2012
DOI: 10.1016/j.neulet.2012.07.040
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Intranasal delivery of HMGB1-binding heptamer peptide confers a robust neuroprotection in the postischemic brain

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Cited by 33 publications
(26 citation statements)
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“…Interestingly, NMDAR activation also causes HMGB1 cytoplasmic translocation and release. Cytosolic HMGB1 can bind to Beclin-1 to limit death by upregulated autophagy (Perez-Carrion and Cena, 2013), whereas extracellular HMGB1 plays both negative and positive roles in the regulation of neuronal cell death (Kim et al, 2010a; Kim et al, 2012c; Kim et al, 2006; Kim et al, 2012d; Kim et al, 2011b). A recent coimmunoprecipitation study demonstrated that HMGB1 physiologically interacts with GluN1 and GluN2B subunits of NMDAR via a specific region of HMGB1 localized in the B box upstream from the RAGE and downstream from the TLR4 binding sites (Pedrazzi et al, 2012).…”
Section: Hmgb1 Receptors (Figure 7)mentioning
confidence: 99%
“…Interestingly, NMDAR activation also causes HMGB1 cytoplasmic translocation and release. Cytosolic HMGB1 can bind to Beclin-1 to limit death by upregulated autophagy (Perez-Carrion and Cena, 2013), whereas extracellular HMGB1 plays both negative and positive roles in the regulation of neuronal cell death (Kim et al, 2010a; Kim et al, 2012c; Kim et al, 2006; Kim et al, 2012d; Kim et al, 2011b). A recent coimmunoprecipitation study demonstrated that HMGB1 physiologically interacts with GluN1 and GluN2B subunits of NMDAR via a specific region of HMGB1 localized in the B box upstream from the RAGE and downstream from the TLR4 binding sites (Pedrazzi et al, 2012).…”
Section: Hmgb1 Receptors (Figure 7)mentioning
confidence: 99%
“…Also, this nose to brain route bypasses the BBB and avoids drug elimination by the liver and gastrointestinal tract and filtration through the kidney [44,45]. Especially, we demonstrated the potency of the intranasal approach using siRNA or protein-containing nanoparticles in post-ischemic brain [41,46,47]. Therefore, we estimated the possibility of the NCs for ATP delivery via an intranasal administration route.…”
Section: Basementioning
confidence: 89%
“…Furthermore, the study provides evidence that HBHP suppresses LCM-induced microglial activation, and that this is achieved by its direct binding to HMGB1 A box. In a previous report, we found that intranasal delivered HBHP ameliorates neuronal damage in the postischemic rat brain, and that HBHP confers neuroprotection to NMDA- or Zn 2+ -treated primary cortical cultures, wherein HBHP interacts with accumulated HMGB1 in NMDA-conditioned media [19]. Under pathological conditions, including that of the postischemic brain, where HMGB1 might be released from neurons after an excitotoxic insult [3] or secreted from activated microglia (Figs.…”
Section: Discussionmentioning
confidence: 99%
“…In a previous study, we found that a HMGB1-binding heptamer peptide (HBHP) with the HMSKPVQ sequence, which directly binds with HMGB1 under cell free conditions and in NMDA-conditioned media (MCM), exerted a neuroprotective effect in the rat postischemic brain [19]. Moreover, intranasally delivered HBHP suppressed infarct formation in the rat brain after MCAO and ameliorated neurological deficits [19]. In the present study, we investigated whether HBHP confers anti-inflammatory effects on cultured primary microglia, and whether its effects are attributable to direct binding to HMGB1.…”
Section: Introductionmentioning
confidence: 99%