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AuthorMustafa A.G.
AuthorAlfaqih M.A.
AuthorAl-Shboul O.
Available date2020-03-03T06:19:34Z
Publication Date2018
Publication NameExperimental and Therapeutic Medicine
ResourceScopus
ISSN17920981
URIhttp://dx.doi.org/10.3892/etm.2018.6419
URIhttp://hdl.handle.net/10576/13181
AbstractLipid peroxidation is associated with several metabolic diseases. Lipid peroxidation causes cellular damage through reactive aldehyde species such as 4-hydroxyonenal (4-HNE). The exact mechanism(s) by which 4-HNE causes damage in the intravascular compartment is not yet exactly understood. Using an in vitro system, the damage induced by 4-HNE on the blood was investigated by measuring protein carbonyl groups and thiobarbituric acid reactive substances (TBARS) following 4-HNE treatment. The findings demonstrated that treatment with 4-HNE increased the carbonylation of protein and the formation of TBARS in the blood plasma. It was also tested whether phenelzine, a scavenger of aldehyde species, or U-83836E, a scavenger of lipid peroxy radicals, attenuated the damage caused by 4-HNE. It was demonstrated that phenelzine or U-83836E both mitigated the effects of 4-HNE on the proteins and the lipids of the blood plasma. The findings of the current study suggest that phenelzine, U-83836E or functionally similar therapeutics may prevent or treat diseases that involve an increased production of 4-HNE in the intravascular compartment.
SponsorThe present study was supported by the Deanship of Research at Jordan University of Science and Technology (grant no. 301/2014).
Languageen
PublisherSpandidos Publications
SubjectLipid peroxidation
Oxidative stress
Phenelzine
Reactive oxygen species
Thiobarbituric acid reactive substances
TitleThe 4-hydroxynonenal mediated oxidative damage of blood proteins and lipids involves secondary lipid peroxidation reactions
TypeArticle
Pagination2132 - 2137
Issue Number3
Volume Number16


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