2008
DOI: 10.1152/ajprenal.00391.2007
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Inhibition of proinflammatory genes in anti-GBM glomerulonephritis by targeted dexamethasone-loaded AbEsel liposomes

Abstract: E-selectin-directed targeted drug delivery was analyzed in anti-glomerular basement membrane glomerulonephritis. Liposomes conjugated with anti-E-selectin antibodies (Ab(Esel) liposomes) were internalized by activated endothelial cells in vitro through E-selectin-mediated endocytosis. At the onset of glomerulonephritis in mice, E-selectin was expressed on glomerular endothelial cells, which resulted in homing of Ab(Esel) liposomes to glomeruli after intravenous administration. Accumulation of Ab(Esel) liposome… Show more

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Cited by 87 publications
(48 citation statements)
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“…Specific targeted delivery of therapeutic agents to kidneys, and even to specific renal cells in the glomeruli or the tubulointerstitium, seems feasible (442)(443)(444)(445)(446)(447) and might open the possibility of using drugs that would otherwise be limited by systemic toxicity. Such approaches may also be combined with contrast agents for non-invasive imaging allowing a ''theranostic'' strategy which is currently mainly being developed for cancer applications.…”
Section: Getting Anti-fibrotic Therapies To the Clinicmentioning
confidence: 99%
“…Specific targeted delivery of therapeutic agents to kidneys, and even to specific renal cells in the glomeruli or the tubulointerstitium, seems feasible (442)(443)(444)(445)(446)(447) and might open the possibility of using drugs that would otherwise be limited by systemic toxicity. Such approaches may also be combined with contrast agents for non-invasive imaging allowing a ''theranostic'' strategy which is currently mainly being developed for cancer applications.…”
Section: Getting Anti-fibrotic Therapies To the Clinicmentioning
confidence: 99%
“…Also, anti-E-selectin ILs loaded with dexamethasone have been tested in vivo and display binding and internalization in a mouse model of skin inflammation [141]. Dexamethasone-loaded Ls conjugated with anti-E-selectin antibodies were shown to be internalized by activated endothelial cells in vitro through E-selectin-mediated endocytosis in an injury model characterized by glomerular renal inflammation [142,303]. These ILs not only show an accumulation in the inflamed kidney 3.6 times higher than non-targeted IgG Ls, but also reduce inflammatory gene expression without affecting blood glucose levels, a severe side effect of administration of free dexamethasone.…”
Section: Inflammatory Diseasesmentioning
confidence: 99%
“…It remains to be determined whether the siRNA/CDP NP system can facilitate gene knockdown in mouse models of kidney disease. However, reports examining nanoparticle delivery to the diseased kidney in animal models [6,9,[32][33][34][35] suggest that nanoparticles have a higher propensity for glomerular deposition in glomerulonephritic states, likely due to increased vascular permeability and inflammation. Thus, the healthy, rather than the diseased kidney, may provide the more restrictive condition for nanoparticle delivery.…”
Section: Discussionmentioning
confidence: 99%