ST8SIA2 promotes oligodendrocyte differentiation and the integrity of myelin and axons

Szewczyk, Łukasz Mateusz; Brożko, Nikola; Nagalski, Andrzej; Röckle, Iris; Werneburg, Sebastian; Hildebrandt, Herbert; Wisniewska, M.; Kuźnicki, Jacek

doi:10.1002/glia.23048

Cited by 17 publications

(14 citation statements)

References 90 publications

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“…In addition, although to our knowledge there was no previous study detailing the impact of St8sia2 deficiency on neonatal amygdala development, several studies have revealed alterations in other brain regions occurring after birth in St8sia2−/− mice. The reported alterations include a decrease in GABA neurons in the prefrontal cortex observed at P1, but not E16.5; [81] deficits in olfactory interneurons only seen at P5; [82] and a decrease in myelination observed from P15 onwards [83]. More generally, polysialylation is an essential process involved in the migration and clustering of neural and glial precursors [23,81,84], axonal growth and fasciculation [85], synapse formation and plasticity [86,87], and myelination [83].…”

Section: Discussionmentioning

confidence: 99%

Amygdala GluN2B-NMDAR dysfunction is critical in abnormal aggression of neurodevelopmental origin induced by St8sia2 deficiency

et al. 2018

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Aggression is frequently observed in neurodevelopmental psychiatric disorders such as schizophrenia, autism, and bipolar disorder. Due to a lack of understanding of its underlying mechanisms, effective treatments for abnormal aggression are still missing. Recently, genetic variations in Sialyltransferase 2 (St8sia2) have been linked to these disorders and aggression. Here we identify abnormal aggressive behaviors and concomitant blunted fear learning in St8sia2 knockout (-/-) mice. It is worth noting that the amygdala of St8sia2-/- mice shows diminished threat-induced activation, as well as alterations in synaptic structure and function, including impaired GluN2B-containing NMDA receptor-mediated synaptic transmission and plasticity. Pharmacological rescue of NMDA receptor activity in the amygdala of St8sia2-/- mice with the partial agonist D-cycloserine restores synaptic plasticity and normalizes behavioral aberrations. Pathological aggression and associated traits were recapitulated by specific amygdala neonatal St8sia2 silencing. Our results establish a developmental link between St8sia2 deficiency and a pathological aggression syndrome, specify synaptic targets for therapeutic developments, and highlight D-cycloserine as a plausible treatment.

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Section: Discussionmentioning

confidence: 99%

Amygdala GluN2B-NMDAR dysfunction is critical in abnormal aggression of neurodevelopmental origin induced by St8sia2 deficiency

et al. 2018

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“…ST8SIA2 knock out mouse models exhibit delayed myelination and decreased myelin content, including thinner sheaths, irregularly shaped axons, and increased white matter lesions in adulthood. ST8SIA2 knockout mice also exhibit increases in the number of immature oligodendrocytes in the cortex and the corpus callosum that may imply a blockade of OPC differentiation to myelinating oligodendrocytes (Szewczyk et al, ).…”

Section: Psychiatric Disordersmentioning

confidence: 99%

Bad wrap: Myelin and myelin plasticity in health and disease

Gibson

Geraghty

Monje

2017

Developmental Neurobiology

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Human central nervous system myelin development extends well into the fourth decade of life, and this protracted period underscores the potential for experience to modulate myelination. The concept of myelin plasticity implies adaptability in myelin structure and function in response to experiences during development and beyond. Mounting evidence supports this concept of neuronal activity-regulated changes in myelin-forming cells, including oligodendrocyte precursor cell proliferation, oligodendrogenesis and modulation of myelin microstructure. In healthy individuals, myelin plasticity in associative white matter structures of the brain is implicated in learning and motor function in both rodents and humans. Activity-dependent changes in myelin-forming cells may influence the function of neural networks that depend on the convergence of numerous neural signals on both a temporal and spatial scale. However, dysregulation of myelin plasticity can disadvantageously alter myelin microstructure and result in aberrant circuit function or contribute to pathological cell proliferation. Emerging roles for myelin plasticity in normal neurological function and in disease are discussed. © 2017 Wiley Periodicals, Inc. Develop Neurobiol 78: 123-135, 2018.

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“…Cells with nuclear Olig2 expression were negative for GS or GFAP. Extranuclear signal in the Olig2-channel occurred in both lowDeg and highDeg samples, in the presence and absence of primary antibodies, and was mainly interpreted as unspecific secondary antibody binding (Supporting Information,Figures S4 and S5, white circles),(Rhee et al, 2009;Szewczyk et al, 2017). However, atypical cytosolic/extranuclear expression of Olig2 as a possible consequence of the disease cannot be excluded.…”

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confidence: 99%

Astrocytic glutamine synthetase is expressed in the neuronal somatic layers and down‐regulated proportionally to neuronal loss in the human epileptic hippocampus

Papageorgiou

Valous

Lahrmann

et al. 2018

Glia

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Human mesial temporal lobe epilepsy (MTLE) features subregion-specific hippocampal neurodegeneration and reactive astrogliosis, including up-regulation of the glial fibrillary acidic protein (GFAP) and down-regulation of glutamine synthetase (GS). However, the regional astrocytic expression pattern of GFAP and GS upon MTLE-associated neurodegeneration still remains elusive. We assessed GFAP and GS expression in strict correlation with the local neuronal number in cortical and hippocampal surgical specimens from 16 MTLE patients using immunohistochemistry, stereology and high-resolution image analysis for digital pathology and whole-slide imaging. In the cortex, GS-positive (GS+) astrocytes are dominant in all neuronal layers, with a neuron to GS+ cell ratio of 2:1. GFAP-positive (GFAP+) cells are widely spaced, with a GS+ to GFAP+ cell ratio of 3:1-5:1. White matter astrocytes, on the contrary, express mainly GFAP and, to a lesser extent, GS. In the hippocampus, the neuron to GS+ cell ratio is approximately 1:1. Hippocampal degeneration is associated with a reduction of GS+ astrocytes, which is proportional to the degree of neuronal loss and primarily present in the hilus. Up-regulation of GFAP as a classical hallmark of reactive astrogliosis does not follow the GS-pattern and is prominent in the CA1. Reactive alterations were proportional to the neuronal loss in the neuronal somatic layers (stratum pyramidale and hilus), while observed to a lesser extent in the axonal/dendritic layers (stratum radiatum, molecular layer). We conclude that astrocytic GS is expressed in the neuronal somatic layers and, upon neurodegeneration, is down-regulated proportionally to the degree of neuronal loss.

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ST8SIA2 promotes oligodendrocyte differentiation and the integrity of myelin and axons

Cited by 17 publications

References 90 publications

Amygdala GluN2B-NMDAR dysfunction is critical in abnormal aggression of neurodevelopmental origin induced by St8sia2 deficiency

Amygdala GluN2B-NMDAR dysfunction is critical in abnormal aggression of neurodevelopmental origin induced by St8sia2 deficiency

Bad wrap: Myelin and myelin plasticity in health and disease

Astrocytic glutamine synthetase is expressed in the neuronal somatic layers and down‐regulated proportionally to neuronal loss in the human epileptic hippocampus

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