The ruthenium-based compound imidazolium trans-imidazoledimethylsulfoxide-tetrachlororuthenate (NAMI-A) is free of cytotoxicity up to 1. mM concentration after 1. h in vitro exposure of the LLC-PK1 renal tubule cells. In vivo, one cycle of i.p. administrations of 35. mg/kg/day NAMI-A (1. cycle. =. 6 consecutive days), is free of a measurable toxicity on mouse kidneys. After two cycles with a one-week drug-free washout between cycles, mitochondrial membrane potential of the renal cells drops by 37% (p<. 0.05), serum creatinine increases by 30% (p<. 0.05) and a significant decrease of body weight of 12% (p<. 0.05) occurs. These parameters return to normal within 7. days after the end of treatment. A cycle-dependent alteration of glomeruli and a diffused swelling of renal tubules are also evident leading to a significant alteration of these structures after the third cycle. These effects are completely prevented if a 2-week drug free washout is used between two consecutive cycles. These data support the toxic accumulation of NAMI-A or of its products of transformation in the kidneys and stress the need of at least 14. days washout between two treatment cycles when the drug is given daily for 6 consecutive days.

Features and full reversibility of the renal toxicity of the ruthenium-based drug NAMI-A in mice

PACOR, SABRINA;VITA, FRANCESCA;ZORZET, SONIA;SAVA, GIANNI
2013-01-01

Abstract

The ruthenium-based compound imidazolium trans-imidazoledimethylsulfoxide-tetrachlororuthenate (NAMI-A) is free of cytotoxicity up to 1. mM concentration after 1. h in vitro exposure of the LLC-PK1 renal tubule cells. In vivo, one cycle of i.p. administrations of 35. mg/kg/day NAMI-A (1. cycle. =. 6 consecutive days), is free of a measurable toxicity on mouse kidneys. After two cycles with a one-week drug-free washout between cycles, mitochondrial membrane potential of the renal cells drops by 37% (p<. 0.05), serum creatinine increases by 30% (p<. 0.05) and a significant decrease of body weight of 12% (p<. 0.05) occurs. These parameters return to normal within 7. days after the end of treatment. A cycle-dependent alteration of glomeruli and a diffused swelling of renal tubules are also evident leading to a significant alteration of these structures after the third cycle. These effects are completely prevented if a 2-week drug free washout is used between two consecutive cycles. These data support the toxic accumulation of NAMI-A or of its products of transformation in the kidneys and stress the need of at least 14. days washout between two treatment cycles when the drug is given daily for 6 consecutive days.
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11368/2635871
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