Improved resistance to serum oxidation in Gilbert's Syndrome: a mechanism for cardiovascular protection

Article


Bulmer, Andrew C., Blanchfield, Joanne T., Toth, Istvan, Fassett, Robert G. and Coombes, Jeff S.. 2008. "Improved resistance to serum oxidation in Gilbert's Syndrome: a mechanism for cardiovascular protection." Atherosclerosis. 199, pp. 390-396. https://doi.org/10.1016/j.atherosclerosis.2007.11.022
Article Title

Improved resistance to serum oxidation in Gilbert's Syndrome: a mechanism for cardiovascular protection

ERA Journal ID15748
Article CategoryArticle
AuthorsBulmer, Andrew C. (Author), Blanchfield, Joanne T. (Author), Toth, Istvan (Author), Fassett, Robert G. (Author) and Coombes, Jeff S. (Author)
Journal TitleAtherosclerosis
Journal Citation199, pp. 390-396
Number of Pages7
Year2008
Place of PublicationIreland
ISSN0021-9150
1879-1484
Digital Object Identifier (DOI)https://doi.org/10.1016/j.atherosclerosis.2007.11.022
Abstract

Bilirubin is a potent antioxidant, however, uncertainty surrounds its physiological importance. Individuals with Gilbert’s syndrome (GS)have increased circulating bilirubin and a reduced prevalence of cardiovascular disease (CVD). The aim of this study was to investigate mechanisms that may link bilirubin to protection from CVD seen in GS by examining markers of antioxidant and oxidative stress status and the susceptibility of serum to oxidation. Nine individuals with GS and twelve controls, matched for age, height and weight, were assessed for plasma antioxidant status, red blood cell antioxidant enzyme activities, plasma malondialdehyde, the susceptibility of serum to copper (Cu2+) induced oxidation and blood lipid profile. Individuals with GS had significantly elevated unconjugated bilirubin (GS: 26.0±6.4; control: 9.7±3.0!mol/L; P < 0.001), increased trolox equivalent antioxidant capacity (GS: 1.59±0.07; control: 1.52±0.07 mmol/L trolox Equ; P = 0.035) and ferric reducing ability of plasma (GS: 1.09±0.16; control: 0.92±0.14 mmol/L Fe2+ Equ; P = 0.024). The lag phase of serum oxidation was significantly longer in the GS group (GS: 121.4±10.5; control: 106.8±14.6 min; P = 0.020) and was positively correlated with the bilirubin concentration (r = 0.451, P = 0.040). A trend toward elevated HDL:LDL ratio was observed in GS (GS 0.96±0.31; control: 0.73±0.21; P = 0.072). In summary, individuals with GS have an increased circulating antioxidant status and an improved resistance to serum oxidation which may partially explain their reduced prevalence of CVD.

KeywordsCardiovascular disease; Bilirubin; Superoxide; Glutathione; catalase; Trolox equivalent antioxidant capacity; ferric reducing ability of plasma; high and low density lipoprotein cholesterol
ANZSRC Field of Research 2020320199. Cardiovascular medicine and haematology not elsewhere classified
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Byline AffiliationsUniversity of Queensland
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