N-methyl-d-aspartate receptor inhibition by an apolipoprotein E-derived peptide relies on low-density lipoprotein receptor-associated protein

Sheng, Zhenyu; Prorok, Mary; Brown, Brigid E.; Castellino, Francis J.

doi:10.1016/j.neuropharm.2008.05.016

Cited by 35 publications

(30 citation statements)

References 59 publications

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“…Another protective mechanism is related to glutamate excitotoxicity. Both apoE protein, as well as its mimetic peptide COG133, can prevent primary neurons from excitotoxicity-induced calcium influx and subsequent cell death (Aono et al, 2002(Aono et al, , 2003 through binding to the low-density lipoprotein receptor-associated protein (Sheng et al, 2008). A similar protective effect of COG112 was recently validated by our laboratory (F.-Q.…”

Section: Discussionmentioning

confidence: 67%

“…Similar to holo-apoE3 protein, COG133 inhibits lipopolysaccharide (LPS)-stimulated microglia activation, reduces TNF-␣ and NO production in vitro (Laskowitz et al, 2001), and suppresses brain and systemic inflammatory responses in LPS-injected mice . Likewise, apoE-mimetic peptides retain the ability to bind LRP1 and other LDL receptors (Croy et al, 2004) and simulate the neuroprotective effect of apoE protein against N-methyl-D-aspartate excitotoxicity (Sheng et al, 2008). To enhance transmembrane permeability, COG133 has been molecularly modified by fusion with a protein transduction domain (PTD) derived from Drosophila antennapedia protein (Antp) to create COG112.…”

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confidence: 99%

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An Apolipoprotein E-Mimetic Stimulates Axonal Regeneration and Remyelination after Peripheral Nerve Injury

Fowler²,

Neil³

et al. 2010

J Pharmacol Exp Ther

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Elevated apolipoprotein E (apoE) synthesis within crushed sciatic nerves advocates that apoE could benefit axonal repair and reconstruction of axonal and myelin membranes. We created an apoE-mimetic peptide, COG112 (acetyl-RQIKIWFQNRRMK-WKKCLRVRLASHLRKLRKRLL-amide), and found that postinjury treatment with COG112 significantly improved recovery of motor and sensory function following sciatic nerve crush in C57BL/6 mice. Morphometric analysis of injured sciatic nerves revealed that COG112 promoted axonal regrowth after 2 weeks of treatment. More strikingly, the thickness of myelin sheaths was increased by COG112 treatment. Consistent with these histological findings, COG112 potently elevated growth associated protein 43 (GAP-43) and peripheral myelin protein zero (P0), which are markers of axon regeneration and remyelination, respectively. Electron microscopic examination further suggested that the apoE-mimetic COG112 may increase clearance of myelin debris. Schwann cell uptake of cholesterol-containing low-density lipoprotein particles was selectively enhanced by COG112 treatment in a Schwann cell line S16. Moreover, COG112 significantly promoted axon elongation in primary dorsal root ganglion cultures from rat pups. Considering that cholesterol and lipids are needed for reconstructing myelin sheaths and axon extension, these data support a hypothesis where supplementation with exogenous apoE-mimetics such as COG112 may be a promising strategy for restoring lost functional and structural elements following nerve injury.

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Section: Discussionmentioning

confidence: 67%

mentioning

confidence: 99%

An Apolipoprotein E-Mimetic Stimulates Axonal Regeneration and Remyelination after Peripheral Nerve Injury

Fowler²,

Neil³

et al. 2010

J Pharmacol Exp Ther

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“…In neurons, LRP1 signaling requires the NMDA-R as an essential co-receptor (Bacskai et al, 2000;Qiu et al, 2002;Samson et al, 2008;Martin et al, 2008;Sheng et al, 2008;Mantuano et al, 2013). Other LRP1 co-receptors in neurons include Trk receptors and p75 NTR (Shi et al, 2009;Yoon et al, 2013;Stiles et al, 2013).…”

Section: Nmda-r Is Necessary For Lrp1 Signaling In Schwann Cellsmentioning

confidence: 99%

“…Based on its interaction with LRP1, the NMDA-R functions as an essential signaling co-receptor for LRP1 ligands, including α 2 -macroglobulin (α 2 M), tissue-type plasminogen activator (tPA) and apolipoprotein E (Bacskai et al, 2000;Qiu et al, 2002;Samson et al, 2008;Martin et al, 2008;Sheng et al, 2008;Mantuano et al, 2013). LRP1 ligands have been implicated in neuronal survival (Hayashi et al, 2007;Fuentealba et al, 2009) and in neurite outgrowth (Mantuano et al, 2008a,b;Shi et al, 2009;Yoon et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

The NMDA receptor functions independently and as an LRP1 co-receptor to promote Schwann cell survival and migration

Mantuano

Lam

Shibayama

et al. 2015

Journal of Cell Science

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NMDA receptors (NMDA-Rs) are ionotropic glutamate receptors, which associate with LDL-receptor-related protein-1 (LRP1) to trigger cell signaling in response to protein ligands in neurons. Here, we demonstrate for the first time that the NMDA-R is expressed by rat Schwann cells and functions independently and with LRP1 to regulate Schwann cell physiology. The NR1 (encoded by GRIN1) and NR2b (encoded by GRIN2B) NMDA-R subunits were expressed by cultured Schwann cells and upregulated in sciatic nerves following crush injury. The ability of LRP1 ligands to activate ERK1/2 (also known as MAPK3 and MAPK1, respectively) and promote Schwann cell migration required the NMDA-R. NR1 gene silencing compromised Schwann cell survival. Injection of the LRP1 ligands tissue-type plasminogen activator (tPA, also known as PLAT) or MMP9-PEX into crush-injured sciatic nerves activated ERK1/2 in Schwann cells in vivo, and the response was blocked by systemic treatment with the NMDA-R inhibitor MK801. tPA was unique among the LRP1 ligands examined because tPA activated cell signaling and promoted Schwann cell migration by interacting with the NMDA-R independently of LRP1, albeit with delayed kinetics. These results define the NMDA-R as a Schwann cell signaling receptor for protein ligands and a major regulator of Schwann cell physiology, which may be particularly important in peripheral nervous system (PNS) injury.

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“…Protective effects of apoE have been observed in the context of coagulation, macrophage function, oxidative processes, central nervous system physiology, infl ammation, and cell signaling ( 98,99 ). Data suggest that anti-infl ammatory reduce infl ammatory injury in murine models of multiple sclerosis and traumatic brain injury, respectively, and are thought to mediate their effects via binding to LRP (128)(129)(130).…”

Section: Anti-atherogenic Mechanisms Of Apoe Actionmentioning

confidence: 99%

Anti-inflammatory and cholesterol-reducing properties of apolipoprotein mimetics: a review

White

Garber

Anantharamaiah

2014

Journal of Lipid Research

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N-methyl-d-aspartate receptor inhibition by an apolipoprotein E-derived peptide relies on low-density lipoprotein receptor-associated protein

Cited by 35 publications

References 59 publications

An Apolipoprotein E-Mimetic Stimulates Axonal Regeneration and Remyelination after Peripheral Nerve Injury

An Apolipoprotein E-Mimetic Stimulates Axonal Regeneration and Remyelination after Peripheral Nerve Injury

The NMDA receptor functions independently and as an LRP1 co-receptor to promote Schwann cell survival and migration

Anti-inflammatory and cholesterol-reducing properties of apolipoprotein mimetics: a review

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