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邻苯二甲酸二(2-乙基己基)酯(DEHP)在大鼠和狨猴体内的比较药代动力学及亚急性毒性:从啮齿动物效应推断对人类的影响

Comparative pharmacokinetics and subacute toxicity of di(2-ethylhexyl) phthalate (DEHP) in rats and marmosets: extrapolation of effects in rodents to man.

作者信息

Rhodes C, Orton T C, Pratt I S, Batten P L, Bratt H, Jackson S J, Elcombe C R

出版信息

Environ Health Perspect. 1986 Mar;65:299-307. doi: 10.1289/ehp.8665299.

Abstract

Certain phthalate esters and hypolipidemic agents are known to induce morphological and biochemical changes in the liver of rodents, which have been associated with an increased incidence of hepatocellular tumors in these species. There is evidence that hypolipidemic agents do not induce these effects in either subhuman primates or man. The oral and intraperitoneal administration of di(2-ethylhexyl) phthalate (DEHP) to the marmoset monkey at doses up to 5 mmole DEHP/kg body weight/day for 14 days did not induce morphological or biochemical changes in the liver or testis comparable with those obtained in rats given the same amount of DEHP. In the marmoset, the excretion profile of [14C]-DEHP following oral, IP, and IV administration and the lower tissue levels of radioactivity demonstrated a considerably reduced absorption in this species compared to the rat. The urinary metabolite pattern in the marmoset was in many respects qualitatively similar to but quantitatively different from that in the rat; the marmoset excreted principally conjugated metabolites derived from omega- 1 oxidation. The pharmacokinetic differences between these two species indicate that the tissues of the marmoset are exposed to a level of DEHP metabolites equivalent to the complete absorption of a dose of Ca. 0.1 to 0.25 mmole DEHP/kg body weight/day without significant toxicological effects. These exposure levels are at least 100-fold greater than the worst estimates of incidental human exposure (ca. 0.0015 mmole/kg/day). They are comparable with the human therapeutic dose of many hypolipidemic drugs (ca. 0.15 mmole/kg/day), a dose at which it is claimed that there is an absence of morphological or biochemical changes to human or subhuman primate liver.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

已知某些邻苯二甲酸酯和降血脂药物会在啮齿动物肝脏中引起形态学和生化变化,这与这些物种肝细胞肿瘤发病率增加有关。有证据表明,降血脂药物在非人灵长类动物或人类中不会引发这些效应。以高达5毫摩尔二(2-乙基己基)邻苯二甲酸酯(DEHP)/千克体重/天的剂量,对狨猴进行14天的口服和腹腔注射,并未在肝脏或睾丸中引发与给予相同剂量DEHP的大鼠所观察到的类似的形态学或生化变化。在狨猴中,口服、腹腔注射和静脉注射[14C]-DEHP后的排泄情况以及较低的组织放射性水平表明,与大鼠相比,该物种的吸收显著降低。狨猴的尿液代谢物模式在许多方面在质量上与大鼠相似,但在数量上有所不同;狨猴主要排泄源自ω-1氧化的结合代谢物。这两个物种之间的药代动力学差异表明,狨猴组织接触的DEHP代谢物水平相当于每天完全吸收约0.1至0.25毫摩尔DEHP/千克体重,且无明显毒理学效应。这些接触水平比人类偶然接触的最坏估计值(约0.0015毫摩尔/千克/天)至少高100倍。它们与许多降血脂药物的人类治疗剂量(约0.15毫摩尔/千克/天)相当,据称在该剂量下,人类或非人灵长类动物肝脏不存在形态学或生化变化。(摘要截取自250字)

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