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血小板活化因子拮抗剂BN52021对家兔的影响:在庆大霉素肾毒性中的作用

Effect of the platelet activating factor antagonist BN52021 in rabbits: role in gentamicin nephrotoxicity.

作者信息

Hanslik T, Blanchet F, Nochy D, Pirotzky E, Guilmard C, Seta N, Carbon C

机构信息

INSERM U13, CHU Bichat, Paris, France.

出版信息

Toxicol Appl Pharmacol. 1994 Sep;128(1):111-5. doi: 10.1006/taap.1994.1187.

Abstract

Platelet activating factor (PAF) is an ubiquitous phospholipid that acts as a mediator of numerous pathophysiological conditions, including drug nephrotoxicity. Aminoglycosides are potent antibiotics but their use is limited by their nephrotoxic potential. We assumed that PAF could participate in inducing gentamicin nephrotoxicity, and we used the PAF antagonist BN52021 to test this hypothesis. We studied renal glomerular and tubular function by clearance techniques and renal histology in four groups of New Zealand male rabbits treated for 7 days with isotonic saline, BN52021, gentamicin, or gentamicin + BN52021. BN52021 alone reduced only fractional excretions (FE) of sodium and chloride, without modifying the other parameters studied. Renal histology was not altered. Gentamicin reduced glomerular filtration rate and renal plasma flow. Free water clearance was not modified. Sodium, potassium, chloride, calcium, and magnesium FEs were raised. Renal histology showed a massive and diffuse tubular necrosis. BN52021 did not modify gentamicin glomerular, tubular, or histopathological alterations. These data suggest that PAF might physiologically affect tubular function in New Zealand male rabbits, increasing sodium and chloride excretions, and in a minute manner, potassium, calcium, and magnesium excretions. Under our experimental conditions, there was no evidence for a role of PAF in gentamicin nephrotoxicity.

摘要

血小板活化因子(PAF)是一种普遍存在的磷脂,在包括药物肾毒性在内的多种病理生理状况中作为介质发挥作用。氨基糖苷类是强效抗生素,但其使用因具有肾毒性潜力而受到限制。我们推测PAF可能参与诱导庆大霉素肾毒性,于是使用PAF拮抗剂BN52021来验证这一假设。我们采用清除技术和肾脏组织学方法,对四组用等渗盐水、BN52021、庆大霉素或庆大霉素+BN52021处理7天的新西兰雄性兔的肾小球和肾小管功能进行了研究。单独使用BN52021仅降低了钠和氯的分数排泄(FE),而未改变所研究的其他参数。肾脏组织学未发生改变。庆大霉素降低了肾小球滤过率和肾血浆流量。自由水清除率未改变。钠、钾、氯、钙和镁的FE升高。肾脏组织学显示大量弥漫性肾小管坏死。BN52021未改变庆大霉素的肾小球、肾小管或组织病理学改变。这些数据表明,PAF可能在生理上影响新西兰雄性兔的肾小管功能,增加钠和氯的排泄,并轻微增加钾、钙和镁的排泄。在我们的实验条件下,没有证据表明PAF在庆大霉素肾毒性中起作用。

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