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Down-regulation of the hepatic cytochrome P450 by an acute inflammatory reaction: implication of mediators in human and animal serum and in the liver

机译:急性炎症反应下调肝细胞色素P450的作用:人和动物血清以及肝脏中介质的影响

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摘要

Infection and inflammation trigger a cascade of mediators that eventually will down-regulate the hepatic cytochrome P450 (P450). The present study aimed to characterize the mediators contained in the serum of rabbits with an acute inflammatory reaction (AIR) induced by the s.c. injection of turpentine (5 ml), and in the serum of humans with an acute upper respiratory tract viral infection.Hepatocytes from control (HCONT) rabbits and rabbits with an AIR (HINFLA) were isolated and cultured. Compared with HCONT in HINFLA the production of theophylline metabolites, 3-methylxanthine (3MX), 1-methyluric acid (1MU), and 1,3-dimethyluric acid (1,3DMU) was reduced as was the amount of total P450, while lipid peroxidation was increased. Incubation of HINFLA with serum of rabbits with an AIR (RSINFLA) for 4 h further reduced the formation of the metabolites of theophylline as well as the amount of P450, and enhanced the lipid peroxidation. RSINFLA obtained 6, 12 and 24 h after the injection of turpentine showed the same ability to down-regulate hepatic P450 as the serum obtained at 48 h.The efficacy (Emax) of RSINFLA to inhibit the formation of theophylline metabolites differed, i.e. 1,3DMU>1MU>3MX, and the potency of serum mediators (IC50) was similar for 3MX and 1MU, but lower for 1,3DMU.Incubation of serum of human volunteers (HSINFLA) with a viral infection with HCONT or HINFLA reduced the production of theophylline metabolites, as well as the amount of P450, and increased the lipid peroxidation. HSINFLA depressed 1,3DMU more efficiently than 3MX and 1MU. HSINFLA reduced 3MX with greater efficacy than did RSINFLA. Potency was very variable but not different from rabbits.It is concluded that the serum of rabbits with an AIR or of humans with a viral infection contain several mediators that inhibit noncompetitively various isoenzymes of the hepatic P450. The decrease in P450 induced by HSINFLA or RSINFLA is closely associated with the increase in lipid peroxidation (r2= 0.8870) suggesting that lipid peroxidation could directly or indirectly be involved in the P450 down-regulation.
机译:感染和炎症会触发一系列的介质,最终会下调肝细胞色素P450(P450)。本研究旨在表征由兔皮疹引起的急性炎症反应(AIR)的兔血清中所含的介质。注射松节油(5 ml),并在患有急性上呼吸道病毒感染的人的血清中。分离并培养对照(HCONT)兔和AIR(HINFLA)兔的肝细胞。与HINFLA中的HCONT相比,茶碱代谢产物,3-甲基黄嘌呤(3MX),1-甲基尿酸(1MU)和1,3-二甲基尿酸(1,3DMU)的生成减少了,而总P450的数量减少了,而脂质过氧化增加。用AIR(RSINFLA)在兔子的血清中孵育HINFLA 4小时,可进一步减少茶碱代谢产物的形成以及P450的含量,并增强脂质过氧化作用。松节油注射后6、12和24 h获得的RSINFLA具有与48 h获得的血清相同的下调肝P450的能力.RSINFLA抑制茶碱代谢物形成的功效(Emax)不同,即1, 3DMU> 1MU> 3MX,并且3MX和1MU的血清介体效能(IC50)相似,但1,3DMU较低。茶碱代谢产物以及P450的量增加了脂质的过氧化作用。 HSINFLA比3MX和1MU更有效地抑制了1,3DMU。与RSINFLA相比,HSINFLA降低了3MX的疗效。效力变化很大,但与兔子无异。结论是,患有AIR的兔子或患有病毒感染的人的血清含有几种介体,这些介体可以非竞争性地抑制肝P450的各种同工酶。 HSINFLA或RSINFLA诱导的P450的降低与脂质过氧化的增加密切相关(r2 = 0.8870),表明脂质过氧化可以直接或间接参与P450的下调。

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