2012
DOI: 10.4161/pri.20197
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Brain delivery of AAV9 expressing an anti-PrP monovalent antibody delays prion disease in mice

Abstract: (2012) Brain delivery of AAV9 expressing an anti-PrP monovalent antibody delays prion disease in mice, Prion, 6:4,[383][384][385][386][387][388][389][390]

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Cited by 27 publications
(27 citation statements)
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References 39 publications
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“…Recently, passive immunization has been extensively investigated ( Figure 1). 63,68,96,[108][109][110][111][112][113] Transgenic expression of the µ heavy chain of anti-PrP antibody 6H4 in PRNP -/-mice was found to completely prevent prion infection after intraperitoneal PrP Sc administration. 68 The most common way of administering anti-prion antibodies to prion-infected mice is peripherally.…”
Section: Passive Immunizationmentioning
confidence: 99%
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“…Recently, passive immunization has been extensively investigated ( Figure 1). 63,68,96,[108][109][110][111][112][113] Transgenic expression of the µ heavy chain of anti-PrP antibody 6H4 in PRNP -/-mice was found to completely prevent prion infection after intraperitoneal PrP Sc administration. 68 The most common way of administering anti-prion antibodies to prion-infected mice is peripherally.…”
Section: Passive Immunizationmentioning
confidence: 99%
“…Novel scFv variants with improved stability can be selected from large randomly mutated phage-displayed libraries with a specific antigen, [120][121][122] and phage display has been successfully used in engineering anti-prion antibodies. 110,123 An scFv version of a PrP-specific full-length antibody (6H4) has been demonstrated therapeutic 63,68 and to increase PrP Sc clearance when secreted from stably transfected and cultured cells. 117 Serotype 2 of AAV (AAV2) is one of the most commonly used vectors for brain delivery.…”
Section: Passive Immunizationmentioning
confidence: 99%
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“…The advantage of VHs and scFvs is the single polypeptide sequence used for the gene transfer-based passive immunisation. Studies conducted by Moda et al [124] and Wuertzer et al [125] investigated vectors for antibody gene delivery to both periphery and brain areas and highlighted two: AAV2 and AAV9 showing a promising delay in the onset of clinical signs of the disease, prolonged survival time, milder neuropathological changes, reduced PrP SC in brain and more importantly, no inflammation and neurotoxicity. An additional benefit of intrabodies is the ability to design them to target a specific cellular compartment.…”
Section: Transmissible Spongiform Encephalopathy: Targeting Prionmentioning
confidence: 99%