Human GPM6A Is Associated With Differentiation and Neuronal Migration of Neurons Derived from Human Embryonic Stem Cells

Michibata, Hideo; Okuno, Taketoshi; Konishi, Nae; Kyono, Kiyoshi; Wakimoto, Koji; Aoki, Kosuke; Kondo, Yasushi; Takata, Kazuyuki; Kitamura, Yoshihisa; Taniguchi, Takashi

doi:10.1089/scd.2008.0215

Cited by 53 publications

(41 citation statements)

References 32 publications

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“…Remarkably, the myelin proteolipid protein (PLP/DM20) family members, such as GPM6A, GPM6B, and PLP1 transcript variant DM20, but not PLP1 (Fernandez et al, 2010), have been shown to be involved in the processes of neurite outgrowth and filopodium formation (Lagenaur et al, 1992; Mukobata et al, 2002; Alfonso et al, 2005; Michibata et al, 2008; Zhao et al, 2008; Fuchsova et al, 2009; Brocco et al, 2010; Scorticati et al, 2011). GPM6A, in particular, is also required for filopodium motility and synaptogenesis (Fuchsova et al, 2009; Brocco et al, 2010), and it has been implicated in neuronal differentiation of human stem cells (Michibata et al, 2009) and PC12 cells (Mukobata et al, 2002). When siRNA methodology is used, GPM6A low-expressing neurons display decreased filopodia numbers and a lower density of synaptophysin clusters (Alfonso et al, 2005).…”

Section: Introductionmentioning

confidence: 99%

Altered expression of neuroplasticity-related genes in the brain of depressed suicides

et al. 2015

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Background Expression of the neuronal membrane glycoprotein M6a (GPM6A), the proteolipid protein (PLP/DM20) family member, is downregulated in the hippocampus of chronically stressed animals. Its neuroplastic function involves a role in neurite formation, filopodium outgrowth and synaptogenesis through an unknown mechanism. Disruptions in neuroplasticity mechanisms have been shown to play a significant part in the etiology of depression. Thus, the current investigation examined whether GPM6A expression is also altered in human depressed brain. Methods Expression levels and coexpression patterns of GPM6A, GPM6B, and PLP1 (two other members of PLP/DM20 family) as well as of the neuroplasticity-related genes identified to associate with GPM6A were determined using quantitative polymerase chain reaction (qPCR) in postmortem samples from the hippocampus (n =18) and the prefrontal cortex (PFC) (n= 25) of depressed suicide victims and compared with control subjects (hippocampus n= 18; PFC n =25). Neuroplasticity-related proteins that form complexes with GPM6A were identified by coimmunoprecipitation technique followed by mass spectrometry. Results Results indicated transcriptional downregulation of GPM6A and GPM6B in the hippocampus of depressed suicides. The expression level of calcium/calmodulin-dependent protein kinase II alpha (CAMK2A) and coronin1A (CORO1A) was also significantly decreased. Subsequent analysis of coexpression patterns demonstrated coordinated gene expression in the hippocampus and in the PFC indicating that the function of these genes might be coregulated in the human brain. However, in the brain of depressed suicides this coordinated response was disrupted. Conclusions Disruption of coordinated gene expression as well as abnormalities in GPM6A and GPM6B expression and expression of the components of GPM6A complexes were detected in the brain of depressed suicides.

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Section: Introductionmentioning

confidence: 99%

Altered expression of neuroplasticity-related genes in the brain of depressed suicides

et al. 2015

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“…Regarding the polygenic nature of neural disorders, the fact that GPM6A is able to cause claustrophobia disorder highlights its importance. The GPM6A encodes the glycoprotein M6A that associated with the differentiation and neuronal migration of neurons derived from undifferentiated human stem cells [39]. Association of the GPM6A with the subgroup of schizophrenia patients reinforces the key role of this gene in regulation of central nervous system (CNS) [8].…”

Section: Discussionmentioning

confidence: 99%

Unique ability of pandemic influenza to downregulate the genes involved in neuronal disorders

et al. 2015

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Pandemic influenza remains as a substantial threat to humans with a widespread panic worldwide. In contrast, seasonal (non-pandemic) has a mild non-lethal infection each year. The underlying mechanisms governing the detrimental effects of pandemic influenza are yet to be known. Transcriptomic-based network discovery and gene ontology (GO) analysis of host response to pandemic influenza, compared to seasonal influenza, can shed light on the differential mechanisms which pandemic influenza is employed during evolution. Here, using microarray data of infected ferrets with pandemic and seasonal influenza (as a model), we evaluated the possible link between altered genes after pandemic infection with activation of neuronal disorders. To this end, we utilized novel computational biology techniques including differential transcriptome analysis, network construction, GO enrichment, and GO network to investigate the underlying mechanisms of pandemic influenza infection and host interaction. In comparison to seasonal influenza, pandemic influenza differentially altered the expression of 31 genes with direct involvement in activity of central nervous system (CNS). Network topology highlighted the high interactions of IRF1, NKX2-1 and NR5A1 as well as MIR27A, MIR19A, and MIR17. TGFB2, NCOA3 and SP1 were the central transcription factors in the networks. Pandemic influenza remarkably downregulated GPM6A and GTPase. GO network demonstrated the key roles of GPM6A and GTPase in regulation of important functions such as synapse assembly and neuron projection. For the first time, we showed that besides interference with cytokine/chemokine storm and neuraminidase enzyme, H1N1 pandemic influenza is able to directly affect neuronal gene networks. The possibility of application of some key regulators such as GPM6A protein, MIR128, and MIR367 as candidate therapeutic agents is discussed. The presented approach established a new way to unravel unknown pathways in virus-associated CNS dysfunction by utilizing global transcriptomic data, network and GO analysis.

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“…Notably, other neuronal surface molecules besides L1 have been shown to promote neuronal differentiation in vitro, which further supports the hypothesis that an overexpression of neuronal cell adhesion molecules in ES cells is a suitable approach towards their application in vivo. ES cells overexpressing the glycoprotein M6A, which is a cell adhesion molecule expressed on neurons in the CNS, differentiated more efficiently into neurons when compared to non-modified control ES cells (Michibata et al, 2009) and the L1-binding partner molecule NCAM significantly increased neuronal differentiation of embryonic neural precursor cells into mature neurons in vitro when added into medium of cultured cells (Shin et al, 2002). However, in contrast to L1, the beneficial effects of ES cells overexpressing these molecules have not been tested in animal models of disease to date.…”

Section: The Effects Of L1 On Neuroectodermal Differentiation Of Es Cmentioning

confidence: 99%

Embryonic Stem Cells Overexpressing the Recognition Molecules L1 and Tenascin-R Enhance Regeneration in Mouse Models of Acute and Chronic Neurological Disorders

Hargus¹,

Bernreuther²

2011

Embryonic Stem Cells - Recent Advances in Pluripotent Stem Cell-Based Regenerative Medicine

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Human GPM6A Is Associated With Differentiation and Neuronal Migration of Neurons Derived from Human Embryonic Stem Cells

Cited by 53 publications

References 32 publications

Altered expression of neuroplasticity-related genes in the brain of depressed suicides

Altered expression of neuroplasticity-related genes in the brain of depressed suicides

Unique ability of pandemic influenza to downregulate the genes involved in neuronal disorders

Embryonic Stem Cells Overexpressing the Recognition Molecules L1 and Tenascin-R Enhance Regeneration in Mouse Models of Acute and Chronic Neurological Disorders

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