Literature DB >> 25488607

Surviving mossy cells enlarge and receive more excitatory synaptic input in a mouse model of temporal lobe epilepsy.

Wei Zhang1, Ajoy K Thamattoor, Christopher LeRoy, Paul S Buckmaster.   

Abstract

Numerous hypotheses of temporal lobe epileptogenesis have been proposed, and several involve hippocampal mossy cells. Building on previous hypotheses we sought to test the possibility that after epileptogenic injuries surviving mossy cells develop into super-connected seizure-generating hub cells. If so, they might require more cellular machinery and consequently have larger somata, elongate their dendrites to receive more synaptic input, and display higher frequencies of miniature excitatory synaptic currents (mEPSCs). To test these possibilities pilocarpine-treated mice were evaluated using GluR2-immunocytochemistry, whole-cell recording, and biocytin-labeling. Epileptic pilocarpine-treated mice displayed substantial loss of GluR2-positive hilar neurons. Somata of surviving neurons were 1.4-times larger than in controls. Biocytin-labeled mossy cells also were larger in epileptic mice, but dendritic length per cell was not significantly different. The average frequency of mEPSCs of mossy cells recorded in the presence of tetrodotoxin and bicuculline was 3.2-times higher in epileptic pilocarpine-treated mice as compared to controls. Other parameters of mEPSCs were similar in both groups. Average input resistance of mossy cells in epileptic mice was reduced to 63% of controls, which is consistent with larger somata and would tend to make surviving mossy cells less excitable. Other intrinsic physiological characteristics examined were similar in both groups. Increased excitatory synaptic input is consistent with the hypothesis that surviving mossy cells develop into aberrantly super-connected seizure-generating hub cells, and soma hypertrophy is indirectly consistent with the possibility of axon sprouting. However, no obvious evidence of hyperexcitable intrinsic physiology was found. Furthermore, similar hypertrophy and hyper-connectivity has been reported for other neuron types in the dentate gyrus, suggesting mossy cells are not unique in this regard. Thus, findings of the present study reveal epilepsy-related changes in mossy cell anatomy and synaptic input but do not strongly support the hypothesis that mossy cells develop into seizure-generating hub cells.
© 2014 Wiley Periodicals, Inc.

Entities:  

Keywords:  GluR2; dendrites; dentate gyrus; hypertrophy; miniature EPSC

Mesh:

Substances:

Year:  2014        PMID: 25488607      PMCID: PMC4412767          DOI: 10.1002/hipo.22396

Source DB:  PubMed          Journal:  Hippocampus        ISSN: 1050-9631            Impact factor:   3.899


  82 in total

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2.  Axon sprouting in a model of temporal lobe epilepsy creates a predominantly excitatory feedback circuit.

Authors:  Paul S Buckmaster; Guo Feng Zhang; Ruth Yamawaki
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3.  Synaptic connections of dentate granule cells and hilar neurons: results of paired intracellular recordings and intracellular horseradish peroxidase injections.

Authors:  H E Scharfman; D D Kunkel; P A Schwartzkroin
Journal:  Neuroscience       Date:  1990       Impact factor: 3.590

4.  Survival of dentate hilar mossy cells after pilocarpine-induced seizures and their synchronized burst discharges with area CA3 pyramidal cells.

Authors:  H E Scharfman; K L Smith; J H Goodman; A L Sollas
Journal:  Neuroscience       Date:  2001       Impact factor: 3.590

5.  "Dormant basket cell" hypothesis revisited: relative vulnerabilities of dentate gyrus mossy cells and inhibitory interneurons after hippocampal status epilepticus in the rat.

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9.  Loss of glutamate decarboxylase mRNA-containing neurons in the rat dentate gyrus following pilocarpine-induced seizures.

Authors:  A Obenaus; M Esclapez; C R Houser
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Authors:  R S Sloviter
Journal:  Science       Date:  1987-01-02       Impact factor: 47.728

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10.  Excitatory Synaptic Input to Hilar Mossy Cells under Basal and Hyperexcitable Conditions.

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