Vertical Bias in Dendritic Trees of Non-pyramidal Neocortical Neurons Expressing GAD67-GFP In Vitro

doi:10.1093/cercor/11.7.666

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Cerebral Cortex, Vol. 11, No. 7, 666-678, July 2001
© 2001 Oxford University Press

Vertical Bias in Dendritic Trees of Non-pyramidal Neocortical Neurons Expressing GAD67–GFP In Vitro

X. Jin¹^,4, P. H. Mathers²^,3, G. Szabo⁵, Z. Katarova⁵ and A. Agmon¹^,3

¹ Department of Neurobiology and Anatomy, , ² Departments of Otolaryngology and Biochemistry, , ³ Sensory Neuroscience Research Center and the , ⁴ Neuroscience Graduate Program, West Virginia University, Morgantown, WV 26506, USA and , ⁵ Laboratory of Molecular Biology and Genetics, Institute of Experimental Medicine, Hungarian Academy of Sciences, H-1450 Budapest, Hungary

The neocortical neuropil has a strong vertical (orthogonal topia) orientation, constraining the intracortical flow of informationand forming the basis for the functional parcellation of thecortex into semi-independent vertical columns or ‘modules’.Apical dendrites of excitatory pyramidal neurons are a majorcomponent of this vertical neuropil, but the extent to whichinhibitory, GABAergic neurons conform to this structural andfunctional design is less well documented. We used a gene gunto transfect organotypic slice cultures of mouse and rat neocortexwith the enhanced green fluorescent protein (eGFP) gene drivenby the promoter for glutamic acid decarboxylase 67 (GAD67),an enzyme expressed exclusively in GABAergic cells. Many GAD67–GFPexpressing cells were highly fluorescent, and their dendriticmorphologies and axonal patterns, revealed in minute detail,were characteristic of GABAergic neurons. We traced 150 GFP-expressingneurons from confocal image stacks, and estimated the degreeof vertical bias in their dendritic trees using a novel computationalmetric. Over 70% of the neurons in our sample had dendritictrees with a highly significant vertical bias. We conclude thatGABAergic neurons make an important contribution to the verticalneocortical neuropil, and are likely to integrate synaptic inputsfrom axons terminating within their own module.

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