A retrospective analysis of phosphatase catalytic subunit gene variants in patients with rare disorders identifies novel candidate neurodevelopmental disease genes

Lyulcheva-Bennett, Ekaterina; Consortium, Genomics England Research; Bennett, Daimark

doi:10.3389/fcell.2023.1107930

Cited by 2 publications

(1 citation statement)

References 58 publications

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“…Interestingly, neurodevelopmental disorders related to increased cortical neurons are often associated with impaired neuronal phenotypes and behavioral alterations ( Fang et al, 2014 ). Regarding the role of PTPRD in neurogenesis, our observations align with this hypothesis since previous studies have found that PTPRD KO mice have aberrant dendritic processes ( Nakamura et al, 2017 ), impaired synaptic development and function ( Takahashi et al, 2012 ; Park et al, 2020 ; Sclip and Südhof, 2020 ), and behavioral deficits ( Drgonova et al, 2015 ; Uhl et al, 2018 ; Park et al, 2020 ; Ho et al, 2023 ), which could explain the contribution of PTRPD mutations to neurodevelopmental disorders ( Schormair et al, 2008 ; Elia et al, 2010 ; Pinto et al, 2010 ; Levy et al, 2011 ; Yang et al, 2011 ; Gai et al, 2012 ; Gazzellone et al, 2016 ; Liu et al, 2016 ; Li et al, 2018 ; Li et al, 2023 ; Lyulcheva-Bennett and Bennett, 2023 ).…”

Section: Discussionsupporting

confidence: 88%

Neural conditional ablation of the protein tyrosine phosphatase receptor Delta PTPRD impairs gliogenesis in the developing mouse brain cortex

Cornejo,

Franchini,

Cortés

et al. 2024

Front. Cell Dev. Biol.

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Neurodevelopmental disorders are characterized by alterations in the development of the cerebral cortex, including aberrant changes in the number and function of neural cells. Although neurogenesis is one of the most studied cellular processes in these pathologies, little evidence is known about glial development. Genetic association studies have identified several genes associated with neurodevelopmental disorders. Indeed, variations in the PTPRD gene have been associated with numerous brain disorders, including autism spectrum disorder, restless leg syndrome, and schizophrenia. We previously demonstrated that constitutive loss of PTPRD expression induces significant alterations in cortical neurogenesis, promoting an increase in intermediate progenitors and neurons in mice. However, its role in gliogenesis has not been evaluated. To assess this, we developed a conditional knockout mouse model lacking PTPRD expression in telencephalon cells. Here, we found that the lack of PTPRD in the mouse cortex reduces glial precursors, astrocytes, and oligodendrocytes. According to our results, this decrease in gliogenesis resulted from a reduced number of radial glia cells at gliogenesis onset and a lower gliogenic potential in cortical neural precursors due to less activation of the JAK/STAT pathway and reduced expression of gliogenic genes. Our study shows PTPRD as a regulator of the glial/neuronal balance during cortical neurodevelopment and highlights the importance of studying glial development to understand the etiology of neurodevelopmental diseases.

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Section: Discussionsupporting

confidence: 88%

Neural conditional ablation of the protein tyrosine phosphatase receptor Delta PTPRD impairs gliogenesis in the developing mouse brain cortex

Cornejo,

Franchini,

Cortés

et al. 2024

Front. Cell Dev. Biol.

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. Detecţia prenatală a deleţiei 2q21.1 la un făt cu restricţie severă precoce de creştere intrauterină: prezentare de caz şi review al literaturii

Muntean,

Săsăran,

Luca

et al. 2024

Obstetrica şi Ginecologia

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Background. Early-onset fetal growth restriction (FGR) has a wide range of etiologies, including impaired placentation, congenital infections, genetic abnormalities, and toxic or environmental exposure. Depending on the size and location of the genomic region involved, 2q21.1 deletion can be associated with various clinical manifestations. Method and results. A 30-year-old primigravida was referred for early-onset severe symmetrical FGR at 22 weeks of gestational age, without any ultrasound signs of malformations. The karyotype of the fetus was 46,XY. Single-nucleotide polymorphism (SNP) microarray revealed a heterozygous deletion of 350kb in the chromosomal region 2q21.1, which contained five OMIM genes: SMPD4, MZT2B, CCDC115, IMP4, and PTPN18. The evolution of pregnancy was uneventful until 37+4 weeks, when a male infant weighing 1880 g was delivered by caesarean section, with Apgar scores of 6 and 9 at 1 and 5 minutes. The infant was discharged alive ten days after birth. Conclusions. The result of this study may be helpful for antenatal counseling of pregnant women with severe early onset of intrauterine growth restriction.

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A retrospective analysis of phosphatase catalytic subunit gene variants in patients with rare disorders identifies novel candidate neurodevelopmental disease genes

Cited by 2 publications

References 58 publications

Neural conditional ablation of the protein tyrosine phosphatase receptor Delta PTPRD impairs gliogenesis in the developing mouse brain cortex

Neural conditional ablation of the protein tyrosine phosphatase receptor Delta PTPRD impairs gliogenesis in the developing mouse brain cortex

. Detecţia prenatală a deleţiei 2q21.1 la un făt cu restricţie severă precoce de creştere intrauterină: prezentare de caz şi review al literaturii

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