Abstract
Epsilon toxin (ET) produced by C. perfringens types B and D is a highly potent pore-forming toxin. ET-intoxicated animals express severe neurological disorders that are thought to result from the formation of vasogenic brain edemas and indirect neuronal excitotoxicity. The cerebellum is a predilection site for ET damage. ET has been proposed to bind to glial cells such as astrocytes and oligodendrocytes. However, the possibility that ET binds and attacks the neurons remains an open question. Using specific anti-ET mouse polyclonal antibodies and mouse brain slices preincubated with ET, we found that several brain structures were labeled, the cerebellum being a prominent one. In cerebellar slices, we analyzed the co-staining of ET with specific cell markers, and found that ET binds to the cell body of granule cells, oligodendrocytes, but not astrocytes or nerve endings. Identification of granule cells as neuronal ET targets was confirmed by the observation that ET induced intracellular Ca2+ rises and glutamate release in primary cultures of granule cells. In cultured cerebellar slices, whole cell patch-clamp recordings of synaptic currents in Purkinje cells revealed that ET greatly stimulates both spontaneous excitatory and inhibitory activities. However, pharmacological dissection of these effects indicated that they were only a result of an increased granule cell firing activity and did not involve a direct action of the toxin on glutamatergic nerve terminals or inhibitory interneurons. Patch-clamp recordings of granule cell somata showed that ET causes a decrease in neuronal membrane resistance associated with pore-opening and depolarization of the neuronal membrane, which subsequently lead to the firing of the neuronal network and stimulation of glutamate release. This work demonstrates that a subset of neurons can be directly targeted by ET, suggesting that part of ET-induced neuronal damage observed in neuronal tissue is due to a direct effect of ET on neurons.
Highlights
Epsilon toxin (ET) is a protein of 30 kDa produced by Clostridium perfringens types B and D with a very high lethality (,400.000 mouse LD100/mg protein)
ET binds to defined regions of the cerebellar cortex Whole brain acute sagittal slices taken from adult (P25–P30)
In the presence of 1027 M ET the staining was marked in several brain regions, including cerebellum (Fig. 1B), hippocampus, thalamus, striatum, olfactive bulb, the colliculi, and cerebral white matter
Summary
Epsilon toxin (ET) is a protein of 30 kDa produced by Clostridium perfringens types B and D with a very high lethality (,400.000 mouse LD100/mg protein) This ranks this toxin among the 10 most potent poisonous substances so far known. ET is secreted in the gut lumen as a proto-toxin and following its activation by endoproteases the toxin compromises the intestinal barrier [2]. This allows ET to spread through the blood-stream, affecting the lungs, kidneys and the brain [1,3,4]. The causal link between pore formation and altered functions remains unclear: in conditions that prevent ET heptamerization ET can cause cell death [12]
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