Chronic enzyme replacement therapy ameliorates neuropathology in alpha‐mannosidosis mice

Damme, Markus; Lüdemann, Meike; Rothaug, Michelle; Lüllmann‐Rauch, Renate; Beck, Hans Christian; Ericsson, Annika; Andersson, Claes; Fogh, Jørgen; D’Hooge, Rudi; Säftig, Paul; Blanz, Judith

doi:10.1002/acn3.245

Cited by 8 publications

(7 citation statements)

References 55 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Storage material was prepared for mass spectrometry analysis as previously described ( Damme et al, 2015 ). Briefly urine samples and water extracts of TLC-isolated compounds were centrifuged at 14,000 g for 20 min, and 10 µl of extract were mixed with 10 µl of a 0.01 nmol/µl maltotriose internal standard.…”

Section: Methodsmentioning

confidence: 99%

A mouse model for fucosidosis recapitulates storage pathology and neurological features of the milder form of the human disease

Wolf

Damme

D’Hooge

et al. 2016

Disease Models &Amp; Mechanisms

Self Cite

View full text Add to dashboard Cite

Fucosidosis is a rare lysosomal storage disorder caused by the inherited deficiency of the lysosomal hydrolase α-L-fucosidase, which leads to an impaired degradation of fucosylated glycoconjugates. Here, we report the generation of a fucosidosis mouse model, in which the gene for lysosomal α-L-fucosidase (Fuca1) was disrupted by gene targeting. Homozygous knockout mice completely lack α-L-fucosidase activity in all tested organs leading to highly elevated amounts of the core-fucosylated glycoasparagine Fuc(α1,6)-GlcNAc(β1-N)-Asn and, to a lesser extent, other fucosylated glycoasparagines, which all were also partially excreted in urine. Lysosomal storage pathology was observed in many visceral organs, such as in the liver, kidney, spleen and bladder, as well as in the central nervous system (CNS). On the cellular level, storage was characterized by membrane-limited cytoplasmic vacuoles primarily containing water-soluble storage material. In the CNS, cellular alterations included enlargement of the lysosomal compartment in various cell types, accumulation of secondary storage material and neuroinflammation, as well as a progressive loss of Purkinje cells combined with astrogliosis leading to psychomotor and memory deficits. Our results demonstrate that this new fucosidosis mouse model resembles the human disease and thus will help to unravel underlying pathological processes. Moreover, this model could be utilized to establish diagnostic and therapeutic strategies for fucosidosis.

show abstract

Section: Methodsmentioning

confidence: 99%

A mouse model for fucosidosis recapitulates storage pathology and neurological features of the milder form of the human disease

Wolf

Damme

D’Hooge

et al. 2016

Disease Models &Amp; Mechanisms

Self Cite

View full text Add to dashboard Cite

show abstract

“…As a next step, we studied the uptake and processing of rhCTSD in CTSD-deficient mice (ctsd -/-). For this purpose, a range of enzyme concentrations was firstly tested taking into account previous studies with other recombinant lysosomal enzymes (not shown) [18][19][20]. Based on these preliminary tests, we decided to give postnatal day 20 (P20) ctsd -/animals a dose of 25 mg/kg of rhCTSD by intravenous (i.v.)…”

Section: Uptake Of Rhctsd In the Cln10 Mouse Modelmentioning

confidence: 99%

“…ERT aims to replace the defective hydrolase by a recombinantly produced enzyme, typically administered by intravenous injection and delivered to the lysosomes via receptor-mediated endocytosis. We have previously developed an ERT strategy to treat αmannosidosis, a LSD caused by the deficiency of the lysosomal acid hydrolase MAN/α-mannosidase [18][19][20]. The treatment of patients with the engineered human MAN/α-mannosidase (velmanase alfa) has been recently approved in Europe [21].…”

Section: Introductionmentioning

confidence: 99%

Enzyme replacement therapy with recombinant pro-CTSD (cathepsin D) corrects defective proteolysis and autophagy in neuronal ceroid lipofuscinosis

et al. 2019

Self Cite

View full text Add to dashboard Cite

CTSD (cathepsin D) is one of the major lysosomal proteases indispensable for the maintenance of cellular proteostasis by turning over substrates of endocytosis, phagocytosis and autophagy. Consequently, CTSD deficiency leads to a strong impairment of the lysosomal-autophagy machinery. In mice and humans CTSD dysfunction underlies the congenital variant (CLN10) of neuronal ceroid lipofuscinosis (NCL). NCLs are distinct lysosomal storage disorders (LSDs) sharing various hallmarks, namely accumulation of protein aggregates and ceroid lipofuscin leading to neurodegeneration and blindness. The most established and clinically approved approach to treat LSDs is enzyme replacement therapy (ERT) aiming to replace the defective hydrolase with an exogenously applied recombinant protein. Here we reveal that recombinant human pro-CTSD produced in a mammalian expression system can be efficiently taken up by a variety of cell models, is correctly targeted to lysosomes and processed to the active mature form of the protease. In proof-of-principle experiments we provide evidence that recombinant human CTSD (rhCTSD) can improve the biochemical phenotype of CTSDdeficient hippocampal slice cultures in vitro and retinal cells in vivo. Furthermore, we demonstrate that dosing of rhCTSD in the murine CLN10 model leads to a correction of lysosomal hypertrophy, storage accumulation and impaired autophagic flux in the viscera and central nervous system (CNS). We establish that direct delivery of the recombinant protease to the CNS is required for improvement of neuropathology and lifespan extension. Together these data support the continuation of the pre-clinical studies for the application of rhCTSD in the treatment of NCL.

show abstract

“…High doses are probably necessary because the injected enzyme is quickly captured by visceral organs and thus the bioavailability of the enzyme is rapidly reduced. Recently, to overcome the immunological problems associated with ERT in alpha-mannosidosis mice, an immune-tolerant mouse model of alpha-mannosidosis was generated [ 66 ]. This mouse model allowed for an evaluation of the effect of high-dose long-term ERT on CSF pathology using rhLAMAN.…”

Section: Enzyme Replacement Therapymentioning

confidence: 99%

Alpha-Mannosidosis: Therapeutic Strategies

Ceccarini

Codini

Conte

et al. 2018

IJMS

View full text Add to dashboard Cite

Alpha-mannosidosis (α-mannosidosis) is a rare lysosomal storage disorder with an autosomal recessive inheritance caused by mutations in the gene encoding for the lysosomal α-d-mannosidase. So far, 155 variants from 191 patients have been identified and in part characterized at the biochemical level. Similarly to other lysosomal storage diseases, there is no relationship between genotype and phenotype in alpha-mannosidosis. Enzyme replacement therapy is at the moment the most effective therapy for lysosomal storage disease, including alpha-mannosidosis. In this review, the genetic of alpha-mannosidosis has been described together with the results so far obtained by two different therapeutic strategies: bone marrow transplantation and enzyme replacement therapy. The primary indication to offer hematopoietic stem cell transplantation in patients affected by alpha-mannosidosis is preservation of neurocognitive function and prevention of early death. The results obtained from a Phase I–II study and a Phase III study provide evidence of the positive clinical effect of the recombinant enzyme on patients with alpha-mannosidosis.

show abstract

Chronic enzyme replacement therapy ameliorates neuropathology in alpha‐mannosidosis mice

Cited by 8 publications

References 55 publications

A mouse model for fucosidosis recapitulates storage pathology and neurological features of the milder form of the human disease

A mouse model for fucosidosis recapitulates storage pathology and neurological features of the milder form of the human disease

Enzyme replacement therapy with recombinant pro-CTSD (cathepsin D) corrects defective proteolysis and autophagy in neuronal ceroid lipofuscinosis

Alpha-Mannosidosis: Therapeutic Strategies

Contact Info

Product

Resources

About