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J Neurophysiol (January 24, 2007). doi:10.1152/jn.00646.2006
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Submitted on June 20, 2006
Accepted on January 19, 2007

IDENTIFICATION OF GIANT SPONTANEOUS DEPOLARIZING POTENTIALS IN THE DEVELOPING THALAMIC RETICULAR NUCLEUS

Susanne M Pangratz-Fuehrer1, Uwe Rudolph2, and John R. Huguenard1*

1 Department of Neurology and Neurological Sciences, Stanford University Medical Center, Stanford, California, United States
2 Laboratory of Genetic Neuropharmacology, Harvard Medical School, McLean Hospital, Mailman Research Center, Boston, Massachusetts, United States

* To whom correspondence should be addressed. E-mail: john.huguenard{at}stanford.edu.

The thalamic reticular nucleus (nRt) provides a major source of inhibition in the thalamo-cortical circuit and is critically involved in the generation of spindle oscillations. Here, we describe the properties of thalamic giant depolarizing potentials (tGDPs) that were observed in nRt during early development. tGDPs persisted in presence of ionotropic glutamate antagonists but were completely abolished by GABAAR antagonist SR 35591. tGDPs occurred primarily between p3 and p8 (in 30-50% of cells) and occasionally up until p15. tGDPs lasted 0.4-3 sec with peak conductances of 2-13 nS and occurred at frequencies between 0.02 and 0.06 Hz. We used mice with a benzodiazepine-insensitive {alpha}3 subunit [{alpha}3(H126R)] to probe for the identity of the GABAA receptors responsible for tGDP generation. Benzodiazepine enhancement of tGDP amplitude persisted in nRt neurons in {alpha}3(H126R) mice indicating that the GABAARs containing {alpha}3 are not critical for tGDP generation, and suggests that tGDPs are mediated by GABAARs containing the {alpha}5 subunit, which is transiently expressed in nRt neurons in early postnatal development. Furthermore, we found that exogenous GABA application depolarized nRt neurons younger than p8, indicating elevated [Cl-]i at this developmental stage. Taken together, these data suggest that in immature nRt long-lasting depolarizing responses mediated by GABA receptors could trigger Ca2+ entry and play a role in functional development of the spindle generating circuitry.




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