Developmentally regulated mannose 6-phosphate receptor-mediated transport of a lysosomal enzyme across the blood-brain barrier

Urayama, Akihiko; Grubb, Jeffrey H.; Sly, William S.; Banks, William A.

doi:10.1073/pnas.0405042101

Cited by 146 publications

(147 citation statements)

References 40 publications

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“…injection. To determine the extent of delivery of sGCmApoB and sGFPmApoB to the CNS, adult mice (Ͼ8 weeks) were used to mimic the BBB environment observed in the patient (12).…”

Section: Resultsmentioning

confidence: 99%

Targeted delivery of proteins across the blood–brain barrier

Spencer

Verma

2007

Proc. Natl. Acad. Sci. U.S.A.

208

163

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Treatment of many neuronal degenerative disorders will require delivery of a therapeutic protein to neurons or glial cells across the whole CNS. The presence of the blood-brain barrier hampers the delivery of these proteins from the blood, thus necessitating a new method for delivery. Receptors on the blood-brain barrier bind ligands to facilitate their transport to the CNS; therefore, we hypothesized that by targeting these receptors, we may be able to deliver proteins to the CNS for therapy. Here, we report the use of the lentivirus vector system to deliver the lysosomal enzyme glucocerebrosidase and a secreted form of GFP to the neurons and astrocytes in the CNS. We fused the low-density lipoprotein receptor-binding domain of the apolipoprotein B to the targeted protein. This approach proved to be feasible for delivery of the protein and could possibly be used as a general method for delivery of therapeutic proteins to the CNS. fusion protein ͉ lentiviral vectors ͉ low-density lipoprotein receptor

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“…injection. To determine the extent of delivery of sGCmApoB and sGFPmApoB to the CNS, adult mice (Ͼ8 weeks) were used to mimic the BBB environment observed in the patient (12).…”

Section: Resultsmentioning

confidence: 99%

Targeted delivery of proteins across the blood–brain barrier

Spencer

Verma

2007

Proc. Natl. Acad. Sci. U.S.A.

208

163

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“…To visualize the distribution of endosomal compartments, we used antibodies against early endosome antigen 1 (EEA1) [26][27][28] and cation-independent mannose-6-phosphate receptor (CI-MPR) 26,35 as the early and late endosomal markers, respectively. As shown in Figure 3a, the early and the late endosomal markers were largely separated.…”

Section: Tracking Of Viral Transport Through Endosomesmentioning

confidence: 99%

Visualization of targeted transduction by engineered lentiviral vectors

Joo

Wang

2008

Gene Ther

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“…According to Sly and coworkers using recombinant GUS in preclinical ERT studies with MPSVII mice,24, 34 mannose‐6 phosphate receptors (MPRs) that are responsible for intracellular lysosomal targeting of most lysosomes enzymes and their cellular uptake35, 36 cannot account for the uptake of recombinant lysosomal enzymes into adult brain due to their restricted expression in brain endothelial cells within the perinatal period (2 weeks after birth). In adult animals which lack expression of endothelial MPRs, administration of recombinant enzymes bearing mannose 6‐phosphate (M6P) residues might even diminish their uptake into brain as demonstrated for GUS 24, 30, 34. Of note, recombinant rhLAMAN which, in comparison with other lysosomal enzymes, is highly efficient in clearance of brain primary substrate storage is only marginally phosphorylated, suggesting primarily M6P‐independent uptake 16.…”

Section: Discussionmentioning

confidence: 99%

Chronic enzyme replacement therapy ameliorates neuropathology in alpha‐mannosidosis mice

Damme

Lüdemann

Rothaug

et al. 2015

Ann Clin Transl Neurol

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ObjectiveThe lysosomal storage disease alpha‐mannosidosis is caused by the deficiency of the lysosomal acid hydrolase alpha‐mannosidase (LAMAN) leading to lysosomal accumulation of neutral mannose‐linked oligosaccharides throughout the body, including the brain. Clinical findings in alpha‐mannosidosis include skeletal malformations, intellectual disabilities and hearing impairment. To date, no curative treatment is available. We previously developed a beneficial enzyme replacement therapy (ERT) regimen for alpha‐mannosidase knockout mice, a valid mouse model for the human disease. However, humoral immune responses against the injected recombinant human alpha‐mannosidase (rhLAMAN) precluded long‐term studies and chronic treatment.MethodsHere, we describe the generation of an immune‐tolerant alpha‐mannosidosis mouse model that allowed chronic injection of rhLAMAN by transgenic expression of a catalytically inactive variant of human LAMAN in the knockout background.ResultsChronic ERT of rhLAMAN revealed pronounced effects on primary substrate storage throughout the brain, normalization of lysosomal enzyme activities and morphology as well as a decrease in microglia activation. The positive effect of long‐term ERT on neuronal lysosomal function was reflected by an improvement of cognitive deficits and exploratory activity. in vivo and in vitro uptake measurements indicate rapid clearance of rhLAMAN from circulation and a broad uptake into different cell types of the nervous system.InterpretationOur data contribute to the understanding of neurological disorders treatment by demonstrating that lysosomal enzymes such as rhLAMAN can penetrate into the brain and is able to ameliorate neuropathology.

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Developmentally regulated mannose 6-phosphate receptor-mediated transport of a lysosomal enzyme across the blood-brain barrier

Cited by 146 publications

References 40 publications

Targeted delivery of proteins across the blood–brain barrier

Targeted delivery of proteins across the blood–brain barrier

Visualization of targeted transduction by engineered lentiviral vectors

Chronic enzyme replacement therapy ameliorates neuropathology in alpha‐mannosidosis mice

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