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7. Clinical onset and course, response to treatment and outcome in 24 patients with the cblE or cblG remethylation defect complemented by genetic and in vitro enzyme study data

Author

Huemer, M., primary, Bürer, C., additional, Ješina, P., additional, Kožich, V., additional, Landolt, M. A., additional, Suormala, T., additional, Fowler, B., additional, Augoustides‐ Savvopoulou, P., additional, Blair, E., additional, Brennerova, K., additional, Broomfield, A., additional, De Meirleir, L., additional, Gökcay, G., additional, Hennermann, J., additional, Jardine, P., additional, Koch, J., additional, Lorenzl, S., additional, Lotz‐Havla, A. S., additional, Noss, J., additional, Parini, R., additional, Peters, H., additional, Plecko, B., additional, Ramos, F. J., additional, Schlune, A., additional, Tsiakas, K., additional, Zerjav Tansek, M., additional, and Baumgartner, M. R., additional

Published
2014
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8. Mortality and cause of death in mucopolysaccharidosis type II-a historical review based on data from the Hunter Outcome Survey (HOS)

Author

Jones, S.A., Almássy, Z., Beck, Miroslav, Burt, K., Clarke, J.T., Giugliani, R., Hendriksz, C., Kroepfl, T., Lavery, L., Lin, S.P., Malm, G., Ramaswami, U., Tincheva, R., Wraith, J.E., Bodamer, O., De Meirleir, L., Melgar, D., Boy, R., Horovitz, D., Clarke, J., Clarke, L., Mabe, P., Barišić, Ingeborg, Barić, Ivo, Zeman, J., Lund, A.M., Guffon, N., Valayannopoulos, V., Héron, B., Beck, M., Frenking, G.S., Muschol, N., Zafeiriou, D., Gabrielli, O., Cicognani, A., DiRocco, M., Parini, R., and Scarpa, M.

Subjects
Adult, Male, medicine.medical_specialty, Pediatrics, Adolescent, Idursulfase, Iduronate Sulfatase, Cohort Studies, Young Adult, Cause of Death, Epidemiology, Genetics, medicine, Humans, Mucopolysaccharidosis type II, Young adult, Child, Genetics (clinical), Cause of death, Mucopolysaccharidosis II, Retrospective Studies, MPS type II, business.industry, Data Collection, Age Factors, Infant, Hunter syndrome, Enzyme replacement therapy, medicine.disease, Surgery, Treatment Outcome, Child, Preschool, Female, Settore MED/35 - MALATTIE CUTANEE E VENEREE, business, medicine.drug, Cohort study
Abstract

Mucopolysaccharidosis type II (MPS II or Hunter syndrome) is a progressive, multisystemic disease caused by a deficiency of iduronate-2-sulfatase. Patients with the severe form of the disease have cognitive impairment and typically die in the second decade of life. Patients with the less severe form do not experience significant cognitive involvement and may survive until the fifth or sixth decade of life. We studied the relationship of both severity of MPS II and the time period in which patients died with age at death in 129 patients for whom data were entered retrospectively into HOS (Hunter Outcome Survey), the only large-scale, multinational observational study of patients with MPS II. Median age at death was significantly lower in patients with cognitive involvement compared with those without cognitive involvement (11.7 versus 14.1 years ; p = 0.024). These data indicate that cognitive involvement is indicative of more severe disease and lower life expectancy in patients with MPS II. Median age at death was significantly lower in patients who died in or before 1985 compared with those who died after 1985 (11.3 versus 14.1 years ; p alpha 0.001). The difference in age at death between patients dying in or before, relative to after, the selected cut-off date of 1985 may reflect improvements in patient identification, care and management over the past two decades. Data from patients who died after 1985 could serve as a control in analyses of the effects of enzyme replacement therapy with idursulfase on mortality in patients with MPS II.

Published
2008

9. Methylmalonic acidaemia: Examination of genotype and biochemical data in 32 patients belonging to mut, cblA or cblB complementation group

Author

Merinero, B., primary, Pérez, B., additional, Pérez-Cerdá, C., additional, Rincón, A., additional, Desviat, L. R., additional, Martínez, M. A., additional, Sala, P. Ruiz, additional, García, M. J., additional, Aldamiz-Echevarría, L., additional, Campos, J., additional, Cornejo, V., additional, del Toro, M., additional, Mahfoud, A., additional, Martínez-Pardo, M., additional, Parini, R., additional, Pedrón, C., additional, Peña-Quintana, L., additional, Pérez, M., additional, Pourfarzam, M., additional, and Ugarte, M., additional

Published
2007
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10. Clinical onset and course, response to treatment and outcome in 24 patients with the cblE or cblG remethylation defect complemented by genetic and in vitro enzyme study data.

Author

Huemer, M., Bürer, C., Ješina, P., Kožich, V., Landolt, M., Suormala, T., Fowler, B., Augoustides- Savvopoulou, P., Blair, E., Brennerova, K., Broomfield, A., Meirleir, L., Gökcay, G., Hennermann, J., Jardine, P., Koch, J., Lorenzl, S., Lotz-Havla, A., Noss, J., and Parini, R.

Abstract

Background: The cobalamin E (cblE) (MTRR, methionine synthase reductase) and cobalamin G (cblG) (MTR, methionine synthase) defects are rare inborn errors of cobalamin metabolism leading to impairment of the remethylation of homocysteine to methionine. Methods: Information on clinical and laboratory data at initial full assessment and during the course of the disease, treatment, outcome and quality of life was obtained in a survey-based, retrospective study from physicians caring for patients with the CblE or CblG defect. In addition, data on enzyme studies in cultured skin fibroblasts and mutations in the MTRR and MTR gene were analysed. Results: In 11 cblE and 13 cblG patients, failure to thrive, feeding problems, delayed milestones, muscular hypotonia, cognitive impairment and macrocytic anaemia were the most frequent symptoms. Delay in diagnosis depended on age at first symptom and clinical pattern at presentation and correlated significantly with impaired communication abilities at follow-up. Eighteen/22 patients presented with brain atrophy or white matter disease. Biochemical response to treatment with variable combinations of betaine, cobalamin, folate was significant. The overall course was considered improving ( n = 8) or stable ( n = 15) in 96 % of patients, however the average number of CNS symptoms per patient increased significantly over time and 16 of 23 patients were classified as developmentally delayed or severely handicapped. In vitro enzyme analysis data showed no correlation with outcome. Predominantly private mutations were detected and no genotype- phenotype correlations evident. Conclusions: The majority of patients with the cblE and cblG defect show limited clinical response to treatment and have neurocognitive impairment. [ABSTRACT FROM AUTHOR]

Published
2015
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11. Maple syrup urine disease (MSUD): Screening for known mutations in Italian patients

Author

Parrella, T., primary, Surrey, S., additional, Iolascon, A., additional, Sartore, M., additional, Heidenreich, R., additional, Diamond, G., additional, Ponzone, A., additional, Guardamagna, O., additional, Burlina, A. B., additional, Cerone, R., additional, Parini, R., additional, Dionisi-Vici, C., additional, Rappaport, E., additional, and Fortina, P., additional

Published
1994
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12. Medium-chain triglyceride loading test in carnitine–acylcarnitine translocase deficiency: Insights on treatment.

Author

Parini, R., Invernizzi, F., Menni, F., Garavaglia, B., Melotti, D., Rimoldi, M., Salera, S., Tosetto, C., and Taroni, F.

Abstract

The results of a medium-chain triglyceride loading test in a patient with severe carnitine–acylcarnitine translocase deficiency clearly demonstrated impaired in vivo utilization of medium-chain triglycerides. The loading test was performed at the ages of 7 and 36 months. The diet was adjusted accordingly. The clinical course has been favourable and the child is now in very good condition at age 4 years. We conclude that the utilization of medium-chain triglycerides is only partial in carnitine–acylcarnitine translocase deficiency and cannot reasonably be considered an optimal source of energy for these patients. Careful adjustment of dietetic treatment may help to improve prognosis. [ABSTRACT FROM AUTHOR]

Published
1999
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13. Presentation of the data of the Italian registry for oculocutaneous tyrosinaemia

Author

Fois, A., primary, Borgogni, P., additional, Cioni, M., additional, Molinelli, M., additional, Frezzotti, R., additional, Bardelli, A. M., additional, Lasorella, G., additional, Barberi, L., additional, Durand, P., additional, Di Rocco, M., additional, Romano, C., additional, Parini, R., additional, Corbetta, C., additional, Giovannini, M., additional, Riva, E., additional, Balato, N., additional, Sartorio, R., additional, Mollica, F., additional, Zammarchi, E., additional, and Battini, M. L., additional

Published
1986
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14. Dietary lipids in glycogen storage disease type III

Author

A. Bordugo, Irene J Hoogeveen, Surekha Pendyal, Foekje de Boer, Chiara Montanari, Serena Gasperini, Giancarlo Parenti, Vanessa B Bastek, Carmen Campana, U. Meyer, A. Rossi, Daniela Melis, Pietro Strisciuglio, Arianna Maiorana, Miriam Rigoldi, S. Paci, Terry G J Derks, Priya S. Kishnani, A. Dianin, Rossella Parini, Center for Liver, Digestive and Metabolic Diseases (CLDM), Rossi, A., Hoogeveen, I. J., Bastek, V. B., de Boer, F., Montanari, C., Meyer, U., Maiorana, A., Bordugo, A., Dianin, A., Campana, C., Rigoldi, M., Kishnani, P. S., Pendyal, S., Strisciuglio, P., Gasperini, S., Parenti, G., Parini, R., Paci, S., Melis, D., and Derks, T. G. J.

Subjects
medicine.medical_specialty, high fat, Dietary lipid, Cardiomyopathy, glycogen storage diseases, Glycogen storage disease type III, Triglyceride, Glycogen Storage Disease Type III, 03 medical and health sciences, glycogen storage disease, dietary intervention, medium‐chain triglycerides, Internal medicine, Genetics, Humans, Medicine, Child, Myopathy, Triglycerides, Genetics (clinical), Cardiomyopathie, Monitoring, Physiologic, 030304 developmental biology, 0303 health sciences, medium-chain triglycerides, metabolic control, biology, business.industry, 030305 genetics & heredity, Original Articles, medicine.disease, Dietary Fats, Liver, Hepatocellular carcinoma, Cohort, biology.protein, Original Article, Creatine kinase, medicine.symptom, Literature study, Cardiomyopathies, business, medium-chain triglyceride, Human
Abstract

A potential role of dietary lipids in the management of hepatic glycogen storage diseases (GSDs) has been proposed, but no consensus on management guidelines exists. The aim of this study was to describe current experiences with dietary lipid manipulations in hepatic GSD patients. An international study was set up to identify published and unpublished cases describing hepatic GSD patients with a dietary lipid manipulation. A literature search was performed according to the Cochrane Collaboration methodology through PubMed and EMBASE (up to December 2018). All delegates who attended the dietetics session at the IGSD2017, Groningen were invited to share unpublished cases. Due to multiple biases, only data on GSDIII were presented. A total of 28 cases with GSDIII and a dietary lipid manipulation were identified. Main indications were cardiomyopathy and/or myopathy. A high fat diet was the most common dietary lipid manipulation. A decline in creatine kinase concentrations (n = 19, P

Published
2020

15. Dietary lipids in glycogen storage disease type III: A systematic literature study, case studies, and future recommendations.

Author

Rossi A, Hoogeveen IJ, Bastek VB, de Boer F, Montanari C, Meyer U, Maiorana A, Bordugo A, Dianin A, Campana C, Rigoldi M, Kishnani PS, Pendyal S, Strisciuglio P, Gasperini S, Parenti G, Parini R, Paci S, Melis D, and Derks TGJ

Subjects
Cardiomyopathies physiopathology, Child, Glycogen Storage Disease Type III complications, Humans, Liver pathology, Monitoring, Physiologic, Triglycerides blood, Cardiomyopathies etiology, Dietary Fats, Glycogen Storage Disease Type III diet therapy
Abstract

A potential role of dietary lipids in the management of hepatic glycogen storage diseases (GSDs) has been proposed, but no consensus on management guidelines exists. The aim of this study was to describe current experiences with dietary lipid manipulations in hepatic GSD patients. An international study was set up to identify published and unpublished cases describing hepatic GSD patients with a dietary lipid manipulation. A literature search was performed according to the Cochrane Collaboration methodology through PubMed and EMBASE (up to December 2018). All delegates who attended the dietetics session at the IGSD2017, Groningen were invited to share unpublished cases. Due to multiple biases, only data on GSDIII were presented. A total of 28 cases with GSDIII and a dietary lipid manipulation were identified. Main indications were cardiomyopathy and/or myopathy. A high fat diet was the most common dietary lipid manipulation. A decline in creatine kinase concentrations (n = 19, P < .001) and a decrease in cardiac hypertrophy in paediatric GSDIIIa patients (n = 7, P < .01) were observed after the introduction with a high fat diet. This study presents an international cohort of GSDIII patients with different dietary lipid manipulations. High fat diet may be beneficial in paediatric GSDIIIa patients with cardiac hypertrophy, but careful long-term monitoring for potential complications is warranted, such as growth restriction, liver inflammation, and hepatocellular carcinoma development., (© 2020 The Authors. Journal of Inherited Metabolic Disease published by John Wiley & Sons Ltd on behalf of SSIEM.)

Published
2020
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16. Resting energy expenditure in argininosuccinic aciduria and in other urea cycle disorders.

Author

Brambilla A, Bianchi ML, Cancello R, Galimberti C, Gasperini S, Pretese R, Rigoldi M, Tursi S, and Parini R

Subjects
Adolescent, Adult, Body Composition, Calorimetry, Indirect, Child, Child, Preschool, Cohort Studies, Female, Humans, Male, Middle Aged, Young Adult, Argininosuccinic Aciduria metabolism, Energy Metabolism physiology, Rest physiology, Urea Cycle Disorders, Inborn metabolism
Abstract

No data are available on the specific energy needs of patients affected with Urea Cycle disorders (UCD) and especially argininosuccinic aciduria (ASA). In our experience, ASA patients tend to develop central adiposity and hypertriglyceridemia when treated with apparently adequate energy intake, while the other UCD do not. The aim of this study was to evaluate anthropometric parameters, body composition, risk of metabolic syndrome (MS) and resting energy expenditure (REE), both by indirect calorimetry (IC) and predictive equations, in UCD patients. Hypertension (5/13), pathological waist circumference-to-height ratio (WtHr) (6/13), hypertriglyceridemia (12/13), reduced HDL cholesterol (12/13), and MS (5/13) were found in ASA group. In the ASA cohort, the mean and median IC-REE were 88% of what was predicted by Food and Agriculture Organization of the United Nations and Harris-Benedict equations. The "other UCD" cohort did not show hypertension, dyslipidaemia nor MS; IC-REE was similar to the REE predicted by equations. A significant difference was seen for the presence of hypertension, dyslipidaemia, pathological WtHr, MS and IC-REE/predictive equations-REE in the two cohorts. ASA patients have a risk of overfeeding if their energy requirement is not assessed individually with IC. Excessive energy intake might increase the cardiovascular risk of ASA patients. We suggest to test ASA individuals with IC every year if the patient is sufficiently collaborative. We speculate that most of the features seen in ASA patients might depend on an imbalance of Krebs cycle. Further studies are needed to verify this hypothesis., (© 2019 SSIEM.)

Published
2019
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17. Chronic liver involvement in urea cycle disorders.

Author

Ranucci G, Rigoldi M, Cotugno G, Bernabei SM, Liguori A, Gasperini S, Goffredo BM, Martinelli D, Monti L, Francalanci P, Candusso M, Parini R, and Dionisi-Vici C

Subjects
Adolescent, Adult, Aged, Child, Child, Preschool, Chronic Disease, Cohort Studies, Cross-Sectional Studies, Disease Progression, Female, Follow-Up Studies, Humans, Infant, Italy, Liver diagnostic imaging, Liver pathology, Liver Diseases diagnosis, Liver Diseases pathology, Liver Diseases surgery, Liver Function Tests, Liver Transplantation, Male, Middle Aged, Urea Cycle Disorders, Inborn diagnosis, Urea Cycle Disorders, Inborn surgery, Young Adult, Liver Diseases etiology, Urea Cycle Disorders, Inborn complications, Urea Cycle Disorders, Inborn pathology
Abstract

The increased survival of urea cycle disorders (UCDs) patients has led the attention to clinical manifestations that characterize the long-term disease course. Acute and chronic liver disease have been anecdotally reported since the very first description of UCDs. However, a detailed analysis of long-term liver involvement in large patient cohorts is still needed. Chronic liver damage in UCDs has probably a multifactorial origin, but the specific underlying mechanisms of liver disease have not yet been well elucidated. In this study, we report on chronic liver involvement and on associated metabolic abnormalities in a large cohort of 102 UCD patients, followed by two reference centers in Italy. Chronic liver involvement was observed in over 60% of UCDs patients, and comparison between individual diseases showed a significant higher frequency in argininosuccinate lyase deficiency (ASLD) and in hyperornithinemia-hyperammonemia-homocitrullinemia (HHH) syndrome with elevation of transaminases and of gamma-GT in ASLD, and of alpha-fetoprotein in HHH syndrome. Also, consistent with a chronic hepatic dysfunction, ultrasound examination revealed more pronounced abnormalities in ASLD and in HHH syndrome, when compared to other UCDs. Our study highlights in a large UCDs patients' cohort that chronic liver disease is a common finding in UCDs, often with a distinct phenotype between different diseases. Furthers studies are needed to elucidate the specific involvement of different metabolic pathways in the pathogenesis of liver dysfunction in UCDs., (© 2019 SSIEM.)

Published
2019
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18. Enzyme replacement therapy outcomes across the disease spectrum: Findings from the mucopolysaccharidosis VI Clinical Surveillance Program.

Author

Harmatz PR, Lampe C, Parini R, Sharma R, Teles EL, Johnson J, Sivam D, and Sisic Z

Subjects
Adolescent, Adult, Child, Child, Preschool, Drug-Related Side Effects and Adverse Reactions, Female, Follow-Up Studies, Heart Function Tests, Humans, Infant, Infant, Newborn, Male, Middle Aged, Mucopolysaccharidosis VI urine, Recombinant Proteins therapeutic use, Registries, Respiratory Function Tests, Severity of Illness Index, Walk Test, Young Adult, Enzyme Replacement Therapy, Glycosaminoglycans urine, Mucopolysaccharidosis VI drug therapy, N-Acetylgalactosamine-4-Sulfatase therapeutic use
Abstract

The impact of galsulfase enzyme replacement therapy in patients with mucopolysaccharidosis (MPS) VI with phenotypes at either end of the disease spectrum was evaluated. The MPS VI Clinical Surveillance Program (CSP) was established to collect long-term observational data from routine clinical and laboratory assessments. A subanalysis of the CSP was performed in patients with pretreatment urinary glycosaminoglycan (uGAG) levels <100 μg/mg and ≥200 μg/mg creatinine (low- and high-uGAG) who had received galsulfase for ≥6 months. uGAG, 6-minute walk test (6MWT), 3-minute stair climb test (3MSCT), pulmonary function measures, height/growth, cardiac function, and safety were evaluated. Patients with a high-uGAG level at pre-treatment baseline (N = 68) showed greater impairments in endurance and pulmonary function than those with low-baseline uGAG levels (N = 39). From pre-treatment baseline, the distance walked on the 6MWT in the low- and high-uGAG groups increased by a mean (±SD) of 49 (±151) meters and 42 (±165) meters (median follow-up 5.5 and 7.7 years), respectively. The number of stairs/min climbed in the 3MSCT in the low- and high-uGAG groups increased by a mean of 18 (±33) and 30 (±45) (median follow-up 2.8 and 3.5 years), respectively. Overall, pulmonary function remained unchanged for both groups. No impact was seen on cardiac function. Galsulfase was generally well tolerated in both groups, with most adverse events being MPS-related complications unrelated to galsulfase. Results of this CSP sub-analysis suggest that galsulfase stabilizes MPS VI in the long-term and has an acceptable safety profile, regardless of baseline disease severity., (© 2019 The Authors. Journal of Inherited Metabolic Disease published by John Wiley & Sons Ltd on behalf of SSIEM.)

Published
2019
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19. Impact of long-term elosulfase alfa treatment on respiratory function in patients with Morquio A syndrome.

Author

Hendriksz CJ, Berger KI, Parini R, AlSayed MD, Raiman J, Giugliani R, Mitchell JJ, Burton BK, Guelbert N, Stewart F, Hughes DA, Matousek R, Jurecki E, Decker C, and Harmatz PR

Subjects
Adolescent, Adult, Aged, Child, Child, Preschool, Double-Blind Method, Enzyme Replacement Therapy methods, Female, Humans, Long-Term Care, Male, Middle Aged, Respiratory Function Tests methods, Young Adult, Chondroitinsulfatases therapeutic use, Forced Expiratory Volume drug effects, Mucopolysaccharidosis IV drug therapy, Respiration drug effects
Abstract

Objective: To present long-term respiratory function outcomes from an open-label, multi-center, phase 3 extension study (MOR-005) of elosulfase alfa enzyme replacement therapy (ERT) in patients with Morquio A syndrome., Methods: In part 1 of MOR-005, patients initially randomized to ERT in the 24-week pivotal study (MOR-004) remained on their regimen (2.0 mg/kg/week or every other week); placebo patients were re-randomized to one of the two regimens. During part 2, all patients received elosulfase alfa 2.0 mg/kg/week. Respiratory function was one of the efficacy endpoints evaluated in MOR-005. Change from MOR-004 baseline to 120 weeks of treatment for the combined population was determined and compared with results from untreated patients from a Morquio A natural history study (MorCAP)., Results: Maximum voluntary ventilation (MVV) improved up to week 72 and then stabilized; forced vital capacity (FVC) and forced expiratory volume in 1 s (FEV 1 ) increased continuously over 120 weeks. Mean increases in the modified per-protocol population was 9.2 % for FVC, 8.8 % for FEV 1 , and 6.1 % for MVV after 120 weeks. All patients ≤14 years showed respiratory improvements, presumably in part related to growth; however, these were greater in treated patients. For those >14 years, treated patients showed improvements, while deterioration occurred in untreated. Altogether, the improvements were significantly greater (P < 0.05) in treated patients., Conclusions: Long-term ERT is associated with sustained improvements in respiratory function in Morquio A. In younger patients (≤14 years), some improvement may be ascribed to growth. In older patients, other mechanisms, e.g., decreased glycosaminoglycan storage, are likely involved., Competing Interests: Compliance with ethics standards Competing interest C J Hendriksz has received consulting fees and travel support from BioMarin Pharmaceutical Inc., Alexion, Actelion, Amicus, Genzyme, and Shire; K I Berger has received consulting fees from BioMarin Pharmaceutical Inc., Teva, Vertex, Sarepta and Genzyme; R Parini has received travel grants and honoraria for scientific presentations or advisory boards from BioMarin Pharmaceutical Inc., Shire and Genzyme; M AlSayed has received honorarium and travel reimbursement from BioMarin Pharmaceutical Inc., Shire, and Genzyme; J Raiman has received travel support and speakers fees from BioMarin, Shire, Genzyme and Actelion; R Giugliani has received investigator fees, travel grants, and speaker honoraria from BioMarin Pharmaceutical, Inc.; J J Mitchell has received consulting fees and travel reimbursement from BioMarin Pharmaceutical Inc. and Genzyme and honoraria from BioMarin Pharmaceutical Inc. and Shire; B K Burton has received royalties from McGraw-Hill and clinical trial funding, consulting fees and/or honoraria from BioMarin Pharmaceutical Inc., Shire, Genzyme, Horizon Pharma, Alexion, ReGenX Bio, Armagen, and Cytonet; N Guelbert has received honorarium and travel reimbursement from Biomarin Pharmaceutical Inc., Shire and Genzyme; F Stewart has received honorarium and travel reimbursement from BioMarin Pharmaceutical Inc., Shire, and Genzyme; D A Hughes has received travel grants and honoraria for advisory boards from BioMarin Pharmaceutical Inc.; R Matousek, E Jurecki, and C Decker are employees of BioMarin Pharmaceutical Inc.; P R Harmatz has provided consulting support to BioMarin Pharmaceutical Inc., received research grants, participated in advisory panels, and received speaker honorarium from BioMarin Pharmaceutical Inc. He has also received clinical trial funding, consulting fees and/or honoraria from Armagen, Shire, Genzyme, Enobia (now Alexion), ReGenX Bio, Ciesi, PTC, and Inventiva. Details of funding This study and support in the process of manuscript development were funded by BioMarin Pharmaceutical Inc. The site in Monza (Dr. Parini) received continuous economical support to the clinical work of the Center from Fondazione Pierfranco and Luisa Mariani. This publication was supported in part (Dr. Harmatz) by the National Center for Advancing Translational Sciences, National Institutes of Health (NIH), through UCSF-CTSI Grant Number UL1 TR000004. Its contents are solely the responsibility of the authors and do not necessarily represent the official views of the NIH.

Published
2016
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20. Clinical pattern, mutations and in vitro residual activity in 33 patients with severe 5, 10 methylenetetrahydrofolate reductase (MTHFR) deficiency.

Author

Huemer M, Mulder-Bleile R, Burda P, Froese DS, Suormala T, Zeev BB, Chinnery PF, Dionisi-Vici C, Dobbelaere D, Gökcay G, Demirkol M, Häberle J, Lossos A, Mengel E, Morris AA, Niezen-Koning KE, Plecko B, Parini R, Rokicki D, Schiff M, Schimmel M, Sewell AC, Sperl W, Spiekerkoetter U, Steinmann B, Taddeucci G, Trejo-Gabriel-Galán JM, Trefz F, Tsuji M, Vilaseca MA, von Kleist-Retzow JC, Walker V, Zeman J, Baumgartner MR, and Fowler B

Subjects
Ataxia genetics, Betaine therapeutic use, Child, Female, Folic Acid therapeutic use, Genetic Association Studies methods, Homocystinuria drug therapy, Humans, Intellectual Disability genetics, Male, Methionine therapeutic use, Muscle Spasticity drug therapy, Mutation genetics, Phenotype, Psychotic Disorders drug therapy, Psychotic Disorders enzymology, Psychotic Disorders genetics, Retrospective Studies, Spinal Cord Diseases genetics, Vitamin B 12 therapeutic use, Homocystinuria enzymology, Homocystinuria genetics, Methylenetetrahydrofolate Reductase (NADPH2) deficiency, Methylenetetrahydrofolate Reductase (NADPH2) genetics, Muscle Spasticity enzymology, Muscle Spasticity genetics
Abstract

Background: Severe methylenetetrahydrofolate reductase (MTHFR) deficiency is a rare inborn defect disturbing the remethylation of homocysteine to methionine (<200 reported cases). This retrospective study evaluates clinical, biochemical genetic and in vitro enzymatic data in a cohort of 33 patients., Methods: Clinical, biochemical and treatment data was obtained from physicians by using a questionnaire. MTHFR activity was measured in primary fibroblasts; genomic DNA was extracted from cultured fibroblasts., Results: Thirty-three patients (mean age at follow-up 11.4 years; four deceased; median age at first presentation 5 weeks; 17 females) were included. Patients with very low (<1.5%) mean control values of enzyme activity (n = 14) presented earlier and with a pattern of feeding problems, encephalopathy, muscular hypotonia, neurocognitive impairment, apnoea, hydrocephalus, microcephaly and epilepsy. Patients with higher (>1.7-34.8%) residual enzyme activity had mainly psychiatric symptoms, mental retardation, myelopathy, ataxia and spasticity. Treatment with various combinations of betaine, methionine, folate and cobalamin improved the biochemical and clinical phenotype. During the disease course, patients with very low enzyme activity showed a progression of feeding problems, neurological symptoms, mental retardation, and psychiatric disease while in patients with higher residual enzyme activity, myelopathy, ataxia and spasticity increased. All other symptoms remained stable or improved in both groups upon treatment as did brain imaging in some cases. No clear genotype-phenotype correlation was obvious., Discussion: MTHFR deficiency is a severe disease primarily affecting the central nervous system. Age at presentation and clinical pattern are correlated with residual enzyme activity. Treatment alleviates biochemical abnormalities and clinical symptoms partially.

Published
2016
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21. Brain and spine MRI features of Hunter disease: frequency, natural evolution and response to therapy.

Author

Manara R, Priante E, Grimaldi M, Santoro L, Astarita L, Barone R, Concolino D, Di Rocco M, Donati MA, Fecarotta S, Ficcadenti A, Fiumara A, Furlan F, Giovannini I, Lilliu F, Mardari R, Polonara G, Procopio E, Rampazzo A, Rossi A, Sanna G, Parini R, and Scarpa M

Subjects
Adolescent, Adult, Bone Diseases, Developmental etiology, Bone Diseases, Developmental therapy, Child, Child, Preschool, Disease Progression, Female, Humans, Incidence, Magnetic Resonance Imaging, Male, Mucopolysaccharidosis II complications, Phenotype, Radiography, Treatment Outcome, Young Adult, Bone Diseases, Developmental diagnostic imaging, Bone Diseases, Developmental epidemiology, Brain diagnostic imaging, Mucopolysaccharidosis II diagnostic imaging, Mucopolysaccharidosis II therapy, Spinal Canal diagnostic imaging
Abstract

Background: Hunter disease is a rare X-linked mucopolysaccharidosis. Despite frequent neurological involvement, characterizing the severe phenotype, neuroimaging studies are scarce., Objectives: To determine frequency and severity of neuroradiological mucopolysaccharidosis-related features; to correlate them with clinical phenotype; to evaluate their natural evolution and the impact of intravenous enzymatic replacement therapy (ERT)., Methods: Sixty nine brain MRI examinations of 36 Italian patients (mean-age 10.4 years; age-range 2.2-30.8; severe phenotype in 22 patients) were evaluated. Twenty patients had multiple MRIs (median follow-up 3.1 years, range 1-16.9): among them 15 had MRIs before and after ERT, six had repeated MRIs without being on ERT and five while on ERT. Perivascular, subarachnoid and ventricle space enlargement, white matter abnormality (WMA) burden, pituitary sella/skull/posterior fossa abnormalities, periodontoid thickening, spinal stenosis, dens hypoplasia, myelopathy, vertebral and intervertebral disc abnormalities were graded by means of dedicated scales., Results: Perivascular spaces enlargement (89%), WMAs (97%), subarachnoid space enlargement (83%), IIIrd-ventricle dilatation (100%), pituitary sella abnormalities (80%), cranial hyperostosis (19%), craniosynostosis (19%), enlarged cisterna magna (39%), dens hypoplasia (66%), periodontoid thickening (94%), spinal stenosis (46%), platyspondylia (84%) and disc abnormalities (79%) were frequently detected. WMAs, IIIrd-ventricle dilatation and hyperostosis correlated with the severe phenotype (p < 0.05). Subarachnoid spaces and ventricle enlargement, WMAs and spinal stenosis progressed despite ERT, while other MR features showed minimal or no changes., Conclusions: The spectrum of brain and spine MRI abnormalities in Hunter disease is extremely wide and requires a thorough evaluation. WMAs, atrophy/communicating hydrocephalus and spinal stenosis progress over time and might represent possible disease severity markers for new treatment efficacy assessment.

Published
2011
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22. Long-term observational, non-randomized study of enzyme replacement therapy in late-onset glycogenosis type II.

Author

Bembi B, Pisa FE, Confalonieri M, Ciana G, Fiumara A, Parini R, Rigoldi M, Moglia A, Costa A, Carlucci A, Danesino C, Pittis MG, Dardis A, and Ravaglia S

Subjects
Adolescent, Adult, Age of Onset, Aged, Child, Female, Follow-Up Studies, Glycogen Storage Disease Type II enzymology, Glycogen Storage Disease Type II epidemiology, Glycogen Storage Disease Type II rehabilitation, Humans, Male, Middle Aged, Observation, Time Factors, Treatment Outcome, Young Adult, Enzyme Replacement Therapy methods, Glycogen Storage Disease Type II drug therapy, alpha-Glucosidases therapeutic use
Abstract

Objectives: Type II glycogenosis (GSDII) is a lysosomal storage disorder due to acid alpha-glucosidase (GAA) deficiency. Enzyme replacement therapy (ERT) with human recombinant alpha-glucosidase (rhGAA) has been demonstrated to be effective in the treatment of infantile forms of GSDII, but little information is available concerning late-onset phenotypes. Long-term follow-up studies are not available at present. The aim of this study was to evaluate the ERT long-term effects in late-onset GSDII., Methods: Twenty-four patients, including 7 juveniles and 17 adults, received bi-weekly infusion of rhGAA (20 mg/kg) for at least 36 months. Clinical conditions, muscular function (6-min walking test, 6MWT; Walton scale, WS), respiratory function (vital capacity, VC; forced expiratory volume, FEV1; arterial pCO(2)), and muscle enzymes were assessed every 6 months., Results: The 6MWT improved in both juvenile and adult patients (p = 0.01, p = 0.0002, respectively), as well as in patients with moderate to severe muscle function impairment (WS >3.5; p = 0.002). An overall improvement in WS was also observed (p = 0.0003). VC and FEV1 remained unchanged, while pCO(2) decreased (p = 0.017). Muscle enzymes decreased significantly (p < 0.0001). Two patients (8%) showed transient secondary events during ERT., Conclusions: Long-term ERT with rhGAA was shown to be safe, well tolerated, and effective in improving motor function and in stabilizing respiratory function in late-onset GSDII. The response pattern showed a progressive clinical improvement during the follow-up period in juvenile patients, while in adults it reached and maintained a plateau after the first year of treatment.

Published
2010
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