Abstract

Converging lines of evidence indicate that schizophrenia is characterized by impairments of synaptic machinery within cerebral cortical circuits. Efforts to localize these alterations in brain tissue from subjects with schizophrenia have frequently been limited to the quantification of structures that are non-selectively identified (e.g., dendritic spines labeled in Golgi preparations, axon boutons labeled with synaptophysin), or to quantification of proteins using methods unable to resolve relevant cellular compartments. Multiple label fluorescence confocal microscopy represents a means to circumvent many of these limitations, by concurrently extracting information regarding the number, morphology, and relative protein content of synaptic structures. An important adaptation required for studies of human disease is coupling this approach to stereologic methods for systematic random sampling of relevant brain regions. In this review article we consider the application of multiple label fluorescence confocal microscopy to the mapping of synaptic alterations in subjects with schizophrenia and describe the application of a novel, readily automated, iterative intensity/morphological segmentation algorithm for the extraction of information regarding synaptic structure number, size, and relative protein level from tissue sections obtained using unbiased stereological principles of sampling. In this context, we provide examples of the examination of pre- and post-synaptic structures within excitatory and inhibitory circuits of the cerebral cortex.

Highlights

  • HUMAN NEUROSCIENCEMapping synaptic pathology within cerebral cortical circuits in subjects with schizophrenia

  • Evidence for localized impairments of cerebral cortical circuits in schizophrenia Evidence from in vivo imaging and electrophysiologic studies, and from examination of postmortem tissue, indicate that schizophrenia is characterized by selective impairments of the synaptic machinery within cerebral cortical circuits

  • Postmortem studies of the dorsolateral prefrontal cortex (DLPFC) of subjects with schizophrenia have found disturbances in GABA neuron networks, in particular of PV+ neurons, which may contribute to impaired gamma oscillations in the DLPFC

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Summary

HUMAN NEUROSCIENCE

Mapping synaptic pathology within cerebral cortical circuits in subjects with schizophrenia. In this review article we consider the application of multiple label fluorescence confocal microscopy to the mapping of synaptic alterations in subjects with schizophrenia and describe the application of a novel, readily automated, iterative intensity/morphological segmentation algorithm for the extraction of information regarding synaptic structure number, size, and relative protein level from tissue sections obtained using unbiased stereological principles of sampling. In this context, we provide examples of the examination of pre- and post-synaptic structures within excitatory and inhibitory circuits of the cerebral cortex

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