Your search keyword '"Steven Q. Le"' showing total 66 results

1. Combining angiotensin receptor blockade and enzyme replacement therapy for vascular disease in mucopolysaccharidosis type I

Author

Sarah C. Hurt, Moin U. Vera, Steven Q. Le, Shih-hsin Kan, Quang Bui, and Patricia I. Dickson

Subjects

Lysosomal storage disease, Hurler, Scheie, Hurler-Scheie, Losartan, Alpha-L-iduronidase, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Vascular involvement in the genetic disorder mucopolysaccharidosis type I (MPS I) has features of atherosclerotic disease near branch points of arterial vasculature, such as intimal thickening with disruption of the internal elastic lamina, and proliferation of macrophages and myofibroblasts. Inflammatory pathways are implicated in the pathogenesis of vascular disease in MPS I animal models, evidenced by cytokines like CD18 and TGF-β within arterial plaques. The angiotensin II-mediated inflammatory pathway is well studied in human atherosclerotic coronary artery disease. Recent work indicates treatment with the angiotensin receptor blocker losartan may improve vascular MPS I disease in mouse models. Here, we combined losartan with the standard therapy for MPS I, enzyme replacement therapy (ERT), to measure effects on cytokines in serum and aortic vasculature. Each treatment group (losartan, ERT, and their combination) equally normalized levels of cytokines that were largely differential between normal and mutant mice. Some cytokines, notably CD30 ligand, Eotaxin-2, LIX, IL-13, IL-15, GM-CSF, MCP-5, MIG, and CCL3 showed elevations in mice treated with ERT above normal or mutant levels; these elevations were reduced or absent in mice that received losartan or combination therapy. The observations suggest that losartan may impact inflammatory cascades due to MPS I and may also blunt inflammation in combination with ERT.

Published

2024

2. Brain transplantation of genetically corrected Sanfilippo type B neural stem cells induces partial cross-correction of the disease

Author

Yewande Pearse, Don Clarke, Shih-hsin Kan, Steven Q. Le, Valentina Sanghez, Anna Luzzi, Ivy Pham, Lina R. Nih, Jonathan D. Cooper, Patricia I. Dickson, and Michelina Iacovino

Subjects

Sanfilippo type B, MPS, LSD, neural progenitor cells, cell therapy, Genetics, QH426-470, Cytology, QH573-671

Abstract

Sanfilippo syndrome type B (mucopolysaccharidosis type IIIB) is a recessive genetic disorder that severely affects the brain due to a deficiency in the enzyme α-N-acetylglucosaminidase (NAGLU), leading to intra-lysosomal accumulation of partially degraded heparan sulfate. There are no effective treatments for this disorder. In this project, we carried out an ex vivo correction of neural stem cells derived from Naglu−/− mice (iNSCs) induced pluripotent stem cells (iPSC) using a modified enzyme in which human NAGLU is fused to an insulin-like growth factor II receptor binding peptide in order to improve enzyme uptake. After brain transplantation of corrected iNSCs into Naglu−/− mice and long-term evaluation of their impact, we successfully detected NAGLU-IGFII activity in all transplanted animals. We found decreased lysosomal accumulation and reduced astrocytosis and microglial activation throughout transplanted brains. We also identified a novel neuropathological phenotype in untreated Naglu−/− brains with decreased levels of the neuronal marker Map2 and accumulation of synaptophysin-positive aggregates. Upon transplantation, we restored levels of Map2 expression and significantly reduced formation of synaptophysin-positive aggregates. Our findings suggest that genetically engineered iNSCs can be used to effectively deliver the missing enzyme to the brain and treat Sanfilippo type B-associated neuropathology.

Published

2022

3. Cross-species efficacy of enzyme replacement therapy for CLN1 disease in mice and sheep

Author

Hemanth R. Nelvagal, Samantha L. Eaton, Sophie H. Wang, Elizabeth M. Eultgen, Keigo Takahashi, Steven Q. Le, Rachel Nesbitt, Joshua T. Dearborn, Nicholas Siano, Ana C. Puhl, Patricia I. Dickson, Gerard Thompson, Fraser Murdoch, Paul M. Brennan, Mark Gray, Stephen N. Greenhalgh, Peter Tennant, Rachael Gregson, Eddie Clutton, James Nixon, Chris Proudfoot, Stefano Guido, Simon G. Lillico, C. Bruce A. Whitelaw, Jui-Yun Lu, Sandra L. Hofmann, Sean Ekins, Mark S. Sands, Thomas M. Wishart, and Jonathan D. Cooper

Subjects

Neuroscience, Therapeutics, Medicine

Abstract

CLN1 disease, also called infantile neuronal ceroid lipofuscinosis (NCL) or infantile Batten disease, is a fatal neurodegenerative lysosomal storage disorder resulting from mutations in the CLN1 gene encoding the soluble lysosomal enzyme palmitoyl-protein thioesterase 1 (PPT1). Therapies for CLN1 disease have proven challenging because of the aggressive disease course and the need to treat widespread areas of the brain and spinal cord. Indeed, gene therapy has proven less effective for CLN1 disease than for other similar lysosomal enzyme deficiencies. We therefore tested the efficacy of enzyme replacement therapy (ERT) by administering monthly infusions of recombinant human PPT1 (rhPPT1) to PPT1-deficient mice (Cln1–/–) and CLN1R151X sheep to assess how to potentially scale up for translation. In Cln1–/– mice, intracerebrovascular (i.c.v.) rhPPT1 delivery was the most effective route of administration, resulting in therapeutically relevant CNS levels of PPT1 activity. rhPPT1-treated mice had improved motor function, reduced disease-associated pathology, and diminished neuronal loss. In CLN1R151X sheep, i.c.v. infusions resulted in widespread rhPPT1 distribution and positive treatment effects measured by quantitative structural MRI and neuropathology. This study demonstrates the feasibility and therapeutic efficacy of i.c.v. rhPPT1 ERT. These findings represent a key step toward clinical testing of ERT in children with CLN1 disease and highlight the importance of a cross-species approach to developing a successful treatment strategy.

Published

2022

4. Genetically Corrected iPSC-Derived Neural Stem Cell Grafts Deliver Enzyme Replacement to Affect CNS Disease in Sanfilippo B Mice

Author

Don Clarke, Yewande Pearse, Shih-hsin Kan, Steven Q. Le, Valentina Sanghez, Jonathan D. Cooper, Patricia I. Dickson, and Michelina Iacovino

Subjects

Genetics, QH426-470, Cytology, QH573-671

Abstract

Sanfilippo syndrome type B (mucopolysaccharidosis type IIIB [MPS IIIB]) is a lysosomal storage disorder primarily affecting the brain that is caused by a deficiency in the enzyme α-N-acetylglucosaminidase (NAGLU), leading to intralysosomal accumulation of heparan sulfate. There are currently no treatments for this disorder. Here we report that, ex vivo, lentiviral correction of Naglu−/− neural stem cells derived from Naglu−/− mice (iNSCs) corrected their lysosomal pathology and allowed them to secrete a functional NAGLU enzyme that could be taken up by deficient cells. Following long-term transplantation of these corrected iNSCs into Naglu−/− mice, we detected NAGLU activity in the majority of engrafted animals. Successfully transplanted Naglu−/− mice showed a significant decrease in storage material, a reduction in astrocyte activation, and complete prevention of microglial activation within the area of engrafted cells and neighboring regions, with beneficial effects extending partway along the rostrocaudal axis of the brain. Our results demonstrate long-term engraftment of iNSCs in the brain that are capable of cross-correcting pathology in Naglu−/− mice. Our findings suggest that genetically engineered iNSCs could potentially be used to deliver enzymes and treat MPS IIIB. Keywords: MPS IIIB, lysosomal storage disorder, stem cell therapy

Published

2018

5. A Humoral Immune Response Alters the Distribution of Enzyme Replacement Therapy in Murine Mucopolysaccharidosis Type I

Author

Steven Q. Le, Shih-hsin Kan, Don Clarke, Valentina Sanghez, Martin Egeland, Kristen N. Vondrak, Terence M. Doherty, Moin U. Vera, Michelina Iacovino, Jonathan D. Cooper, Mark S. Sands, and Patricia I. Dickson

Subjects

lysosomal disease, alpha-l-iduronidase, Hurler, Scheie, glycosaminoglycan, Genetics, QH426-470, Cytology, QH573-671

Abstract

Antibodies against recombinant proteins can significantly reduce their effectiveness in unanticipated ways. We evaluated the humoral response of mice with the lysosomal storage disease mucopolysaccharidosis type I treated with weekly intravenous recombinant human alpha-l-iduronidase (rhIDU). Unlike patients, the majority of whom develop antibodies to recombinant human alpha-l-iduronidase, only approximately half of the treated mice developed antibodies against recombinant human alpha-l-iduronidase and levels were low. Serum from antibody-positive mice inhibited uptake of recombinant human alpha-l-iduronidase into human fibroblasts by partial inhibition compared to control serum. Tissue and cellular distributions of rhIDU were altered in antibody-positive mice compared to either antibody-negative or naive mice, with significantly less recombinant human alpha-l-iduronidase activity in the heart and kidney in antibody-positive mice. In the liver, recombinant human alpha-l-iduronidase was preferentially found in sinusoidal cells rather than in hepatocytes in antibody-positive mice. Antibodies against recombinant human alpha-l-iduronidase enhanced uptake of recombinant human alpha-l-iduronidase into macrophages obtained from MPS I mice. Collectively, these results imply that a humoral immune response against a therapeutic protein can shift its distribution preferentially into macrophage-lineage cells, causing decreased availability of the protein to the cells that are its therapeutic targets.

Published

2018

6. Neuropathology of murine Sanfilippo D syndrome

Author

Shih-hsin Kan, Matthew J. Jansen, Jonathan D. Cooper, Keigo Takahashi, Patricia I. Dickson, and Steven Q. Le

Subjects

Male, Pathology, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Mucopolysaccharidosis, Thalamus, Hippocampus, Neuropathology, Striatum, Biology, Hippocampal formation, Biochemistry, Mice, Mucopolysaccharidosis III, Endocrinology, Genetics, medicine, Animals, Gliosis, Molecular Biology, Brain, Lysosome-Associated Membrane Glycoproteins, Mitochondrial Proton-Translocating ATPases, medicine.disease, Female, Microglia, Primary motor cortex, Immunostaining

Abstract

Sanfilippo D syndrome (mucopolysaccharidosis type IIID) is a lysosomal storage disorder caused by the deficiency of N-acetylglucosamine-6-sulfatase (GNS). A mouse model was generated by constitutive knockout of the Gns gene. We studied affected mice and controls at 12, 24, 36, and 48 weeks of age for neuropathological markers of disease in the somatosensory cortex, primary motor cortex, ventral posterior nuclei of the thalamus, striatum, hippocampus, and lateral and medial entorhinal cortex. We found significantly increased immunostaining for glial fibrillary associated protein (GFAP), CD68 (a marker of activated microglia), and lysosomal-associated membrane protein-1 (LAMP-1) in Sanfilippo D mice compared to controls at 12 weeks of age in all brain regions. Intergroup differences were marked for GFAP and CD68 staining, with levels in Sanfilippo D mice consistently above controls at all age groups. Intergroup differences in LAMP-1 staining were more pronounced in 12- and 24-week age groups compared to 36- and 48-week groups, as control animals showed some LAMP-1 staining at later timepoints in some brain regions. We also evaluated the somatosensory cortex, medial entorhinal cortex, reticular nucleus of the thalamus, medial amygdala, and hippocampal hilus for subunit c of mitochondrial ATP synthase (SCMAS). We found a progressive accumulation of SCMAS in most brain regions of Sanfilippo D mice compared to controls by 24 weeks of age. Cataloging the regional neuropathology of Sanfilippo D mice may aid in understanding the disease pathogenesis and designing preclinical studies to test brain-directed treatments.

Published

2021

7. Biochemical evaluation of intracerebroventricular rhNAGLU-IGF2 enzyme replacement therapy in neonatal mice with Sanfilippo B syndrome

Author

Brett E. Crawford, Mark S. Sands, Ibrahim Elsharkawi, Steven Q. Le, Patricia I. Dickson, Jonathan D. Cooper, Linley Mangini, Roger Lawrence, Shih-hsin Kan, and Heather Prill

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Recombinant Fusion Proteins, Endocrinology, Diabetes and Metabolism, Mucopolysaccharidosis, 030105 genetics & heredity, Biochemistry, Article, Mice, Mucopolysaccharidosis III, 03 medical and health sciences, chemistry.chemical_compound, Dogs, 0302 clinical medicine, Endocrinology, Insulin-Like Growth Factor II, Internal medicine, Acetylglucosaminidase, Genetics, Animals, Humans, Medicine, Enzyme Replacement Therapy, Dosing, Molecular Biology, Sanfilippo syndrome, Mice, Knockout, business.industry, Therapeutic effect, nutritional and metabolic diseases, Heparan sulfate, Enzyme replacement therapy, medicine.disease, Fusion protein, Disease Models, Animal, Infusions, Intraventricular, Animals, Newborn, chemistry, Sanfilippo B syndrome, Heparitin Sulfate, Nervous System Diseases, business, 030217 neurology & neurosurgery

Abstract

Mucopolysaccharidosis IIIB (MPS IIIB, Sanfilippo syndrome type B) is caused by a deficiency in α-N-acetylglucosaminidase (NAGLU) activity, which leads to the accumulation of heparan sulfate (HS). MPS IIIB causes progressive neurological decline, with affected patients having an expected lifespan of approximately 20 years. No effective treatment is available. Recent preclinical studies have shown that intracerebroventricular (ICV) ERT with a fusion protein of rhNAGLU-IGF2 is a feasible treatment for MPS IIIB in both canine and mouse models. In this study, we evaluated the biochemical efficacy of a single dose of rhNAGLU-IGF2 via ICV-ERT in brain and liver tissue from Naglu(−/−) neonatal mice. Twelve weeks after treatment, NAGLU activity levels in brain were 0.75-fold those of controls. HS and β-hexosaminidase activity, which are elevated in MPS IIIB, decreased to normal levels. This effect persisted for at least 4 weeks after treatment. Elevated NAGLU and reduced β-hexosaminidase activity levels were detected in liver; these effects persisted for up to 4 weeks after treatment. The overall therapeutic effects of single dose ICV-ERT with rhNAGLU-IGF2 in Naglu(−/−) neonatal mice were long-lasting. These results suggest a potential benefit of early treatment, followed by less-frequent ICV-ERT dosing, in patients diagnosed with MPS IIIB.

Published

2021

8. Brain transplantation of genetically corrected Sanfilippo B Neural Stem Cells induces partial cross-correction of the disease

Author

Yewande Pearse, Don Clarke, Shih-hsin Kan, Steven Q. Le, Valentina Sanghez, Anna Luzzi, Ivy Pham, Lina R. Nih, Jonathan D. Cooper, Patricia I. Dickson, and Michelina Iacovino

Abstract

Sanfilippo syndrome type B (Mucopolysaccharidosis type IIIB or MPS IIIB) is a recessive genetic disorder that severely affects the brain due to a deficiency in the enzyme α-N-acetylglucosaminidase (NAGLU), leading to intralysosomal accumulation of partially degraded heparan sulfate. There are no effective treatments for this disorder. In this project, we carried out an ex vivo lentiviral correction of neural stem cells derived from Naglu-/- mice (iNSCs) using a modified enzyme in which the NAGLU is fused to an Insulin-like Growth Factor II receptor (IGFIIR) binding peptide in order to improve the cross-correction efficiency. After brain transplantation of these corrected iNSCs into Naglu-/- mice and long-term evaluation of the cross-correction, we successfully detected NAGLU-IGFII activity in all transplanted animals, as well as decreased lysosomal accumulation and reduced astrocytic and microglial activation throughout the transplanted brain. In addition, we identified a novel neuropathological phenotype in untreated brains characterized by decreased levels of MAP2 protein and accumulation of synaptophysin-positive aggregates in the brain. Following transplantation, this Naglu-/- -specific phenotype was altered with restored levels of MAP2 expression and significantly reduced formation of synaptophysin-positive aggregates. Our results demonstrate the feasibility and long-term benefit of genetically corrected iNSCs transplantation in the Sanfilippo B brain and effective cross-correction of Sanfilippo-associated pathology in Naglu-/- mice. Our findings suggest that genetically engineered iNSCs can be used to effectively deliver the missing enzyme to the brain and treat Sanfilippo type B-associated neuropathology.

Published

2022

9. Enzyme Replacement Therapy for Mucopolysaccharidosis IIID using Recombinant Human α-N-Acetylglucosamine-6-Sulfatase in Neonatal Mice

Author

Shan Li, Sean Ekins, Feng Wang, Steven Q. Le, Tsui-Fen Chou, Chelsee Sauni, Brett Lomenick, Xiaoyi Zhang, Patricia I. Dickson, Shih Hsin Kan, Srikanth Singamsetty, Jill Wood, and Derek R. Moen

Subjects

Mucopolysaccharidosis Type IIID, Mucopolysaccharidosis, Pharmaceutical Science, 02 engineering and technology, Heparan sulfate, Enzyme replacement therapy, Pharmacology, 021001 nanoscience & nanotechnology, medicine.disease, N-acetylglucosamine-6-sulfatase, 030226 pharmacology & pharmacy, Glycosaminoglycan, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, Drug Discovery, medicine, Molecular Medicine, 0210 nano-technology, Receptor, Sanfilippo syndrome

Abstract

There is currently no cure or effective treatment available for mucopolysaccharidosis type IIID (MPS IIID, Sanfilippo syndrome type D), a lysosomal storage disorder (LSD) caused by the deficiency of α-N-acetylglucosamine-6-sulfatase (GNS). The clinical symptoms of MPS IIID, like other subtypes of Sanfilippo syndrome, are largely localized to the central nervous system (CNS), and any treatments aiming to ameliorate or reverse the catastrophic and fatal neurologic decline caused by this disease need to be delivered across the blood–brain barrier. Here, we report a proof-of-concept enzyme replacement therapy (ERT) for MPS IIID using recombinant human α-N-acetylglucosamine-6-sulfatase (rhGNS) via intracerebroventricular (ICV) delivery in a neonatal MPS IIID mouse model. We overexpressed and purified rhGNS from CHO cells with a specific activity of 3.9 × 10⁴ units/mg protein and a maximal enzymatic activity at lysosomal pH (pH 5.6), which was stable for over one month at 4 °C in artificial cerebrospinal fluid (CSF). We demonstrated that rhGNS was taken up by MPS IIID patient fibroblasts via the mannose 6-phosphate (M6P) receptor and reduced intracellular glycosaminoglycans to normal levels. The delivery of 5 μg of rhGNS into the lateral cerebral ventricle of neonatal MPS IIID mice resulted in normalization of the enzymatic activity in brain tissues; rhGNS was found to be enriched in lysosomes in MPS IIID-treated mice relative to the control. Furthermore, a single dose of rhGNS was able to reduce the accumulated heparan sulfate and β-hexosaminidase. Our results demonstrate that rhGNS delivered into CSF is a potential therapeutic option for MPS IIID that is worthy of further development.

Published

2020

10. Elucidating expression of a corrective enzyme for MPS I through administration of an adenoviral vector targeted to endothelial cells

Author

Sarah Hurt, Steven Q. Le, Samir Mendonça, Alexander Sorensen, David T. Curiel, and Patricia I. Dickson

Subjects

Endocrinology, Endocrinology, Diabetes and Metabolism, Genetics, Molecular Biology, Biochemistry

Published

2023

11. Membrane-tethered form of NAGLU used to elucidate pathogenesis of heparan sulfate in MPS IIIB mice

Author

Steven Q. Le, Alexander Sorensen, and Patricia I. Dickson

Subjects

Endocrinology, Endocrinology, Diabetes and Metabolism, Genetics, Molecular Biology, Biochemistry

Published

2023

12. Recombinant NAGLU-IGF2 prevents physical and neurological disease and improves survival in Sanfilippo B syndrome

Author

Steven Q. Le, Shih-hsin Kan, Marie S. Roberts, Joshua T. Dearborn, Feng Wang, Shan Li, Elizabeth M. Snella, Jackie K. Jens, Bethann N. Valentine, Hemanth R. Nelvagal, Alexander Sorensen, Keerthana Chintalapati, Kevin Ohlemiller, Carole Vogler, Jonathan D. Cooper, Tsui-Fen Chou, N. Matthew Ellinwood, Jodi D. Smith, Mark S. Sands, and Patricia I. Dickson

Subjects

medicine.medical_specialty, business.industry, Neurodegeneration, Mannose, Inflammation, Enzyme replacement therapy, Heparan sulfate, medicine.disease, law.invention, chemistry.chemical_compound, Endocrinology, chemistry, law, Internal medicine, medicine, Lysosomal storage disease, Recombinant DNA, medicine.symptom, business, Receptor

Abstract

Recombinant human alpha-N-acetylglucosaminidase-insulin-like growth factor-2 (rhNAGLU-IGF2) is an investigational enzyme replacement therapy for Sanfilippo B, a lysosomal storage disease. Because recombinant human NAGLU (rhNAGLU) is poorly mannose 6-phosphorylated, we generated a fusion protein of NAGLU with IGF2 to permit its binding to the cation-independent mannose 6-phosphate receptor. We previously administered rhNAGLU-IGF2 intracerebroventricularly to Sanfilippo B mice, and demonstrated therapeutic restoration of NAGLU, normalization of lysosomal storage, and improvement in markers of neurodegeneration and inflammation. Here, we studied repeated intracerebroventricular rhNAGLU-IGF2 delivery in both murine and canine Sanfilippo B to determine potential effects on their behavioral phenotypes and survival. Treated mice showed improvement in disease markers such as heparan sulfate glycosaminoglycans, beta-hexosaminidase, microglial activation, and lysosomal-associated membrane protein-1. Sanfilippo B mice treated with rhNAGLU-IGF2 displayed partial normalization of their stretch attend postures, a defined fear pose in mice (p

Published

2021

13. Enzyme Replacement Therapy for Mucopolysaccharidosis IIID using Recombinant Human α

Author

Feng, Wang, Derek R, Moen, Chelsee, Sauni, Shih-Hsin, Kan, Shan, Li, Steven Q, Le, Brett, Lomenick, Xiaoyi, Zhang, Sean, Ekins, Srikanth, Singamsetty, Jill, Wood, Patricia I, Dickson, and Tsui-Fen, Chou

Subjects

Neurons, Brain, CHO Cells, Receptor, IGF Type 2, Recombinant Proteins, Article, Lysosomal Storage Diseases, Disease Models, Animal, Mice, Mucopolysaccharidosis III, Cricetulus, Animals, Newborn, Liver, Animals, Humans, Enzyme Replacement Therapy, Heparitin Sulfate, Sulfatases, Lysosomes, Glycosaminoglycans

Abstract

There is currently no cure or effective treatment available for mucopolysaccharidosis type IIID (MPS IIID, Sanfilippo syndrome type D), a lysosomal storage disorder (LSD) caused by the deficiency of α-N-acetylglucosamine-6-sulfatase (GNS). The clinical symptoms of MPS IIID, like other subtypes of Sanfilippo syndrome, are largely localized to the central nervous system (CNS), and any treatments aiming to ameliorate or reverse the catastrophic and fatal neurologic decline caused by this disease need to be delivered across the blood-brain barrier. Here, we report a proof-of-concept enzyme replacement therapy (ERT) for MPS IIID using recombinant human α-N-acetylglucosamine-6-sulfatase (rhGNS) via intracerebroventricular (ICV) delivery in a neonatal MPS IIID mouse model. We overexpressed and purified rhGNS from CHO cells with specific activity of 3.9x10(4) units/mg protein, with a maximal enzymatic activity at lysosomal pH (pH 5.6), and which was stable for over one month at 4°C in artificial cerebrospinal fluid (CSF). We demonstrated that rhGNS was taken up by MPS IIID patient fibroblasts via the mannose 6-phosphate (M6P) receptor and reduced intracellular glycosaminoglycans to normal levels. Delivery of 5 micrograms of rhGNS into the lateral cerebral ventricle of neonatal MPS IIID mice resulted in normalization of the enzymatic activity in brain tissues; rhGNS was found to be enriched in lysosomes in MPS IIID treated mice relative to control. Furthermore, a single dose of rhGNS was able to reduce the accumulated heparan sulfate and β-hexosaminidase. Our results demonstrate that rhGNS delivered into CSF is a potential therapeutic option for MPS IIID worthy of further development.

Published

2020

14. Myelin and lipid composition of the corpus callosum in mucopolysaccharidosis type I mice

Author

Rong Guo, Igor Nestrasil, Patricia I. Dickson, David Elashoff, Jonathan D. Cooper, Steven Q. Le, Jennifer K. Yee, Shih hsin Kan, Martin T. Egeland, and Jakub Tolar

Subjects

0301 basic medicine, Male, Ceramide, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, Mucopolysaccharidosis I, Phospholipid, Gene Expression, Biochemistry, Article, Corpus Callosum, White matter, 03 medical and health sciences, chemistry.chemical_compound, Mucopolysaccharidosis type I, Myelin, Internal medicine, medicine, Animals, skin and connective tissue diseases, Myelin Sheath, Mice, Knockout, 030109 nutrition & dietetics, biology, Cholesterol, Organic Chemistry, nutritional and metabolic diseases, Myelin Basic Protein, Cell Biology, Lipids, Myelin basic protein, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, chemistry, Case-Control Studies, biology.protein, Female, Sphingomyelin

Abstract

Mucopolysaccharidosis type I (MPS I) is a lysosomal disease with progressive central nervous system involvement. This study examined the lipid, cholesterol, and myelin basic protein composition of white matter in the corpus callosum of MPS I mice. We studied 50 week-old, male MPS I mice and littermate, heterozygote controls (n = 12 per group). Male MPS I mice showed lower phosphatidylcholine and ether-linked phosphatidylcholine quantities than controls (p < 0.05). Twenty-two phospholipid or ceramide species showed significant differences in percent of total. Regarding specific lipid species, MPS I mice exhibited lower quantities of sphingomyelin 18:1, phosphatidylserine 38:3, and hexosylceramide d18:1(22:1) mH(2)O than controls. Principal components analyses of polar, ceramide and hexosylceramide lipids, respectively, showed some separation of MPS I and control mice. We found no significant differences in myelin gene expression, myelin basic protein, or total cholesterol in the MPS I mice versus heterozygous controls. There was a trend towards lower proteolipid protein-1 levels in MPS I mice (p = 0.06). MPS I mice show subtle changes in white matter composition, with an unknown impact on pathogenesis in this model.

Published

2020

15. Spinal cord pathology in murine Sanfilippo syndrome type B

Author

Steven Q. Le, Alexander Sorensen, Keerthana Chintalapati, Shih-hsin Kan, Hemanth R. Nelvagal, Jonathan D. Cooper, and Patricia I. Dickson

Subjects

Endocrinology, Endocrinology, Diabetes and Metabolism, Genetics, Molecular Biology, Biochemistry

Published

2022

16. An adenoviral mediated gene therapy for mucopolysaccharidosis type I

Author

Sarah Hurt, Steven Q. Le, Samir Mendonca, Patricia Dickson, and David T. Curiel

Subjects

Endocrinology, Endocrinology, Diabetes and Metabolism, Genetics, Molecular Biology, Biochemistry

Published

2022

17. Co-expression of S1S3 phosphotransferase in production cell line improves mannose 6-phosphorylation and cellular uptake of alpha--acetylglucosaminidase (Sanfilippo syndrome type B)

Author

Patricia I. Dickson, Steven Q. Le, Alexander Sorensen, Balraj Doray, Shou Liu, Yicheng Zhao, Russell Gotschall, Stuart Kornfeld, and Lin Liu

Subjects

Endocrinology, Endocrinology, Diabetes and Metabolism, Genetics, Molecular Biology, Biochemistry

Published

2022

18. Efficacy of recombinant human PPT1 enzyme replacement therapy in mouse and sheep models of CLN1 disease

Author

Hemanth R. Nelvagal, Samantha L. Eaton, Sophie H. Wang, Elizabeth M. Eultgen, Keigo Takahashi, Steven Q. Le, LaRachel Nesbitt, Joshua T. Dearborn, Ana C. Puhl, Patricia I. Dickson, Paul M. Brennan, Gerard Thompson, Sandra L. Hofmann, Sean Ekins, Mark S. Sands, Thomas M. Wishart, and Jonathan D. Cooper

Subjects

Endocrinology, Endocrinology, Diabetes and Metabolism, Genetics, Molecular Biology, Biochemistry

Published

2022

19. A Humoral Immune Response Alters the Distribution of Enzyme Replacement Therapy in Murine Mucopolysaccharidosis Type I

Author

Moin Vera, Terence M. Doherty, Shih hsin Kan, Kristen N. Vondrak, Michelina Iacovino, Martin T. Egeland, Steven Q. Le, Patricia I. Dickson, Jonathan D. Cooper, Mark S. Sands, Valentina Sanghez, and Don Clarke

Subjects

0301 basic medicine, lcsh:QH426-470, Hurler, Pharmacology, Article, law.invention, Scheie, 03 medical and health sciences, Mucopolysaccharidosis type I, 0302 clinical medicine, Immune system, law, Genetics, medicine, Lysosomal storage disease, glycosaminoglycan, lcsh:QH573-671, Molecular Biology, Kidney, biology, lcsh:Cytology, lysosomal disease, Enzyme replacement therapy, medicine.disease, 3. Good health, lcsh:Genetics, 030104 developmental biology, medicine.anatomical_structure, Immunology, biology.protein, Recombinant DNA, Molecular Medicine, Antibody, Iduronidase, 030217 neurology & neurosurgery, alpha-l-iduronidase

Abstract

Antibodies against recombinant proteins can significantly reduce their effectiveness in unanticipated ways. We evaluated the humoral response of mice with the lysosomal storage disease mucopolysaccharidosis type I treated with weekly intravenous recombinant human alpha-l-iduronidase (rhIDU). Unlike patients, the majority of whom develop antibodies to recombinant human alpha-l-iduronidase, only approximately half of the treated mice developed antibodies against recombinant human alpha-l-iduronidase and levels were low. Serum from antibody-positive mice inhibited uptake of recombinant human alpha-l-iduronidase into human fibroblasts by partial inhibition compared to control serum. Tissue and cellular distributions of rhIDU were altered in antibody-positive mice compared to either antibody-negative or naive mice, with significantly less recombinant human alpha-l-iduronidase activity in the heart and kidney in antibody-positive mice. In the liver, recombinant human alpha-l-iduronidase was preferentially found in sinusoidal cells rather than in hepatocytes in antibody-positive mice. Antibodies against recombinant human alpha-l-iduronidase enhanced uptake of recombinant human alpha-l-iduronidase into macrophages obtained from MPS I mice. Collectively, these results imply that a humoral immune response against a therapeutic protein can shift its distribution preferentially into macrophage-lineage cells, causing decreased availability of the protein to the cells that are its therapeutic targets.

Published

2018

20. Comparison of dermatan sulfate and heparan sulfate concentrations in serum, cerebrospinal fluid and urine in patients with mucopolysaccharidosis type I receiving intravenous and intrathecal enzyme replacement therapy

Author

Ashlee R. Stiles, Steven Q. Le, David S. Millington, Haoyue Zhang, Patricia I. Dickson, Sarah P. Young, Patricia McCaw, Agnes Chen, and James Beasley

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Mucopolysaccharidosis, Mucopolysaccharidosis I, Clinical Biochemistry, Dermatan Sulfate, Urine, Biochemistry, Dermatan sulfate, 03 medical and health sciences, chemistry.chemical_compound, Mucopolysaccharidosis type I, 0302 clinical medicine, Cerebrospinal fluid, Tandem Mass Spectrometry, Internal medicine, medicine, Humans, Enzyme Replacement Therapy, Chondroitin sulfate, Glycosaminoglycans, Chemistry, Biochemistry (medical), nutritional and metabolic diseases, General Medicine, Heparan sulfate, Enzyme replacement therapy, medicine.disease, 030104 developmental biology, Endocrinology, 030220 oncology & carcinogenesis, Heparitin Sulfate, Chromatography, Liquid

Abstract

Aims To validate a liquid chromatography-tandem mass spectrometry (UPLC-MS/MS) method for the measurement of glycosaminoglycans (GAGs) in plasma and serum. To establish plasma, cerebrospinal fluid (CSF) and urine reference intervals. To compare GAGs in serum with that in urine and CSF from patients with MPS I. Methods Dermatan sulfate (DS), heparan sulfate (HS), and chondroitin sulfate (CS) in serum/plasma, urine and CSF were methanolysed into dimers and analyzed using pseudo isotope dilution UPLC-MS/MS assay. Serum, CSF and urine DS and HS were quantified for 11 patients with mucopolysaccharidosis (MPS) type I before and after treatment with Aldurazyme® (laronidase) enzyme replacement therapy (ERT). Results The method showed acceptable imprecision and recovery for the quantification of serum/plasma CS, DS, and HS. The serum, urine, and CSF DS and HS concentrations were reduced after 26 weeks of ERT in 4 previously untreated patients. Serum DS and HS concentrations normalized in some patients, and were mildly elevated in others after ERT. In contrast, urine and CSF DS and HS values remained elevated above the reference ranges. Compared with serum GAGs, urine and CSF DS and HS were more sensitive biomarkers for monitoring the ERT treatment of patients with MPS I.

Published

2019

21. Intrathecal enzyme replacement for cognitive decline in mucopolysaccharidosis type I, a randomized, open-label, controlled pilot study

Author

Agnes Chen, Steven Q. Le, Igor Nestrasil, Alexander M. Kaizer, Alena Svátková, Haoyue Zhang, Jacqueline Madden, Paul Harmatz, Sarah P. Young, Patricia I. Dickson, Lynda E. Polgreen, Kelly King, Kyle Rudser, Julie B. Eisengart, and Amy Wakumoto

Subjects

0301 basic medicine, Male, Lysosomal disease, Mucopolysaccharidoses (MPS), Endocrinology, Diabetes and Metabolism, Mucopolysaccharidosis, Mucopolysaccharidosis I, Cognitive decline, Pilot Projects, 030105 genetics & heredity, Regenerative Medicine, Biochemistry, Iduronidase, 0302 clinical medicine, Endocrinology, Prospective Studies, Child, Injections, Spinal, Genetics & Heredity, Pain Research, Intrathecal enzyme replacement therapy, Enzyme replacement therapy, Middle Aged, Recombinant Proteins, Research Design, 6.1 Pharmaceuticals, Neurological, Female, Adult, medicine.medical_specialty, Randomization, Spinal, Adolescent, Clinical Trials and Supportive Activities, Clinical Sciences, Hurler, Article, Injections, 03 medical and health sciences, Mucopolysaccharidosis type I, Young Adult, Rare Diseases, Clinical Research, Spinal cord compression, Neck spasm, Internal medicine, Genetics, medicine, Humans, Cognitive Dysfunction, Enzyme Replacement Therapy, Adverse effect, Molecular Biology, business.industry, Neurosciences, Evaluation of treatments and therapeutic interventions, Stem Cell Research, medicine.disease, Brain Disorders, Glycosaminoglycan, business, 030217 neurology & neurosurgery

Abstract

Central nervous system manifestations of mucopolysaccharidosis type I (MPS I) such as cognitive impairment, hydrocephalus, and spinal cord compression are inadequately treated by intravenously-administered enzyme replacement therapy with laronidase (recombinant human alpha-L-iduronidase). While hematopoietic stem cell transplantation treats neurological symptoms, this therapy is not generally offered to attenuated MPS I patients. This study is a randomized, open-label, controlled pilot study of intrathecal laronidase in eight attenuated MPS I patients with cognitive impairment. Subjects ranged between 12years and 50years old with a median age of 18years. All subjects had received intravenous laronidase prior to the study over a range of 4 to 10years, with a mean of 7.75years. Weekly intravenous laronidase was continued throughout the duration of the study. The randomization period was one year, during which control subjects attended all study visits and assessments, but did not receive any intrathecal laronidase. After the first year, all eight subjects received treatment for one additional year. There was no significant difference in neuropsychological assessment scores between control or treatment groups, either over the one-year randomized period or at 18 or 24months. However, there was no significant decline in scores in the control group either. Adverse events included pain (injection site, back, groin), headache, neck spasm, and transient blurry vision. There were seven serious adverse events, one judged as possibly related (headache requiring hospitalization). There was no significant effect of intrathecal laronidase on cognitive impairment in older, attenuated MPS I patients over a two-year treatment period. A five-year open-label extension study is underway.

Published

2019

22. Evaluation of non-reducing end pathologic glycosaminoglycan detection method for monitoring therapeutic response to enzyme replacement therapy in human mucopolysaccharidosis I

Author

Alla Victoroff, Merry Passage, Jillian R. Brown, Moin Vera, Agnes Chen, Steven Q. Le, Patricia I. Dickson, Lynda E. Polgreen, and Brett E. Crawford

Subjects

0301 basic medicine, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Mucopolysaccharidosis, Mucopolysaccharidosis I, Urine, 030105 genetics & heredity, Biochemistry, Article, law.invention, Glycosaminoglycan, 03 medical and health sciences, chemistry.chemical_compound, Iduronidase, 0302 clinical medicine, Endocrinology, law, Internal medicine, Genetics, medicine, Humans, Enzyme Replacement Therapy, Molecular Biology, Glycosaminoglycans, biology, business.industry, Clinical Laboratory Techniques, Enzyme replacement therapy, Heparan sulfate, medicine.disease, Enzyme assay, chemistry, biology.protein, Recombinant DNA, Drug Monitoring, business, 030217 neurology & neurosurgery, Biomarkers

Abstract

Therapeutic development and monitoring require demonstration of effects on disease phenotype. However, due to the complexity of measuring clinically-relevant effects in rare multisystem diseases, robust biomarkers are essential. For the mucopolysaccharidoses (MPS), the measurement of glycosaminoglycan levels is relevant as glycosaminoglycan accumulation is the primary event that occurs due to reduced lysosomal enzyme activity. Traditional dye-based assays that measure total glycosaminoglycan levels have a high background, due to a normal, baseline glycosaminoglycan content in unaffected individuals. An assay that selectively detects the disease-specific non-reducing ends of heparan sulfate glycosaminoglycans that remain undegraded due to deficiency of a specific enzyme in the catabolic pathway avoids the normal background, increasing sensitivity and specificity. We evaluated glycosaminoglycan content by dye-based and non-reducing end methods using urine, serum, and cerebrospinal fluid from MPS I human samples before and after treatment with intravenous recombinant human alpha-l-iduronidase. We found that both urine total glycosaminoglycans and serum heparan sulfate derived non-reducing end levels were markedly decreased compared to baseline after 26 weeks and 52 weeks of therapy, with a significantly greater percentage reduction in serum non-reducing end (89.8% at 26 weeks and 81.3% at 52 weeks) compared to urine total glycosaminoglycans (68.3% at 26 weeks and 62.4% at 52 weeks, p

Published

2019

23. Devising effective enzyme replacement therapy for infantile onset neuronal ceroid lipofuscinosis (CLN1 disease)

Author

Keigo Takahashi, Sophie H. Wang, Hemanth R. Nelvagal, Elizabeth M. Eultgen, Jonathan D. Cooper, Ana C. Puhl, Steven Q. Le, and Sean Ekins

Subjects

Pathology, medicine.medical_specialty, business.industry, Endocrinology, Diabetes and Metabolism, Disease, Enzyme replacement therapy, medicine.disease, Biochemistry, Endocrinology, Genetics, Medicine, Neuronal ceroid lipofuscinosis, Infantile onset, business, Molecular Biology

Published

2021

24. Intracerebroventricular sulfamidase delivery to the brain

Author

Steven Q. Le, Bryan E. Thacker, Farhan A. Hussain, Patricia I. Dickson, Charles A. Glass, Jeffrey D. Esko, and Jillian R. Brown

Subjects

Endocrinology, Endocrinology, Diabetes and Metabolism, Genetics, Molecular Biology, Biochemistry

Published

2020

25. Genetically Corrected iPSC-Derived Neural Stem Cell Grafts Deliver Enzyme Replacement to Affect CNS Disease in Sanfilippo B Mice

Author

Patricia I. Dickson, Shih-hsin Kan, Valentina Sanghez, Steven Q. Le, Jonathan D. Cooper, Michelina Iacovino, Don Clarke, and Yewande Pearse

Subjects

0301 basic medicine, lcsh:QH426-470, Mucopolysaccharidoses (MPS), medicine.medical_treatment, Regenerative Medicine, stem cell therapy, Article, 03 medical and health sciences, chemistry.chemical_compound, Rare Diseases, Genetics, medicine, Secretion, lcsh:QH573-671, Molecular Biology, Metabolic and endocrine, Sanfilippo syndrome, chemistry.chemical_classification, Transplantation, 5.2 Cellular and gene therapies, lcsh:Cytology, Neurosciences, Heparan sulfate, Stem-cell therapy, medicine.disease, Stem Cell Research, Neural stem cell, 3. Good health, lcsh:Genetics, 030104 developmental biology, Enzyme, medicine.anatomical_structure, chemistry, Neurological, Cancer research, MPS IIIB, Molecular Medicine, lysosomal storage disorder, Development of treatments and therapeutic interventions, Astrocyte, Biotechnology

Abstract

Sanfilippo syndrome type B (mucopolysaccharidosis type IIIB [MPS IIIB]) is a lysosomal storage disorder primarily affecting the brain that is caused by a deficiency in the enzyme α-N-acetylglucosaminidase (NAGLU), leading to intralysosomal accumulation of heparan sulfate. There are currently no treatments for this disorder. Here we report that, ex vivo, lentiviral correction of Naglu−/− neural stem cells derived from Naglu−/− mice (iNSCs) corrected their lysosomal pathology and allowed them to secrete a functional NAGLU enzyme that could be taken up by deficient cells. Following long-term transplantation of these corrected iNSCs into Naglu−/− mice, we detected NAGLU activity in the majority of engrafted animals. Successfully transplanted Naglu−/− mice showed a significant decrease in storage material, a reduction in astrocyte activation, and complete prevention of microglial activation within the area of engrafted cells and neighboring regions, with beneficial effects extending partway along the rostrocaudal axis of the brain. Our results demonstrate long-term engraftment of iNSCs in the brain that are capable of cross-correcting pathology in Naglu−/− mice. Our findings suggest that genetically engineered iNSCs could potentially be used to deliver enzymes and treat MPS IIIB. Keywords: MPS IIIB, lysosomal storage disorder, stem cell therapy

Published

2018

26. Data from subjects receiving intrathecal laronidase for cervical spinal stenosis due to mucopolysaccharidosis type I

Author

Alla Victoroff, Patricia I. Dickson, Paul Harmatz, Anton Mlikotic, Ilkka Kaitila, Merry Passage, Agnes Chen, Jacqueline Madden, Steven Q. Le, David E. Naylor, Medicum, and Department of Medical and Clinical Genetics

Subjects

Pathology, medicine.medical_specialty, education, lcsh:Computer applications to medicine. Medical informatics, Pulmonary function testing, 03 medical and health sciences, Mucopolysaccharidosis type I, 0302 clinical medicine, Cerebrospinal fluid, medicine, Adverse effect, lcsh:Science (General), Data Article, 0303 health sciences, Multidisciplinary, medicine.diagnostic_test, business.industry, 030302 biochemistry & molecular biology, Cervical spinal stenosis, Magnetic resonance imaging, Spinal cord, medicine.disease, 3. Good health, medicine.anatomical_structure, Somatosensory evoked potential, Anesthesia, lcsh:R858-859.7, 3111 Biomedicine, business, 030217 neurology & neurosurgery, lcsh:Q1-390

Abstract

Five subjects with mucopolysaccharidosis type I and symptomatic cervical spinal stenosis received intrathecal laronidase in a 4-month pilot study and/or a 12-month extension study [1]. Clinical descriptions of study subjects, nonserious adverse events, individual data tables, and scoring system methods are provided. There were ten nonserious adverse events that occurred in more than one study subject. Somatosensory evoked potentials were absent in two subjects and normal in two subjects, limiting their utility as an endpoint. There were no significant changes in magnetic resonance imaging of cervical spinal cord or brain, pulmonary function tests, or cerebrospinal fluid opening pressure. These data are presented along with the scoring methods used in evaluation of the study subjects.

Published

2015

27. Safety of laronidase delivered into the spinal canal for treatment of cervical stenosis in mucopolysaccharidosis I

Author

Anton Mlikotic, Alla Victoroff, Paul Harmatz, Steven Q. Le, Jacqueline Madden, Merry Passage, Patricia I. Dickson, Ilkka Kaitila, David E. Naylor, and Agnes Chen

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Mucopolysaccharidosis I, Endocrinology, Diabetes and Metabolism, Cervix Uteri, Constriction, Pathologic, Biochemistry, Article, Iduronidase, Young Adult, Mucopolysaccharidosis type I, Myelopathy, Endocrinology, Lumbar, Spinal cord compression, Genetics, medicine, Humans, Spinal canal, Child, Spinal Meninges, Molecular Biology, business.industry, Enzyme replacement therapy, medicine.disease, Recombinant Proteins, 3. Good health, Surgery, medicine.anatomical_structure, Female, business, Spinal Canal

Abstract

Enzyme replacement therapy with laronidase (recombinant human alpha-l-iduronidase) is successfully used to treat patients with mucopolysaccharidosis type I (MPS I). However, the intravenously-administered enzyme is not expected to treat or prevent neurological deterioration. As MPS I patients suffer from spinal cord compression due in part to thickened spinal meninges, we undertook a phase I clinical trial of lumbar intrathecal laronidase in MPS I subjects age 8 years and older with symptomatic (primarily cervical) spinal cord compression. The study faced significant challenges, including a heterogeneous patient population, difficulty recruiting subjects despite an international collaborative effort, and an inability to include a placebo-controlled design due to ethical concerns. Nine serious adverse events occurred in the subjects. All subjects reported improvement in symptomatology and showed improved neurological examinations, but objective outcome measures did not demonstrate change. Despite limitations, we demonstrated the safety of this approach to treating neurological disease due to MPS I.

Published

2015

28. Enzyme replacement therapy for mucopolysaccharidosis type IIID

Author

Jill Wood, Derek R. Moen, Sean Ekins, Tsui-Fen Chou, Steven Q. Le, Xiaoyi Zhang, Shih-hsin Kan, Patricia I. Dickson, Chelsee Sauni, and Feng Wang

Subjects

Mucopolysaccharidosis Type IIID, medicine.medical_specialty, Endocrinology, business.industry, Endocrinology, Diabetes and Metabolism, Internal medicine, Genetics, medicine, Enzyme replacement therapy, business, Molecular Biology, Biochemistry

Published

2019

29. Behavioral deficits and cholinergic pathway abnormalities in male Sanfilippo B mice

Author

Shih-hsin Kan, Patricia I. Dickson, Jesse D. Cushman, Quang D. Bui, Steven Q. Le, Mark S. Sands, and Braeden Benedict

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Elevated plus maze, Mucopolysaccharidosis, Spatial Learning, Water maze, Anxiety, Open field, Article, Choline O-Acetyltransferase, 03 medical and health sciences, Behavioral Neuroscience, chemistry.chemical_compound, Mice, Mucopolysaccharidosis III, 0302 clinical medicine, Internal medicine, medicine, Animals, Radial arm maze, Brain, Fear, medicine.disease, Acetylcholinesterase, Acetylcholine, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Endocrinology, Memory, Short-Term, chemistry, Rotarod Performance Test, Cholinergic, Psychology, 030217 neurology & neurosurgery, Locomotion, medicine.drug

Abstract

Sanfilippo B syndrome is a progressive neurological disorder caused by inability to catabolize heparan sulfate glycosaminoglycans. We studied neurobehavior in male Sanfilippo B mice and heterozygous littermate controls from 16–20 weeks of age. Affected mice showed reduced anxiety, with a decrease in the number of stretch-attend postures during the elevated plus maze (p = 0.001) and an increased tendency to linger in the center of an open field (p = 0.032). Water maze testing showed impaired spatial learning, with reduced preference for the target quadrant (p = 0.01). In radial arm maze testing, affected mice failed to achieve above-chance performance in a win-shift working memory task (t-test relative to 50% chance: p = 0.289), relative to controls (p = 0.037). We found a 12.4% reduction in mean acetylcholinesterase activity (p < 0.001) and no difference in choline acetyltransferase activity or acetylcholine in whole brain of affected male animals compared to controls. Cholinergic pathways are affected in adult-onset dementias, including Alzheimer disease. Our results suggest that male Sanfilippo B mice display neurobehavioral deficits at a relatively early age, and that as in adult dementias, they may display deficits in cholinergic pathways.

Published

2016

30. Specific antibody titer alters the effectiveness of intrathecal enzyme replacement therapy in canine mucopolysaccharidosis I

Author

Jillian R. Brown, N. Matthew Ellinwood, Patricia I. Dickson, Steven Q. Le, Merry Passage, Moin Vera, Brett E. Crawford, and Robert G. Witt

Subjects

Mucopolysaccharidosis I, Endocrinology, Diabetes and Metabolism, Mucopolysaccharidosis, Pharmacology, Cisterna magna, Biochemistry, Article, law.invention, Glycosaminoglycan, Iduronidase, Dogs, Endocrinology, Antibody Specificity, law, Immune Tolerance, Genetics, medicine, Animals, Humans, Enzyme Replacement Therapy, Molecular Biology, Injections, Spinal, Glycosaminoglycans, business.industry, Brain, Enzyme replacement therapy, medicine.disease, Disease Models, Animal, Titer, Immunoglobulin G, Immunology, Cyclosporine, Recombinant DNA, business, Immunosuppressive Agents

Abstract

Intrathecal enzyme replacement therapy is an experimental option to treat central nervous system disease due to lysosomal storage. Previous work shows that MPS I dogs receiving enzyme replacement with recombinant human alpha-L-iduronidase into the cisterna magna showed normal brain glycosaminoglycan (GAG) storage after three or four doses. We analyzed MPS I dogs that received intrathecal enzyme in a previous study using an assay that detects only pathologic GAG (pGAG). To quantify pGAG in MPS I, the assay measures only those GAG which display terminal iduronic acid residues on their non-reducing ends. Mean cortical brain pGAG in six untreated MPS I dogs was 60.9 ± 5.93 pmol per mg wet weight, and was 3.83 ± 2.64 in eight normal or unaffected carrier animals (p

Published

2012

31. Biochemical characterization of fluorescent-labeled recombinant human alpha-l-iduronidase in vitro

Author

Shih-hsin Kan, Steven Q. Le, Amanda K. Todd, Brigette L. Tippin, Larisa A. Troitskaya, and Patricia I. Dickson

Subjects

Mucopolysaccharidosis I, Biomedical Engineering, Bioengineering, Biology, Applied Microbiology and Biotechnology, Article, Receptor, IGF Type 2, law.invention, Iduronidase, In vivo, Confocal microscopy, law, Drug Discovery, medicine, Humans, Hurler syndrome, Cells, Cultured, Fluorescent Dyes, Glycosaminoglycans, Process Chemistry and Technology, General Medicine, Fibroblasts, Subcellular localization, medicine.disease, Recombinant Proteins, In vitro, Molecular Weight, Biochemistry, Recombinant DNA, Molecular Medicine, Lysosomes, Ex vivo, Biotechnology

Abstract

In vivo tracking of the delivery of therapeutic proteins is a useful tool for preclinical studies. However, many labels are too large to use without disrupting the normal uptake, function, or other properties of the protein. Low-molecular weight fluorescent labels allow in vivo and ex vivo tracking of the distribution of therapeutic proteins, and should not alter the protein’s characteristics. We tested the in vitro properties of fluorescent-labeled recombinant human alpha-L-iduronidase (rhIDU, the enzyme deficient in Hurler syndrome) and compared labeled to unlabeled protein. Labeled rhIDU retained full enzymatic activity and showed similar kinetics to non-labeled rhIDU. Uptake of labeled rhIDU into human Hurler fibroblasts, measured by activity assay, was equivalent to unlabeled rhIDU enzyme and showed an uptake constant of 0.72 nM. Labeled rhIDU was also able to enter cells via the mannose 6-phospate receptor pathway and reduce glycosaminoglycan (GAG) storage in Hurler fibroblasts. Subcellular localization was verified within lysosomes by confocal microscopy. These findings suggest that fluorescent labeling does not significantly interfere with enzymatic activity, stability, or uptake, and validates this method as a way to track exogenously administered enzyme.

Published

2011

32. Glycosaminoglycan storage in neuroanatomical regions of mucopolysaccharidosis I dogs following intrathecal recombinant human iduronidase

Author

Elizabeth M. Snella, Agnes Chen, Patricia I. Dickson, Merry Passage, Catalina Guerra, Michael F. McEntee, Carole Vogler, Steven Q. Le, N. Matthew Ellinwood, Stephen Hanson, and Jackie K. Jens

Subjects

Microbiology (medical), medicine.medical_specialty, Cerebellum, Thalamus, Hippocampus, General Medicine, Anatomy, Biology, Hippocampal formation, Frontal lobe/cortex, Pathology and Forensic Medicine, Endocrinology, medicine.anatomical_structure, Frontal lobe, Internal medicine, Basal ganglia, medicine, Immunology and Allergy, Brainstem

Abstract

Intrathecal (IT) recombinant human α-L-iduronidase (rhIDU) has been shown to reduce mean brain glycosaminoglycans (GAGs) to normal levels in MPS I dogs. In this study, we examined storage in neuroanatomical regions of the MPS I dog brain, including frontal lobe, cerebellum, basal ganglia, thalamus, hippocampal formation, and brainstem, to determine the response of these functional regions to treatment with IT rhIDU. GAG storage in untreated MPS I dogs was significantly different from normal dogs in all examined sections. GAG levels in normal dogs varied by region: frontal lobe (mean 2.36 ± 0.54 µg/mg protein), cerebellum (2.67 ± 0.33), basal ganglia and thalamus (3.51 ± 0.60), hippocampus (3.30 ± 0.40), and brainstem (3.73 ± 1.10). Following intrathecal treatment, there was a reduction in GAG storage in each region in all treatment groups, except for the brainstem. Percent reduction in GAG levels from untreated to treated MPS I dogs in the deeper regions of the brain was 30% for basal ganglia and thalamus and 30% for hippocampus, and storage reduction was greater in superficial regions, with 61% reduction in the frontal lobe and 54% in the cerebellum compared to untreated MPS I dogs. Secondary lipid storage in neurons was also reduced in frontal lobe, but not in the other brain regions examined. Response to therapy appeared to be greater in more superficial regions of the brain, particularly in the frontal lobe cortex.

Published

2011

33. Neural stem cells provide continuous enzyme replacement therapy and reduce neuropathology in Sanfilippo syndrome type B mice

Author

Don Clarke, Yewande Pearse, Patricia I. Dickson, Valentina Sanghez, Steven Q. Le, Kan Shih-hsin, Jonathan D. Cooper, and Michelina Iacovino

Subjects

Pathology, medicine.medical_specialty, business.industry, Endocrinology, Diabetes and Metabolism, Enzyme replacement therapy, Neuropathology, medicine.disease, Biochemistry, Neural stem cell, Endocrinology, Genetics, Medicine, business, Molecular Biology, Sanfilippo syndrome

Published

2018

34. Pilot enzyme replacement therapy with recombinant human glucosamine (N-acetyl)-6-sulfatase in mucopolysaccharidosis type IIID mouse model

Author

Patricia I. Dickson, Steven Q. Le, Betty Anderson, Jill Wood, Tsui-Fen Chou, Chelsee Sauni, Shih-hsin Kan, Sean Ekins, and Feng Wang

Subjects

0301 basic medicine, Mucopolysaccharidosis Type IIID, 6-Sulfatase, Endocrinology, Diabetes and Metabolism, Enzyme replacement therapy, Biochemistry, Molecular biology, law.invention, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Endocrinology, chemistry, Glucosamine, law, Genetics, Recombinant DNA, Molecular Biology

Published

2018

35. Continuous infusion of enzyme replacement therapy is inferior to weekly infusions in MPS I dogs

Author

Merry Passage, Emil D. Kakkis, Steven Q. Le, Maryn Peinovich, A. W. Krieger, Thomas Lester, and Patricia I. Dickson

Subjects

Continuous infusion, Mucopolysaccharidosis I, Article, Iduronidase, Dogs, Genetics, Animals, Humans, Medicine, Enzyme Replacement Therapy, Dosing, Infusions, Intravenous, Adverse effect, Infusion Pumps, Genetics (clinical), Glycosaminoglycans, business.industry, Enzyme replacement therapy, Recombinant Proteins, Disease Models, Animal, Treatment Outcome, Peak plasma, Weekly dose, Anesthesia, business

Abstract

Intravenous enzyme replacement therapy with recombinant human α-L-iduronidase (rhIDU) is used weekly to treat mucopolysaccharidosis (MPS) I. We tested continuous administration of rhIDU at two dosing levels (0.58 mg/kg per week and 2 mg/kg per week) in MPS I dogs, and compared the efficacy of continuous infusion with the clinically used 0.58 mg/kg weekly three-hour infusion. Peak plasma concentrations of rhIDU were much higher in weekly-treated dogs (mean 256 units/ml) than steady-state concentrations in dogs treated with continuous infusion (mean 1.97 units/ml at 0.58 mg/kg per week; 8.44 units/ml at 2 mg/kg per week). Dogs receiving continuous IV rhIDU, even at a higher (2 mg/kg per week) dose, had consistently lower iduronidase levels in tissues than dogs receiving a weekly (0.58 mg/kg per week) dose. GAG storage was also less improved by continuous intravenous infusion. Adverse events were similar in all dosing groups. We found that continuous administration of 2 mg/kg per week rhIDU to MPS I dogs was insufficient to achieve GAG storage reduction comparable to 0.58 mg/kg weekly dosing.

Published

2009

36. Intrathecal enzyme replacement therapy: Successful treatment of brain disease via the cerebrospinal fluid

Author

Maryn Peinovich, Carole Vogler, Stephen Hanson, Michael F. McEntee, Patricia I. Dickson, Steven Q. Le, Merry Passage, Emil D. Kakkis, and Beth Levy

Subjects

medicine.medical_specialty, Mucopolysaccharidosis I, Endocrinology, Diabetes and Metabolism, Central nervous system, Pharmacology, Biochemistry, Article, Iduronidase, Dogs, Meninges, Endocrinology, Cerebrospinal fluid, Genetics, medicine, Animals, Humans, Tissue Distribution, Hurler syndrome, Spinal Meninges, Molecular Biology, Injections, Spinal, Glycosaminoglycans, Brain Diseases, Dose-Response Relationship, Drug, business.industry, Brain, Enzyme replacement therapy, medicine.disease, Recombinant Proteins, Surgery, Disease Models, Animal, medicine.anatomical_structure, Spinal Cord, Ependyma, business

Abstract

Treatment of brain disease with recombinant proteins is difficult due to the blood-brain barrier. As an alternative to direct injections into the brain, we studied whether application of high concentrations of therapeutic enzymes via intrathecal (IT) injections could successfully drive uptake across the ependyma to treat brain disease. We studied IT enzyme replacement therapy with recombinant human iduronidase (rhIDU) in canine mucopolysaccharidosis I (MPS I, Hurler syndrome), a lysosomal storage disorder with brain and meningeal involvement. Monthly or quarterly IT treatment regimens with rhIDU achieved supranormal iduronidase enzyme levels in the brain, spinal cord, and spinal meninges. All regimens normalized total brain glycosaminoglycan (GAG) storage and reduced spinal meningeal GAG storage by 58-70%. The improvement in GAG storage levels persisted three months after the final IT dose. The successful use of enzyme therapy via the CSF represents a potentially useful approach for lysosomal storage disorders.

Published

2007

37. 602. Stem Cell Transplantation in a Novel, Long-Lived, and Highly Engraftable Immunodeficient Mouse Model of Mucopolysaccharidosis Type I

Author

Anthony D. Rangel, Alexander E. Stover, Daniel C. Mendez, Philip H. Schwartz, Omar Khalid, Patricia I. Dickson, Steven Q. Le, and Shih-hsin Kan

Subjects

Pharmacology, Biology, Neural stem cell, Transplantation, Haematopoiesis, Mucopolysaccharidosis type I, Gliosis, Immunology, Drug Discovery, medicine, Genetics, Molecular Medicine, Stem cell, medicine.symptom, Iduronidase, Molecular Biology, Hexosaminidase activity

Abstract

Mucopolysaccharidosis type I (MPS I) is an inherited α-L-iduronidase (IDUA, I) deficiency in which glycosaminoglycan (GAG) accumulation causes progressive multi-system organ dysfunction, neurological impairment, and death. We developed a new MPS I model based on a NOD/SCID/Il2rγ (NSG) background. This model lives longer than one year and is tumor-free during that time. NSG MPS I (NSGI) mice exhibit the typical phenotypic features of MPS I including coarsened fur and facial features, reduced/abnormal gait, kyphosis, and corneal clouding. IDUA is undetectable in all tissues examined while GAG levels are dramatically higher in most tissues. NSGI brain shows a significant inflammatory response and prominent gliosis. Neurological MPS I manifestations are evidenced by impaired performance in behavioral tests. Human neural and hematopoietic stem cells (HSCs) were found to readily engraft, with human cells detectable for at least one year post-transplantation. HSC transplantation at birth gave rise to improvement in behavioral parameters that lasted at least 3 months after transplantation. View Large Image | Download PowerPoint SlideBy 6 months, however, these effects were no longer present. Biochemical and cytometric analyses at 9 months after HSC transplantation showed that iduronidase activity in the liver and hexosaminidase activity in the brain were correlated with levels of HSC engraftment. Behavior at 9 months, however, was not correlated with levels of HSC engraftment suggesting that HSC engraftment, in and of itself, was insufficient to give a prolonged behavioral effect. Future studies will examine the effects of neural stem cells engraftment, with and without concomitant HSC engraftment.

Published

2015

38. Cardiovascular-related proteins identified in human plasma by the HUPO Plasma Proteome Project Pilot Phase

Author

Richard C. Jones, Aaron Huang, Peipei Ping, David A. Liem, Xin Qiao, Beniam Berhane, Steven Q. Le, Ricky D. Edmondson, Thomas M. Vondriska, Julian P. Whitelegge, and Chenggong Zong

Subjects

Genetic Markers, Proteomics, Proteome, Transcription, Genetic, Arteriosclerosis, Myocardial Infarction, Myocardial Ischemia, Pilot Projects, Inflammation, Computational biology, Disease, Biology, Cardiovascular System, Biochemistry, Mass Spectrometry, medicine, Humans, Databases, Protein, Receptor, Molecular Biology, Transcription factor, Cytoskeleton, Cell Proliferation, Proteomic Profiling, Blood Proteins, Blood proteins, Cardiovascular Diseases, Immunology, medicine.symptom, Peptides

Abstract

Proteomic profiling of accessible bodily fluids, such as plasma, has the potential to accelerate biomarker/biosignature development for human diseases. The HUPO Plasma Proteome Project pilot phase examined human plasma with distinct proteomic approaches across multiple laboratories worldwide. Through this effort, we confidently identified 3020 proteins, each requiring a minimum of two high-scoring MS/MS spectra. A critical step subsequent to protein identification is functional annotation, in particular with regard to organ systems and disease. Performing exhaustive literature searches, we have manually annotated a subset of these 3020 proteins that have cardiovascular-related functions on the basis of an existing body of published information. These cardiovascular-related proteins can be organized into eight groups: markers of inflammation and/or cardiovascular disease, vascular and coagulation, signaling, growth and differentiation, cytoskeletal, transcription factors, channels/receptors and heart failure and remodeling. In addition, analysis of the peptide per protein ratio for MS/MS identification reveals group-specific trends. These findings serve as a resource to interrogate the functions of plasma proteins, and moreover, the list of cardiovascular-related proteins in plasma constitutes a baseline proteomic blueprint for the future development of biosignatures for diseases such as myocardial ischemia and atherosclerosis.

Published

2005

39. Intrathecal enzyme replacement therapy reduces lysosomal storage in the brain and meninges of the canine model of MPS I

Author

Emil D. Kakkis, Patricia I. Dickson, Stephen Hanson, Beth Levy, William C. Mobley, Steven Q. Le, Merry Passage, Michael F. McEntee, Carole Vogler, and Pavel V. Belichenko

Subjects

Pathology, medicine.medical_specialty, Mucopolysaccharidosis I, Endocrinology, Diabetes and Metabolism, Central nervous system, Biochemistry, Iduronidase, Dogs, Meninges, Endocrinology, Cerebrospinal fluid, Immune system, Reference Values, Genetics, Lysosomal storage disease, Animals, Humans, Medicine, Tissue Distribution, Molecular Biology, Injections, Spinal, Glycosaminoglycans, Dose-Response Relationship, Drug, business.industry, Brain, Enzyme replacement therapy, medicine.disease, Recombinant Proteins, Disease Models, Animal, medicine.anatomical_structure, Immune System, Lysosomes, business

Abstract

Enzyme replacement therapy (ERT) has been developed for several lysosomal storage disorders, including mucopolysaccharidosis I (MPS I), and is effective at reducing lysosomal storage in many tissues and in ameliorating clinical disease. However, intravenous ERT does not adequately treat storage disease in the central nervous system (CNS), presumably due to effects of the blood-brain barrier on enzyme distribution. To circumvent this barrier, we studied whether intrathecal (IT) recombinant human alpha-L-iduronidase (rhIDU) could penetrate and treat the brain and meninges. An initial dose-response study showed that doses of 0.46-4.14 mg of IT rhIDU successfully penetrated the brain of normal dogs and reached tissue levels 5.6 to 18.9-fold normal overall and 2.7 to 5.9-fold normal in deep brain sections lacking CSF contact. To assess the efficacy and safety in treating lysosomal storage disease, four weekly doses of approximately 1 mg of IT rhIDU were administered to MPS I-affected dogs resulting in a mean 23- and 300-fold normal levels of iduronidase in total brain and meninges, respectively. Quantitative glycosaminoglycan (GAG) analysis showed that the IT treatment reduced mean total brain GAG to normal levels and achieved a 57% reduction in meningeal GAG levels accompanied by histologic improvement in lysosomal storage in all cell types. The dogs did develop a dose-dependent immune response against the recombinant human protein and a meningeal lymphocytic/plasmacytic infiltrate. The IT route of ERT administration may be an effective way to treat the CNS disease in MPS I and could be applicable to other lysosomal storage disorders.

Published

2004

40. A novel, long-lived, and highly engraftable immunodeficient mouse model of mucopolysaccharidosis type I

Author

Daniel C. Mendez, Philip H. Schwartz, Patricia I. Dickson, Alexander E. Stover, Cian McGuire, Andrew Wong, James V. Jester, Anthony D. Rangel, Marissa A. Torres, Hubert E. Nethercott, Steven Q. Le, Jonathan D. Cooper, Shih hsin Kan, Edwin S. Monuki, David J. Brick, and Omar Khalid

Subjects

lcsh:QH426-470, Nod, Article, 03 medical and health sciences, Mucopolysaccharidosis type I, 0302 clinical medicine, Genetics, medicine, lcsh:QH573-671, Induced pluripotent stem cell, Molecular Biology, 030304 developmental biology, 0303 health sciences, business.industry, lcsh:Cytology, Organ dysfunction, Transplantation, Haematopoiesis, lcsh:Genetics, Gliosis, Immunology, Molecular Medicine, medicine.symptom, Stem cell, business, 030217 neurology & neurosurgery

Abstract

Mucopolysaccharidosis type I (MPS I) is an inherited α-L-iduronidase (IDUA, I) deficiency in which glycosaminoglycan (GAG) accumulation causes progressive multisystem organ dysfunction, neurological impairment, and death. Current MPS I mouse models, based on a NOD/SCID (NS) background, are short-lived, providing a very narrow window to assess the long-term efficacy of therapeutic interventions. They also develop thymic lymphomas, making the assessment of potential tumorigenicity of human stem cell transplantation problematic. We therefore developed a new MPS I model based on a NOD/SCID/Il2rγ (NSG) background. This model lives longer than 1 year and is tumor-free during that time. NSG MPS I (NSGI) mice exhibit the typical phenotypic features of MPS I including coarsened fur and facial features, reduced/abnormal gait, kyphosis, and corneal clouding. IDUA is undetectable in all tissues examined while GAG levels are dramatically higher in most tissues. NSGI brain shows a significant inflammatory response and prominent gliosis. Neurological MPS I manifestations are evidenced by impaired performance in behavioral tests. Human neural and hematopoietic stem cells were found to readily engraft, with human cells detectable for at least 1 year posttransplantation. This new MPS I model is thus suitable for preclinical testing of novel pluripotent stem cell-based therapy approaches.

Published

2015

41. Delivery of an enzyme-IGFII fusion protein to the mouse brain is therapeutic for mucopolysaccharidosis type IIIB

Author

Shih-hsin Kan, Zhi Chen, Stuart Bunting, Brett E. Crawford, Wesley Wong, Anil Bagri, Evan G. Adintori, John Holtzinger, Melanie J. Lo, Elizabeth F. Neufeld, Danielle Crippen-Harmon, Paul A. Fitzpatrick, Jillian R. Brown, Josh C. Woloszynek, Pascale M.N. Tiger, Kristen N. Vondrak, Diana S. Cheung, Kazuhiro Ohmi, Jon Vincelette, Sherry Bullens, Jonathan H. LeBowitz, Chuck Hague, Steven Q. Le, Roger Lawrence, Terri Christianson, Bryan K. Yip, Daniel J. Wendt, Katherine A. Webster, Mika Aoyagi-Scharber, and Patricia I. Dickson

Subjects

Aging, Mucopolysaccharidoses (MPS), Neurodegenerative, Alzheimer's Disease, chemistry.chemical_compound, Mice, Mucopolysaccharidosis III, Drug Delivery Systems, Cricetinae, Lysosomal storage disease, Cells, Cultured, Sanfilippo syndrome, Neurons, Multidisciplinary, Cultured, LAMP1, Brain, Heparan sulfate, Enzyme replacement therapy, Biological Sciences, Endocytosis, beta-N-Acetylhexosaminidases, Liver, Neurological, Biotechnology, Protein Binding, Protein subunit, Cells, Intraventricular, Recombinant Fusion Proteins, CHO Cells, Biology, Injections, Rare Diseases, Cricetulus, Insulin-Like Growth Factor II, Acetylglucosaminidase, medicine, Acquired Cognitive Impairment, Animals, Humans, Metabolic and endocrine, Injections, Intraventricular, Neurosciences, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Lysosome-Associated Membrane Glycoproteins, Fibroblasts, medicine.disease, Fusion protein, Molecular biology, Brain Disorders, Orphan Drug, chemistry, Dementia, Heparitin Sulfate, Biomarkers

Abstract

Mucopolysaccharidosis type IIIB (MPS IIIB, Sanfilippo syndrome type B) is a lysosomal storage disease characterized by profound intellectual disability, dementia, and a lifespan of about two decades. The cause is mutation in the gene encoding α–N-acetylglucosaminidase (NAGLU), deficiency of NAGLU, and accumulation of heparan sulfate. Impediments to enzyme replacement therapy are the absence of mannose 6-phosphate on recombinant human NAGLU and the blood–brain barrier. To overcome the first impediment, a fusion protein of recombinant NAGLU and a fragment of insulin-like growth factor II (IGFII) was prepared for endocytosis by the mannose 6-phosphate/IGFII receptor. To bypass the blood–brain barrier, the fusion protein (“enzyme”) in artificial cerebrospinal fluid (“vehicle”) was administered intracerebroventricularly to the brain of adult MPS IIIB mice, four times over 2 wk. The brains were analyzed 1–28 d later and compared with brains of MPS IIIB mice that received vehicle alone or control (heterozygous) mice that received vehicle. There was marked uptake of the administered enzyme in many parts of the brain, where it persisted with a half-life of approximately 10 d. Heparan sulfate, and especially disease-specific heparan sulfate, was reduced to control level. A number of secondary accumulations in neurons [β-hexosaminidase, LAMP1(lysosome-associated membrane protein 1), SCMAS (subunit c of mitochondrial ATP synthase), glypican 5, β-amyloid, P-tau] were reduced almost to control level. CD68, a microglial protein, was reduced halfway. A large amount of enzyme also appeared in liver cells, where it reduced heparan sulfate and β-hexosaminidase accumulation to control levels. These results suggest the feasibility of enzyme replacement therapy for MPS IIIB.

Published

2014

42. Intra-articular Enzyme Replacement Therapy with rhIDUA is Safe, Well-Tolerated, and Reduces Articular GAG Storage in the Canine Model of Mucopolysaccharidosis Type I

Author

Jeffrey D. Esko, Raymond Y. Wang, Shih-hsin Kan, Catalina Guerra, Calogera M. Simonaro, Patricia I. Dickson, Afshin Aminian, N. Matthew Ellinwood, Roger Lawrence, Michael F. McEntee, Steven Q. Le, and William C. Lamanna

Subjects

musculoskeletal diseases, Cartilage, Articular, Pathology, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Mucopolysaccharidosis, Mucopolysaccharidosis I, Clinical Sciences, Plasma Cells, Biochemistry, Article, Antibodies, Mucopolysaccharidosis type I, Iduronidase, Endocrinology, Chondrocytes, Dogs, Synovial Fluid, Genetics, medicine, Synovial fluid, Animals, Humans, Enzyme Replacement Therapy, Molecular Biology, Glycosaminoglycans, Genetics & Heredity, business.industry, Cartilage, Synovial Membrane, Enzyme replacement therapy, medicine.disease, Recombinant Proteins, Disease Models, Animal, medicine.anatomical_structure, Treatment Outcome, Synovial membrane, business

Abstract

Background: Treatment with intravenous enzyme replacement therapy and hematopoietic stem cell transplantation for mucopolysaccharidosis (MPS) type I does not address joint disease, resulting in persistent orthopedic complications and impaired quality of life. A proof-of-concept study was conducted to determine the safety, tolerability, and efficacy of intra-articular recombinant human iduronidase (IA-rhIDUA) enzyme replacement therapy in the canine MPS I model. Methods: Four MPS I dogs underwent monthly rhIDUA injections (0.58. mg/joint) into the right elbow and knee for 6. months. Contralateral elbows and knees concurrently received normal saline. No intravenous rhIDUA therapy was administered. Monthly blood counts, chemistries, anti-rhIDUA antibody titers, and synovial fluid cell counts were measured. Lysosomal storage of synoviocytes and chondrocytes, synovial macrophages and plasma cells were scored at baseline and 1. month following the final injection. Results: All injections were well-tolerated without adverse reactions. One animal required prednisone for spinal cord compression. There were no clinically significant abnormalities in blood counts or chemistries. Circulating anti-rhIDUA antibody titers gradually increased in all dogs except the prednisone-treated dog; plasma cells, which were absent in all baseline synovial specimens, were predominantly found in synovium of rhIDUA-treated joints at study-end. Lysosomal storage in synoviocytes and chondrocytes following 6. months of IA-rhIDUA demonstrated significant reduction compared to tissues at baseline, and saline-treated tissues at study-end. Mean joint synovial GAG levels in IA-rhIDUA joints were 8.62 ± 5.86 μg/mg dry weight and 21.6 ± 10.4 μg/mg dry weight in control joints (60% reduction). Cartilage heparan sulfate was also reduced in the IA-rhIDUA joints (113 ± 39.5. ng/g wet weight) compared to saline-treated joints (142 ± 56.4. ng/g wet weight). Synovial macrophage infiltration, which was present in all joints at baseline, was abolished in rhIDUA-treated joints only. Conclusions: Intra-articular rhIDUA is well-tolerated and safe in the canine MPS I animal model. Qualitative and quantitative assessments indicate that IA-rhIDUA successfully reduces tissue and cellular GAG storage in synovium and articular cartilage, including cartilage deep to the articular surface, and eliminates inflammatory macrophages from synovial tissue. Clinical relevance: The MPS I canine IA-rhIDUA results suggest that clinical studies should be performed to determine if IA-rhIDUA is a viable approach to ameliorating refractory orthopedic disease in human MPS I. © 2014 Elsevier Inc.

Published

2014

43. Immune response to intrathecal enzyme replacement therapy in mucopolysaccharidosis I patients

Author

David E. Naylor, Shih hsin Kan, Agnes Chen, Anton Mlikotic, Hermes Garban, Moin Vera, Patricia I. Dickson, Ilkka Kaitila, Paul Harmatz, and Steven Q. Le

Subjects

Adult, Male, Spinal, Mucopolysaccharidoses (MPS), animal diseases, Mucopolysaccharidosis I, chemical and pharmacologic phenomena, Bioinformatics, Intrathecal, Pediatrics, Article, Injections, Paediatrics and Reproductive Medicine, Iduronidase, Young Adult, Immune system, Rare Diseases, Clinical Research, Medicine, Humans, Young adult, Child, Preschool, Injections, Spinal, business.industry, Pain Research, Neurosciences, Infant, Enzyme replacement therapy, biochemical phenomena, metabolism, and nutrition, Recombinant Proteins, Child, Preschool, Pediatrics, Perinatology and Child Health, Immunology, Public Health and Health Services, bacteria, Female, business

Abstract

BackgroundIntrathecal (IT) enzyme replacement therapy with recombinant human α-L-iduronidase (rhIDU) has been studied to treat glycosaminoglycan storage in the central nervous system of mucopolysaccharidosis (MPS) I dogs and is currently being studied in MPS I patients.MethodsWe studied the immune response to IT rhIDU in MPS I subjects with spinal cord compression who had been previously treated with intravenous rhIDU. We measured the concentrations of specific antibodies and cytokines in serum and cerebrospinal fluid (CSF) collected before monthly IT rhIDU infusions and compared the serologic findings with clinical adverse event (AE) reports to establish temporal correlations with clinical symptoms.ResultsFive MPS I subjects participating in IT rhIDU trials were studied. One subject with symptomatic spinal cord compression had evidence of an inflammatory response with CSF leukocytosis, elevated interleukin-5, and elevated immunoglobulin G. This subject also complained of lower back pain and buttock paresthesias temporally correlated with serologic abnormalities. Clinical symptoms were managed with oral medication, and serologic abnormalities were resolved, although this subject withdrew from the trial to have spinal decompressive surgery.ConclusionIT rhIDU was generally well tolerated in the subjects studied, although one subject had moderate to severe clinical symptoms and serologic abnormalities consistent with an immune response.

Published

2013

44. Insulin-like growth factor II peptide fusion enables uptake and lysosomal delivery of α-N-acetylglucosaminidase to mucopolysaccharidosis type IIIB fibroblasts

Author

Larisa A. Troitskaya, Amanda K. Todd, Patricia I. Dickson, Brigette L. Tippin, Shih hsin Kan, Karyn Haitz, Ariana Di Stefano, Carolyn S. Sinow, and Steven Q. Le

Subjects

medicine.medical_treatment, Recombinant Fusion Proteins, Amino Acid Motifs, Mannose, CHO Cells, Biology, Endocytosis, Biochemistry, Article, chemistry.chemical_compound, Mucopolysaccharidosis III, Cricetulus, Downregulation and upregulation, Insulin-Like Growth Factor II, Cell Line, Tumor, Cricetinae, Acetylglucosaminidase, medicine, Animals, Humans, Receptor, Molecular Biology, Binding Sites, Growth factor, Chinese hamster ovary cell, Cell Biology, Enzyme replacement therapy, Fibroblasts, Molecular biology, Up-Regulation, chemistry, Cell culture, Lysosomes, Protein Binding

Abstract

Enzyme replacement therapy for MPS IIIB (mucopolysaccharidosis type IIIB; also known as Sanfilippo B syndrome) has been hindered by inadequate mannose 6 phosphorylation and cellular uptake of rhNAGLU (recombinant human α-N-acetylglucosaminidase). We expressed and characterized a modified rhNAGLU fused to the receptor-binding motif of IGF-II (insulin-like growth factor 2) (rhNAGLU–IGF-II) to enhance its ability to enter cells using the cation-independent mannose 6-phosphate receptor, which is also the receptor for IGF-II (at a different binding site). RhNAGLU–IGF-II was stably expressed in CHO (Chinese-hamster ovary) cells, secreted and purified to apparent homogeneity. The Km and pH optimum of the fusion enzyme was similar to those reported for rhNAGLU. Both intracellular uptake and confocal microscopy suggested that MPS IIIB fibroblasts readily take up the fusion enzyme via receptor-mediated endocytosis that was inhibited significantly (P

Published

2013

45. Characterization on the cellular distribution of enzyme replacement therapy (ERT) under the influence of humoral immune response in MPS I mouse model

Author

Patti Dickson, Michelina Iacovino, Don Clarke, Kristen N. Vondrak, Shih-hsin Kan, Steven Q. Le, Mark S. Sands, Valentina Sanghez, and Moin Vera

Subjects

Endocrinology, Immune system, business.industry, Endocrinology, Diabetes and Metabolism, Immunology, Cellular distribution, Genetics, Medicine, Enzyme replacement therapy, business, Molecular Biology, Biochemistry

Published

2017

46. AAAV5-mediated gene therapy with choroid plexus-directed α-n-acetyl-glucosaminidase expression in Sanfilippo syndrome type B mice

Author

Shih-hsin Kan, Patricia I. Dickson, and Steven Q. Le

Subjects

Genetics, business.industry, Endocrinology, Diabetes and Metabolism, Genetic enhancement, medicine.disease, Biochemistry, Molecular biology, Endocrinology, Medicine, Choroid plexus, Glucosaminidase, business, Molecular Biology, Sanfilippo syndrome

Published

2017

47. Corpus callosum white matter myelination by neuroimaging and myelin composition analysis in murine mucopolysaccharidosis type I

Author

Jennifer K. Yee, Shih-hsin Kan, Jakub Tolar, Patricia I. Dickson, Igor Nestrasil, Steven Q. Le, Ivan Tkáč, and Nathan Grant

Subjects

Pathology, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Composition analysis, Biology, Corpus callosum, Biochemistry, White matter, Myelin, Mucopolysaccharidosis type I, Endocrinology, medicine.anatomical_structure, Neuroimaging, Genetics, medicine, Molecular Biology

Published

2017

48. 615. Choroid Plexus-Targeted Viral Gene Therapy for Lysosomal Storage Diseases

Author

Stephen G. Kaler, Shih-hsin Kan, Patricia I. Dickson, Steven Q. Le, and Eun-Young Choi

Subjects

Pharmacology, medicine.medical_specialty, Genetic enhancement, Ventricular system, Biology, Cerebrospinal fluid, medicine.anatomical_structure, Endocrinology, Immune system, Cerebral cortex, Internal medicine, Drug Discovery, Immunology, Genetics, medicine, Molecular Medicine, Choroid plexus, Choroid, Molecular Biology, Tropism

Abstract

Lysosomal storage diseases (LSDs) represent a category of approximately 60 inherited neurometabolic illnesses with considerable morbidity and mortality in children and adults. The burden of LSD is high due to the chronic progressive decline in the neurocognitive function of affected individuals that profoundly limits their societal integration. Current therapy for LSDs has focused on recombinant enzyme replacement therapy (ERT), which while promising, is not ideal for numerous reasons, including the short half-lives of ERT with weekly or monthly administration, potential immune responses against ERT may also reduce the effectiveness for the treatment and inefficient passage through the blood-brain barrier. The choroid plexuses are vascularized structures that project into the cerebrospinal fluid (CSF) and feature specialized polarized epithelia derived from neuroectoderm that are post-mitotic, i.e., do not undergo turnover, and produce CSF by transporting water and ions into the brain ventricles. We hypothesized that remodeling these epithelia to secrete missing lysosomal enzymes by one-time administration of a recombinant AAV vector with selective tropism for choroid plexus (e.g., serotype 5) would be an attractive strategy for long-term treatment of LSDs. Potentially this approach would result in steady secretion of the missing enzyme into the CSF, which normally carries molecules throughout the ventricular system into the subarachnoid space, and ultimately deliver enzyme to the entire brain. The cross-correction phenomenon in many LSDs would provide a further advantage. To evaluate this hypothesis in preclinical animal models, we chose two prototypical LSDs, α-mannosidosis and mucopolysaccharidosis type IIIB (MPS IIIB or Sanfilippo B syndrome). We cloned the respective cDNAs (human (h) LAMAN and NAGLU) into rAAV shuttle plasmids and generated high titer of rAAV5 expressing the enzymes. We administered viral particles to the lateral cerebroventricles sof homozygous mutant mice on day 2 or 3 of life at doses of 5 × 109 or 5 × 1010 vector genomes. In the LAMAN deficient mice, we documented dose-dependent transduction and hLAMAN mRNA expression confined to the choroid plexuses of rAAV5-treated animals. Brain biochemical analyses at 1, 2 and 6 months post-treatment documented sustained, highly statistically significant increases of LAMAN enzyme activity in the brain globally (olfactory bulb, cerebral cortex, cerebellum, brainstem). By 8 months of age, untreated mutant mice showed prominent lysosomal vacuoles in hippocampal neurons, in contrast to rAAV5-hLAMAN treated mutants for which brain histopathology was comparable to wild-type. Lysosomal associated membrane protein 1 (Lamp1) levels were normalized in AAV5-hLAMAN treated mutant brain. In MPS IIIB mutant mice, levels of NAGLU enzyme activity were 2-8 fold higher in brain sections six weeks after rAAV5-hNAGLU treatment compared to normal controls. β-Hexosaminidase activity, which is elevated in MPS IIIB, was reduced to heterozygote carrier levels. Tissue evaluations by immunohistochemistry showed robust hNAGLU expression in the choroid plexus epithelia. Lamp1 expression was significantly reduced in hippocampus and frontal cortex of treated mice. The approach outlined herein challenges existing treatment modalities for LSDs, by exploiting the ability of choroid plexus-targeted gene therapy to restore missing or defective lysosomal enzymes at concentrations and distributions in CSF suitable for disease correction. The potential impact on clinical practice in the field of LSD is high since, if these results extend to larger animal disease models, nonhuman primates, and human subjects, the largest current barriers to health for affected patients would be circumvented.

Published

2016

49. Initial characterization of a murine model of Sanfilippo syndrome type IIID shows similar pathology to other murine models of Sanfilippo syndrome

Author

Patricia I. Dickson, Barbara C. Birtcil, N. Matthew Ellinwood, Jodi D. Smith, Shih-hsin Kan, Steven Q. Le, Maryam Jamil, and Elizabeth M. Snella

Subjects

Pathology, medicine.medical_specialty, business.industry, Endocrinology, Diabetes and Metabolism, 02 engineering and technology, 021001 nanoscience & nanotechnology, medicine.disease, 030226 pharmacology & pharmacy, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Murine model, Genetics, medicine, 0210 nano-technology, business, Molecular Biology, Sanfilippo syndrome

Published

2016

50. Quantification of dermatan sulfate and heparan sulfate in cerebrospinal fluid using liquid chromatography-tandem mass spectrometry for therapeutic monitoring of patients with mucopolysaccharidoses

Author

Steven Q. Le, David S. Millington, Patricia I. Dickson, Marla Weetall, Sarah P. Young, Agnes Chen, and Haoyue Zhang

Subjects

chemistry.chemical_compound, Endocrinology, Chromatography, Cerebrospinal fluid, Chemistry, Liquid chromatography–mass spectrometry, Endocrinology, Diabetes and Metabolism, Genetics, Heparan sulfate, Molecular Biology, Biochemistry, Dermatan sulfate, Therapeutic monitoring

Published

2016