2016
DOI: 10.1523/jneurosci.0322-16.2016
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Roles of Cbln1 in Non-Motor Functions of Mice

Abstract: The cerebellum is thought to be involved in cognitive functions in addition to its well established role in motor coordination and motor learning in humans. Cerebellin 1 (Cbln1) is predominantly expressed in cerebellar granule cells and plays a crucial role in the formation and function of parallel fiber-Purkinje cell synapses. Although genes encoding Cbln1 and its postsynaptic receptor, the delta2 glutamate receptor (GluD2), are suggested to be associated with autistic-like traits and many psychiatric disorde… Show more

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Cited by 61 publications
(52 citation statements)
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References 56 publications
(49 reference statements)
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“…Only Cbln1 KO mice have been analyzed in detail, and exhibit a phenotype that is virtually identical to that of GluD2 KO mice (Hirai et al, 2005; Otsuka et al, 2016; Kusnoor et al, 2010; Ito-Ishida et al, 2008 and 2014). The fact that Nrxn1 and Nrxn3 are essential for survival (Missler et al, 2003; Aoto et al, 2015), but their binding partners cerebellins and GluD2 are not, may be due to the interactions of neurexins with many different postsynaptic partners, whereas Cbln1 and Cbln2 and GluD2 appear to only bind to each other and to neurexins, and thus only mediate part of the overall functions of neurexins.…”
Section: Cerebellinsmentioning
confidence: 99%
See 1 more Smart Citation
“…Only Cbln1 KO mice have been analyzed in detail, and exhibit a phenotype that is virtually identical to that of GluD2 KO mice (Hirai et al, 2005; Otsuka et al, 2016; Kusnoor et al, 2010; Ito-Ishida et al, 2008 and 2014). The fact that Nrxn1 and Nrxn3 are essential for survival (Missler et al, 2003; Aoto et al, 2015), but their binding partners cerebellins and GluD2 are not, may be due to the interactions of neurexins with many different postsynaptic partners, whereas Cbln1 and Cbln2 and GluD2 appear to only bind to each other and to neurexins, and thus only mediate part of the overall functions of neurexins.…”
Section: Cerebellinsmentioning
confidence: 99%
“…The loss of Cbln1 signaling may cause distinct downstream, region-dependent effects on synapse stability, accounting for the different phenotypes of Cbln1-deficient cerebellum and striatum. Moreover, Cbln1 was shown to be essential for hippocampal learning by an unknown mechanism, even though cerebellins are not expressed in the hippocampus proper (Otsuka et al, 2016). Thus, our understanding of Cbln1 function is incomplete, and even less is known about the functions of Cbln2 and Cbln4.…”
Section: Cerebellinsmentioning
confidence: 99%
“…Here, Cbln1‐deficient thalamic axons exhibited an increase in synaptic spine density instead of a synapse loss, suggesting that cerebellins may in general perform a signaling function instead of a synapse‐formation function. Moreover, Cbln1 was shown to be essential for hippocampal learning by an unknown mechanism (Otsuka et al, ). Although our understanding of Cbln1 function is thus incomplete, even less is known about the expression patterns and functions of Cbln2 and Cbln4.…”
Section: Introductionmentioning
confidence: 99%
“…Two out of the remaining five neuronal clusters can be classified as GABAergic interneurons (GIs, neurod6a+ and gabrb3+ ) (Butt et al, 2007; Lujan et al, 2005; Ohtsuka et al, 2011) and based on Parvalbumin expression can be separated into pvalb7a+ GIs (GIs+) and pvalb7a− GIs (GIs−) (Figure 2; Dataset S1B). The remaining three clusters are comprised of commissural neurons (CN, cbln1+ and eomesa+ ) (Cameron et al, 2012; Otsuka et al, 2016), corticospinal projection/Cajal-Retzius neurons (CPN, lhx5+ and tbr1b+ ) (Bedogni et al, 2010; Miquelajauregui et al, 2010) and motor neuron progenitors/excitatory neuron progenitors (MNP, eomesa+ and ets2+ ) (Cameron et al, 2012; Lake et al, 2016). We could also verify the initial clustering of cell types with further markers such as endothelium ( cd9b , aplnrb ) (Klein-Soyer et al, 2000; Reaux et al, 2001), neuroepithelium ( krt18 , tagln2 ) (Lee et al, 2014; Merrick et al, 1995; Pollen et al, 2015) and mixed immune cells ( pfn1 and cd74 ) (Fan et al, 2014; Gil-Yarom et al, 2017).…”
Section: Resultsmentioning
confidence: 99%