Disruption of hippocampal development
            <i>in vivo</i>
            by CR-50 mAb against Reelin

Nakajima, Kazunori; Mikoshiba, Katsuhiko; Miyata, Takaki; Kudo, Chikako; Ogawa, Michio

doi:10.1073/pnas.94.15.8196

Cited by 160 publications

(119 citation statements)

References 40 publications

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“…After binding to lipoprotein receptors on the cell surface, Reln is internalized into vesicles. Binding of Reln to the receptors is inhibited by mAb CR-50, which blocks Reln function in vivo and in vitro (D'Arcangelo et al 1995(D'Arcangelo et al , 1999Ogawa et al 1995;Del Rio et al 1997;Nakajima et al 1997). These findings imply that Reln is a physiological ligand for lipoprotein receptors in the brain.…”

Section: Reln Is a Ligand For Lipoprotein Receptorsmentioning

confidence: 57%

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Mutant mice with scrambled brains: understanding the signaling pathways that control cell positioning in the CNS

Rice¹,

Curran²

1999

Genes & Development

141

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Section: Reln Is a Ligand For Lipoprotein Receptorsmentioning

confidence: 57%

“…1). This abnormality can be recapitulated in rotating cultures of reeler neurons or by incubating normal neurons with the CR-50 antibody, which inhibits Reln function (Ogawa et al 1995;Nakajima et al 1997). The mechanism responsible for this phenotype is not clear.…”

Section: Reln and Cortical Developmentmentioning

confidence: 99%

Mutant mice with scrambled brains: understanding the signaling pathways that control cell positioning in the CNS

Rice¹,

Curran²

1999

Genes & Development

141

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“…It also increases their gating (25). NR2 phosphorylation by Reelin is greatly reduced in the presence of a high concentration of 1 M A␤ [25][26][27][28][29][30][31][32][33][34][35] (Fig. 2 A, lane 4).…”

Section: Resultsmentioning

confidence: 94%

“…1B, closed circles). This suppression was again fully reversible by co-application of Reelin (closed triangles), indicating that LTP suppression induced by low concentrations of A␤ 1-42 or A␤ [25][26][27][28][29][30][31][32][33][34][35] was not caused by a non-specific cytotoxic effect.We have reported earlier (20) that Reelin increases tyrosine phosphorylation of NR2A as well as NR2B subunits (Fig. 2A, lane 2, Upper and Lower, respectively).…”

mentioning

confidence: 88%

“…Consistent with the findings in other laboratories, monomeric A␤ 1-42 (1°) was ineffective. A truncated form of the A␤ peptide consisting only of amino acids 25 to 35 (A␤ [25][26][27][28][29][30][31][32][33][34][35] ), which form the minimal fibrillogenic region was also able to potently suppress baseline LTP at consistently lower concentrations (100 nM; Fig. 1B, closed circles).…”

mentioning

confidence: 99%

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Reelin signaling antagonizes β-amyloid at the synapse

Durakoglugil¹,

Chen²,

White³

et al. 2009

Proc. Natl. Acad. Sci. U.S.A.

137

138

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Abnormal processing of the amyloid precursor protein (APP) and ␤-amyloid (A␤) plaque accumulation are defining features of Alzheimer disease (AD), a genetically complex neurodegenerative disease that is characterized by progressive synapse loss and neuronal cell death. A␤ induces synaptic dysfunction in part by altering the endocytosis and trafficking of AMPA and NMDA receptors. Reelin is a neuromodulator that increases glutamatergic neurotransmission by signaling through the postsynaptic ApoE receptors Apoer2 and Vldlr and thereby potently enhances synaptic plasticity. Here we show that Reelin can prevent the suppression of long-term potentiation and NMDA receptors, which is induced by levels of A␤ comparable to those present in an AD-afflicted brain. This reversal is dependent upon the activation of Src family tyrosine kinases. At high concentrations of A␤ peptides, Reelin can no longer overcome the A␤ induced functional suppression and this coincides with a complete blockade of the Reelin-dependent phosphorylation of NR2 subunits. We propose a model in which A␤, Reelin, and ApoE receptors modulate neurotransmission and thus synaptic stability as opposing regulators of synaptic gain control.Alzheimer disease ͉ apolipoprotein E ͉ long-term potentiation ͉ NMDA receptor ͉ A␤ oligomer A lzheimer disease (AD) is a complex genetic neurodegenerative disease that afflicts an increasing fraction of our aging population (1). A characteristic feature of AD is the accumulation of oligomeric and higher-order aggregates of the A␤ 1-42 form of the amyloid-␤ (A␤) peptide, which is physiologically released by sequential proteolytic cleavage from the amyloid-␤ precursor protein (APP) (2, 3). Abnormal, amyloidogenic A␤ processing and plaque formation progressively lead to synaptic dysfunction, synapse loss, and ultimately neuronal death.Recent insight into the pathophysiological functions of A␤ came from studies that demonstrated a potent negative impact of A␤ oligomers on synaptic functions that underlie long-term synaptic plasticity (4-6). Incubation of hippocampal neurons and slices with A␤ oligomers leads to intracellular trapping or functional impairment of AMPA and NMDA-type glutamate receptors (7-9), thereby decreasing long-term potentiation (LTP), an enhancement of synaptic strength that is correlated with memory (4, 5, 10-13). Consistent with these in vitro findings, Palop et al. (14,15) showed that overexpression of mutant APP forms in mice resulted in a global dysregulation of neuronal network activity in vivo.Reelin is a signaling protein that is produced by interneurons in the brain and that has an effect on synaptic functions that is opposite to that of A␤ oligomers. Reelin addition to hippocampal slices results in enhanced LTP (16) as a result of the activation of Src family tyrosine kinases (SFKs) (17-19), which increase NMDA receptor activity by tyrosine phosphorylation of their NR2 subunits (20,21). These effects of Reelin are mediated by a pair of homologous cell surface receptors designated apolipoprotein E r...

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Integrin ?1 localization in murine central and peripheral nervous system

Murase

Hayashi

1998

J. Comp. Neurol.

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The distribution of neurons expressing integrin alpha1 subunit protein (INTalpha1) was examined in adult mouse tissues of not only the central nervous system, but also the sympathetic ganglia, and the adrenal gland by immunohistochemistry and immunoelectron microscopy. INTalpha1-positive neurons were observed in most tissues examined, and most of them were found to coexpress tyrosine hydroxylase (TH) except for Purkinje cells and hippocampal neurons. Expression of INTalpha1 was also observed in the malpositioned cortical neurons in reeler mutants, and appeared not to be affected by the aberrant cell migration of the reeler cortical neurons. In situ hybridization showed that the expression of INTalpha1 mRNA was correlated with synthesis of the INTalpha1 protein in each case, and this finding indicated that expression of the protein was controlled by transcriptional regulation of the INTalpha1 gene.

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Disruption of hippocampal development in vivo by CR-50 mAb against Reelin

Cited by 160 publications

References 40 publications

Mutant mice with scrambled brains: understanding the signaling pathways that control cell positioning in the CNS

Mutant mice with scrambled brains: understanding the signaling pathways that control cell positioning in the CNS

Reelin signaling antagonizes β-amyloid at the synapse

Integrin ?1 localization in murine central and peripheral nervous system

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