trimethyltin-hydroxide and Seizures

Insulin-like growth factor-1 (IGF-1) protects neurons from apoptosis and in vivo offers neuroprotective support to hippocampal CA1 pyramidal neurons following ischemia or seizure. IGF-1 signals through IGF-1 receptors activating phosphytidylinositol 3-kinase (PI3K)/Akt or pMAPK pathways. IGF-1 can be induced with injury and microglia and astrocytes may serve as a source of this neurotrophic factor to promote neuronal survival. An acute systemic injection of trimethyltin (TMT; 2 mg/kg, ip) to mice induces apoptosis of dentate granule neurons within 24 h and a differential response of microglia with ramified microglia present in the CA-1 region. Using this model, we studied the role of IGF-1 in the survival of CA-1 pyramidal neurons under conditions of altered synaptic input due to changes in the dentate gyrus. Within 24 h of injection, IGF-1 mRNA levels were elevated in the hippocampus and IGF-1 protein detected in both astrocytes and microglia. IGF-1 was redistributed within the CA-1 neurons corresponding with an increase in cytoplasmic pAkt, elevated PKBalpha/Akt protein levels, and a decrease in the antagonist, Rho. pMAPK was not detected in CA-1 neurons and ERK2 showed a transient decrease followed by a significant increase, suggesting a lack of recruitment of the pMAPK signaling pathway for neuronal survival. In mice deficient for IGF-1, a similar level of apoptosis was observed in dentate granule neurons as compared to wildtype; however, TMT induced a significant level CA-1 neuronal death, further supporting a role for IGF-1 in the survival of CA-1 neurons.

Topics: Animals; Animals, Newborn; Brain Injuries; CA1 Region, Hippocampal; Caspase 3; Dentate Gyrus; Disease Models, Animal; Fluoresceins; Gene Expression Regulation; Glial Fibrillary Acidic Protein; Glycoproteins; Insulin-Like Growth Factor I; Mice; Mice, Knockout; Microglia; Mitogen-Activated Protein Kinase Kinases; Nerve Tissue Proteins; Neurons; Oncogene Protein v-akt; Organic Chemicals; Seizures; Signal Transduction; Time Factors; Trimethyltin Compounds

Trimethyltin (TMT) causes a pattern of hippocampal damage in rats that is similar to that caused by convulsant chemicals or seen in the brains of some human epileptics. Therefore, we investigated the possible role that TMT-induced seizure activity might play in the hippocampal damage produced by this organotin. The morphologic effects of systemically administered TMT were compared to those of kainic acid given by the same route. Unlike kainate, TMT produced seizures in only a subset of treated animals and with a latency of days rather than minutes. Evaluation of morphology during the acute seizure period revealed that TMT-induced seizures were associated with a variable pattern of granule and pyramidal cell necrosis and acute dendritic swelling in the two associational/commissural hippocampal pathways, one from CA3 to CA1-CA3 and the other from the hilus to the proximal dendrites of dentate granule cells. The TMT-induced damage contrasted sharply with the acute pattern of kainate-induced damage that consisted of acute dendritic swellings in the distal granule cell dendrites, hilus and mossy fiber region. TMT-treated rats that did not exhibit seizures in the one week after injection exhibited minimal pathology during this period. These results suggest that at least part of the damage to granule and pyramidal cells produced by TMT is mediated by the seizure activity produced by this compound. Although the resulting lesions to the CA1-CA3 pyramidal cells may appear similar in both TMT- and kainate-treated rats long after injection, evaluation of acute pathology during the active seizure phase indicates that these compounds induce seizure activity in different hippocampal pathways and cause different patterns of irreversible neuronal damage as a result.

Topics: Animals; Brain Diseases; Hippocampus; Male; Microscopy, Electron; Rats; Rats, Inbred Strains; Seizures; Trialkyltin Compounds; Trimethyltin Compounds