Your search keyword '"Mucopolysaccharidoses genetics"' showing total 434 results

1. α-mannosidosis diagnosis in Brazilian patients with MPS-like symptoms.

Author

Marins M, Curiati MA, Gomes CP, Martin RP, Nicolicht-Amorim P, Yamamoto JUDS, D'Almeida V, Martins AM, and Pesquero JB

Subjects

Humans, Brazil, Female, Male, Child, Child, Preschool, Adolescent, Mucopolysaccharidoses diagnosis, Mucopolysaccharidoses genetics, Infant, Adult, alpha-Mannosidosis diagnosis, alpha-Mannosidosis genetics, alpha-Mannosidase genetics, alpha-Mannosidase metabolism

Abstract

Background: α-mannosidosis is an inborn error of metabolism caused by the deficiency of the lysosomal enzyme α-mannosidase, which is encoded by the MAN2B1 gene and inherited in an autosomal recessive manner. The impairment of affected individuals is multisystemic and very similar to the observed in some mucopolysaccharidosis (MPS) patients. The aim of this study was to search for α-mannosidosis cases in individuals with clinical suspicion of MPS without a confirmed diagnosis. Biochemical and molecular analysis were standardized by our group for this study. Two hundred and fifty samples from patients with clinical suspicion of MPS, but with inconclusive MPS biochemical and/or molecular analysis, were screened for α-mannosidase activity. Subsequently the MAN2B1 gene was sequenced in samples from 53 patients by the Sanger method., Results: The measurement of enzymatic activity detected fifty-three samples with abnormal results, suggesting α-mannosidosis. Molecular analysis confirmed three affected families, which presented the nonsense variant p.Ser899Ter. This variant generates a premature stop codon in exon 22, resulting in a truncated protein with no residual enzymatic activity., Conclusion: In conclusion, this work brings data for the beginning of a genetic characterization of α-mannosidosis in the Brazilian population. It also shows that α-mannosidosis cases may be underdiagnosed due to the clinical similarity to MPS and the lack of information about this ultra-rare disease. Based on our data, we strongly recommend to all screening centers to consider α-mannosidosis testing together with screening for MPS as a tool for diagnosis to MPS-like phenotype individuals, since the phenotype similarity between these diseases poses a significant challenge for clinicians worldwide and often leads to the failure of the correct clinical diagnosis and treatment., Competing Interests: Declarations. Ethics approval and consent to participate: The medical records and samples for retrospective studies were approved by the Ethics Committee in Research of Universidade Federal de São Paulo, and the consent to participate was obtained from the legal guardian (CEP: 0791–2016). Consent for publication: The consent for image publication was obtained from the legal guardian. Disclosures: The authors report no disclosures. Competing interests: The authors declare no conflict of interest and confirm independence from the sponsors. The sponsors have not influenced the content of the article., (© 2024. The Author(s).)

Published

2024

2. Anti-amyloid treatment is broadly effective in neuronopathic mucopolysaccharidoses and synergizes with gene therapy in MPS-IIIA.

Author

Giaccio M, Monaco A, Galiano L, Parente A, Borzacchiello L, Rubino R, Klärner FG, Killa D, Perna C, Piccolo P, Marotta M, Pan X, Khijniak M, Siddique I, Schrader T, Pshezhetsky AV, Sorrentino NC, Bitan G, and Fraldi A

Subjects

Animals, Mice, Humans, Mucopolysaccharidosis III therapy, Mucopolysaccharidosis III genetics, Mucopolysaccharidosis III metabolism, Combined Modality Therapy, Amyloid metabolism, Mucopolysaccharidoses therapy, Mucopolysaccharidoses genetics, Mucopolysaccharidoses metabolism, Biological Products, Recombinant Fusion Proteins, Genetic Therapy methods, Disease Models, Animal, Dependovirus genetics, Genetic Vectors administration & dosage, Genetic Vectors genetics

Abstract

Mucopolysaccharidoses (MPSs) are childhood diseases caused by inherited deficiencies in glycosaminoglycan degradation. Most MPSs involve neurodegeneration, which to date is untreatable. Currently, most therapeutic strategies aim at correcting the primary genetic defect. Among these strategies, gene therapy has shown great potential, although its clinical application is challenging. We have shown previously in an MPS-IIIA mouse model that the molecular tweezer (MT) CLR01, a potent, broad-spectrum anti-amyloid small molecule, inhibits secondary amyloid storage, facilitates amyloid clearance, and protects against neurodegeneration. Here, we demonstrate that combining CLR01 with adeno-associated virus (AAV)-mediated gene therapy, targeting both the primary and secondary pathologic storage in MPS-IIIA mice, results in a synergistic effect that improves multiple therapeutic outcomes compared to each monotherapy. Moreover, we demonstrate that CLR01 is effective therapeutically in mouse models of other forms of neuronopathic MPS, MPS-I, and MPS-IIIC. These strongly support developing MTs as an effective treatment option for neuronopathic MPSs, both on their own and in combination with gene therapy, to improve therapeutic efficacy and translation into clinical application., Competing Interests: Declaration of interests The compositions of matter (patent 1, application 2) and methods of use (applications 3 and 4) of CLR01 are protected by the patents and patent applications listed below. G.B. and T.S. are co-inventors on 1 and 2. A.F. and G.B. are co-inventors on 3 and 4., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

3. Oral Problems in Brazilian Individuals with Rare Genetic Diseases That Affect Skeletal Development.

Author

Rabello F, Celestino MLS, Carneiro NCR, Reis-Oliveira J, Prado HV, Abreu MHNG, and Borges-Oliveira AC

Subjects

Humans, Brazil epidemiology, Male, Female, Adult, Cross-Sectional Studies, Child, Child, Preschool, Adolescent, Young Adult, Middle Aged, Prevalence, Mucopolysaccharidoses epidemiology, Mucopolysaccharidoses genetics, Mouth Diseases epidemiology, Malocclusion epidemiology, Dental Caries epidemiology, Osteogenesis Imperfecta epidemiology, Osteogenesis Imperfecta genetics, Rare Diseases epidemiology, Rare Diseases genetics

Abstract

The present study aimed to compare the prevalence of oral problems between individuals with rare genetic diseases that affect skeletal development and individuals without rare diseases. A cross-sectional study was conducted with 210 individuals between two and fifty-four years of age: 105 with rare genetic diseases (27 with mucopolysaccharidosis [MPS] and 78 with osteogenesis imperfecta [OI]) and 105 without rare diseases. The rare genetic disease group was recruited from hospital units that provide care for patients with MPS and OI in five states of Brazil, and the other group was recruited from the same location. The participants were examined with regards to malocclusion, dental anomalies, dental caries, and gingivitis. A questionnaire was administered addressing individual, sociodemographic, and behavioral characteristics as well as dental history. A descriptive analysis was performed, followed by unadjusted and adjusted binary logistic regression analyses. The mean age was 14.1 ± 12.2 years. Individuals with a rare disease were 12.9-fold more likely to have some type of oral problem (95% CI: 3.7-44.7) compared to the group without rare diseases. The prevalence of oral problems was higher among Brazilians with MPS and OI compared to normotypical individuals.

Published

2024

4. Mucopolysaccharidosis-Plus Syndrome: Is This a Type of Mucopolysaccharidosis or a Separate Kind of Metabolic Disease?

Author

Cyske Z, Gaffke L, Pierzynowska K, and Węgrzyn G

Subjects

Humans, Glycosaminoglycans metabolism, Glycosaminoglycans urine, Mutation, Lysosomes metabolism, Metabolic Diseases metabolism, Metabolic Diseases genetics, Vesicular Transport Proteins genetics, Vesicular Transport Proteins metabolism, Syndrome, Mucopolysaccharidoses genetics, Mucopolysaccharidoses metabolism

Abstract

Several years ago, dozens of cases were described in patients with symptoms very similar to mucopolysaccharidosis (MPS). This new disease entity was described as mucopolysaccharidosis-plus syndrome (MPSPS). The name of the disease indicates that in addition to the typical symptoms of conventional MPS, patients develop other features such as congenital heart defects and kidney and hematopoietic system disorders. The symptoms are highly advanced, and patients usually do not survive past the second year of life. MPSPS is inherited in an autosomal recessive manner and is caused by a homozygous-specific mutation in the gene encoding the VPS33A protein. To date, it has been described in 41 patients. Patients with MPSPS exhibited excessive excretion of glycosaminoglycans (GAGs) in the urine and exceptionally high levels of heparan sulfate in the plasma, but the accumulation of substrates is not caused by a decrease in the activity of any lysosomal enzymes. Here, we discuss the pathomechanisms and symptoms of MPSPS, comparing them to those of MPS. Moreover, we asked the question whether MPSPS should be classified as a type of MPS or a separate disease, as contrary to 'classical' MPS types, despite GAG accumulation, no defects in lysosomal enzymes responsible for degradation of these compounds could be detected in MPSPS. The molecular mechanism of the appearance of GAG accumulation in MPSPS is suggested on the basis of results available in the literature.

Published

2024

5. Causes of death in mucopolysaccharidoses.

Author

Rintz E, Banacki M, Ziemian M, Kobus B, and Wegrzyn G

Subjects

Humans, Male, Child, Female, Child, Preschool, Adolescent, Infant, Adult, Young Adult, Infant, Newborn, Glycosaminoglycans metabolism, Middle Aged, Mucopolysaccharidosis II genetics, Mucopolysaccharidosis II mortality, Mucopolysaccharidoses genetics, Mucopolysaccharidoses complications, Cause of Death

Abstract

Mucopolysaccharidoses are inherited metabolic diseases caused by mutations in genes encoding enzymes required for degradation of glycosaminoglycans. A lack or severe impairment of activity of these enzymes cause accumulation of GAGs which is the primary biochemical defect. Depending on the kind of the deficient enzyme, there are 12 types and subtypes of MPS distinguished. Despite the common primary metabolic deficit (inefficient GAG degradation), the course and symptoms of various MPS types can be different, though majority of the diseases from the group are characterized by severe symptoms and significantly shortened live span. Here, we analysed the frequency of specific, direct causes of death of patients with different MPS types, the subject which was not investigated comprehensively to date. We examined a total of 1317 cases of death among MPS patients, including 393 cases of MPS I, 418 cases of MPS II, 232 cases of MPS III, 45 cases of MPS IV, 208 cases of MPS VI, and 22 cases of MPS VII. Our analyses indicated that the most frequent causes of death differ significantly between MPS types, with cardiovascular and respiratory failures being predominant in MPS I, MPS II, and MPS VI, neurological deficits in MPS III, respiratory issues in MPS IV, and hydrops fetalis in MPS VII. Results of such studies suggest what specific clinical problems should be considered with the highest priority in specific MPS types, apart from attempts to correct the primary causes of the diseases, to improve the quality of life of patients and to prolong their lives., Competing Interests: Declaration of competing interest The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

6. Identification and characterization of novel genetic variants in the first Chinese family of mucopolysaccharidosis IIIC (Sanfilippo C syndrome).

Author

Zhao H, Wang L, Zhang M, Wang H, Zhang S, Wu J, and Tang Y

Subjects

Humans, Acetylation, Acetyltransferases, Asian People genetics, China, Mucopolysaccharidoses genetics, Mucopolysaccharidosis III genetics

Abstract

Mucopolysaccharidosis type IIIC (MPS IIIC) is one of inherited lysosomal storage disorders, caused by deficiencies in lysosomal hydrolases degrading acidic mucopolysaccharides. The gene responsible for MPS IIIC is HGSNAT, which encodes an enzyme that catalyses the acetylation of the terminal glucosamine residues of heparan sulfate. So far, few studies have focused on the genetic landscape of MPS IIIC in China, where IIIA and IIIB were the major subtypes. In this study, we utilized whole-exome sequencing (WES) to identify novel compound heterozygous variants in the HGSNAT gene from a Chinese patient with typical MPS IIIC symptoms: c.743G>A; p.Gly248Glu and c.1030C>T; p.Arg344Cys. We performed in silico analysis and experimental validation, which confirmed the deleterious pathogenic nature of both variants, as evidenced by the loss of HGSNAT activity and failure of lysosomal localization. To the best of our knowledge, the MPS IIIC is first confirmed by clinical, biochemical and molecular genetic findings in China. Our study thus expands the spectrum of MPS IIIC pathogenic variants, which is of importance to dissect the pathogenesis and to carry out clinical diagnosis of MPS IIIC. Moreover, this study helps to depict the natural history of Chinese MPS IIIC populations., (© 2024 The Authors. Journal of Cellular and Molecular Medicine published by Foundation for Cellular and Molecular Medicine and John Wiley & Sons Ltd.)

Published

2024

7. Molecular Mechanisms in Pathophysiology of Mucopolysaccharidosis and Prospects for Innovative Therapy.

Author

Ago Y, Rintz E, Musini KS, Ma Z, and Tomatsu S

Subjects

Humans, Therapies, Investigational, Antibodies, Monoclonal, Glycosaminoglycans, Inflammation, Mucopolysaccharidoses genetics, Mucopolysaccharidoses therapy, Osteochondrodysplasias

Abstract

Mucopolysaccharidoses (MPSs) are a group of inborn errors of the metabolism caused by a deficiency in the lysosomal enzymes required to break down molecules called glycosaminoglycans (GAGs). These GAGs accumulate over time in various tissues and disrupt multiple biological systems, including catabolism of other substances, autophagy, and mitochondrial function. These pathological changes ultimately increase oxidative stress and activate innate immunity and inflammation. We have described the pathophysiology of MPS and activated inflammation in this paper, starting with accumulating the primary storage materials, GAGs. At the initial stage of GAG accumulation, affected tissues/cells are reversibly affected but progress irreversibly to: (1) disruption of substrate degradation with pathogenic changes in lysosomal function, (2) cellular dysfunction, secondary/tertiary accumulation (toxins such as GM2 or GM3 ganglioside, etc.), and inflammatory process, and (3) progressive tissue/organ damage and cell death (e.g., skeletal dysplasia, CNS impairment, etc.). For current and future treatment, several potential treatments for MPS that can penetrate the blood-brain barrier and bone have been proposed and/or are in clinical trials, including targeting peptides and molecular Trojan horses such as monoclonal antibodies attached to enzymes via receptor-mediated transport. Gene therapy trials with AAV, ex vivo LV, and Sleeping Beauty transposon system for MPS are proposed and/or underway as innovative therapeutic options. In addition, possible immunomodulatory reagents that can suppress MPS symptoms have been summarized in this review.

Published

2024

8. Gene therapies for mucopolysaccharidoses.

Author

Rossi A and Brunetti-Pierri N

Subjects

Humans, Brain, Genetic Therapy, Enzyme Replacement Therapy, Mucopolysaccharidoses genetics, Mucopolysaccharidoses therapy, Hematopoietic Stem Cell Transplantation

Abstract

Current specific treatments for mucopolysaccharidoses (MPSs) include enzyme replacement therapy (ERT) and hematopoietic stem cell transplantation (HSCT). Both treatments are hampered by several limitations, including lack of efficacy on brain and skeletal manifestations, need for lifelong injections, and high costs. Therefore, more effective treatments are needed. Gene therapy in MPSs is aimed at obtaining high levels of the therapeutic enzyme in multiple tissues either by engrafted gene-modified hematopoietic stem progenitor cells (ex vivo) or by direct infusion of a viral vector expressing the therapeutic gene (in vivo). This review focuses on the most recent clinical progress in gene therapies for MPSs. The various gene therapy approaches with their strengths and limitations are discussed., (© 2023 The Authors. Journal of Inherited Metabolic Disease published by John Wiley & Sons Ltd on behalf of SSIEM.)

Published

2024

9. Adenotonsillar pathology in mucopolysaccharidoses - lysosomal storage predominates in paracortical CD63+ cells.

Author

Murgasova L, Hulkova H, Baresova V, Jurovcik M, Stritesky J, Jurickova K, Magner M, and Sikora J

Subjects

Humans, Lymphoid Tissue pathology, Lysosomes, Enzyme Replacement Therapy, Tetraspanin 30, Mucopolysaccharidoses diagnosis, Mucopolysaccharidoses drug therapy, Mucopolysaccharidoses genetics

Abstract

Despite the adenoids are regularly removed in patients with mucopolysaccharidoses (MPS), the underlying tissue and cellular pathologies remain understudied. We characterized an (immuno)histopathologic and ultrastructural phenotype dominated by lysosomal storage changes in a specific subset of adenotonsillar paracortical cells in 8 MPS patients (3 MPS I, 3 MPS II, and 2 MPS IIIA). These abnormal cells were effectively detected by an antibody targeting the lysosomal membrane tetraspanin CD63. Important, CD63+ storage vacuoles in these cells lacked the monocytes/macrophages lysosomal marker CD68. Such a distinct patterning of CD63 and CD68 was not present in a patient with infantile neurovisceral variant of acid sphingomyelinase deficiency. The CD63+ storage pathology was absent in two MPS I patients who either received enzyme-replacement therapy or underwent hematopoietic stem cells transplantation prior the adenoidectomy. Our study demonstrates novel features of lysosomal storage patterning and suggests diagnostic utility of CD63 detection in adenotonsillar lymphoid tissue of MPS patients., (© 2023. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature.)

Published

2024

10. Endogenous, non-reducing end glycosaminoglycan biomarkers for the mucopolysaccharidoses: Accurate diagnosis and elimination of false positive newborn screening results.

Author

Saville JT, Herbst ZM, Gelb MH, and Fuller M

Subjects

Infant, Newborn, Humans, Neonatal Screening methods, Tandem Mass Spectrometry methods, Biomarkers, Hydrolases, Glycosaminoglycans metabolism, Mucopolysaccharidoses diagnosis, Mucopolysaccharidoses genetics, Mucopolysaccharidoses metabolism

Abstract

The mucopolysaccharidoses (MPS) are a family of inborn errors of metabolism resulting from a deficiency in a lysosomal hydrolase responsible for the degradation of glycosaminoglycans (GAG). From a biochemical standpoint, excessive urinary excretion of GAG has afforded first-tier laboratory investigations for diagnosis whereas newborn screening programs employ lysosomal hydrolase measurements. Given false positives are not uncommon, second-tier diagnostic testing relies on lysosomal hydrolase measurements following elevated urinary GAG, and newborn screening results are often corroborated with GAG determinations. Molecular genetics requires acknowledgement, as identifying pathogenic variants in the hydrolase genes confirms the diagnosis and allows cascade testing for families, but genetic variants of uncertain significance complicate this paradigm. Initiating cellular, tissue and organ damage that leads to an MPS phenotype is undoubtedly the accumulation of partially degraded GAG, and with mass spectrometry technologies now readily available in the biochemical genetics' laboratory, the ability to properly measure these GAG fragments has been realized. The most common approach involves bacterial lyase/hydrolase digestion of the long chain GAG polymers into their disaccharide units that can be measured by mass spectrometry. Another, less well-known method, the endogenous, non-reducing end method, does not require depolymerization of GAG but rather relies on the mass spectrometric measurement of the naturally produced oligosaccharides that arise from the enzyme deficiency. All MPS can be identified by this one method, and evidence to date shows it to be the only GAG analysis method that gives no false positives when employed as a first-tier laboratory diagnostic test and second-tier newborn screening test., Competing Interests: Declaration of Competing Interest MF, JTS and ZMH have no conflicts of interest to declare, and MHG is a co-founder of GelbChem, LLC., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published

2023

11. Dysregulation of genes coding for proteins involved in metabolic processes in mucopolysaccharidoses, evidenced by a transcriptomic approach.

Author

Pierzynowska K, Deresz P, Węgrzyn G, and Gaffke L

Subjects

Humans, Glycosaminoglycans genetics, Glycosaminoglycans metabolism, Cell Line, Lysosomes metabolism, Transcriptome genetics, Mucopolysaccharidoses genetics, Mucopolysaccharidoses pathology

Abstract

Mucopolysaccharidoses (MPS) are a group of lysosomal storage diseases (LSD) caused by mutations in genes coding for enzymes responsible for degradation of glycosaminoglycans (GAGs). Most types of these severe disorders are characterized by neuronopathic phenotypes. Although lysosomal accumulation of GAGs is the primary metabolic defect in MPS, secondary alterations in biochemical processes are considerable and influence the course of the disease. Early hypothesis suggested that these secondary changes might be due to lysosomal storage-mediated impairment of activities of other enzymes, and subsequent accumulation of various compounds in cells. However, recent studies indicated that expression of hundreds of genes is changed in MPS cells. Therefore, we asked whether metabolic effects observed in MPS are caused primarily by GAG-mediated inhibition of specific biochemical reactions or appear as results of dysregulation of expression of genes coding for proteins involved in metabolic processes. Transcriptomic analyses of 11 types of MPS (using RNA isolated from patient-derived fibroblasts), performed in this study, showed that a battery of the above mentioned genes is dysregulated in MPS cells. Some biochemical pathways might be especially affected by changes in expression of many genes, including GAG metabolism and sphingolipid metabolism which is especially interesting as secondary accumulation of various sphingolipids is one of the best known additional (while significantly enhancing neuropathological effects) metabolic defects in MPS. We conclude that severe metabolic disturbances, observed in MPS cells, can partially arise from changes in the expression of many genes coding for proteins involved in metabolic processes., (© 2023. The Author(s).)

Published

2023

12. Contribution of vesicle trafficking dysregulation to the pathomechanism of mucopolysaccharidosis.

Author

Gaffke L, Pierzynowska K, Cyske Z, Podlacha M, and Węgrzyn G

Subjects

Mice, Animals, Cell Line, Glycosaminoglycans metabolism, Golgi Matrix Proteins metabolism, Adaptor Proteins, Signal Transducing metabolism, Mucopolysaccharidoses genetics, Mucopolysaccharidoses drug therapy, Mucopolysaccharidoses metabolism

Abstract

Although mucopolysaccharidoses (MPS) are monogenic diseases, caused by mutations in genes coding for enzymes involved in degradation of glycosaminoglycans (GAGs), recent studies suggested that changes in expressions of various genes might cause secondary and tertiary cellular dysfunctions modulating the course of these diseases. In this report, we demonstrate that vesicle trafficking regulation is affected in fibroblasts derived from patients suffering from 11 different types of MPS due to changes in levels of crucial proteins (estimated by automated Western-blotting) involved in this process, including caveolin, clathrin, huntingtin (Htt), APPL1, EEA1, GOPC, Rab5, and Rab7. Microscopic studies confirmed these results, while investigations of tissue samples derived from the MPS I mouse model indicated differences between various organs in this matter. Moreover, transcriptomic analyses provided a global picture for changes in expressions of genes related to vesicle trafficking in MPS cells. We conclude that vesicle trafficking is dysregulated in MPS cells and changes in this process might contribute to the molecular mechanisms of this disease. Most probably, primary GAG storage might cause a cellular stress response leading to dysregulation of expression of many genes which, in turn, results in changes in cellular processes like vesicle trafficking. This can significantly modulate the course of the disease due to enhancing accumulation of GAGs and altering crucial cellular processes. This hypothesis has been supported by normalization of levels of clathrin in MPS cells treated with either an active form of the deficient GAG-degrading enzyme or a compound (5,7-dihydroxy-3-(4-hydroxyphenyl)-4H-1-benzopyran-4-one) indirectly reducing the efficiency of GAG synthesis., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2023

13. Intraparenchymal convection enhanced delivery of AAV in sheep to treat Mucopolysaccharidosis IIIC.

Author

O'Leary C, Forte G, Mitchell NL, Youshani AS, Dyer A, Wellby MP, Russell KN, Murray SJ, Jolinon N, Jones SA, Stacey K, Davis DM, Henckaerts E, Palmer DN, Kamaly-Asl I, and Bigger BW

Subjects

Animals, Acetyltransferases genetics, Acetyltransferases metabolism, Brain, Dependovirus genetics, Disease Models, Animal, Genetic Vectors, Heparitin Sulfate metabolism, Mucopolysaccharidoses genetics, Mucopolysaccharidoses therapy, Sheep, Genetic Therapy, Mucopolysaccharidosis III genetics, Mucopolysaccharidosis III metabolism, Mucopolysaccharidosis III therapy

Abstract

Background: Mucopolysaccharidosis IIIC (MPSIIIC) is one of four Sanfilippo diseases sharing clinical symptoms of severe cognitive decline and shortened lifespan. The missing enzyme, heparan sulfate acetyl-CoA: α-glucosaminide-N-acetyltransferase (HGSNAT), is bound to the lysosomal membrane, therefore cannot cross the blood-brain barrier or diffuse between cells. We previously demonstrated disease correction in MPSIIIC mice using an Adeno-Associated Vector (AAV) delivering HGSNAT via intraparenchymal brain injections using an AAV2 derived AAV-truetype (AAV-TT) serotype with improved distribution over AAV9., Methods: Here, intraparenchymal AAV was delivered in sheep using catheters or Hamilton syringes, placed using Brainlab cranial navigation for convection enhanced delivery, to reduce proximal vector expression and improve spread., Results: Hamilton syringes gave improved AAV-GFP distribution, despite lower vector doses and titres. AAV-TT-GFP displayed moderately better transduction compared to AAV9-GFP but both serotypes almost exclusively transduced neurons. Functional HGSNAT enzyme was detected in 24-37% of a 140g gyrencephalic sheep brain using AAV9-HGSNAT with three injections in one hemisphere., Conclusions: Despite variabilities in volume and titre, catheter design may be critical for efficient brain delivery. These data help inform a clinical trial for MPSIIIC., (© 2023. The Author(s).)

Published

2023

14. Mucopolysaccharidoses Differential Diagnosis by Mass Spectrometry-Based Analysis of Urine Free Glycosaminoglycans-A Diagnostic Prediction Model.

Author

D'Avanzo F, Zanetti A, Dardis A, Scarpa M, Volpi N, Gatto F, and Tomanin R

Subjects

Humans, Tandem Mass Spectrometry, Diagnosis, Differential, Hydrolases genetics, Glycosaminoglycans, Mucopolysaccharidoses diagnosis, Mucopolysaccharidoses genetics, Mucopolysaccharidoses metabolism

Abstract

Impaired glycosaminoglycans (GAGs) catabolism may lead to a cluster of rare metabolic and genetic disorders called mucopolysaccharidoses (MPSs). Each subtype is caused by the deficiency of one of the lysosomal hydrolases normally degrading GAGs. Affected tissues accumulate undegraded GAGs in cell lysosomes and in the extracellular matrix, thus leading to the MPS complex clinical phenotype. Although each MPS may present with recognizable signs and symptoms, these may often overlap between subtypes, rendering the diagnosis difficult and delayed. Here, we performed an exploratory analysis to develop a model that predicts MPS subtypes based on UHPLC-MS/MS measurement of a urine free GAG profile (or GAGome). We analyzed the GAGome of 78 subjects (38 MPS, 37 healthy and 3 with other MPS symptom-overlapping disorders) using a standardized kit in a central-blinded laboratory. We observed several MPS subtype-specific GAGome changes. We developed a multivariable penalized Lasso logistic regression model that attained 91.2% balanced accuracy to distinguish MPS type II vs. III vs. any other subtype vs. not MPS, with sensitivity and specificity ranging from 73.3% to 91.7% and from 98.4% to 100%, depending on the predicted subtype. In conclusion, the urine GAGome was revealed to be useful in accurately discriminating the different MPS subtypes with a single UHPLC-MS/MS run and could serve as a reliable diagnostic test for a more rapid MPS biochemical diagnosis.

Published

2023

15. Mucopolysaccharidoses: Cellular Consequences of Glycosaminoglycans Accumulation and Potential Targets.

Author

Leal AF, Benincore-Flórez E, Rintz E, Herreño-Pachón AM, Celik B, Ago Y, Alméciga-Díaz CJ, and Tomatsu S

Subjects

Humans, Glycosaminoglycans therapeutic use, Lysosomes, Enzyme Replacement Therapy, Mucopolysaccharidoses genetics, Lysosomal Storage Diseases drug therapy

Abstract

Mucopolysaccharidoses (MPSs) constitute a heterogeneous group of lysosomal storage disorders characterized by the lysosomal accumulation of glycosaminoglycans (GAGs). Although lysosomal dysfunction is mainly affected, several cellular organelles such as mitochondria, endoplasmic reticulum, Golgi apparatus, and their related process are also impaired, leading to the activation of pathophysiological cascades. While supplying missing enzymes is the mainstream for the treatment of MPS, including enzyme replacement therapy (ERT), hematopoietic stem cell transplantation (HSCT), or gene therapy (GT), the use of modulators available to restore affected organelles for recovering cell homeostasis may be a simultaneous approach. This review summarizes the current knowledge about the cellular consequences of the lysosomal GAGs accumulation and discusses the use of potential modulators that can reestablish normal cell function beyond ERT-, HSCT-, or GT-based alternatives.

Published

2022

16. Gene editing strategies to treat lysosomal disorders: The example of mucopolysaccharidoses.

Author

Fachel FNS, Frâncio L, Poletto É, Schuh RS, Teixeira HF, Giugliani R, Baldo G, and Matte U

Subjects

Animals, Gene Editing, Enzyme Replacement Therapy methods, Lysosomes, Mucopolysaccharidoses genetics, Mucopolysaccharidoses therapy, Mucopolysaccharidoses diagnosis, Lysosomal Storage Diseases therapy, Lysosomal Storage Diseases drug therapy

Abstract

Lysosomal storage disorders are a group of progressive multisystemic hereditary diseases with a combined incidence of 1:4,800. Here we review the clinical and molecular characteristics of these diseases, with a special focus on Mucopolysaccharidoses, caused primarily by the lysosomal storage of glycosaminoglycans. Different gene editing techniques can be used to ameliorate their symptoms, using both viral and nonviral delivery methods. Whereas these are still being tested in animal models, early results of phase I/II clinical trials of gene therapy show how this technology may impact the future treatment of these diseases. Hurdles related to specific hard-to-reach organs, such as the central nervous system, heart, joints, and the eye must be tackled. Finally, the regulatory framework necessary to advance into clinical practice is also discussed., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published

2022

17. Mucopolysaccharidosis-Plus Syndrome: Report on a Polish Patient with a Novel VPS33A Variant with Comparison with Other Described Patients.

Author

Lipiński P, Szczałuba K, Buda P, Zakharova EY, Baydakova G, Ługowska A, Różdzyńska-Świątkowska A, Cyske Z, Węgrzyn G, Pollak A, Płoski R, and Tylki-Szymańska A

Subjects

Chondroitin Sulfates urine, Glycosaminoglycans urine, Humans, Mutation, Poland, Sphingolipids blood, Mucopolysaccharidoses blood, Mucopolysaccharidoses diagnosis, Mucopolysaccharidoses genetics, Mucopolysaccharidoses urine, Vesicular Transport Proteins genetics

Abstract

Eleven patients from Yakutia with a new lysosomal disease assumed then as mucopolysaccharidosis-plus syndrome (MPS-PS) were reported by Gurinova et al. in 2014. Up to now, a total number of 39 patients have been reported; in all of them, the c.1492C>T (p.Arg498Trp) variant of the VPS33A gene was detected. Here, we describe the first Polish MPS-PS patient with a novel homozygous c.599G>C (p.Arg200Pro) VPS33A variant presenting over 12 years of follow-up with some novel clinical features, including fetal ascites (resolved spontaneously), recurrent joint effusion and peripheral edemas, normal growth, and visceral obesity. Functional analyses revealed a slight presence of chondroitin sulphate (only) in urine glycosaminoglycan electrophoresis, presence of sialooligosaccharides in urine by thin-layer chromatography, and normal results of lysosomal enzymes activity and lysosphingolipids concentration in dried blood spot. The comparison with other MPS-PS described cases was also provided. The presented description of the natural history of MPS-PS in our patient may broaden the spectrum of phenotypes in this disease.

Published

2022

18. Delivery and assessment of a CRISPR/nCas9-based genome editing system on in vitro models of mucopolysaccharidoses IVA assisted by magnetite-based nanoparticles.

Author

Leal AF, Cifuentes J, Torres CE, Suárez D, Quezada V, Gómez SC, Cruz JC, Reyes LH, Espejo-Mojica AJ, and Alméciga-Díaz CJ

Subjects

Clustered Regularly Interspaced Short Palindromic Repeats, Ferrosoferric Oxide therapeutic use, Gene Editing, Glycosaminoglycans, Humans, Chondroitinsulfatases genetics, Mucopolysaccharidoses genetics, Mucopolysaccharidoses therapy, Mucopolysaccharidosis IV genetics, Mucopolysaccharidosis IV therapy, Nanoparticles

Abstract

Mucopolysaccharidosis IV A (MPS IVA) is a lysosomal disorder caused by mutations in the GALNS gene. Consequently, the glycosaminoglycans (GAGs) keratan sulfate and chondroitin 6-sulfate accumulate in the lysosomal lumen. Although enzyme replacement therapy has shown essential advantages for the patients, several challenges remain to overcome, such as the limited impact on the bone lesion and recovery of oxidative profile. Recently, we validated a CRISPR/nCas9-based gene therapy with promising results in an in vitro MPS IVA model. In this study, we have expanded the use of this CRISPR/nCas9 system to several MPS IVA fibroblasts carrying different GALNS mutations. Considering the latent need to develop more safety vectors for gene therapy, we co-delivered the CRISPR/nCas9 system with a novel non-viral vector based on magnetoliposomes (MLPs). We found that the CRISPR/nCas9 treatment led to an increase in enzyme activity between 5 and 88% of wild-type levels, as well as a reduction in GAGs accumulation, lysosomal mass, and mitochondrial-dependent oxidative stress, in a mutation-dependent manner. Noteworthy, MLPs allowed to obtain similar results to those observed with the conventional transfection agent lipofectamine. Overall, these results confirmed the potential of CRISPR/nCas9 as a genome editing tool for treating MPS IVA. We also demonstrated the potential use of MLPs as a novel delivery system for CRISPR/nCas9-based therapies., (© 2022. The Author(s).)

Published

2022

19. Updated Confirmatory Diagnosis for Mucopolysaccharidoses in Taiwanese Infants and the Application of Gene Variants.

Author

Chuang CK, Tu YR, Lee CL, Lo YT, Chang YH, Liu MY, Liu HY, Chen HJ, Kao SM, Wang LY, Ho HJ, Lin HY, and Lin SP

Subjects

Disaccharides, Glycosaminoglycans genetics, Humans, Infant, Infant, Newborn, Tandem Mass Spectrometry methods, Mucopolysaccharidoses diagnosis, Mucopolysaccharidoses genetics, Mucopolysaccharidosis I, Mucopolysaccharidosis II

Abstract

Mucopolysaccharidosis (MPS) is a lysosomal storage disease caused by genetic defects that result in deficiency of one specific enzyme activity, consequently impairing the stepwise degradation of glycosaminoglycans (GAGs). Except for MPS II, the other types of MPS have autosomal recessive inheritance in which two copies of an abnormal allele must be present in order for the disease to develop. In this study, we present the status of variant alleles and biochemistry results found in infants suspected of having MPS I, II, IVA, and VI. A total of 324 suspected infants, including 12 for MPS I, 223 for MPS II, 72 for MPS IVA, and 17 for MPS VI, who were referred for MPS confirmation from newborn screening centers in Taiwan, were enrolled. In all of these infants, one specific enzyme activity in dried blood spot filter paper was lower than the cut-off value in the first blood sample, as well asin a second follow-up sample. The confirmatory methods used in this study included Sanger sequencing, next-generation sequencing, leukocyte enzyme fluorometric assay, and GAG-derived disaccharides in urine using tandem mass spectrometry assays. The results showed that five, nine, and six infants had MPS I, II, and IVA, respectively, and all of them were asymptomatic. Thus, a laboratory diagnosis is extremely important to confirm the diagnosis of MPS. The other infants with identified nucleotide variations and reductions in leukocyte enzyme activities were categorized as being highly suspected cases requiring long-term and intensive follow-up examinations. In summary, the final confirmation of MPS depends on the most powerful biomarkers found in urine, i.e., the quantification of GAG-derived disaccharides including dermatan sulfate, heparan sulfate, and keratan sulfate, and analysis of genetic variants can help predict outcomes and guide treatment.

Published

2022

20. Cell cycle disturbances in mucopolysaccharidoses: Transcriptomic and experimental studies on cellular models.

Author

Brokowska J, Gaffke L, Pierzynowska K, Cyske Z, and Węgrzyn G

Subjects

Humans, Cyclin D1 metabolism, Transcriptome genetics, Cell Line, Glycosaminoglycans, Cell Cycle genetics, Cell Division, Genistein pharmacology, Genistein therapeutic use, Mucopolysaccharidoses genetics, Mucopolysaccharidoses metabolism, Mucopolysaccharidoses therapy

Abstract

Mucopolysaccharidoses (MPS) are a group of lysosomal storage diseases caused by defects in genes coding for proteins involved in degradation of glycosaminoglycans (GAGs). These complex carbohydrates accumulate in cells causing their serious dysfunctions. Apart from the physical GAG storage, secondary and tertiary changes may contribute significantly to the pathomechanism of the disease. Among processes which were not systematically investigated in MPS cells to date there is the cell cycle. Here, we studied perturbances in this crucial cellular process in majority of MPS types. Transcriptomic analyses indicated that expression of many genes coding for proteins involved in the cell cycle is dysregulated in all tested MPS cells. Importantly, levels of transcripts of particular genes were changed in the same manner (i.e. either up- or down-regulated) in most or all types of the disease, indicating a common mechanism of the dysregulation. Flow cytometric studies demonstrated that the cell cycle is disturbed in all MPS types, with increased fractions of cells in the G 0 /G 1 phase in most types and decreased fractions of cells in the G 2 /M phase in all types. We found that increased levels of cyclin D1 and disturbed timing of its appearance during the cell cycle may contribute to the mechanism of dysregulation of this process in MPS. Reduction of GAG levels by either a specific enzyme or genistein-mediated inhibition of synthesis of these compounds improved, but not fully corrected, the cell cycle in MPS fibroblasts. Therefore, it is suggested that combination of the therapeutic approaches devoted to reduction of GAG levels with cyclin D1 inhibitors might be considered in further works on developing effective treatment procedures for MPS.

Published

2022

21. Ex Vivo and In Vivo Gene Therapy for Mucopolysaccharidoses: State of the Art.

Author

Consiglieri G, Bernardo ME, Brunetti-Pierri N, and Aiuti A

Subjects

Cost of Illness, Enzyme Replacement Therapy methods, Genetic Therapy methods, Humans, Hematopoietic Stem Cell Transplantation methods, Mucopolysaccharidoses complications, Mucopolysaccharidoses genetics, Mucopolysaccharidoses therapy

Abstract

Enzyme replacement therapy (ERT) and allogeneic hematopoietic stem cell transplantation (HSCT) are standard treatments for some mucopolysaccharidoses. Nevertheless, ERT is not curative, and HSCT is associated with significant mortality and morbidity, leaving a substantial disease burden of brain and skeletal manifestations. To overcome these limitations, different gene therapy (GT) strategies are under preclinical and clinical development. Data from ex-vivo GT clinical trials have demonstrated encouraging biochemical and early clinical outcomes. In-vivo GT, based on local brain delivery or systemic intravenous injections, resulted in biochemical and clinical stabilization of the disease., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published

2022

22. Hematopoietic Disorders, Renal Impairment and Growth in Mucopolysaccharidosis-Plus Syndrome.

Author

Sofronova V, Iwata R, Moriya T, Loskutova K, Gurinova E, Chernova M, Timofeeva A, Shvedova A, Vasilev F, Novgorodova S, Terawaki S, Moriwaki T, Sukhomyasova A, Maksimova N, and Otomo T

Subjects

Glycosaminoglycans metabolism, Humans, Mutation, Eye Diseases, Hematologic Diseases complications, Mucopolysaccharidoses genetics

Abstract

Mucopolysaccharidoses (MPS) are rare lysosomal storage disorders (LSD) characterized by the excessive accumulation of glycosaminoglycans (GAG). Conventional MPS, caused by inborn deficiencies of lysosomal enzymes involved in GAG degradation, display various multisystemic symptoms-including progressive neurological complications, ophthalmological disorders, hearing loss, gastrointestinal and hepatobiliary issues, cardiorespiratory problems, bone and joint abnormalities, dwarfism, and coarse facial features. Mucopolysaccharidosis-Plus Syndrome (MPSPS), an autosomal recessive disease caused by a mutation in the endo-lysosomal tethering protein VPS33A, shows additional renal and hematopoietic abnormalities ("Plus symptoms") uncommon in conventional MPS. Here, we analyze data from biochemical, histological, and physical examinations-particularly of blood counts and kidney function-to further characterize the clinical phenotype of MPSPS. A series of blood tests indicate hematopoietic symptoms including progressive anemia and thrombocytopenia, which correlate with histological observations of hypoplastic bone marrow. High urinary excretion of protein (caused by impairments in renal filtration), hypoalbuminemia, and elevated levels of creatinine, cholesterol, and uric acid indicate renal dysfunction. Histological analyses of MPSPS kidneys similarly suggest the extensive destruction of glomerular structures by foamy podocytes. Height and weight did not significantly deviate from the average, but in some cases, growth began to decline at around six months or one year of age.

Published

2022

23. Separating gene clustering in the rare mucopolysaccharidosis disease.

Author

Bobrowski L, Łukaszuk T, Gaffke L, Cyske Z, Ferenc M, Pierzynowska K, and Węgrzyn G

Subjects

Cluster Analysis, Humans, Transcriptome genetics, Mucopolysaccharidoses genetics, Rare Diseases

Abstract

Rare disease datasets are typically structured such that a small number of patients (cases) are represented by multidimensional feature vectors. In this report, we considered a rare disease, mucopolysaccharidosis (MPS). This disease is divided into 11 types and subtypes, depending on the genetic defect, type of deficient enzyme, and nature of accumulated glycosaminoglycan(s). Among them, 7 types are known as possibly neuronopathic and 4 are non-neuronopathic, and in the case of the former group, prediction of the course of the disease is crucial for patient's treatment and the management. Here, we have used transcriptomic data available for one patient from each MPS type/subtype. The approach to gene grouping considered by us was based on the minimization of the perceptron criterion in the form of convex and piecewise linear function (CPL). This approach allows designing complexes of linear classifiers on the basis of small samples of multivariate vectors. As a result, distinguishing neuronopathic and non-neuronopathic forms of MPS was possible on the basis of bioinformatic analysis of gene expression patterns where each MPS type was represented by only one patient. This approach can be potentially used also for assessing other features of patients suffering from rare diseases, for which large body of data (like transcriptomic data) is available from only one or a few representatives., (© 2022. The Author(s), under exclusive licence to Institute of Plant Genetics Polish Academy of Sciences.)

Published

2022

24. Molecular characterization of a large cohort of mucopolysaccharidosis patients: Iran Mucopolysaccharidosis RE-diagnosis study (IMPRESsion).

Author

Ghaffari SR, Rafati M, Shadnoush M, Pourbabaee S, Aghighi M, Mirab Samiee S, Kermanchi J, Alaei MR, Salehpour S, Amirkashani D, Setoodeh A, Sarkhail P, Badv RS, Aminzadeh M, Shiva S, Eshraghi P, Moravej H, Hashemipour M, Rostampour N, Hamidieh AA, Shamsian BS, Shams S, Zamanfar D, Ebrahimi A, Otadi A, Tara SZ, Barati Z, Fakhri L, Hoseini A, Amiri H, Ramandi S, Mostofinezhad N, Kani ZP, Mohammadyari E, Khosravi M, Saadati M, Hoseininasab F, Khorram Khorshid HR, and Modaberisaber Y

Subjects

DNA Copy Number Variations, Humans, Iran epidemiology, Chondroitinsulfatases genetics, Mucopolysaccharidoses diagnosis, Mucopolysaccharidoses genetics, Mucopolysaccharidosis I diagnosis, Mucopolysaccharidosis I epidemiology, Mucopolysaccharidosis I genetics, Mucopolysaccharidosis VI genetics

Abstract

Mucopolysaccharidoses (MPSs) are rare, heterogeneous inborn errors of metabolism (IEM) diagnosed through a combination of clinical, biochemical, and genetic investigations. The aim of this study was molecular characterization of the largest cohort of Iranian MPS patients (302 patients from 289 unrelated families), along with tracking their ethnicity and geographical origins. 185/289 patients were studied using an IEM-targeted NGS panel followed by complementary Sanger sequencing, which led to the diagnosis of 154 MPS patients and 5 non-MPS IEMs (diagnostic yield: 85.9%). Furthermore, 106/289 patients who were referred with positive findings went through reanalysis and confirmatory tests which confirmed MPS diagnosis in 104. Among the total of 258 MPS patients, 225 were homozygous, 90 harbored novel variants, and 9 had copy number variations. MPS IV was the most common type (34.8%) followed by MPS I (22.7%) and MPS VI (22.5%). Geographical origin analysis unveiled a pattern of distribution for frequent variants in ARSB (c.430G>A, c.962T>C [p.Leu321Pro], c.281C>A [p.Ser94*]), GALNS (c.319G>A [p.Ala107Thr], c.860C>T [p.Ser287Leu], c.1042A>G [p.Thr348Ala]), and IDUA (c.1A>C [p.Met1Leu], c.1598C>G [p.Pro533Arg], c.1562_1563insC [p.Gly522Argfs*50]). Our extensive patient cohort reveals the genetic and geographic landscape of MPS in Iran, which provides insight into genetic epidemiology of MPS and can facilitate a more cost-effective, time-efficient diagnostic approach based on the region-specific variants., (© 2022 Wiley Periodicals LLC.)

Published

2022

25. Complex Changes in the Efficiency of the Expression of Many Genes in Monogenic Diseases, Mucopolysaccharidoses, May Arise from Significant Disturbances in the Levels of Factors Involved in the Gene Expression Regulation Processes.

Author

Cyske Z, Gaffke L, Pierzynowska K, and Węgrzyn G

Subjects

Cell Cycle Proteins genetics, Gene Expression Regulation genetics, Glycosaminoglycans genetics, Glycosaminoglycans metabolism, Humans, Repressor Proteins genetics, Serine-Arginine Splicing Factors genetics, Transcriptome, Lysosomal Storage Diseases, Mucopolysaccharidoses genetics, Mucopolysaccharidoses metabolism

Abstract

Monogenic diseases are primarily caused by mutations in a single gene; thus, they are commonly recognized as genetic disorders with the simplest mechanisms. However, recent studies have indicated that the molecular mechanisms of monogenic diseases can be unexpectedly complicated, and their understanding requires complex studies at the molecular level. Previously, we have demonstrated that in mucopolysaccharidoses (MPS), a group of monogenic lysosomal storage diseases, several hundreds of genes reveal significant changes in the expression of various genes. Although the secondary effects of the primary biochemical defect and the inefficient degradation of glycosaminoglycans (GAGs) might be considered, the scale of the changes in the expression of a large fraction of genes cannot be explained by a block in one biochemical pathway. Here, we demonstrate that in cellular models of 11 types of MPS, the expression of genes coding for proteins involved in the regulation of the expression of many other genes at various stages (such as signal transduction, transcription, splicing, RNA degradation, translation, and others) is significantly disturbed relative to the control cells. This conclusion was based on transcriptomic studies, supported by biochemical analyses of levels of selected proteins encoded by genes revealing an especially high level of dysregulation in MPS (EXOSC9, SRSF10, RPL23, and NOTCH3 proteins were investigated). Interestingly, the reduction in GAGs levels, through the inhibition of their synthesis normalized the amounts of EXOSC9, RPL23, and NOTCH3 in some (but not all) MPS types, while the levels of SRSF10 could not be corrected in this way. These results indicate that different mechanisms are involved in the dysregulation of the expression of various genes in MPS, pointing to a potential explanation for the inability of some therapies (such as enzyme replacement therapy or substrate reduction therapy) to fully correct the physiology of MPS patients. We suggest that the disturbed expression of some genes, which appears as secondary or tertiary effects of GAG storage, might not be reversible, even after a reduction in the amounts of the storage material.

Published

2022

26. Mucopolysaccharidosis-Plus Syndrome, a Rapidly Progressive Disease: Favorable Impact of a Very Prolonged Steroid Treatment on the Clinical Course in a Child.

Author

Faraguna MC, Musto F, Crescitelli V, Iascone M, Spaccini L, Tonduti D, Fedeli T, Kullmann G, Canonico F, Cattoni A, Dell'Acqua F, Rizzari C, and Gasperini S

Subjects

Child, Child, Preschool, Humans, Male, Quality of Life, Steroids, Syndrome, Lymphohistiocytosis, Hemophagocytic diagnosis, Lymphohistiocytosis, Hemophagocytic drug therapy, Lymphohistiocytosis, Hemophagocytic genetics, Mucopolysaccharidoses genetics

Abstract

Mucopolysaccharidosis-plus syndrome (MPS-PS) is a novel autosomal recessive disorder caused by a mutation in the VPS33A gene. This syndrome presents with typical symptoms of mucopolysaccharidosis, as well as congenital heart defects, renal, and hematopoietic system disorders. To date, twenty-four patients have been described. There is no specific therapy for MPS-PS; clinical management is therefore limited to symptoms management. The clinical course is rapidly progressive, and most patients die before 1-2 years of age. We describe a currently 6-year-old male patient with MPS-PS presenting with multiorgan involvement. Symptoms started at four months of age when he progressively suffered from numerous acute and potentially life-threatening events. When he was two years old, he developed secondary hemophagocytic lymphohistiocytosis (HLH), which was successfully treated with steroids. To date, this child represents the oldest patient affected by MPS-PS described in the literature and the first one presenting with a life-threatening secondary HLH. The prolonged steroid treatment allowed a stabilization of his general and hematological conditions and probably determined an improvement of his psychomotor milestones and new neurological acquisitions with an improvement of quality of life. HLH should be suspected and adequately treated in MPS-PS patients presenting with suggestive symptoms of the disease. The usefulness of a prolonged steroid treatment to improve the clinical course of children with MPS-PS deserves further investigation.

Published

2022

27. The experiences and support needs of siblings of people with mucopolysaccharidosis.

Author

Grant N, Von Handorf R, Karaa A, and Skotko BG

Subjects

Adolescent, Adult, Caregivers psychology, Female, Humans, Internet, Male, Middle Aged, Mucopolysaccharidoses epidemiology, Mucopolysaccharidoses pathology, Siblings psychology, Young Adult, Emotions, Mucopolysaccharidoses genetics, Mucopolysaccharidoses psychology, Surveys and Questionnaires

Abstract

The mucopolysaccharidoses (MPS) are a group of rare genetic disorders characterized by progressive multisystem disease. We sought to identify the perceptions and support needs of siblings, who often have lifelong relationships and assume important roles for their brothers and sisters with MPS. We designed an online survey to ask siblings about their experiences through a series of Likert statements and open-ended questions. A mixed methods approach was used to analyze the results. We analyzed eligible responses from 97 participants, ages 18.1-61.2 years, who have brothers and sisters with MPS I, II, III, IV, and VI. Participants reported serving as caregivers for their siblings with MPS, at all ages. While over 62% of siblings often felt sad because they have a brother or sister with MPS, over 90% of siblings reported that they like their brothers and sisters and expressed feelings of pride. Siblings wanted information about MPS, guidance for caregiving activities, genetic counseling, and opportunities to connect with other siblings. Families and professionals should acknowledge the unique experiences and needs of siblings, include siblings in medical conversations and care plans when appropriate, and connect siblings to resources for informational and emotional support., (© 2021 Wiley Periodicals LLC.)

Published

2021

28. Homozygous missense VPS16 variant is associated with a novel disease, resembling mucopolysaccharidosis-plus syndrome in two siblings.

Author

Yıldız Y, Koşukcu C, Aygün D, Akçaboy M, Öztek Çelebi FZ, Taşcı Yıldız Y, Şahin G, Aytekin C, Yüksel D, Lay İ, Özgül RK, and Dursun A

Subjects

Abnormalities, Multiple, Female, Homozygote, Humans, Infant, Male, Mucopolysaccharidoses pathology, Pedigree, Phenotype, Siblings, Syndrome, Mucopolysaccharidoses genetics, Mutation, Missense, Vesicular Transport Proteins genetics

Abstract

Disorders of intracellular trafficking are a group of inherited disorders, which often display multisystem phenotypes. Vacuolar protein sorting (VPS) subunit C, composed of VPS11, VPS18, VPS16, and VPS33A proteins, is involved in tethering of endosomes, lysosomes, and autophagosomes. Our group and others have previously described patients with a specific homozygous missense VPS33A variant, exhibiting a storage disease phenotype resembling mucopolysaccharidosis (MPS), termed "MPS-plus syndrome." Here, we report two siblings from a consanguineous Turkish-Arabic family, who have overlapping features of MPS and intracellular trafficking disorders, including short stature, coarse facies, developmental delay, peripheral neuropathy, splenomegaly, spondylar dysplasia, congenital neutropenia, and high-normal glycosaminoglycan excretion. Whole exome sequencing and familial segregation analyses led to the homozygous NM_022575.3:c.540G>T; p.Trp180Cys variant in VPS16 in both siblings. Multiple bioinformatic methods supported the pathogenicity of this variant. Different monoallelic null VPS16 variants and a homozygous missense VPS16 variant had been previously associated with dystonia. A biallelic intronic, probably splice-altering variant in VPS16, causing an MPS-plus syndrome-like disease has been very recently reported in two individuals. The siblings presented herein display no dystonia, but have features of a multisystem storage disorder, representing a novel MPS-plus syndrome-like disease, associated for the first time with VPS16 missense variants., (© 2021 John Wiley & Sons A/S . Published by John Wiley & Sons Ltd.)

Published

2021

29. Gene Therapy for Neuronopathic Mucopolysaccharidoses: State of the Art.

Author

de Castro MJ, Del Toro M, Giugliani R, and Couce ML

Subjects

Animals, Blood-Brain Barrier metabolism, Gene Editing methods, Genetic Vectors genetics, Humans, Mucopolysaccharidoses genetics, Genetic Therapy methods, Mucopolysaccharidoses therapy

Abstract

The need for long-lasting and transformative therapies for mucopolysaccharidoses (MPS) cannot be understated. Currently, many forms of MPS lack a specific treatment and in other cases available therapies, such as enzyme replacement therapy (ERT), do not reach important areas such as the central nervous system (CNS). The advent of newborn screening procedures represents a major step forward in early identification and treatment of individuals with MPS. However, the treatment of brain disease in neuronopathic MPS has been a major challenge to date, mainly because the blood brain barrier (BBB) prevents penetration of the brain by large molecules, including enzymes. Over the last years several novel experimental therapies for neuronopathic MPS have been investigated. Gene therapy and gene editing constitute potentially curative treatments. However, despite recent progress in the field, several considerations should be taken into account. This review focuses on the state of the art of in vivo and ex vivo gene therapy-based approaches targeting the CNS in neuronopathic MPS, discusses clinical trials conducted to date, and provides a vision for the future implications of these therapies for the medical community. Recent advances in the field, as well as limitations relating to efficacy, potential toxicity, and immunogenicity, are also discussed.

Published

2021

30. MPSBase: Comprehensive repository of differentially expressed genes for mucopolysaccharidoses.

Author

Soares LDF, Villalba Silva GC, Kubaski F, Giugliani R, and Matte U

Subjects

Animals, Biomarkers, Dogs, Gene Ontology, Humans, Lysosomal Storage Diseases physiopathology, Mice, Mucopolysaccharidoses physiopathology, Rats, Databases, Genetic, Gene Expression, Lysosomal Storage Diseases genetics, Mucopolysaccharidoses genetics

Abstract

Mucopolysaccharidoses (MPS) are lysosomal storage diseases (LSDs) caused by the deficiency of enzymes essential for the metabolism of extracellular matrix components called glycosaminoglycans (GAGs). To understand the physiopathology and alterations due to the lysosomal accumulation resulting from enzymatic deficiencies and their secondary outcomes can improve the diagnosis and treatment of rare genetic diseases. This work presents a database for differentially expressed genes from different public MPS data. We developed our database, including 13 studies previously deposited in the GEO (https://www.ncbi.nlm.nih.gov/geo/). The website is hosted in the UFRGS data processing center (CPD) and is available at . The site was constructed in PHP, and the analyses were performed in R. The organisms represented by the datasets are Canis lupus familiaris, Homo sapiens, Mus musculus, and Rattus norvegicus. The user can search for the differentially expressed genes and ontologies by species, MPS type, or tissue type. For each comparison, a heatmap with the 50 top differentially expressed genes is available as well as dot plots for the 30 top ontologies divided by biological process, cellular component, KEGG pathways, and molecular function. This data is also fully available in tables. There are 54 possible comparisons involving about 5000 to 10,000 genes each. This website is the only specific database for MPS with filtering and presenting their results in a one-click approach to the best of our knowledge. The development of such analytical and automated strategies accessible to health professionals is essential for fostering MPS research. The MPSBase is a web user-friendly, comprehensive repository of differentially expressed genes and ontologies regarding the MPS data., Competing Interests: Declaration of Competing Interest The authors declare they have no competing interests., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

31. Update in the Mucopolysaccharidoses.

Author

McBride KL and Flanigan KM

Subjects

Central Nervous System, Genetic Therapy, Glycosaminoglycans, Humans, Infant, Newborn, Neonatal Screening, Mucopolysaccharidoses diagnosis, Mucopolysaccharidoses genetics, Mucopolysaccharidoses therapy

Abstract

The mucopolysaccharidoses (MPS) are a genetically heterogenous group of enzyme deficiencies marked by accumulation of glycosaminoglycans in lysosomes leading to multisystem disease. Although significant therapeutic advances have been made for the MPS disorders, including recombinant enzyme replacement approaches, the neuronopathic features of MPS lack adequate treatment. Gene therapies, including adeno-associated virus vectors targeting the central nervous system, hold significant promise for this group of disorders. Optimal outcomes of all therapies will require early disease identification and treatment, ideally by newborn screening., (Copyright © 2021. Published by Elsevier Inc.)

Published

2021

32. Changes in cellular processes occurring in mucopolysaccharidoses as underestimated pathomechanisms of these diseases.

Author

Gaffke L, Pierzynowska K, Podlacha M, Brokowska J, and Węgrzyn G

Subjects

Animals, Apoptosis, Autophagy, Humans, Mitochondria metabolism, Models, Genetic, Mucopolysaccharidoses genetics, Cells pathology, Mucopolysaccharidoses pathology

Abstract

Mucopolysaccharidoses (MPS) are a group of genetic disorders belonging to lysosomal storage diseases. They are caused by genetic defects leading to a lack or severe deficiency of activity of one of lysosomal hydrolases involved in degradation of glycosaminoglycans (GAGs). Partially degraded GAGs accumulate in lysosomes, which results in dysfunctions of cells, tissues, and organs. Until recently, it was assumed that GAG accumulation in cells is the major, if not the only, mechanism of pathogenesis in MPS, as GAGs may be a physical ballast for lysosomes causing inefficiency of cells due to a large amount of a stored material. However, recent reports suggest that in MPS cells there are changes in many different processes, which might be even more important for pathogenesis than lysosomal accumulation of GAGs per se. Moreover, there are many recently published results indicating that lysosomes not only are responsible for degradation of various macromolecules, but also play crucial roles in the regulation of cellular metabolism. Therefore, it appears plausible that previous failures in treatment of MPS (i.e., possibility to correct only some symptoms and slowing down of the disease rather than fully effective management of MPS) might be caused by underestimation of changes in cellular processes and concentration solely on decreasing GAG levels in cells., (© 2019 International Federation for Cell Biology.)

Published

2021

33. Expression of genes involved in apoptosis is dysregulated in mucopolysaccharidoses as revealed by pilot transcriptomic analyses.

Author

Brokowska J, Pierzynowska K, Gaffke L, Rintz E, and Węgrzyn G

Subjects

Adult, Caspase 3 metabolism, Caspase 7 metabolism, Humans, RNA, Messenger genetics, RNA, Messenger metabolism, Apoptosis genetics, Gene Expression Profiling, Gene Expression Regulation, Mucopolysaccharidoses genetics

Abstract

Mucopolysaccharidoses (MPS), a group of lysosomal storage diseases (LSD), are inherited disorders caused by mutations in genes coding for enzymes involved in the degradation of glycosaminoglycans (GAGs). Therefore, accumulated GAGs in lysosomes lead to severe symptoms in patients and significantly shortened life span. Although GAG accumulation in cells is the primary cellular defect in MPS, recent reports indicated that severe changes in cellular processes occur there as secondary or tertiary effects, which may contribute significantly to the disease pathomechanism. Apoptosis is one of such process, while mechanisms leading to dysregulation of this process in MPS remain largely unknown. To learn about these mechanisms, we have performed transcriptomic studies using cultures of fibroblasts derived from patients suffering from all types and subtypes of MPS, and assessed genes related to apoptosis. We found that there are significant changes in expression levels of many such genes relative to control fibroblasts (Human Dermal Fibroblasts-adult cell line), and the number of down- or up-regulated transcripts was between 19 and 73 in different MPS types. We have identified apoptosis-related genes, which were considerably dysregulated in many MPS types, as well as those in which expression was significantly changed in specific MPS types. BNIP3, C1D, CLU, GPER1, KREMEN1, and PRKCD genes displayed the most changed expression profiles in most MPS types relative to control cells. Caspase 3/7 activity was increased in MPS IVA and IX. These results indicate that changes in apoptosis, observed in MPS, may arise, at least partially, from dysregulation of genes coding for proteins involved in this process., (© 2020 International Federation for Cell Biology.)

Published

2021

34. Mucopolysaccharidosis III: Molecular basis and treatment.

Author

Spahiu L, Behluli E, Peterlin B, Nefic H, Hadziselimovic R, Liehr T, and Temaj G

Subjects

Glycosaminoglycans, Humans, Mutation, Mucopolysaccharidoses drug therapy, Mucopolysaccharidoses genetics, Mucopolysaccharidosis I, Mucopolysaccharidosis III

Abstract

Mucopolysaccharidoses (MPSs) are known as rare genetic diseases which are caused by mutation in the enzyme heparin sulfate, which normally leads to degradation and accumulation of glycosaminoglycans in the cells. There are 11 types of MPSs, whereby neuropathy may occur in seven of them (MPS I, II, IIIA, IIIB, IIIC, IIID and VII). Accumulation of degraded heparin sulfate in lysosomes causes cellular dysfunction and malfunction of several organs. However, the exact molecular mechanism how protein degradation and storage leads to cellular dysfunction is not understood, yet. Nonetheless, several genetic and biochemical methods for diagnosis of MPSs are available nowadays. Here we provide an overview on known molecular basis of MPS in general, including enzyme defects and symptoms of MPS; however, the main focus is on MPS type III together with potential and perspective therapy-options.

Published

2021

35. Genome editing in mucopolysaccharidoses and mucolipidoses.

Author

Santos HS, Poletto E, Schuh R, Matte U, and Baldo G

Subjects

Animals, Gene Editing, Genetic Therapy, Glycosaminoglycans, Humans, Mucolipidoses genetics, Mucopolysaccharidoses genetics, Mucopolysaccharidoses therapy

Abstract

Mucopolysaccharidoses (MPS) and mucolipidoses (ML) are disorders that alter lysosome function. While MPS are caused by mutation in enzymes that degrade glycosaminoglycans, the ML are disorders characterized by reduced function in the phosphotransferase enzyme. Multiple clinical features are associated with these diseases and the exact mechanisms that could explain such different clinical manifestations in patients are still unknown. Furthermore, there are no curative treatment for any of MPS and ML conditions so far. Gene editing holds promise as a tool for the creation of cell and animal models to help explain disease pathogenesis, as well as a platform for gene therapy. In this chapter, we discuss the main studies involving genome editing for MPS and the prospect applications for ML., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

36. Changes in expressions of genes involved in the regulation of cellular processes in mucopolysaccharidoses as assessed by fibroblast culture-based transcriptomic analyses.

Author

Gaffke L, Pierzynowska K, Krzelowska K, Piotrowska E, and Węgrzyn G

Subjects

Cell Line, Cells, Cultured, Fibroblasts pathology, Gene Expression, Humans, Mucopolysaccharidoses pathology, Cellular Microenvironment physiology, Fibroblasts metabolism, Mucopolysaccharidoses genetics, Mucopolysaccharidoses metabolism, Transcriptome physiology

Abstract

Recent studies indicated that apart from lysosomal storage of glycosaminoglycans (GAGs), secondary and tertiary changes in cellular processes may significantly contribute to development of disorders and symptoms occurring in mucopolysaccharidoses (MPS), a group of lysosomal storage diseases in which neurodegeneration is specific for most types and subtypes. In this report, using transcriptomic data, we demonstrate that regulation of hundreds of genes coding for proteins involved in regulations of various cellular processes is changed in cells derived from patients suffering from all types and subtypes of MPS. Among such genes there are 10 which expression is significantly changed in 9 or more (out of 11) MPS types/subtypes; they include IER3IP1, SAR1A, TMEM38B, PLCB4, SIN3B, ABHD5, SH3BP5, CAPG, PCOLCE2, and MN1. Moreover, there are several genes whose expression is changed over log 2  > 4 times in some MPS types relative to control cells. The above analysis indicates that significant changes in expression of genes coding for various regulators of cellular processes may considerably contribute to development of cellular dysfunctions, and further appearance of specific symptoms of MPS, including neurodegeneration.

Published

2020

37. Estimated prevalence of mucopolysaccharidoses from population-based exomes and genomes.

Author

Borges P, Pasqualim G, Giugliani R, Vairo F, and Matte U

Subjects

Exome, Humans, Mutation, Prevalence, Mucopolysaccharidoses epidemiology, Mucopolysaccharidoses genetics, Mucopolysaccharidosis I

Abstract

Background: In this study, the prevalence of different types of mucopolysaccharidoses (MPS) was estimated based on data from the exome aggregation consortium (ExAC) and the genome aggregation database (gnomAD). The population-based allele frequencies were used to identify potential disease-causing variants on each gene related to MPS I to IX (except MPS II)., Methods: We evaluated the canonical transcripts and excluded homozygous, intronic, 3', and 5' UTR variants. Frameshift and in-frame insertions and deletions were evaluated using the SIFT Indel tool. Splice variants were evaluated using SpliceAI and Human Splice Finder 3.0 (HSF). Loss-of-function single nucleotide variants in coding regions were classified as potentially pathogenic, while synonymous variants outside the exon-intron boundaries were deemed non-pathogenic. Missense variants were evaluated by five in silico prediction tools, and only those predicted to be damaging by at least three different algorithms were considered disease-causing., Results: The combined frequencies of selected variants (ranged from 127 in GNS to 259 in IDUA) were used to calculate prevalence based on Hardy-Weinberg's equilibrium. The maximum estimated prevalence ranged from 0.46 per 100,000 for MPSIIID to 7.1 per 100,000 for MPS I. Overall, the estimated prevalence of all types of MPS was higher than what has been published in the literature. This difference may be due to misdiagnoses and/or underdiagnoses, especially of the attenuated forms of MPS. However, overestimation of the number of disease-causing variants by in silico predictors cannot be ruled out. Even so, the disease prevalences are similar to those reported in diagnosis-based prevalence studies., Conclusion: We report on an approach to estimate the prevalence of different types of MPS based on publicly available population-based genomic data, which may help health systems to be better prepared to deal with these conditions and provide support to initiatives on diagnosis and management of MPS.

Published

2020

38. A systematic review and meta-analysis of published cases reveals the natural disease history in multiple sulfatase deficiency.

Author

Schlotawa L, Preiskorn J, Ahrens-Nicklas R, Schiller S, Adang LA, Gärtner J, and Friede T

Subjects

Glycine analogs & derivatives, Glycine genetics, Glycine metabolism, Humans, Leukodystrophy, Metachromatic pathology, Mucopolysaccharidoses pathology, Multiple Sulfatase Deficiency Disease pathology, Protein Processing, Post-Translational genetics, Sulfatases deficiency, Sulfatases genetics, Leukodystrophy, Metachromatic genetics, Mucopolysaccharidoses genetics, Multiple Sulfatase Deficiency Disease genetics, Oxidoreductases Acting on Sulfur Group Donors genetics

Abstract

Multiple Sulfatase Deficiency (MSD, MIM#272200) is an ultra-rare lysosomal storage disorder arising from mutations in the SUMF1 gene, which encodes the formylglycine-generating enzyme (FGE). FGE is necessary for the activation of sulfatases, a family of enzymes that are involved in the degradation of sulfated substrates such as glycosaminoglycans and sulfolipids. SUMF1 mutations lead to functionally impaired FGE and individuals with MSD demonstrate clinical signs of single sulfatase deficiencies, including metachromatic leukodystrophy (MLD) and several mucopolysaccharidosis (MPS) subtypes. Comprehensive information related to the natural history of MSD is missing. We completed a systematic literature review and a meta-analysis on data from published cases reporting on MSD. As available from these reports, we extracted clinical, genetic, biochemical, and brain imaging information. We identified 75 publications with data on 143 MSD patients with a total of 53 unique SUMF1 mutations. The mean survival was 13 years (95% CI 9.8-16.2 years). Seventy-five clinical signs and 11 key clusters of signs were identified. The most frequently affected organs systems were the nervous, skeletal, and integumentary systems. The most frequent MRI features were abnormal myelination and cerebral atrophy. Individuals with later onset MSD signs and survived longer than those with signs at birth. Less severe mutations, low disease burden and achievement of independent walking positively correlated with longer survival. Despite the limitations of our approach, we were able to define clinical characteristics and disease outcomes in MSD. This work will provide the foundation of natural disease history data needed for future clinical trial design., (© 2020 The Authors. Journal of Inherited Metabolic Disease published by John Wiley & Sons Ltd on behalf of SSIEM.)

Published

2020

39. Natural history of multiple sulfatase deficiency: Retrospective phenotyping and functional variant analysis to characterize an ultra-rare disease.

Author

Adang LA, Schlotawa L, Groeschel S, Kehrer C, Harzer K, Staretz-Chacham O, Silva TO, Schwartz IVD, Gärtner J, De Castro M, Costin C, Montgomery EF, Dierks T, Radhakrishnan K, and Ahrens-Nicklas RC

Subjects

Adolescent, Child, Child, Preschool, Female, Genotype, Glycine analogs & derivatives, Glycine genetics, Glycine metabolism, Humans, Infant, Internationality, Leukodystrophy, Metachromatic pathology, Male, Mucopolysaccharidoses pathology, Multiple Sulfatase Deficiency Disease pathology, Mutation, Phenotype, Rare Diseases, Retrospective Studies, Sulfatases deficiency, Sulfatases genetics, Leukodystrophy, Metachromatic genetics, Mucopolysaccharidoses genetics, Multiple Sulfatase Deficiency Disease genetics, Oxidoreductases Acting on Sulfur Group Donors genetics

Abstract

Multiple sulfatase deficiency (MSD) is an ultra-rare neurodegenerative disorder caused by pathogenic variants in SUMF1. This gene encodes formylglycine-generating enzyme (FGE), a protein required for sulfatase activation. The clinical course of MSD results from additive effect of each sulfatase deficiency, including metachromatic leukodystrophy (MLD), several mucopolysaccharidoses (MPS II, IIIA, IIID, IIIE, IVA, VI), chondrodysplasia punctata, and X-linked ichthyosis. While it is known that affected individuals demonstrate a complex and severe phenotype, the genotype-phenotype relationship and detailed clinical course is unknown. We report on 35 cases enrolled in our retrospective natural history study, n = 32 with detailed histories. Neurologic function was longitudinally assessed with retrospective scales. Biochemical and computational modeling of novel SUMF1 variants was performed. Genotypes were classified based on predicted functional change, and each individual was assigned a genotype severity score. The median age at symptom onset was 0.25 years; median age at diagnosis was 2.7 years; and median age at death was 13 years. All individuals demonstrated developmental delay, and only a subset of individuals attained ambulation and verbal communication. All subjects experienced an accumulating systemic symptom burden. Earlier age at symptom onset and severe variant pathogenicity correlated with poor neurologic outcomes. Using retrospective deep phenotyping and detailed variant analysis, we defined the natural history of MSD. We found that attenuated cases can be distinguished from severe cases by age of onset, attainment of ambulation, and genotype. Results from this study can help inform prognosis and facilitate future study design., (© 2020 The Authors. Journal of Inherited Metabolic Disease published by John Wiley & Sons Ltd on behalf of SSIEM.)

Published

2020

40. Transcriptomic analyses suggest that mucopolysaccharidosis patients may be less susceptible to COVID-19.

Author

Pierzynowska K, Gaffke L, and Węgrzyn G

Subjects

Angiotensin-Converting Enzyme 2 genetics, Angiotensin-Converting Enzyme 2 metabolism, COVID-19 metabolism, COVID-19 pathology, COVID-19 prevention & control, Cells, Cultured, Fibroblasts metabolism, Fibroblasts pathology, Fibroblasts virology, Gene Expression Profiling, Genetic Predisposition to Disease, Humans, Mucopolysaccharidoses metabolism, Mucopolysaccharidoses pathology, Mucopolysaccharidoses virology, SARS-CoV-2 pathogenicity, Serine Endopeptidases genetics, Serine Endopeptidases metabolism, Transcriptome, COVID-19 genetics, Mucopolysaccharidoses genetics, SARS-CoV-2 physiology, Virus Internalization

Abstract

We used transcriptomic (RNA-seq) analyses to determine whether patients suffering from all types and subtypes of mucopolysaccharidosis (MPS), a severe inherited metabolic disease, may be more susceptible to coronavirus disease 2019 (COVID-19). The expression levels of genes encoding proteins potentially involved in SARS-CoV-2 development were estimated in MPS cell lines. Four genes (GTF2F2, RAB18, TMEM97, PDE4DIP) coding for proteins potentially facilitating virus development were down-regulated, while two genes (FBN1, MFGE8), the products of which potentially interfere with virus propagation, were up-regulated in most MPS types. Although narrowing of respiratory tract and occurrence of thick mucus, characteristic of MPS, are risk factors for COVID-19, transcriptomic analyses suggest that MPS cells might be less, rather than more, susceptible to SARS-CoV-2 infection., (© 2020 Federation of European Biochemical Societies.)

Published

2020

41. Arylsulfatase K inactivation causes mucopolysaccharidosis due to deficient glucuronate desulfation of heparan and chondroitin sulfate.

Author

Trabszo C, Ramms B, Chopra P, Lüllmann-Rauch R, Stroobants S, Sproß J, Jeschke A, Schinke T, Boons GJ, Esko JD, Lübke T, and Dierks T

Subjects

Animals, Arylsulfatases genetics, Chondroitin Sulfates genetics, Enzyme Activation, Heparitin Sulfate genetics, Mice, Mice, Knockout, Mucopolysaccharidoses genetics, Arylsulfatases metabolism, Chondroitin Sulfates metabolism, Heparitin Sulfate metabolism, Mucopolysaccharidoses metabolism

Abstract

Mucopolysaccharidoses comprise a group of rare metabolic diseases, in which the lysosomal degradation of glycosaminoglycans (GAGs) is impaired due to genetically inherited defects of lysosomal enzymes involved in GAG catabolism. The resulting intralysosomal accumulation of GAG-derived metabolites consequently manifests in neurological symptoms and also peripheral abnormalities in various tissues like liver, kidney, spleen and bone. As each GAG consists of differently sulfated disaccharide units, it needs a specific, but also partly overlapping set of lysosomal enzymes to accomplish their complete degradation. Recently, we identified and characterized the lysosomal enzyme arylsulfatase K (Arsk) exhibiting glucuronate-2-sulfatase activity as needed for the degradation of heparan sulfate (HS), chondroitin sulfate (CS) and dermatan sulfate (DS). In the present study, we investigated the physiological relevance of Arsk by means of a constitutive Arsk knockout mouse model. A complete lack of glucuronate desulfation was demonstrated by a specific enzyme activity assay. Arsk-deficient mice show, in an organ-specific manner, a moderate accumulation of HS and CS metabolites characterized by 2-O-sulfated glucuronate moieties at their non-reducing ends. Pathophysiological studies reflect a rather mild phenotype including behavioral changes. Interestingly, no prominent lysosomal storage pathology like bone abnormalities were detected. Our results from the Arsk mouse model suggest a new although mild form of mucopolysacharidose (MPS), which we designate MPS type IIB., (© 2020 The Author(s). Published by Portland Press Limited on behalf of the Biochemical Society.)

Published

2020

42. Therapy development for the mucopolysaccharidoses: Updated consensus recommendations for neuropsychological endpoints.

Author

van der Lee JH, Morton J, Adams HR, Clarke L, Eisengart JB, Escolar ML, Giugliani R, Harmatz P, Hogan M, Kearney S, Muenzer J, Muschol N, Rust S, Saville BR, Semrud-Clikeman M, Wang R, and Shapiro E

Subjects

Brain pathology, Clinical Trials as Topic, Cognitive Dysfunction physiopathology, Humans, Mucopolysaccharidoses genetics, Mucopolysaccharidoses metabolism, Nervous System Diseases genetics, Nervous System Diseases metabolism, Problem Behavior, Quality of Life, Brain metabolism, Mucopolysaccharidoses therapy, Nervous System Diseases therapy, Physical Therapy Modalities

Abstract

Neurological dysfunction represents a significant clinical component of many of the mucopolysaccharidoses (also known as MPS disorders). The accurate and consistent assessment of neuropsychological function is essential to gain a greater understanding of the precise natural history of these conditions and to design effective clinical trials to evaluate the impact of therapies on the brain. In 2017, an International MPS Consensus Panel published recommendations for best practice in the design and conduct of clinical studies investigating the effects of therapies on cognitive function and adaptive behavior in patients with neuronopathic mucopolysaccharidoses. Based on an International MPS Consensus Conference held in February 2020, this article provides updated consensus recommendations and expands the objectives to include approaches for assessing behavioral and social-emotional state, caregiver burden and quality of life in patients with all mucopolysaccharidoses., Competing Interests: Declaration of Competing Interest Johanna H van der Lee has no conflicts of interest. Jonathan Morton is an employee of Comradis, Oxford, UK, which received payment from conference funds managed by the US National MPS Society for the medical writing support provided during the development of this article, in accordance with Good Publication Practice (GPP3) guidelines (http://www.ismpp.org/gpp3). Heather Adams has served as an advisory board member/consultant for Amicus Therapeutics, Beyond Batten Disease Foundation, Taylor’s Tale, ReGenXBio and Neurogene. She is a member of the Batten Disease Support & Research Association medical advisory board and the co-director of the Tourette Association of America Center of Excellence at University of Rochester. Lorne Clark has received honoraria for advisory boards and educational lectures from BioMarin, JCR Pharmaceutical, ReGenXBio and Sanofi Genzyme. Julie Eisengart has received research support from Lysogene, Sangamo and Shire/Takeda; consulting fees from ArmaGen, Denali Therapeutics, JCR Pharmaceutical, Orchard Therapeutics, ReGenXBio and Shire/Takeda; and honoraria for advisory boards for Amicus Therapeutics, bluebird bio, Orchard Therapeutics, ReGenXBio, Sanofi Genzyme and Shire/Takeda. Maria L Escolar has served as principal investigator and consultant on MPS trials for Abeona Therapeutics, Denali Therapeutics, ReGenXBio and Seelos Therapeutics. Roberto Giugliani has served on as speaker, consultant or advisory board member for Amicus Therapeutics, Abeona Therapeutics, BioMarin, Inventiva, Janssen, JCR Pharmaceuticals, Lysogene, PTC Therapeutics, ReGenXBio, Sanofi Genzyme, Sobi, Takeda and Ultragenyx; has received research grants from Allievex, Amicus Therapeutics, Armagen, BioMarin, GC Pharma, JCR Pharmaceuticals, Lysogene, ReGenXBio, Sanofi Genzyme and Takeda; and has received travel expenses to attend scientific meetings from Amicus Therapeutics, BioMarin, JCR Pharmaceuticals, Sanofi Genzyme, Takeda and Ultragenyx. Paul Harmatz has received research support for studies, served on scientific advisory boards, and provided consulting support for Aeglea Biotherapeutics, Alexion, Amicus Therapeutics, Armagen, Ascendis Pharma, BioMarin, Chiesi, Denali Therapeutics, Homology Medicines, Inventiva Pharma, JCR Pharmaceutical, Orphazyme, Paradigm BioPharma, PTC Therapeutics, QED, ReGenXbio, Sangamo, Sanofi Genzyme, Sobi and Shire/Takeda. Melissa Hogan is a principal consultant with Doulots, LLC through which she has received consulting fees from Denali Therapeutics and Seelos Therapeutics. She has also received stipends and expenses in accordance with her son's participation in a clinical trial and its extension sponsored by Shire (now Takeda). Shauna Kearney has received education and travel sponsorships from Actelion, BioMarin, Denali Therapeutics, Sanofi Genzyme and Shire/Takeda in connection with meetings. She has no conflicts of interest. Joseph Muenzer has received consulting fees from BioMarin, bluebird bio, Denali Therapeutics, Eloxx, Green Cross, JCR Pharmaceuticals, PTC Therapeutics, ReGenXBio, Sangamo, Sanofi Genzyme and Shire/Takeda. He is the principal investigator for Phase I/II and Phase II/III intrathecal enzyme replacement clinical trials for MPS II, a Phase I/II gene editing clinical trial for MPS II and a Phase I/II IV ERT clinical trial for MPS IIIA. Nicole Muschol has received consulting fees from BioMarin, Chiesi, Lysogene, Sanofi Genzyme, Shire/Takeda and Sobi; received grant/research support from BioMarin, Sanofi Genzyme and Shire/Takeda; and received honoraria/travel support from Actelion, Amicus Therapeutics, BioMarin, Sanofi Genzyme and Shire/Takeda. Stewart Rust has received travel grants, speaker fees and conference sponsorship from Takeda. Benjamin R Saville is employed by Berry Consultants, a statistical consulting company specializing in Bayesian adaptive clinical trials. The company has received consulting payments from Abeona Therapeutics in MPS-related trial design Margaret Semrud-Clikeman has no conflicts of interest. Raymond Wang is a principal investigator and has received travel support and honorarium for advisory board participation for Lysogene and ReGenXBio. Elsa Shapiro is the managing partner of Shapiro Neuropsychology Consulting through which she has received fees for providing consultation services on cognitive and behavioural endpoints for all the companies providing support for this conference., (Copyright © 2020 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2020

43. Newborn screening of mucopolysaccharidoses: past, present, and future.

Author

Arunkumar N, Langan TJ, Stapleton M, Kubaski F, Mason RW, Singh R, Kobayashi H, Yamaguchi S, Suzuki Y, Orii K, Orii T, Fukao T, and Tomatsu S

Subjects

Glycosaminoglycans, Humans, Infant, Newborn, Lysosomal Storage Diseases epidemiology, Lysosomal Storage Diseases genetics, Lysosomal Storage Diseases pathology, Mucopolysaccharidoses epidemiology, Mucopolysaccharidoses genetics, Mucopolysaccharidoses pathology, Mucopolysaccharidosis I epidemiology, Mucopolysaccharidosis I genetics, Mucopolysaccharidosis I pathology, Quality of Life, Tandem Mass Spectrometry, Lysosomal Storage Diseases diagnosis, Mucopolysaccharidoses diagnosis, Mucopolysaccharidosis I diagnosis, Neonatal Screening

Abstract

Mucopolysaccharidoses (MPS) are a subtype of lysosomal storage disorders (LSDs) characterized by the deficiency of the enzyme involved in the breakdown of glycosaminoglycans (GAGs). Mucopolysaccharidosis type I (MPS I, Hurler Syndrome) was endorsed by the U.S. Secretary of the Department of Health and Human Services for universal newborn screening (NBS) in February 2016. Its endorsement exemplifies the need to enhance the accuracy of diagnostic testing for disorders that are considered for NBS. The progression of MPS disorders typically incudes irreversible CNS involvement, severe bone dysplasia, and cardiac and respiratory issues. Patients with MPS have a significantly decreased quality of life if untreated and require timely diagnosis and management for optimal outcomes. NBS provides the opportunity to diagnose and initiate treatment plans for MPS patients as early as possible. Most newborns with MPS are asymptomatic at birth; therefore, it is crucial to have biomarkers that can be identified in the newborn. At present, there are tiered methods and different instrumentation available for this purpose. The screening of quick, cost-effective, sensitive, and specific biomarkers in patients with MPS at birth is important. Rapid newborn diagnosis enables treatments to maximize therapeutic efficacy and to introduce immune tolerance during the neonatal period. Currently, newborn screening for MPS I and II has been implemented and/or in pilot testing in several countries. In this review article, historical aspects of NBS for MPS and the prospect of newborn screening for MPS are described, including the potential tiers of screening.

Published

2020

44. Multiple Sulfatase Deficiency: A Disease Comprising Mucopolysaccharidosis, Sphingolipidosis, and More Caused by a Defect in Posttranslational Modification.

Author

Schlotawa L, Adang LA, Radhakrishnan K, and Ahrens-Nicklas RC

Subjects

Glycine analogs & derivatives, Glycine genetics, Glycine metabolism, Humans, Mucopolysaccharidoses pathology, Multiple Sulfatase Deficiency Disease pathology, Mutation genetics, Protein Processing, Post-Translational genetics, Sphingolipidoses pathology, Sulfatases deficiency, Sulfatases genetics, Mucopolysaccharidoses genetics, Multiple Sulfatase Deficiency Disease genetics, Oxidoreductases Acting on Sulfur Group Donors genetics, Sphingolipidoses genetics

Abstract

Multiple sulfatase deficiency (MSD, MIM #272200) is an ultra-rare disease comprising pathophysiology and clinical features of mucopolysaccharidosis, sphingolipidosis and other sulfatase deficiencies. MSD is caused by impaired posttranslational activation of sulfatases through the formylglycine generating enzyme (FGE) encoded by the sulfatase modifying factor 1 ( SUMF1 ) gene, which is mutated in MSD. FGE is a highly conserved, non-redundant ER protein that activates all cellular sulfatases by oxidizing a conserved cysteine in the active site of sulfatases that is necessary for full catalytic activity. SUMF1 mutations result in unstable, degradation-prone FGE that demonstrates reduced or absent catalytic activity, leading to decreased activity of all sulfatases. As the majority of sulfatases are localized to the lysosome, loss of sulfatase activity induces lysosomal storage of glycosaminoglycans and sulfatides and subsequent cellular pathology. MSD patients combine clinical features of all single sulfatase deficiencies in a systemic disease. Disease severity classifications distinguish cases based on age of onset and disease progression. A genotype- phenotype correlation has been proposed, biomarkers like excreted storage material and residual sulfatase activities do not correlate well with disease severity. The diagnosis of MSD is based on reduced sulfatase activities and detection of mutations in SUMF1 . No therapy exists for MSD yet. This review summarizes the unique FGE/ sulfatase physiology, pathophysiology and clinical aspects in patients and their care and outlines future perspectives in MSD., Competing Interests: Authors declare no conflicts of interest.

Published

2020

45. Evading the AAV Immune Response in Mucopolysaccharidoses.

Author

Piechnik M, Sawamoto K, Ohnishi H, Kawamoto N, Ago Y, and Tomatsu S

Subjects

Antibodies immunology, Capsid immunology, Dependovirus immunology, Humans, Mucopolysaccharidoses immunology, Mucopolysaccharidoses therapy, Transgenes genetics, Transgenes immunology, Dependovirus genetics, Genetic Therapy, Immunity, Humoral genetics, Mucopolysaccharidoses genetics

Abstract

The humoral immune response elicited by adeno-associated virus (AAV)-mediated gene therapy for the treatment of mucopolysaccharidoses (MPS) poses a significant challenge to achieving therapeutic levels of transgene expression. Antibodies targeting the AAV capsid as well as the transgene product diminish the production of glycosaminoglycan (GAG)-degrading enzymes essential for the treatment of MPS. Patients who have antibodies against AAV capsid increase in number with age, serotype, and racial background and are excluded from the clinical trials at present. In addition, patients who have undergone AAV gene therapy are often excluded from the additional AAV gene therapy with the same serotype, since their acquired immune response (antibody) against AAV will limit further efficacy of treatment. Several methods are being developed to overcome this immune response, such as novel serotype design, antibody reduction by plasmapheresis and immunosuppression, and antibody evasion using empty capsids and enveloped AAV vectors. In this review, we examine the mechanisms of the anti-AAV humoral immune response and evaluate the strengths and weaknesses of current evasion strategies in order to provide an evidence-based recommendation on evading the immune response for future AAV-mediated gene therapies for MPS., Competing Interests: The authors declare no conflict of interest.

Published

2020

46. Estimated birth prevalence of mucopolysaccharidoses in Brazil.

Author

Federhen A, Pasqualim G, de Freitas TF, Gonzalez EA, Trapp F, Matte U, and Giugliani R

Subjects

Brazil epidemiology, Female, Humans, Iduronidase blood, Live Birth, Male, Mucopolysaccharidoses blood, Mucopolysaccharidoses epidemiology, Mucopolysaccharidoses pathology, Mucopolysaccharidosis I blood, Mucopolysaccharidosis I epidemiology, Mucopolysaccharidosis I genetics, Mucopolysaccharidosis II blood, Mucopolysaccharidosis II epidemiology, Mucopolysaccharidosis II genetics, Mucopolysaccharidosis III blood, Mucopolysaccharidosis III epidemiology, Mucopolysaccharidosis III genetics, Mucopolysaccharidosis VI blood, Mucopolysaccharidosis VI epidemiology, Mucopolysaccharidosis VI genetics, Mutation genetics, Iduronidase genetics, Mucopolysaccharidoses genetics

Abstract

Several studies have been published on the frequency of the mucopolysaccharidoses (MPS) in different countries. The objective of the present study was to estimate the birth prevalence (BP) of MPS in Brazil. MPS diagnosis registered at MPS-Brazil Network and in Instituto Vidas Raras were reviewed. BP was estimated by (a) the number of registered patients born between 1994 and 2015 was divided by the number of live births (LBs), and (b) a sample of 1,000 healthy individuals was tested for the most frequent variant in IDUA gene in MPS I (p.Trp402Ter) to estimate the frequency of heterozygosity and homozygosity. (a) The BP based on total number of LBs was (cases per 100,000 LBs): MPS overall: 1.25; MPS I: 0.24; MPS II: 0.37; MPS III: 0.21; MPS IV: 0.14; MPS VI: 0.28; MPS VII: 0.02. (b) The overall frequency of p.Trp402Ter was 0.002. Considering the frequency of heterozygotes for the p.Trp402Ter IDUA variant in the RS state, the frequency of this variant among MPS I patients and the relative frequency of the different MPSs, we estimated the birth prevalence of MPS in total and of each MPS type, as follows: MPS overall: 4.62; MPS I: 0.95; MPS II: 1.32; MPS III: 0.56; MPS IV: 0.57; MPS VI: 1.02; MPS VII: 0.05. This study provided original data about BP and relative frequency of the MPS types, in Brazil, based on the frequency of the commonest IDUA pathogenic variant and in the records of two large patient databases., (© 2020 Wiley Periodicals, Inc.)

Published

2020

47. An exonic insertion in the NAGLU gene causing Mucopolysaccharidosis IIIB in Schipperke dogs.

Author

Raj K, Ellinwood NM, and Giger U

Subjects

Animals, Base Sequence, Dogs, Mucopolysaccharidoses enzymology, Acetylglucosaminidase genetics, Exons genetics, Mucopolysaccharidoses genetics, Mucopolysaccharidoses veterinary, Mutagenesis, Insertional genetics

Abstract

Mucopolysaccharidosis (MPS) IIIB (Sanfilippo syndrome B; OMIM 252920), is a lysosomal storage disease with progressive neurological signs caused by deficient activity of alpha-N-acetylglucosaminidase (NAGLU, EC 3.2.1.50). Herein we report the causative variant in the NAGLU gene in Schipperke dogs and a genotyping survey in the breed. All six exons and adjacent regions of the NAGLU gene were sequenced from six healthy appearing and three affected Schipperkes. DNA fragment length and TaqMan assays were used to genotype privately owned Schipperkes. A single variant was found in exon 6 of MPS IIIB affected Schipperkes: an insertion consisting of a 40-70 bp poly-A and an 11 bp duplication of the exonic region preceding the poly-A (XM_548088.6:c.2110_2111ins[A(40_70);2100_2110]) is predicted to insert a stretch of 13 or more lysines followed by either an in-frame insertion of a repeat of the four amino acids preceding the lysines, or a frameshift. The clinically affected Schipperkes were homozygous for this insertion, and the sequenced healthy dogs were either heterozygous or homozygous for the wild-type allele. From 2003-2019, 3219 Schipperkes were genotyped. Of these, 1.5% were homozygous for this insertion and found to be clinically affected, and 23.6% were heterozygous for the insertion and were clinically healthy, the remaining 74.9% were homozygous for the wild-type and were also clinically healthy. The number of dogs homozygous and heterozygous for the insertion declined rapidly after the initial years of genotyping, documenting the benefit of a DNA screening program in a breed with a small gene pool. In conclusion, a causative NAGLU variant in Schipperke dogs with MPS IIIB was identified and was found at high frequency in the breed. Through genotyping and informed breeding practices, the prevalence of canine MPS IIIB has been drastically reduced in the Schipperke population worldwide.

Published

2020

48. Underestimated Aspect of Mucopolysaccharidosis Pathogenesis: Global Changes in Cellular Processes Revealed by Transcriptomic Studies.

Author

Gaffke L, Pierzynowska K, Podlacha M, Hoinkis D, Rintz E, Brokowska J, Cyske Z, and Wegrzyn G

Subjects

Cell Line, Fibroblasts metabolism, Gene Expression Regulation, Glycosaminoglycans genetics, Glycosaminoglycans metabolism, Humans, Mucopolysaccharidoses pathology, Mutation, Fibroblasts pathology, Mucopolysaccharidoses genetics, Transcriptome

Abstract

Mucopolysaccharidoses (MPS), a group of inherited metabolic disorders caused by deficiency in enzymes involved in degradation of glycosaminoglycans (GAGs), are examples (and models) of monogenic diseases. Accumulation of undegraded GAGs in lysosomes was supposed to be the major cause of MPS symptoms; however, their complexity and variability between particular types of the disease can be hardly explained by such a simple storage mechanism. Here we show that transcriptomic (RNA-seq) analysis of the material derived from fibroblasts of patients suffering from all types and subtypes of MPS, supported by RT-qPCR results, revealed surprisingly large changes in expression of genes involved in various cellular processes, indicating complex mechanisms of MPS. Although each MPS type and subtype was characterized by specific changes in gene expression profile, there were genes with significantly changed expression relative to wild-type cells that could be classified as common for various MPS types, suggesting similar disturbances in cellular processes. Therefore, both common features of all MPS types, and differences between them, might be potentially explained on the basis of changes in certain cellular processes arising from disturbed regulations of genes' expression. These results may shed a new light on the mechanisms of genetic diseases, indicating how a single mutation can result in complex pathomechanism, due to perturbations in the network of cellular reactions. Moreover, they should be considered in studies on development of novel therapies, suggesting also why currently available treatment methods fail to correct all/most symptoms of MPS. We propose a hypothesis that disturbances in some cellular processes cannot be corrected by simple reduction of GAG levels; thus, combined therapies are necessary which may require improvement of these processes., Competing Interests: The authors declare no conflicts of interest.

Published

2020

49. Genetic Base of Behavioral Disorders in Mucopolysaccharidoses: Transcriptomic Studies.

Author

Pierzynowska K, Gaffke L, Podlacha M, and Węgrzyn G

Subjects

Brain metabolism, Cell Line, Cells, Cultured, Child, Child, Preschool, Female, G(M1) Ganglioside genetics, G(M1) Ganglioside metabolism, Humans, Infant, Male, Mental Disorders etiology, Mucopolysaccharidoses complications, Mental Disorders genetics, Mucopolysaccharidoses genetics, Transcriptome

Abstract

Mucopolysaccharidoses (MPS) are a group of inherited metabolic diseases caused by mutations leading to defective degradation of glycosaminoglycans (GAGs) and their accumulation in cells. Among 11 known types and subtypes of MPS, neuronopathy occurs in seven (MPS I, II, IIIA, IIIB, IIIC, IIID, VII). Brain dysfunctions, occurring in these seven types/subtypes include various behavioral disorders. Intriguingly, behavioral symptoms are significantly different between patients suffering from various MPS types. Molecular base of such differences remains unknown. Here, we asked if expression of genes considered as connected to behavior (based on Gene Ontology, GO terms) is changed in MPS. Using cell lines of all MPS types, we have performed transcriptomic (RNA-seq) studies and assessed expression of genes involved in behavior. We found significant differences between MPS types in this regard, with the most severe changes in MPS IIIA (the type considered as the behaviorally most severely affected), while the lowest changes in MPS IVA and MPS VI (types in which little or no behavioral disorders are known). Intriguingly, relatively severe changes were found also in MPS IVB (in which, despite no behavioral disorder noted, the same gene is mutated as in GM1 gangliosidosis, a severe neurodegenerative disease) and MPS IX (in which only a few patients were described to date, thus, behavioral problems are not well recognized). More detailed analyses of expression of certain genes allowed us to propose an association of specific changes in the levels of transcripts in specific MPS types to certain behavioral disorders observed in patients. Therefore, this work provides a principle for further studies on the molecular mechanism of behavioral changes occurring in MPS patients.

Published

2020

50. Design and applications of gene therapy vectors for mucopolysaccharidosis in Colombia.

Author

Alméciga-Diaz CJ and Barrera LA

Subjects

Colombia, Enzyme Replacement Therapy methods, Genetic Vectors therapeutic use, Humans, Mucopolysaccharidoses genetics, Mucopolysaccharidosis IV genetics, Mucopolysaccharidosis IV therapy, Genetic Therapy methods, Genetic Vectors genetics, Mucopolysaccharidoses therapy

Abstract

The authors briefly describe their work in the construction of viral derived vectors for the use in gene therapy of muchopolysaccharide storage diseases (MPS), especially in Morquio A syndrome. The motivations to undertake that line of research about twenty years ago was the belief that gene therapy was the most plausible treatment for monogenic diseases due to the transient effect and its difficulty to reach bone tissue of the only effective treatment in use, the enzyme replacement therapy. The strategy used to increase the bone targeting was to include in the vectors an aspartic acid octapeptide that increases their affinity for the oppositely charged hydroxyapatite molecule of bone. It is also discussed the difficulties to do front line research in many developing countries, due to the extended belief that their research money should be mainly devoted to projects that render solutions in a very short time. However, the authors argue in favor of doing research in gene therapy, because it is proving to be the solution for many monogenic diseases, and therefore there is a need of people with good command of GT all over the world, in order to make good use of that therapy especially for ex-vivo treatments.

Published

2020