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Published Online: 1 October 2024

Cell Type–Specific Profiles and Developmental Trajectories of Transcriptomes in Primate Prefrontal Layer 3 Pyramidal Neurons: Implications for Schizophrenia

Publication: American Journal of Psychiatry

Abstract

Objective:

In schizophrenia, impaired working memory is associated with transcriptome alterations in layer 3 pyramidal neurons (L3PNs) in the dorsolateral prefrontal cortex (DLPFC). Distinct subtypes of L3PNs that send axonal projections to the DLPFC in the opposite hemisphere (callosal projection [CP] neurons) or the parietal cortex in the same hemisphere (ipsilateral projection [IP] neurons) play critical roles in working memory. However, how the transcriptomes of these L3PN subtypes might shift during late postnatal development when working memory impairments emerge in individuals later diagnosed with schizophrenia is not known. The aim of this study was to characterize and compare the transcriptome profiles of CP and IP L3PNs across developmental transitions from prepuberty to adulthood in macaque monkeys.

Methods:

The authors used retrograde labeling to identify CP and IP L3PNs in the DLPFC of prepubertal, postpubertal, and adult macaque monkeys, and used laser microdissection to capture these neurons for RNA sequencing.

Results:

At all three ages, CP and IP L3PNs had distinct transcriptomes, with the number of genes differentially expressed between neuronal subtypes increasing with age. For IP L3PNs, age-related shifts in gene expression were most prominent between prepubertal and postpubertal animals, whereas for CP L3PNs such shifts were most prominent between postpubertal and adult animals.

Conclusions:

These findings demonstrate the presence of cell type–specific profiles and developmental trajectories of the transcriptomes of PPC-projecting IP and DLPFC-projecting CP L3PNs in monkey DLPFC. The evidence that IP L3PNs reach a mature transcriptome earlier than CP L3PNs suggests that these two subtypes differentially contribute to the maturation of working memory performance across late postnatal development and that they may be differentially vulnerable to the disease process of schizophrenia at specific stages of postnatal development.

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Information & Authors

Information

Published In

Go to American Journal of Psychiatry
Go to American Journal of Psychiatry
American Journal of Psychiatry
Pages: 920 - 934

History

Received: 6 July 2023
Revision received: 4 December 2023
Revision received: 29 February 2024
Accepted: 4 April 2024
Published online: 1 October 2024
Published in print: October 01, 2024

Keywords

  1. Pyramidal Neuron
  2. RNAseq
  3. Schizophrenia
  4. Working Memory
  5. Retrograde Labeling
  6. Laser Microdissection

Authors

Details

Dominique Arion, Ph.D.
Department of Psychiatry (Arion, Enwright, Gonzalez-Burgos, Lewis) and Department of Neuroscience (Lewis), University of Pittsburgh, Pittsburgh.
John F. Enwright III, Ph.D.
Department of Psychiatry (Arion, Enwright, Gonzalez-Burgos, Lewis) and Department of Neuroscience (Lewis), University of Pittsburgh, Pittsburgh.
Guillermo Gonzalez-Burgos, Ph.D.
Department of Psychiatry (Arion, Enwright, Gonzalez-Burgos, Lewis) and Department of Neuroscience (Lewis), University of Pittsburgh, Pittsburgh.
David A. Lewis, M.D. [email protected]
Department of Psychiatry (Arion, Enwright, Gonzalez-Burgos, Lewis) and Department of Neuroscience (Lewis), University of Pittsburgh, Pittsburgh.

Notes

Send correspondence to Dr. Lewis ([email protected]).

Competing Interests

Dr. Lewis receives investigator-initiated research support from Merck. The other authors report no financial relationships with commercial interests.

Funding Information

Supported by NIMH grant MH051234 to Dr. Lewis.

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