Toxic Encephalopathy with Hippocampal Lesions

Krinke, G.; Pericin, C.; Thomann, P.; Hess, R.

doi:10.1111/j.1439-0442.1978.tb00928.x

Cited by 10 publications

(1 citation statement)

References 29 publications

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“…Initially we became interested in the administration of CQ in animals that could serve as negative controls in histochemical studies of zinc-containing pathways (Slomianka et al, 1990) as large single doses (up to 400 mg/kg) of CQ did not show overt toxicity in rats (Kotaki et al, 1983). However, our first observations in mice and early literature on experimental findings in mice, dogs and cats, describing overt tonic-clonic seizures or seizure-like behaviors and associated histopathology in the hippocampus (Püschner and Fankhauser, 1969;Tateishi et al, 1973;Lannek and Jonsson, 1974;Krinke et al, 1978), prompted a more thorough reassessment of the effects of CQ in mice and rats. Effects of CQ may not only help to refine ideas on the function of zinc in the normal CNS, but are also of clinical interest.…”

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confidence: 93%

The hippocampal region of rats and mice after a single i.p. dose of clioquinol: Loss of synaptic zinc, cell death and c-Fos induction

2008

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Clioquinol (CQ) is able to chelate synaptic zinc, which can modulate excitatory and inhibitory neurotransmission. In humans, CQ was associated with cases of transient global amnesia (TGA) and with the neurodegenerative syndrome subacute myelo-optico-neuropathy (SMON). We examined the CQ induced loss of synaptic zinc, cell death and c-Fos induction in rats and mice. In rats, we found a strong reduction of histochemically reactive synaptic zinc no later than 4 h after the injection of the lowest dose of CQ (50 mg/kg) and, for all doses used, a return to control levels after 48 h. There was no evidence of cell death for any dose and up to 1 week after CQ injections. Only a slight induction of c-Fos was seen in the hippocampus for the higher doses used (100-200 mg/kg). In mice injected with 100 mg/kg, CQ also resulted in a fast loss of synaptic zinc. c-Fos was induced after 4 h in cell populations of the hippocampal region and other parts of the telencephalon, and substantially increased after 24 h. One day after the injection we found a pattern of cell loss (hilus, parts of CA3, CA1 and layer III of the medial entorhinal cortex) reminiscent of that seen in models of temporal lobe epilepsy. In conjunction with published data on the behavioral effects of zinc chelation and the modulatory effects of zinc in excitatory neurotransmission, our results indicate that the loss of synaptic zinc may have been involved in TGA and the neuropathology associated with SMON.

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Section: Abbreviationsmentioning

confidence: 93%

The hippocampal region of rats and mice after a single i.p. dose of clioquinol: Loss of synaptic zinc, cell death and c-Fos induction

2008

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The neurotoxicity of trimethyltin chloride in hamsters, gerbils and marmosets

Brown

Verschoyle

Street

et al. 1984

J of Applied Toxicology

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Trimethyltin chloride (TMT) was given to Syrian hamsters, gerbils and marmosets, and the changes in the brain were studied 1 day to 7 weeks later by light and electron microscopy. Within the marmoset brain, TMT was found to be uniformly distributed, similar to that in the rat. In all three species, signs of poisoning included whole-body tremors and prostration, while death might occur in 3-4 days; in marmosets ataxia, agitation, aggression and occasional fits were also observed. Bilateral symmetrical neuronal necrosis and chromatolysis were seen in the majority, which involved the hippocampus, pyriform cortex, amygdaloid nucleus, neocortex, various brain stem nuclei and in marmosets the retina. The probably lethal dose of TMT in all three species is approximately 3 mg kg-1, while the LD50 for the rat is 12.6 mg kg-1. The lower figure is probably related to lack of binding to haemoglobin in contrast to the binding in the rat. TMT does not bind to human haemoglobin and thus the predicted lethal dose for humans may be about 3 mg kg-1 (15.1 mumol kg-1), while the dose required to produce neuronal damage could well be less.

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Neurotoxic Effects of Trimethyltin

Krinke¹

1988

Nervous System

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Toxic Encephalopathy with Hippocampal Lesions

Cited by 10 publications

References 29 publications

The hippocampal region of rats and mice after a single i.p. dose of clioquinol: Loss of synaptic zinc, cell death and c-Fos induction

The hippocampal region of rats and mice after a single i.p. dose of clioquinol: Loss of synaptic zinc, cell death and c-Fos induction

The neurotoxicity of trimethyltin chloride in hamsters, gerbils and marmosets

Neurotoxic Effects of Trimethyltin

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