14 Anatomical studies do support the presence
of input-specific alterations of excitatory connections in the DLPFC in schizophrenia. In the DLPFC, pyramidal neurons (selleckchem Figure 1 C) are the principal source of glutamate neurotransmission, as well as the targets of the majority of glutamate-containing axon terminals. Although the number of these neurons does not appear to be altered in schizophrenia,15,16 neuronal density in the DLPFC has been reported to be increased in schizophrenia.17 Increased cell packing density has been interpreted as evidence of a reduction in the amount of cortical neuropil, Inhibitors,research,lifescience,medical the axon terminals, selleck chem dendritic spines, and glial processes that occupy the space between neurons.18 Consistent with this interpretation, synaptophysin protein, a marker of axon terminals, has been reported to be decreased in the DLPFC of subjects with schizophrenia.19,21 Furthermore, gene expression profiling studies have found reduced Inhibitors,research,lifescience,medical tissue levels of gene transcripts that encode proteins involved in the presynaptic regulation of neurotransmission.22 Dendritic spines are the principal targets of excitatory synapses to pyramidal neurons. Although most dendritic spines present are Inhibitors,research,lifescience,medical stable in number during adulthood,23 they are subject to a number of neuroplastic changes, such as a loss of their presynaptic
excitatory input. In schizophrenia, dendritic spine density in pyramidal neurons has been reported to be lower in the DLPFC24,25; understanding the nature of these neuroplastic responses requires knowledge of the specific circuits that are affected and the developmental mechanisms Inhibitors,research,lifescience,medical that might underlie these changes. Reduced excitatory connections in schizophrenia are specific to a subset of pyramidal neurons Pyramidal
neurons can be divided into subgroups based on the brain region targeted by their Inhibitors,research,lifescience,medical principal axonal projection and the sources of their excitatory inputs; both of these characteristics are associated with the location of pyramidal cell bodies in different layers of the cortex (Figure 1 C). Anacetrapib For example, many pyramidal cells in layers 2 to 3 send axonal projections to other cortical regions, pyramidal neurons in layer 5 tend to project to the striatum and other subcortical structures, and pyramidal neurons in layer 6 furnish projections primarily to the thalamus.26 Studies of basilar dendritic spine density on Golgi-impregnaled pyramidal neurons in each cortical layer of the DLPFC in the same cohort of subjects found a significant effect of diagnosis on spine density only for pyramidal neurons in deep layer 3 (Figure 2).25,27 Figure 2. Pyramidal neuron dendritic spines in the human DLPFC.