2008
DOI: 10.1371/journal.pone.0002469
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A Unique Carrier for Delivery of Therapeutic Compounds beyond the Blood-Brain Barrier

Abstract: BackgroundTherapeutic intervention in many neurological diseases is thwarted by the physical obstacle formed by the blood-brain barrier (BBB) that excludes most drugs from entering the brain from the blood. Thus, identifying efficacious modes of drug delivery to the brain remains a “holy grail” in molecular medicine and nanobiotechnology. Brain capillaries, that comprise the BBB, possess an endogenous receptor that ferries an iron-transport protein, termed p97 (melanotransferrin), across the BBB. Here, we expl… Show more

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Cited by 91 publications
(55 citation statements)
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References 90 publications
(112 reference statements)
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“…Among their many interacting ligands are receptor-associated protein, apolipoprotein E, and melanotransferrin/p97 [131][132][133]. Drug targeting using p97 is perhaps the most studied of these ligands, where injections of the p97-conjugated chemotherapeutics paclitaxel or adriamycin were reported to result in increased brain uptake, with the latter also improving survival in a rat model of intracranial glioma [134]. More recently, Angiochem Inc. has developed a 19-amino-acid peptide against Lrp1, called Angiopep-2, to which paclitaxel was conjugated [135].…”
Section: Other Rmt Targetsmentioning
confidence: 99%
“…Among their many interacting ligands are receptor-associated protein, apolipoprotein E, and melanotransferrin/p97 [131][132][133]. Drug targeting using p97 is perhaps the most studied of these ligands, where injections of the p97-conjugated chemotherapeutics paclitaxel or adriamycin were reported to result in increased brain uptake, with the latter also improving survival in a rat model of intracranial glioma [134]. More recently, Angiochem Inc. has developed a 19-amino-acid peptide against Lrp1, called Angiopep-2, to which paclitaxel was conjugated [135].…”
Section: Other Rmt Targetsmentioning
confidence: 99%
“…To determine the function of mannitol backbone in PMT on BBB permeability, PEI (25 kDa) modified with RVG ligand with bridge of PEG (5 kDa) (R-PEG-PEI) was employed as a control group. Some pharmaceutical nanoparticles use the paracellular route to cross over BBB by accelerating the breakdown of the tight junction [39], while other use the transcellular transport via specific interaction with surface of endothelial cells [14,40]. We examined the integrity of in vitro BBB tight junction at pre-and pro-treatment of complexes to assess the possible risk by breakdown of BBB.…”
Section: In Vitro Bbb Permeability Of R-peg-pmt/sirna Complexesmentioning
confidence: 99%
“…Evidence for BCEC targeting and subsequent brain transport in vivo have been published with peptide vectors (Kumar et al, 2007;Demeule et al, 2008;Hervé et al, 2008), lowdensity lipoprotein receptor (Pan et al, 2004), transferrin (Skarlatos et al, 1995), and melanotransferrin (Demeule et al, 2002;Karkan et al, 2008). However, the most numerous data were obtained with monoclonal antibodies (MAbs) targeting the insulin (Coloma et al, 2000;Zhang et al, 2003a) or transferrin receptors (TfR) Shi and Pardridge, 2000;Zhang et al, 2003b).…”
Section: Introductionmentioning
confidence: 99%