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白三烯D4拮抗剂RG 12525的亚慢性毒性研究。

Subchronic toxicity studies with the leukotriene D4 antagonist RG 12525.

作者信息

Bonnefoi M S, Kelley M F, Wells R E, Sanders J E, Jayyosi Z, Beys E, Kornbrust D J, Langloss J M

机构信息

Rhône-Poulenc Rorer Central Research, Drug Safety Division, Collegeville, Pennsylvania 19426-0107, USA.

出版信息

Fundam Appl Toxicol. 1995 Nov;28(1):129-38. doi: 10.1006/faat.1995.1154.

DOI:10.1006/faat.1995.1154
PMID:8566477
Abstract

Preclinical safety studies with the leukotriene D4 antagonist RG 12525 were conducted by the oral route in mice, rats, and monkeys. Oral administration of RG 12525 was repeated daily in studies up to 6 months in duration. RG 12525 was shown to have limited high-dose toxicity after repeated oral administration. The effects of RG 12525 were strongly dependent upon the species considered. High doses of RG 12525 caused significant increases in liver weight in mice, rats, and monkeys that were associated with diffuse hepatocellular hypertrophy in mice and rats but not in monkeys. No related clinical chemistry changes were observed in any of the species and hepatic activities of peroxisomal enzymes or cytochrome P450 were increased only slightly. Proliferation of brown adipose tissue (BAT) was observed in rats and mice but not in monkeys. The BAT reaction was more pronounced in the interscapular area but it was also observed in other subcutaneous locations as well as in mediastinal and bone marrow fat. In all locations, the RG 12525-induced BAT had some morphological similarities with cold-adapted BAT. Repeated administration of RG 12525 at high doses to female rats resulted in a lack of progression to the luteal phase of the estrous cycle that was reversible after discontinuation of treatment. Finally, RG 12525 was nephrotoxic in mice with males being more sensitive than females.

摘要

对白三烯D4拮抗剂RG 12525进行了临床前安全性研究,研究通过口服途径在小鼠、大鼠和猴子身上开展。在长达6个月的研究中,每日重复口服RG 12525。结果显示,重复口服给药后,RG 12525的高剂量毒性有限。RG 12525的作用在很大程度上取决于所研究的物种。高剂量的RG 12525会使小鼠、大鼠和猴子的肝脏重量显著增加,这与小鼠和大鼠的弥漫性肝细胞肥大有关,但猴子未出现这种情况。在任何物种中均未观察到相关的临床化学变化,过氧化物酶体酶或细胞色素P450的肝脏活性仅略有增加。在大鼠和小鼠中观察到棕色脂肪组织(BAT)增生,但猴子未出现。BAT反应在肩胛间区域更为明显,但在其他皮下部位以及纵隔和骨髓脂肪中也有观察到。在所有部位,RG 12525诱导产生的BAT在形态上与适应寒冷的BAT有一些相似之处。对雌性大鼠高剂量重复给药RG 12525会导致发情周期黄体期无法推进,停药后这种情况可逆转。最后,RG 12525对小鼠具有肾毒性,雄性比雌性更敏感。

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