PSA), surrogate endpoint for prostate cancer initiation or progression, in men with elevated prostate cancer risk. Afro-Caribbean men (n = 81) with high-grade prostatic intraepithelial neoplasia, atypical foci or repeated non-cancerous biopsies, ascertained in a population-based screening program, were randomized to four months intervention with 30 mg/day lycopene (Lyc-O-Mato®) plus a multivitamin, or to multivitamin, only. Serum PSA and lycopene were compared at randomization, 1, and 4 mo using two-sided χ2 and t-tests for independent samples. Treatment groups were similar at baseline. Serum lycopene levels approximately doubled in the lycopene intervention group. Serum PSA declined during the first month of treatment, but returned to randomization level by month 4. The PSA response was nearly identical in both treatment groups. No adverse effects attributed to lycopene supplementation were documented. We conclude that the PSA lowering response to antioxidant supplementation observed in previous 3-wk studies in men awaiting prostatectomy may have been a transient response, perhaps not specific to lycopene. Lowering of serum PSA may not be an appropriate endpoint for the long-term studies needed to evaluate lycopene supplementation for reducing prostate cancer initiation or progression.

AB - This unblinded, randomized, Phase I clinical trial was conducted to determine whether lycopene supplementation lowered serum prostate specific antigen (PSA), surrogate endpoint for prostate cancer initiation or progression, in men with elevated prostate cancer risk. Afro-Caribbean men (n = 81) with high-grade prostatic intraepithelial neoplasia, atypical foci or repeated non-cancerous biopsies, ascertained in a population-based screening program, were randomized to four months intervention with 30 mg/day lycopene (Lyc-O-Mato®) plus a multivitamin, or to multivitamin, only. Serum PSA and lycopene were compared at randomization, 1, and 4 mo using two-sided χ2 and t-tests for independent samples. Treatment groups were similar at baseline. Serum lycopene levels approximately doubled in the lycopene intervention group. Serum PSA declined during the first month of treatment, but returned to randomization level by month 4. The PSA response was nearly identical in both treatment groups. No adverse effects attributed to lycopene supplementation were documented. We conclude that the PSA lowering response to antioxidant supplementation observed in previous 3-wk studies in men awaiting prostatectomy may have been a transient response, perhaps not specific to lycopene. Lowering of serum PSA may not be an appropriate endpoint for the long-term studies needed to evaluate lycopene supplementation for reducing prostate cancer initiation or progression.

UR - http://www.scopus.com/inward/record.url?scp=34447536840&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=34447536840&partnerID=8YFLogxK

U2 - 10.1080/01635580701274046

DO - 10.1080/01635580701274046

M3 - Article

C2 - 17571945

AN - SCOPUS:34447536840

SN - 0163-5581

VL - 57

SP - 130

EP - 137

JO - Nutrition and cancer

JF - Nutrition and cancer

IS - 2

ER -

A randomized trial of lycopene supplementation in Tobago men with high prostate cancer risk

Abstract

All Science Journal Classification (ASJC) codes

UN SDGs

Access to Document

Other files and links

Fingerprint

Cite this