The
            <i>Drosophila</i>
            cell adhesion molecule Klingon is required for long-term memory formation and is regulated by Notch

Matsuno, Motomi; Horiuchi, Junjiro; Tully, Tim; Saitoe, Minoru

doi:10.1073/pnas.0807665106

Cited by 44 publications

(39 citation statements)

References 34 publications

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“…In flies, a number of cell-adhesion molecules have been shown to affect ethanol responses. The Notchregulated cell-adhesion gene klingon is required for normal olfactory memory (Matsuno, Horiuchi, Tully, & Saitoe, 2009) and for ethanol sedation and tolerance (Berger et al, 2008), whereas the neural cell-adhesion molecule FasII is required for normal acute resistance to ethanol as well as for normal olfactory learning (Cheng et al, 2001). Interestingly, FasII protein levels are reduced in the hangover tolerance mutant (Schwenkert et al, 2008), suggesting that the hangover-encoded transcription factor might directly regulate FasII expression and thereby cell adhesion.…”

Section: Cell Adhesion and Structurementioning

confidence: 97%

The Genetics of Alcohol Responses of Invertebrate Model Systems

Rothenfluh

Troutwine

Ghezzi

et al. 2014

Neurobiology of Alcohol Dependence

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Section: Cell Adhesion and Structurementioning

confidence: 97%

The Genetics of Alcohol Responses of Invertebrate Model Systems

Rothenfluh

Troutwine

Ghezzi

et al. 2014

Neurobiology of Alcohol Dependence

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“…Notch has also been implicated in the control of sleep (Seugnet et al, 2011;Singh et al, 2011). Finally, Notch activity is required for memory formation in Drosophila and mice (Costa et al, 2003;Ge et al, 2004;Matsuno et al, 2009;Presente et al, 2004). Intriguingly, loss of function of sca disrupts the formation of memories for ethanol reward without disrupting apparent features of the corresponding neuronal circuitry (Kaun et al, 2011).…”

Section: Intracellular Trafficking Pathways Establish Multiple Layersmentioning

confidence: 99%

dEHBP1 regulates Scabrous secretion during Notch mediated lateral inhibition

Γιαγτζόγλου

Yamamoto

et al. 2013

Journal of Cell Science

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SummaryNotch signaling is an evolutionarily conserved pathway that plays a central role in numerous developmental and disease processes. The versatility of the Notch pathway relies on the activity of context-dependent regulators. These include rab11, sec15, arp3 and Drosophila EHBP1 (dEHBP1), which control Notch signaling and cell fate acquisition in asymmetrically dividing mechanosensory lineages by regulating the trafficking of the ligand Delta. Here, we show that dEHBP1 also controls the specification of R8 photoreceptors, as its loss results in the emergence of supernumerary R8 photoreceptors. Given the requirements for Notch signaling during lateral inhibition, we propose that dEHBP1 regulates distinct aspects of Notch signaling in different developmental contexts. We show that dEHBP1 regulates the exocytosis of Scabrous, a positive regulator of Notch signaling. In conclusion, dEHBP1 provides developmental versatility of intercellular signaling by regulating the trafficking of distinct Notch signaling components.

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“…Interestingly, Wrapper appears to be less conserved. Although it is present in all Drosophilidae and the Drosophila genome harbors a Wrapper-related protein, Klingon (Butler et al, 1997;Matsuno et al, 2009), no clear Wrapper orthologs can be identified in mammals. However, there are several GPI-linked Ig-superfamily proteins in the mouse genome whose expression profiles need to be determined.…”

Section: Research Articlementioning

confidence: 99%

DrosophilaNeurexin IV stabilizes neuron-glia interactions at the CNS midline by binding to Wrapper

et al. 2009

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Ensheathment of axons by glial membranes is a key feature of complex nervous systems ensuring the separation of single axons or axonal fascicles. Nevertheless, the molecules that mediate the recognition and specific adhesion of glial and axonal membranes are largely unknown. We use the Drosophila midline of the embryonic central nervous system as a model to investigate these neuron glia interactions. During development, the midline glial cells acquire close contact to commissural axons and eventually extend processes into the commissures to wrap individual axon fascicles. Here, we show that this wrapping of axons depends on the interaction of the neuronal transmembrane protein Neurexin IV with the glial Ig-domain protein Wrapper. Although Neurexin IV has been previously described to be an essential component of epithelial septate junctions (SJ), we show that its function in mediating glial wrapping at the CNS midline is independent of SJ formation. Moreover, differential splicing generates two different Neurexin IV isoforms. One mRNA is enriched in septate junction-forming tissues, whereas the other mRNA is expressed by neurons and recruited to the midline by Wrapper. Although both Neurexin IV isoforms are able to bind Wrapper, the neuronal isoform has a higher affinity for Wrapper. We conclude that Neurexin IV can mediate different adhesive cell-cell contacts depending on the isoforms expressed and the context of its interaction partners.

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The Drosophila cell adhesion molecule Klingon is required for long-term memory formation and is regulated by Notch

Cited by 44 publications

References 34 publications

The Genetics of Alcohol Responses of Invertebrate Model Systems

The Genetics of Alcohol Responses of Invertebrate Model Systems

dEHBP1 regulates Scabrous secretion during Notch mediated lateral inhibition

DrosophilaNeurexin IV stabilizes neuron-glia interactions at the CNS midline by binding to Wrapper

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