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AuthorVidimce, Josif
AuthorPennell, Evan Noel
AuthorFoo, Maxmilian
AuthorShiels, Ryan Graeme
AuthorShibeeb, Sapha
AuthorWatson, Michael
AuthorBulmer, Andrew Cameron
Available date2023-03-27T07:26:46Z
Publication Date2021-10-01
Publication NameClinical Pharmacology in Drug Development
Identifierhttp://dx.doi.org/10.1002/cpdd.962
CitationVidimce, J., Pennell, E.N., Foo, M., Shiels, R.G., Shibeeb, S., Watson, M. and Bulmer, A.C. (2021), Effect of Silymarin Treatment on Circulating Bilirubin and Cardiovascular Disease Risk Factors in Healthy Men: A Single-Blind, Randomized Crossover Trial. Clinical Pharmacology in Drug Development, 10: 1156-1165. https://doi.org/10.1002/cpdd.962
ISSN2160763X
URIhttps://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85109359066&origin=inward
URIhttp://hdl.handle.net/10576/41328
AbstractThis clinical trial (ACTRN12619001296123) investigated the impact of silymarin (Legalon®) on circulating bilirubin concentration, lipid status, systemic inflammation, and antioxidant status. The study design was a randomized, placebo-controlled, single-blind crossover trial of healthy men (18-65 years), conducted at Griffith University, Gold Coast, Australia. Participants were recruited from Griffith University and were randomized to silymarin (140 mg silymarin capsules thrice daily) or placebo (3 capsules containing mannitol taken daily) for 14 days followed by a ≥4-week washout and crossover to the other arm. The main outcomes were whether silymarin treatment would increase serum bilirubin concentration by >0.29 mg/dL, change serum lipid status (cholesterol and triglycerides), inflammation (c-reactive protein), and antioxidant capacity (ferric reducing ability of plasma) compared with baseline. Silymarin consumption (n = 17) did not affect serum concentrations of unconjugated bilirubin (0.73 versus 0.67 mg/dL, P =.79), cholesterol (185 versus 189 mg/dL, P =.19), triglycerides (94.2 versus 92.3 mg/dL, P =.79), c-reactive protein (0.17 versus 0.09 mg/dL, P =.23), or antioxidant status (6.61 versus 6.67 mg Fe2+/dL, P =.40). These findings challenge previous reports and manufacturer claims of hyperbilirubinemia following silymarin treatment and are critical to guiding researchers toward an effective means to mildly elevate bilirubin, which evidence suggests could protect from cardiovascular disease.
SponsorThis work was supported by an Office of Research Project Grant (20160824) provided by the Endeavour College of Natural Health. This work was also supported by the School of Pharmacy and Medical Science, Griffith University.
Languageen
PublisherWiley
Subjectantioxidant
cholesterol
Legalon
silibinin
silymarin
unconjugated bilirubin
TitleEffect of Silymarin Treatment on Circulating Bilirubin and Cardiovascular Disease Risk Factors in Healthy Men: A Single-Blind, Randomized Crossover Trial
TypeArticle
Pagination1156-1165
Issue Number10
Volume Number10
ESSN2160-7648
dc.accessType Abstract Only


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