髓过氧化物酶
主动脉
化学
超氧化物
胆固醇
吲哚美辛
内科学
内分泌学
过氧化物酶
生物化学
炎症
药理学
环氧合酶
医学
酶
前列腺素内过氧化物合酶
作者
Gábor Békési,H. Heinle,Réka Kakucs,Tamás Pázmány,D Szombath,Mariann Dinya,Zsolt Tulassay,János Fehér,Kàroly Rácz,Béla Székács,Éva Riss,A. Farkas,Ferenc Gódor,G. Illyés
标识
DOI:10.1016/j.exger.2004.12.004
摘要
Our earlier studies have shown that some steroids increase myeloperoxidase enzyme (MPO) release from human granulocytes, and that MPO plasma levels are significantly lower in postclimacteric people. Moreover, we have proven that MPO inhibits production of atherogenic free radical superoxide anion and MPO-inhibitors increase superoxide release. The aim of the present study was to investigate the effect of MPO-inhibitors on the early phase of aortic atherosclerosis, namely the extent of intimal plaques and the thickening of the medial layer. Adult male rabbits were fed with lipid rich food (cholesterol: 1.3%, peanut oil: 8%) for 8 weeks. During this period MPO-inhibitors were also given (4-aminobenzoicacid-hydrazide/ABAH/-13.3 mg/kg/day or indometacin-5 mg/kg/day). All animals developed intimal lipid plaques (raised fatty streaks). The relative plaque-covered areas of the aortas were compared and the media thickness of the aorta was measured on plaque-free as well as plaque-containing areas. The medial smooth muscle density and peroxidase activity of the aortic media were also determined. The media thickness increased (p<0.05) in the cholesterol+ABAH as well as in the cholesterol+indometacin groups up to 375.7 (±60.5) and 442.5 (±123.4) μm, respectively, compared to the control group (cholesterol feeding alone) where it measured only 308.4 (±51.67) μm. The medial peroxidase activity decreased significantly in the indometacin treated group and showed a decreasing tendency using ABAH. In parallel to this there was a tendency of increase in the relative plaque covered areas. The smooth muscle density showed no significant modifications, while inhibitors of the MPO seemed to enhance aortic medial thickness, i.e. the grade of a pre-atherosclerotic lesion, in our animal model. Collectively, the anti-atherogenic effect of certain steroid hormones might be realized through the impact on MPO activity.
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