Differentiation of oligodendrocyte precursors is impaired in the prefrontal cortex in schizophrenia

Mauney, Sarah A.; Pietersen, Charmaine Y.; Sonntag, Kai‐Christian; Woo, Tsung-Ung W.

doi:10.1016/j.schres.2015.10.042

Cited by 83 publications

(65 citation statements)

References 75 publications

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“…In turn, excess of astrocytic human-specific expression differences matches histological differences reported between humans and the other primate species for interlaminar astrocytes, polarized astrocytes, and varicose projection astrocytes [Oberheim et al, 2009;Falcone et al, 2018]. Similarly, oligodendrocyte progenitor cells showing rapid expression evolution in human caudate nucleus were reported to dysfunction in the caudate nucleus of schizophrenia patients [Georgieva et al, 2006;Uranova et al, 2007;Cassoli et al, 2015;Mauney et al, 2015], a disorder suggested to affect aspects of cognition particular to humans [Konopka and Geschwind, 2010;Dean, 2009].…”

Section: Discussionsupporting

confidence: 58%

Single-cell-resolution transcriptome map of human, chimpanzee, bonobo, and macaque brains

Khrameeva

Kurochkin

Han

et al. 2019

Preprint

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Identification of gene expression traits unique to the human brain sheds light on the mechanisms of human cognition. Here we searched for gene expression traits separating humans from other primates by analyzing 88,047 cell nuclei and 422 tissue samples representing 33 brain regions of humans, chimpanzees, bonobos, and macaques. We show that gene expression evolves rapidly within cell types, with more than two-thirds of cell type-specific differences not detected using conventional RNA sequencing of tissue samples. Neurons tend to evolve faster in all hominids, but non-neuronal cell types, such as astrocytes and oligodendrocyte progenitors, show more differences on the human lineage, including alterations of spatial distribution across neocortical layers.

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Section: Discussionsupporting

confidence: 58%

Single-cell-resolution transcriptome map of human, chimpanzee, bonobo, and macaque brains

Khrameeva

Kurochkin

Han

et al. 2019

Preprint

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“…One presumption is that they are consequences of oligodendroglial deficits because variations in the genes that encode oligodendrocyte and myelin proteins, such as OLIG2, MBP, PLP1, MOG, MOBP, CNP, and MAG, have been associated with schizophrenia (reviewed in (Roussos and Haroutunian ), and lower levels of expression of these proteins were observed in schizophrenia brains post‐mortem (Hakak et al, ; Mauney et al, ; Tkachev et al, ). Moreover, a recent study reported a decrease in the density of OLIG2+ cells and an increase in PDGFRA expression in the prefrontal cortex (Mauney et al, ). Highly reminiscent of these findings in schizophrenia, the levels of all the investigated myelin proteins in this study were reduced in the cortex in adult St8sia2 −/− mice, and St8sia2 −/− OPCs exhibited an increase in the level of PDFGRα in vitro .…”

Section: Discussionmentioning

confidence: 99%

ST8SIA2 promotes oligodendrocyte differentiation and the integrity of myelin and axons

Szewczyk

Brożko

Nagalski

et al. 2016

Glia

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ST8SIA2 is a polysialyltransferase that attaches polysialic acid to the glycoproteins NCAM1 and CADM1. Polysialylation is involved in brain development and plasticity. ST8SIA2 is a schizophrenia candidate gene, and St8sia2 −/− mice exhibit schizophrenia‐like behavior. We sought to identify new pathological consequences of ST8SIA2 deficiency. Our proteomic analysis suggested myelin impairment in St8sia2 −/− mice. Histological and immune staining together with Western blot revealed that the onset of myelination was not delayed in St8sia2 −/− mice, but the content of myelin was lower. Ultrastructure analysis of the corpus callosum showed thinner myelin sheaths, smaller and irregularly shaped axons, and white matter lesions in adult St8sia2 −/− mice. Then we evaluated oligodendrocyte differentiation in vivo and in vitro. Fewer OLIG2+ cells in the cortex and corpus callosum, together with the higher percentage of undifferentiated oligodenroglia in St8sia2 −/− mice suggested an impairment in oligodendrocyte generation. Experiment on primary cultures of oligodendrocyte precursor cells (OPCs) confirmed a cell‐autonomous effect of ST8SIA2 in oligodendroglia, and demonstrated that OPC to oligodendrocyte transition is inhibited in St8sia2 −/− mice. Concluding, ST8SIA2‐mediated polysialylation influences on oligodendrocyte differentiation, and oligodendrocyte deficits in St8sia2 mice are a possible cause of the demyelination and degeneration of axons, resembling nerve fiber alterations in schizophrenia. GLIA 2016;65:34–49

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“…Specifically, it is essential for oligodendrocyte and motor neuron development in the spinal cord [Ono et al, 2008], and for oligodendrocyte function, the impairment of which is thought to be a primary pathogenic event in SZ, specifically affecting the prefrontal cortex [Georgieva et al, 2006;Mauney et al, 2015]. Indeed, in our network, OLIG2 is also linked to GFAP , which encodes a hallmark structural component of mature astrocytes.…”

Section: Functional Implication and Biological Interpretation Of Domementioning

confidence: 93%

Schizophrenia and Human Self-Domestication: An Evolutionary Linguistics Approach

et al. 2017

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Schizophrenia (SZ) is a pervasive neurodevelopmental disorder that entails social and cognitive deficits, including marked language problems. Its complex multifactorial etiopathogenesis, including genetic and environmental factors, is still widely uncertain. SZ incidence has always been high and quite stable in human populations, across time and regardless of cultural implications, for unclear reasons. It has been hypothesized that SZ pathophysiology may involve the biological components that changed during the recent human evolutionary history, and led to our distinctive mode of cognition, which includes language skills. In this paper we explore this hypothesis, focusing on the self-domestication of the human species. This has been claimed to account for many human-specific distinctive traits, including aspects of our behavior and cognition, and to favor the emergence of complex languages through cultural evolution. The “domestication syndrome” in mammals comprises the constellation of traits exhibited by domesticated strains, seemingly resulting from the hypofunction of the neural crest. It is our intention to show that people with SZ exhibit more marked domesticated traits at the morphological, physiological, and behavioral levels. We also show that genes involved in domestication and neural crest development and function comprise nearly 20% of SZ candidates, most of which exhibit altered expression profiles in the brain of SZ patients, specifically in areas involved in language processing. Based on these observations, we conclude that SZ may represent an abnormal ontogenetic itinerary for the human faculty of language, resulting, at least in part, from changes in genes important for the domestication syndrome and primarily involving the neural crest.

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Differentiation of oligodendrocyte precursors is impaired in the prefrontal cortex in schizophrenia

Cited by 83 publications

References 75 publications

Single-cell-resolution transcriptome map of human, chimpanzee, bonobo, and macaque brains

Single-cell-resolution transcriptome map of human, chimpanzee, bonobo, and macaque brains

ST8SIA2 promotes oligodendrocyte differentiation and the integrity of myelin and axons

Schizophrenia and Human Self-Domestication: An Evolutionary Linguistics Approach

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