Evaluation of the potential genotoxicity of the phosphate binder lanthanum carbonate

doi:10.1093/mutage/gei003

Mutagenesis Advance Access originally published online on December 29, 2004
Mutagenesis 2005 20(1):29-37; doi:10.1093/mutage/gei003

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Evaluation of the potential genotoxicity of the phosphate binder lanthanum carbonate

S.J.P. Damment^*, C. Beevers¹ and D.G. Gatehouse¹

Biosciences, Shire Pharmaceutical Development Ltd, Chineham, Basingstoke, UK and ¹Covance Laboratories Ltd, Harrogate, North Yorkshire, UK

Lanthanum was evaluated for potential genotoxicity using a rangeof in vitro assays (as the carbonate) in the presence and absenceof post-mitochondrial fraction (S9) and in vivo in three independenttests for mutagenicity and clastogenicity (as the carbonateand chloride). The drug was devoid of mutagenic activity inbacterial assays (maximum concentration 5000 µg/plate)using a range of test strains (Salmonella typhimurium TA1535,TA1537, TA1538, TA98, TA100 and TA102 and Escherichia coli WP2uvrA and WP2 uvrA pkm101). No effects were seen in the hgprtgene mutation assay in Chinese hamster ovary cells in the presenceof S9. In the absence of S9, sporadic increases in revertantnumbers were not dose-related or reproducible in subsequentexperiments and hence were concluded to be chance events. Inan in vitro chromosome aberration assay using Chinese hamsterovary cells, chromosome damage in the presence and absence ofS9 (concentration 200–5000 µg/ml) was attributedto overt cell toxicity. To confirm this, a comprehensive invivo evaluation of the drug was performed. Negative resultswere obtained in two independent rodent micronucleus tests.In the first mice were given oral doses (of carbonate) up to2000 mg/kg, in the second rats were given a single i.v. bolusinjection (of chloride) up to 0.1 mg/kg. Negative results werealso obtained in a rat liver unscheduled DNA synthesis assayafter treatment for 28 days with i.v. bolus injections (of chloride)up to 0.1 mg/kg/day. In these in vivo studies lanthanum plasmaconcentrations were >3000 times higher than the steady-statepeak plasma concentration observed in dialysis patients giventherapeutic doses of lanthanum carbonate. It can be concludedthat lanthanum is not genotoxic and that lanthanum carbonateis unlikely to present a latent hazard in therapeutic use.

^* To whom correspondence should be addressed. Tel: +44 1256 894194; Fax: +44 1256 894703; Email: sdamment{at}uk.shire.com

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