| Literature DB >> 25677510 |
Laura Vicente-Vicente1, Fernando Sánchez-Juanes2, Omar García-Sánchez3, Víctor Blanco-Gozalo4, Moisés Pescador3, María A Sevilla3, José Manuel González-Buitrago5, Francisco J López-Hernández6, José Miguel López-Novoa1, Ana Isabel Morales7.
Abstract
Nephrotoxicity limits the therapeutic efficacy of the antineoplastic drug cisplatin. Due to dosage adjustment and appropriate monitoring, most therapeutic courses with cisplatin produce no or minimal kidney damage. However, we studied whether even sub-nephrotoxic dosage of cisplatin poses a potential risk for the kidneys by predisposing to acute kidney injury (AKI), specifically by lowering the toxicity threshold for a second nephrotoxin. With this purpose rats were treated with a single sub-nephrotoxic dosage of cisplatin (3mg/kg, i.p.) and after two days, with a sub-nephrotoxic regime of gentamicin (50mg/kg/day, during 6 days, i.p.). Control groups received only one of the drugs or the vehicle. Renal function and renal histology were monitored throughout the experiment. Cisplatin treatment did not cause any relevant functional or histological alterations in the kidneys. Rats treated with cisplatin and gentamicin, but not those under single treatments, developed an overt renal failure characterized by both renal dysfunction and massive tubular necrosis. In addition, the urinary excretion of fumarylacetoacetase was increased in cisplatin-treated animals at subtoxic doses, which might be exploited as a cisplatin-induced predisposition marker. In fact, the urinary level of fumarylacetoacetase prior to the second nephrotoxin correlated with the level of AKI triggered by gentamicin in predisposed animals.Entities:
Keywords: Acquired predisposition; Acute kidney injury; Cisplatin; Fumarylacetoacetase; Urinary biomarkers
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Year: 2015 PMID: 25677510 DOI: 10.1016/j.toxlet.2014.11.033
Source DB: PubMed Journal: Toxicol Lett ISSN: 0378-4274 Impact factor: 4.372