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Start Over Author "Mistry, Pramod" Topic lysosomal storage diseases
10 results on '"Mistry, Pramod"'

2. Transformative effect of a Humanitarian Program for individuals affected by rare diseases: building support systems and creating local expertise.

Author

Verma IC, El-Beshlawy A, Tylki-Szymańska A, Martins A, Duan YL, Collin-Histed T, van der Linde MS, Mansour R, Dũng VC, and Mistry PK

Subjects
Child, Delivery of Health Care, Humans, Infant, Newborn, Lysosomal Storage Diseases, Rare Diseases
Abstract

Rare diseases affect > 400 million people globally with a disproportionate burden falling on children, resulting in high morbidity and mortality rates. Affected individuals in some under-resourced countries have limited access to expert care or treatments; moreover, they suffer long diagnostic journeys during which debilitating and life-threatening complications occur. Lysosomal storage disorders (LSD) are prototype rare diseases due, in the main, to inherited deficiencies of lysosomal enzymes/transporters that affect up to 1 in 5000 newborns. Recognizing the need to provide treatment access to people with LSDs everywhere, a collaborative partnership was pioneered and set up 30 years ago. Partnering with local authorities, non-government organizations across six continents, local as well as international experts, a robust, sustainable Humanitarian Program emerged that now represents the most enduring charitable access program for LSD treatment. Here we present the history, process, lasting beneficial effect of the program to develop healthcare systems and infrastructures, and the lessons learned from addressing major unmet needs for LSDs., (© 2022. The Author(s).)

Published
2022
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3. Clinical relevance of endpoints in clinical trials for acid sphingomyelinase deficiency enzyme replacement therapy.

Author

Jones SA, McGovern M, Lidove O, Giugliani R, Mistry PK, Dionisi-Vici C, Munoz-Rojas MV, Nalysnyk L, Schecter AD, and Wasserstein M

Subjects
Carbon Monoxide metabolism, Enzyme Replacement Therapy, Humans, Lung metabolism, Lung pathology, Lysosomal Storage Diseases epidemiology, Lysosomal Storage Diseases pathology, Lysosomal Storage Diseases therapy, Mutation genetics, Niemann-Pick Diseases epidemiology, Niemann-Pick Diseases pathology, Niemann-Pick Diseases therapy, Spleen enzymology, Spleen pathology, Splenomegaly epidemiology, Splenomegaly pathology, Splenomegaly therapy, Lysosomal Storage Diseases genetics, Niemann-Pick Diseases genetics, Sphingomyelin Phosphodiesterase genetics, Splenomegaly genetics
Abstract

Background: Acid sphingomyelinase deficiency (ASMD) also known as Niemann-Pick disease, is a rare lysosomal storage disorder with a diverse disease spectrum that includes slowly progressive, chronic visceral (type B) and neurovisceral forms (intermediate type A/B), in addition to infantile, rapidly progressive fatal neurovisceral disease (type A)., Purpose and Methods: We review the published evidence on the relevance of splenomegaly and reduced lung diffusion capacity to the clinical burden of chronic forms of ASMD. Targeted literature searches were conducted to identify relevant ASMD and non-ASMD studies for associations between diffusing capacity of the lungs for carbon monoxide (DL CO ) and splenomegaly, with clinical parameters and outcome measures., Results: Respiratory disease and organomegaly are primary and independent contributors to mortality, disease burden, and morbidity for patients with chronic ASMD. The degree of splenomegaly correlates with short stature, atherogenic lipid profile, and degree of abnormality of hematologic parameters, and thus may be considered a surrogate marker for bleeding risk, abnormal lipid profiles and possibly, liver fibrosis. Progressive lung disease is a prevalent clinical feature of chronic ASMD, contributing to a decreased quality of life (QoL) and an increased disease burden. In addition, respiratory-related complications are a major cause of mortality in ASMD., Conclusions: The reviewed evidence from ASMD natural history and observational studies supports the use of lung function and spleen volume as clinically meaningful endpoints in ASMD trials that translate into important measures of disease burden for patients., (Copyright © 2020 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2020
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4. Roscoe Owen Brady, MD: Remembrances of co-investigators and colleagues.

Author

Desnick RJ, Barton NW, Furbish S, Grabowski GA, Karlsson S, Kolodny EH, Medin JA, Murray GJ, Mistry PK, Patterson MC, Schiffmann R, and Weinreb NJ

Subjects
Enzyme Replacement Therapy methods, Gaucher Disease drug therapy, History, 20th Century, History, 21st Century, Humans, Research Personnel, Enzyme Replacement Therapy history, Lysosomal Storage Diseases drug therapy
Abstract

To celebrate the research visions and accomplishments of the late Roscoe O. Brady (1923-2016), remembrance commentaries were requested from several of his postdoctoral research fellows and colleagues. These commentaries not only reflect on the accomplishments of Dr. Brady, but they also share some of the backstories and experiences working in the Brady laboratory. They provide insights and perspectives on Brady's research activities, and especially on his efforts to develop an effective treatment for patients with Type 1 Gaucher disease. These remembrances illuminate Brady's efforts to implement the latest scientific advances with an outstanding team of young co-investigators to develop and demonstrate the safety and effectiveness of the first enzyme replacement therapy for a lysosomal storage disease. Brady's pursuit and persistence in accomplishing his research objectives provide insights into this remarkably successful physician scientist who paved the way for the development of treatments for patients with other lysosomal storage diseases., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published
2017
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5. Overcoming the Next Barriers to Successful Therapy.

Author

Cohen IJ, Baris H, Mistry PK, and Sands MS

Subjects
1-Deoxynojirimycin analogs & derivatives, 1-Deoxynojirimycin therapeutic use, Administration, Oral, Cellulose, Daucus carota, Drug Delivery Systems, Drug Discovery, Enzyme Inhibitors therapeutic use, Enzyme Replacement Therapy, Fabry Disease drug therapy, Gaucher Disease drug therapy, Humans, Mucolipidoses drug therapy, Pyrrolidines therapeutic use, Lysosomal Storage Diseases drug therapy, Rare Diseases drug therapy
Published
2016

8. Osteopenia in Gaucher disease develops early in life: Response to imiglucerase enzyme therapy in children, adolescents and adults

Author

Mistry, Pramod K., Weinreb, Neal J., Kaplan, Paige, Cole, J. Alexander, Gwosdow, Andrea R., and Hangartner, Thomas

Subjects
*OSTEOPENIA, *GAUCHER'S disease, *DUAL-energy X-ray absorptiometry, *GLUCOSIDASES, *SPINE, *LYSOSOMAL storage diseases, *BONE diseases in children, *GENETIC polymorphisms
Abstract

Abstract: Background: In Gaucher disease (GD), acid-β-glucosidase (GBA1) gene mutations result in defective glucocerebrosidase and variable combinations of hematological, visceral, and diverse bone disease. Osteopenia is highly prevalent, but its age of onset during the natural course of GD is not known. It is also unclear if the degree of improvement in osteopenia, secondary to imiglucerase enzyme therapy, differs by the age of the patient. Objective: We hypothesized that osteopenia develops early in life, during the natural course of type 1 Gaucher disease (GD1), and that its response to treatment is maximal during this period. Methods: We examined data from the International Collaborative Gaucher Group (ICGG) Gaucher Registry of patients treated with imiglucerase between the ages of 5 and 50years. Lumbar spine bone mineral density (BMD) (determined by dual-energy X-ray absorptiometry (DXA) and expressed as Z-scores) at baseline and for up to 10years on imiglucerase were analyzed in children (ages≥5 to <12years), adolescents (≥12 to <20years), young adults (≥20 to <30years), and older adults (≥30 to <50years). BMD was correlated with other disease characteristics. Pre-treatment, descriptive statistics were applied to 5-year age categories. Non-linear mixed effects regression models were used to analyze DXA Z-scores over time after treatment with imiglucerase. Results: Pre-treatment, low BMD was prevalent in all age groups, most strikingly in adolescents. DXA Z-scores were at or below −1 in 44% of children (n=43), 76% of adolescents (n=41), 54% of young adults (n=56) and 52% of older adults (n=171). The most common GBA1 genotype was N370S heteroallelic. Baseline hematological and visceral manifestations in the 4 age groups were similar. In children with DXA Z-scores≤−1 at baseline, imiglucerase therapy for 6years resulted in improvement of mean DXA Z-scores from −1.38 (95% CI −1.73 to −1.03) to −0.73 (95% CI −1.25 to −0.21); in young adults DXA Z-scores improved from −1.95 (95% CI −2.26 to −1.64) to −0.67 (95% CI −1.09 to −0.26). BMD also improved in older adults, but the magnitude of the improvement was lower compared to younger patients. Conclusions: Low bone density is common in GD1 with the highest prevalence rate in adolescence, a developmental period critical to attainment of peak bone mass. Imiglucerase results in amelioration of osteopenia in all age groups, with the greatest improvements in younger patients. [Copyright &y& Elsevier]

Published
2011
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9. Recommendations for clinical monitoring of patients with acid sphingomyelinase deficiency (ASMD).

Author

Wasserstein, Melissa, Dionisi-Vici, Carlo, Giugliani, Roberto, Hwu, Wuh-Liang, Lidove, Olivier, Lukacs, Zoltan, Mengel, Eugen, Mistry, Pramod K., Schuchman, Edward H., and McGovern, Margaret

Subjects
*NIEMANN-Pick diseases, *LYSOSOMAL storage diseases, *SPHINGOMYELINASE, *BONE marrow, *PATIENT monitoring
Abstract

Abstract Background Acid sphingomyelinase deficiency (ASMD), a rare lysosomal storage disease, results from mutations in SMPD1 , the gene encoding acid sphingomyelinase (ASM). As a result, sphingomyelin accumulates in multiple organs including spleen, liver, lung, bone marrow, lymph nodes, and in the most severe form, in the CNS and peripheral nerves. Clinical manifestations range from rapidly progressive and fatal infantile neurovisceral disease, to less rapidly progressing chronic neurovisceral and visceral forms that are associated with significant morbidity and shorter life span due to respiratory or liver disease. Objectives To provide a contemporary guide of clinical assessments for disease monitoring and symptom management across the spectrum of ASMD phenotypes. Methods An international group of ASMD experts in various research and clinical fields used an evidence-informed consensus process to identify optimal assessments, interventions, and lifestyle modifications. Results Clinical assessment strategies for major organ system involvement, including liver, spleen, cardiovascular, pulmonary, and neurological/developmental are described, as well as symptomatic treatments, interventions, and/or life style modifications that may lessen disease impact. Conclusions There is currently no disease-specific treatment for ASMD, although enzyme replacement therapy with a recombinant human ASM (olipudase alfa) is in clinical development. Current monitoring addresses symptoms and multisystem involvement. Recommended interventions and lifestyle modifications are designed to address morbidity and disease complications and improve patient quality of life. While infantile neurovisceral ASMD is uniformly fatal in early childhood, patients with chronic visceral and chronic neurovisceral ASMD require appropriate management throughout childhood and adulthood by an interdisciplinary clinical team. [ABSTRACT FROM AUTHOR]

Published
2019
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10. Effectiveness of enzyme replacement therapy in 1028 patients with type 1 Gaucher disease after 2 to 5 years of treatment: a report from the Gaucher Registry

Author

Weinreb, Neal J., Charrow, Joel, Andersson, Hans C., Kaplan, Paige, Kolodny, Edwin H., Mistry, Pramod, Pastores, Gregory, Rosenbloom, Barry E., Scott, C. Ronald, Wappner, Rebecca S., and Zimran, Ari

Subjects
*GAUCHER'S disease, *LYSOSOMAL storage diseases
Abstract

: PurposeGaucher disease is the first lysosomal storage disorder to be treated with macrophage-targeted enzyme replacement therapy. Previous studies in relatively small numbers of patients demonstrated short-term efficacy of this treatment. This study describes the effects of 2 to 5 years of treatment on specific manifestations of type 1 Gaucher disease.: Subjects and methodsPhysicians reported data from 1028 patients to the Gaucher Registry. Assessment of response included serial measurements of hemoglobin concentration, platelet count, liver and spleen volumes, and the occurrence of bone pain and bone crises.: ResultsAmong anemic patients, hemoglobin concentration increased to normal or near normal within 6 to 12 months, with a sustained response through 5 years. In thrombocytopenic patients with intact spleens, the most rapid response occurred during the first 2 years, with slower improvement thereafter. The likelihood of achieving a normal platelet count decreased with increasing severity of baseline thrombocytopenia. In patients who had undergone splenectomy, platelet counts returned to normal within 6 to 12 months. Hepatomegaly decreased by 30% to 40% during follow-up; splenomegaly decreased 50% to 60%, but rarely to volumes below five times normal size. In patients with pretreatment bone pain or bone crises, 52% (67/128) were pain free after 2 years and 94% (48/51) reported no additional crises.: ConclusionEnzyme replacement therapy prevents progressive manifestations of Gaucher disease, and ameliorates Gaucher disease–associated anemia, thrombocytopenia, organomegaly, bone pain, and bone crises. [Copyright &y& Elsevier]

Published
2002
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