Your search keyword '"Jeanine R. Jarnes"' showing total 26 results

1. Dose-intensive therapy (DIT) for infantile Pompe disease: A pilot study

Author

Jeanine R. Jarnes, Nishitha R. Pillai, Alia Ahmed, Sofia Shrestha, Molly Stark, and Chester B. Whitley

Subjects

Infantile Pompe disease, Immune tolerance, Neutralizing antibodies, Acid α-glucosidase enzyme, Glycogen, Optimizing therapeutic outcomes, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Background: The current standard of care for infantile-onset Pompe disease (IOPD), a severe form of acid α-glucosidase enzyme activity deficiency is: (1) detection by newborn screening, (2) early initiation of intravenous enzyme replacement therapy (ERT) using recombinant human acid alpha-glucosidase (rhGAA), with higher doses of rhGAA increasingly used to improve clinical outcomes, and (3) immune tolerization induction (ITI) using to prevent anti-rhGAA antibody formation, with methotrexate (MTX), rituximab, and IVIG used for patients who are cross-reactive immunologic material negative (CRIM-) and monotherapy with MTX used in patients who are cross-reactive immunologic material positive (CRIM+). Objectives/methods: A pilot study evaluates a dose-intensive therapy (DIT) using high-dose ERT (40 mg/kg/week) and more frequent exposure to ERT (i.e., 3 times weekly administration) to mitigate anti-rhGAA antibody formation, as an alternative to the standard therapeutic approach for IOPD. Results: In the first patient, DIT resulted in rapid normalization of the following: (1) bi-ventricular hypertrophy, (2) urine HEX-4, (3) CK, (4) liver transaminases. At 7 years of age, the patient continues the DIT regimen. To date, all pediatric developmental milestones have been met on time, anti-rhGAA antibodies have been negative and the patient is able to attend school and maintain normal activities of daily living. Conclusions: Over a 7-year period, DIT for CRIM-positive IOPD was well tolerated in the first patient treated. Excellent clinical outcomes were achieved, and anti-rhGAA antibodies levels were consistently undetectable. Assessments of more patients, that includes patients with CRIM-, as well as CRIM+ IOPD, will determine if this approach consistently achieves improved clinical outcomes and immune tolerization.

Published

2025

2. Identification of a novel fusion Iduronidase with improved activity in the cardiovascular system

Author

Sarah Kim, Michael J. Przybilla, Chester B. Whitley, Li Ou, Mahmoud Al-Kofahi, and Jeanine R. Jarnes

Subjects

Lysosomal diseases, Mucopolysaccharidosis type I, Fusion enzyme, Gene therapy, Pharmacology, Pharmacokinetics, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Background: Lysosomal diseases are a group of over 70 rare genetic conditions in which a protein deficiency (most often an enzyme deficiency) leads to multi-system disease. Current therapies for lysosomal diseases are limited in their ability to treat certain tissues that are major contributors to morbidity and mortality, such as the central nervous system (CNS) and cardiac valves. For this study, the lysosomal disease mucopolysaccharidosis type I (MPS I) was selected as the disease model. In MPS I, mutations in the IDUA gene cause a deficiency of the α-L-iduronidase (IDUA) enzyme activity, leading to disease pathology in tissues throughout the body, including the CNS and cardiac valves. Current therapies have been unable to prevent neurodevelopmental deficits and cardiac valvular disease in patients with MPS I. This study aimed to evaluate the delivery of IDUA enzyme, via a novel gene therapy construct, to target tissues. Methods: MPS I mice were hydrodynamically injected through the tail vein with plasmids containing either a codon-optimized cDNA encoding the wild-type IDUA protein or one of four modified IDUAs under the control of the liver-specific human α1-antitrypsin (hAAT) promoter. Two modified IDUAs contained a ligand for the CB1 receptor, which is a highly expressed receptor in the CNS. Iduronidase activity levels were measured in the tissues and plasma using an enzyme activity assay. Results: The modified IDUAs did not appear to have improved activity levels in the brain compared with the unmodified IDUA. However, one modified IDUA exhibited higher activity levels than the unmodified IDUA in the heart (p = 0.0211). This modified iduronidase (LT-IDUA) contained a sequence for a six amino acid peptide termed LT. LT-IDUA was further characterized using a noncompartmental pharmacokinetic approach that directly analyzed enzyme activity levels after gene delivery. LT-IDUA had a 2-fold higher area under the curve (AUC) than the unmodified IDUA (p = 0.0034) when AUC was estimated using enzyme activity levels in the plasma. Conclusion: The addition of a six amino acid peptide improved iduronidase's activity levels in the heart and plasma. The short length of this LT peptide facilitates its use as fusion enzymes encoded as gene therapy or administered as enzyme replacement therapy. More broadly, the LT peptide may aid in developing therapies for numerous lysosomal diseases.

Published

2022

3. Chitotriosidase as a biomarker for gangliosidoses

Author

Sarah Kim, Chester B. Whitley, and Jeanine R. Jarnes

Subjects

Lysosomal diseases, Chitotriosidase, GM1-gangliosidosis, GM2-gangliosidosis, Mucopolysaccharidosis, Gaucher, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Elevated serum chitotriosidase (CHITO) is an indication of macrophage activation, and its capacity have been explored as a marker of inflammation in a number of disease states. For over a decade, CHITO plasma levels have been used by clinicians as a biomarker of inflammation in the lysosomal disease, Gaucher disease, including monitoring response to therapies in patients with Gaucher disease type I. Although it is becoming increasingly recognized that inflammation is a prominent component of many lysosomal diseases, the relation of CHITO levels to disease burden has not been well-characterized in the large majority of lysosomal diseases. Moreover, the role of CHITO in lysosomal diseases that affect the central nervous system (CNS) has not been systematically studied. In this study, one hundred and thirty-four specimens of CSF and serum were collected from 34 patients with lysosomal diseases affecting the CNS. This study included patients with GM1-gangliosidosis, GM2-gangliosidosis, mucopolysaccharidoses (MPS), multiple sulfatase deficiency and Gaucher disease. CHITO levels in the CSF were significantly higher in patients with more rapidly progressing severe neurological impairment: GM1-gangliosidosis vs MPS (p

Published

2021

4. Examination of a blood-brain barrier targeting β-galactosidase-monoclonal antibody fusion protein in a murine model of GM1-gangliosidosis

Author

Michael J. Przybilla, Christine Stewart, Timothy W. Carlson, Li Ou, Brenda L. Koniar, Rohini Sidhu, Pamela J. Kell, Xuntian Jiang, Jeanine R. Jarnes, M. Gerard O'Sullivan, and Chester B. Whitley

Subjects

GM1-gangliosidosis, Enzyme replacement therapy, Fusion enzyme, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

GM1-gangliosidosis is a lysosomal disease resulting from a deficiency in the hydrolase β-galactosidase (β-gal) and subsequent accumulation of gangliosides, primarily in neuronal tissue, leading to progressive neurological deterioration and eventually early death. Lysosomal diseases with neurological involvement have limited non-invasive therapies due to the inability of lysosomal enzymes to cross the blood-brain barrier (BBB). A novel fusion enzyme, labeled mTfR-GLB1, was designed to act as a ferry across the BBB by fusing β-gal to the mouse monoclonal antibody against the mouse transferrin receptor and tested in a murine model of GM1-gangliosidosis (β-gal−/−). Twelve hours following a single intravenous dose of mTfR-GLB1 (5.0 mg/kg) into adult β-gal−/− mice showed clearance of enzyme activity in the plasma and an increase in β-gal enzyme activity in the liver and spleen. Long-term efficacy of mTfR-GLB1 was assessed by treating β-gal−/− mice intravenously twice a week with a low (2.5 mg/kg) or high (5.0 mg/kg) dose of mTfR-GLB1 for 17 weeks. Long-term studies showed high dose mice gained weight normally compared to vehicle-treated β-gal−/− mice, which are significantly heavier than heterozygous controls. Behavioral assessment at six months of age using the pole test showed β-gal−/− mice treated with mTfR-GLB1 had improved motor function. Biochemical analysis showed an increase in β-gal enzyme activity in the high dose group from negligible levels to 20% and 11% of heterozygous levels in the liver and spleen, respectively. Together, these data show that mTfR-GLB1 is a catalytically active β-gal fusion enzyme in vivo that is readily taken up into tissues.Despite these indications of bioactivity, behavior tests other than the pole test, including the Barnes maze, inverted screen, and accelerating rotarod, showed limited or no improvement of treated mice compared to β-gal−/− mice receiving vehicle only. Further, administration of mTfR-GLB1 was insufficient to create measurable increases in β-gal enzyme activity in the brain or reduce ganglioside content (biochemically and morphologically).

Published

2021

5. Patients with Gaucher disease display systemic oxidative stress dependent on therapy status

Author

Reena V. Kartha, Marcia R. Terluk, Roland Brown, Abigail Travis, Usha R. Mishra, Kyle Rudser, Heather Lau, Jeanine R. Jarnes, James C. Cloyd, and Neal J. Weinreb

Subjects

Gaucher disease, Oxidative stress, Glutathione, Lipid peroxidation, Antioxidants, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Gaucher disease is an autosomal recessive metabolic disorder caused by mutations in GBA1, which encodes for the lysosomal hydrolase enzyme, β-glucocerebrosidase. The resulting misfolded protein can trigger endoplasmic reticulum stress and an unfolded protein response within the affected cells. The enzyme deficiency leads to accumulation of its substrates, glucosylceramide and glucosylsphingosine, within macrophage lysosomes and with prominent disease manifestations in macrophage rich tissues. Resultant lysosomal pathology and impaired autophagy leads to redox imbalance, mitochondrial dysfunction and intracellular oxidative stress. Here we have systematically examined a role for oxidative stress in individuals affected by Gaucher disease. We compared multiple oxidative stress biomarkers in plasma and red blood cell samples from patients who are currently untreated, with those who are stable on standard-of-care therapy, and with healthy controls. We found significant differences in key oxidative stress biomarkers in untreated patients compared to healthy control. In treated patients, results generally fell between the controls and the untreated patients. Interestingly, even asymptomatic and minimally symptomatic untreated patients had evidence of significant systemic oxidative stress. We conclude that underlying oxidative stress may contribute to Gaucher disease pathophysiology including long-term adverse outcomes such as Parkinsonism and malignancies. Therapies targeting oxidative stress may prove useful as adjuvant treatments for Gaucher disease and other lysosomal storage disorders.

Published

2020

6. The juvenile gangliosidoses: A timeline of clinical change

Author

Kelly E. King, Sarah Kim, Chester B. Whitley, and Jeanine R. Jarnes-Utz

Subjects

GM1-gangliosidosis, Tay-Sachs disease, Disease progression, Child, Adolescent, Inherited metabolic diseases, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Background: The gangliosidoses are rare inherited diseases that result in pathologic accumulation of gangliosides in the central nervous system and other tissues, leading to severe and progressive neurological impairment and early death in the childhood forms. No treatments are currently approved for the gangliosidoses, and development of treatments is impaired by limited understanding of the natural history of these diseases. Objective: The objective of this study is to improve understanding of the juvenile gangliosidoses phenotypes and the late-infantile phenotypic subtype. Methods: Through a prospective natural history study of subjects with juvenile GM1- and GM2-gangliosidosis, a timeline of clinical changes was developed for the classic juvenile phenotypes and the late-infantile phenotypes and results of serial neurodevelopmental testing was analyzed. Results: Several candidate ‘outcome measures’ were identified: changes in ambulation and verbalization skills, the communication domain from neurodevelopmental testing and the caregiver-reported socialization domain. Conclusions: The most common symptoms leading caregivers to seek a genetic diagnosis were changes in ambulation and verbalization.

Published

2020

7. Genotype-phenotype correlation of gangliosidosis mutations using in silico tools and homology modeling

Author

Li Ou, Sarah Kim, Chester B. Whitley, and Jeanine R. Jarnes-Utz

Subjects

Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Gangliosidoses, including GM1-gangliosidosis and GM2-gangliosidosis (Tay-Sachs disease and Sandhoff disease), are lysosomal disorders resulting from enzyme deficiencies and accumulation of gangliosides. Phenotypes of gangliosidoses range from infantile, late-infantile, juvenile, and to the adult form. The genotype-phenotype correlation is essential for prognosis and clinical care planning for patients with a gangliosidosis condition. Previously, we have developed a method to establish the genotype-phenotype correlation of another lysosomal disease, mucopolysaccharidosis type I, with in silico tools. This same method was applied to analyze the genotype and phenotype of 38 patients diagnosed with a gangliosidosis disease in the United States. Out of 40 mutations identified, 3 were novel, including p.Tyr192His and p.Phe556Ser of the GLB1 gene and p.Gly461Val of the HEXA gene. Furthermore, the mutant protein structure of all missense mutations was constructed by homology modeling. A systemic structural analysis of these models revealed the specific mechanisms of how each mutation may lead to the disease. In summary, the method developed in this study holds promise as a tool that can be broadly applicable to other lysosomal diseases and monogenic diseases. Keywords: Genotype-phenotype correlation, In silico, Gangliosidosis, Disease subtype, Lysosomal disorder

Published

2019

8. Delayed Infusion Reactions to Enzyme Replacement Therapies

Author

Karimian, Zahra, Whitley, Chester B., Rudser, Kyle D., Utz, Jeanine R. Jarnes, Baumgartner, Matthias R., Series editor, Patterson, Marc, Series editor, Rahman, Shamima, Series editor, Peters, Verena, Series editor, Morava, Eva, Editor-in-chief, Zschocke, Johannes, Series editor, and Baumgartner, Matthias, editor

Published

2017

9. Physiologically‐Based Pharmacokinetic Model Development, Validation, and Application for Prediction of Eliglustat <scp>Drug–Drug</scp> Interactions

Author

Siddhee A. Sahasrabudhe, Shen Cheng, Mahmoud Al‐Kofahi, Jeanine R. Jarnes, Neal J. Weinreb, and Reena V. Kartha

Subjects

Pharmacology, Ketoconazole, Pyrrolidines, Cytochrome P-450 CYP2D6, Drug Interactions, Pharmacology (medical), United States

Abstract

Eliglustat is a glucosylceramide synthase inhibitor indicated as a long-term substrate reduction therapy for adults with type 1 Gaucher disease, a lysosomal rare disease. It is primarily metabolized by cytochrome P450 2D6 (CYP2D6), and variants in the gene encoding this enzyme are important determinants of eliglustat pharmacokinetics (PK) and drug-drug interactions (DDIs). The existing drug label addresses the DDIs to some extent but has omitted scenarios where both metabolizing CYPs (2D6 and 3A4) are mildly or moderately inhibited. The objectives of this study were (i) to develop and validate an eliglustat physiologically-based pharmacokinetic (PBPK) model with and without drug interactions, (ii) to simulate untested DDI scenarios, and (iii) to explore potential dosing flexibility using lower dose strength of eliglustat (commercially not available). PK data from healthy adults receiving eliglustat with or without interacting drugs were obtained from literature and used for the PBPK model development and validation. The model-predicted single-dose and steady-state maximum concentration (C

Published

2022

10. Biomarkers of central nervous system inflammation in infantile and juvenile gangliosidoses

Author

Utz, Jeanine R. Jarnes, Crutcher, Thomas, Schneider, Joseph, Sorgen, Patrick, and Whitley, Chester B.

Published

2015

11. START, a double blind, placebo-controlled pharmacogenetic test of responsiveness to sapropterin dihydrochloride in phenylketonuria patients

Author

Utz, Jeanine R. Jarnes, Lorentz, Cindy Pham, Markowitz, Dorothy, Rudser, Kyle D., Diethelm-Okita, Brenda, Erickson, David, and Whitley, Chester B.

Published

2012

12. Updated interim safety, biomarker, and efficacy data from Imagine-1: A phase 1/2 open-label, multicenter study to assess the safety, tolerability, and efficacy of a single dose, intra-cisterna magna (ICM) administration of PBGM01 in subjects with type I (early onset) and type IIA (late onset) infantile GM1 gangliosidosis (GM1)

Author

Jeanine R. Jarnes, Caroline A. Hastings, Can H. Ficicioglu, Debra-Lynn Day-Salvatore, Roberto Giugliani, Julien Baruteau, Chester B. Whitley, Michal Inbar-Feigenberg, Geneviève Bernard, Fatih S. Ezgü, Yan G. Ni, Michelle Miller, Michael H. Gelb, Pruthvi Nagilla, Rose Johnstone, Patricia Elsasser, Elizabeth Cunningham, Victoria Ballard, Thomas F. Haws, Mark S. Forman, and David A. Weinstein

Subjects

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

Published

2023

13. Long-term intravenous galsulfase in Maroteaux-Lamy syndrome further reduces urine glycosaminoglycans (GAG) after hematopoietic stem cell transplantation and improves cardiac function and endurance

Author

Alia Ahmed, Elizabeth Braunlin, Chester B. Whitley, and Jeanine R. Jarnes

Subjects

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

Published

2023

14. Resolving variants of unknown significance and pseudodeficiency alleles

Author

Nishitha R. Pillai, Jeanine R. Jarnes, Alia Ahmed, Todd Vanyo, and Chester B. Whitley

Subjects

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

Published

2023

15. Delayed Infusion Reactions to Enzyme Replacement Therapies

Author

Karimian, Zahra, primary, Whitley, Chester B., additional, Rudser, Kyle D., additional, and Utz, Jeanine R. Jarnes, additional

Published

2016

16. Maroteaux–Lamy syndrome (mucopolysaccharidosis type VI): A single dose of galsulfase further reduces urine glycosaminoglycans after hematopoietic stem cell transplantation

Author

Whitley, Chester B. and Utz, Jeanine R. Jarnes

Published

2010

17. Prospective longitudinal study of neurological disease trajectory in children living with late-infantile or juvenile onset of GM1 or GM2 gangliosidosis (PRONTO study)

Author

Roberto Giugliani, Benedicte Heron, Jeanine R. Jarnes, Marc C. Patterson, Maurizio Scarpa, Emilie Doppler, and Cecile Paquet Luzy

Subjects

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

Published

2022

18. WORLDSymposiumTM 2022⁎

Author

Chester B. Whitley, Lalitha Belur, Brian Bigger, Elizabeth Braunlin, Philip J. Brooks, Amber R. Brown, Brenda Diethelm-Okita, Roberto Giugliani, Jeanine R. Jarnes, Angela Meader, Jill A. Morris, Uma Ramaswami, Dawn C. Saterdalen, Maurizio Scarpa, Ellen Sidransky, Patroula Smpokou, and Danilo Tagle

Subjects

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

Published

2022

19. Genotype-phenotype correlation of gangliosidosis mutations using in silico tools and homology modeling

Author

Sarah Kim, Jeanine R. Jarnes-Utz, Chester B. Whitley, and Li Ou

Subjects

Lysosomal disorder, Genotype-phenotype correlation, Sandhoff disease, Gangliosidosis, Biology, medicine.disease_cause, Gangliosidoses, 03 medical and health sciences, Mucopolysaccharidosis type I, Disease subtype, 0302 clinical medicine, Endocrinology, Genetics, medicine, Missense mutation, Molecular Biology, lcsh:QH301-705.5, 0303 health sciences, Mutation, lcsh:R5-920, 030305 genetics & heredity, In silico, medicine.disease, Phenotype, 3. Good health, GLB1, lcsh:Biology (General), lcsh:Medicine (General), 030217 neurology & neurosurgery, Research Paper

Abstract

Gangliosidoses, including GM1-gangliosidosis and GM2-gangliosidosis (Tay-Sachs disease and Sandhoff disease), are lysosomal disorders resulting from enzyme deficiencies and accumulation of gangliosides. Phenotypes of gangliosidoses range from infantile, late-infantile, juvenile, and to the adult form. The genotype-phenotype correlation is essential for prognosis and clinical care planning for patients with a gangliosidosis condition. Previously, we have developed a method to establish the genotype-phenotype correlation of another lysosomal disease, mucopolysaccharidosis type I, with in silico tools. This same method was applied to analyze the genotype and phenotype of 38 patients diagnosed with a gangliosidosis disease in the United States. Out of 40 mutations identified, 3 were novel, including p.Tyr192His and p.Phe556Ser of the GLB1 gene and p.Gly461Val of the HEXA gene. Furthermore, the mutant protein structure of all missense mutations was constructed by homology modeling. A systemic structural analysis of these models revealed the specific mechanisms of how each mutation may lead to the disease. In summary, the method developed in this study holds promise as a tool that can be broadly applicable to other lysosomal diseases and monogenic diseases. Keywords: Genotype-phenotype correlation, In silico, Gangliosidosis, Disease subtype, Lysosomal disorder

Published

2019

20. The juvenile gangliosidoses: A timeline of clinical change

Author

Sarah Kim, Jeanine R. Jarnes-Utz, Chester B. Whitley, and Kelly King

Subjects

Pediatrics, medicine.medical_specialty, Adolescent, Tay-Sachs disease, Inherited metabolic diseases, Gangliosidoses, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, GM1-gangliosidosis, Genetics, medicine, Juvenile, Child, lcsh:QH301-705.5, Molecular Biology, lcsh:R5-920, Disease progression, 0303 health sciences, business.industry, 030305 genetics & heredity, Timeline, medicine.disease, Natural history, lcsh:Biology (General), lcsh:Medicine (General), Genetic diagnosis, business, Neurological impairment, 030217 neurology & neurosurgery, Natural history study, Research Paper

Abstract

Background The gangliosidoses are rare inherited diseases that result in pathologic accumulation of gangliosides in the central nervous system and other tissues, leading to severe and progressive neurological impairment and early death in the childhood forms. No treatments are currently approved for the gangliosidoses, and development of treatments is impaired by limited understanding of the natural history of these diseases. Objective The objective of this study is to improve understanding of the juvenile gangliosidoses phenotypes and the late-infantile phenotypic subtype. Methods Through a prospective natural history study of subjects with juvenile GM1- and GM2-gangliosidosis, a timeline of clinical changes was developed for the classic juvenile phenotypes and the late-infantile phenotypes and results of serial neurodevelopmental testing was analyzed. Results Several candidate ‘outcome measures’ were identified: changes in ambulation and verbalization skills, the communication domain from neurodevelopmental testing and the caregiver-reported socialization domain. Conclusions The most common symptoms leading caregivers to seek a genetic diagnosis were changes in ambulation and verbalization.

Published

2020

21. Gene editing to treat GM1-gangliosidosis by heterotopic insertion of GLB1 in a murine model

Author

Michael J. Przybilla, Li Ou, Chester B. Whitley, and Jeanine R. Jarnes-Utz

Subjects

Endocrinology, GLB1, Genome editing, Murine model, Endocrinology, Diabetes and Metabolism, GM1 Gangliosidosis, Genetics, Cancer research, Biology, Molecular Biology, Biochemistry

Published

2020

22. Adding enzyme replacement therapy after hematopoietic stem cell transplantation results in increased metabolic correction in MPS VI

Author

Paul J. Orchard, Elizabeth A. Braunlin, Chester B. Whitley, and Jeanine R. Jarnes-Utz

Subjects

medicine.medical_specialty, Creatinine, business.industry, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Enzyme replacement therapy, Urine, Hematopoietic stem cell transplantation, Biochemistry, Glycosaminoglycan, chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, Mole, Genetics, medicine, business, Molecular Biology, Normal range, Liver size

Abstract

Following allogenic bone marrow transplantation with predominance of donor engraftment, patients with Maroteaux-Lamy syndrome (MPS VI) demonstrate several indications of metabolic correction, such as reduction in liver size, and achieve near-normal levels of urine glycosaminoglycan (GAG). Thus it was somewhat surprising that, a single infusion of galsulfase after 20 years of full donor engraftment resulted in a further decline of GAG into the normal range (Whitley and Jarnes-Utz, Mol Genet Metab 101(4): 346-348, 2010). Urine GAG declined from slightly high pre-treatment levels (7.63 mg GAG/mmol creatinine range 7.0-8.5, N=3) progressively declining below the age-specific normal range (

Published

2019

23. Chitotriosidase as a biomarker for central nervous system inflammation in the gangliosidosis diseases

Author

Donald Bystrom, Jeanine R. Jarnes-Utz, and Chester B. Whitley

Subjects

business.industry, Endocrinology, Diabetes and Metabolism, Central nervous system, Inflammation, Gangliosidosis, medicine.disease, Biochemistry, Endocrinology, medicine.anatomical_structure, Immunology, Genetics, Medicine, Biomarker (medicine), medicine.symptom, business, Molecular Biology

Published

2019

24. Distinct progression patterns of brain disease in infantile and juvenile gangliosidoses: Volumetric quantitative MRI study

Author

Igor Nestrasil, Chester B. Whitley, Josephine M. Utz, Jeanine R. Jarnes-Utz, Kyle Rudser, and Alia Ahmed

Subjects

Male, Pathology, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Sandhoff disease, Corpus callosum, Biochemistry, Article, Gangliosidoses, White matter, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Atrophy, Gangliosidoses, GM2, 030225 pediatrics, Gangliosides, Genetics, medicine, Humans, Longitudinal Studies, Child, Molecular Biology, Gangliosidosis, GM1, business.industry, Putamen, Infant, medicine.disease, Magnetic Resonance Imaging, medicine.anatomical_structure, Cerebellar cortex, Child, Preschool, Brain size, Disease Progression, Female, business, 030217 neurology & neurosurgery

Abstract

GM1-gangliosidosis and GM2-gangliosidosis (Tay-Sachs disease and Sandhoff disease) are unrelenting heritable neurodegenerative conditions of lysosomal ganglioside accumulation. Although progressive brain atrophy is characteristic, longitudinal quantification of specific brain structures has not been systematically studied.The goal of this longitudinal study has been to quantify and track brain MRI volume changes, including specific structure volume changes, at different times in disease progression of childhood gangliosidoses, and to explore quantitative brain MRI volumetry (qMRI) as a non-invasive marker of disease progression for future treatment trials.Brain qMRI studies were performed in 14 patients with gangliosidoses (9 infantile, 5 juvenile) yearly. Cerebellar cortex and white matter, caudate, putamen, corpus callosum, ventricles, total brain, and intracranial volumes were measured, as well as total brain volume. Age-matched controls were available for the patients with the juvenile phenotype.The infantile phenotype of all gangliosidoses showed a consistent pattern of macrocephaly and rapidly increasing intracranial MRI volume with both (a) brain tissue volume (cerebral cortex and other smaller structures) and (b) ventricular volume (P0.01 for all). In contrast to apparent enlargement of the total brain volume, and chiefly the enlarged cerebral cortex, a subset of smaller brain substructures generally decreased in size: the corpus callosum, caudate and putamen became smaller with time. The volume of cerebellar cortex also decreased in patients with infantile GM1-gangliosidosis and juvenile GM1- and GM2-gangliosidosis; however, infantile GM2-gangliosidosis cerebellar cortex was the exception, increasing in size. Elevated intracranial pressure (estimated by lumbar spinal pressure) was a common finding in infantile disease and showed continued increases as the disease progressed, yet lacked MRI signs of hydrocephalus except for increasing ventricular size. Notably, in patients with juvenile gangliosidosis, macrocephaly and elevated intracranial pressure were absent and total brain volume decreased with time compared to controls (P=0.004).The disease course of infantile versus juvenile gangliosidoses is clearly distinguished by the rate of brain disease progression as characterized by qMRI. Assessments by qMRI represent a robust non-invasive method for monitoring CNS changes in the clinical course of gangliosidoses and is ideally suited to monitor effects of novel CNS-directed therapies in future clinical trials.

Published

2017

25. Preliminary N-acetylcysteine results for LDN 6722 - Role of oxidative stress and inflammation in Gaucher disease type 1: Potential use of antioxidant anti-inflammatory medications

Author

Kyle Rudser, Neal J. Weinreb, Reena V. Kartha, Usha Mishra, Paul J. Tuite, James M. Joers, James C. Cloyd, Jeanine R. Jarnes-Utz, Gülin Öz, and Marcia R. Terluk

Subjects

Antioxidant, business.industry, medicine.drug_class, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Inflammation, Pharmacology, medicine.disease_cause, Biochemistry, Anti-inflammatory, Acetylcysteine, Endocrinology, Neurochemical, Genetics, medicine, Biomarker (medicine), Sample collection, medicine.symptom, business, Molecular Biology, Oxidative stress, medicine.drug

Abstract

Enzyme replacement and substrate reduction therapies have significantly improved outcomes in patients with Type 1 Gaucher disease (GD1), but do not completely return glucocerebroside levels to the normal range nor prevent continuing tissue injury. Preliminary biomarker analyses indicate a role for oxidative stress and inflammation in GD1 pathophysiology. Thus, additional treatment strategies that target oxidative stress and inflammation have the potential to ameliorate both systemic and brain symptoms and may alter disease progression. N-acetylcysteine (NAC), a FDA-approved medication with antioxidant/anti-inflammatory activity, is also available as an inexpensive dietary supplement with a good safety profile. Our objective is to determine whether oxidative stress and inflammation in the blood and brains of individuals with GD1 can be altered with orally administered NAC. In this open-label study, we have currently enrolled 13 patients who received NAC at 3600mg/day dose. Blood sample collection for biomarker analysis and brain imaging using magnetic resonance spectroscopy (MRS) was done before and following 3 months of NAC. Total glutathione in red blood cells, which is a measure of oxidative stress, and plasma NAC concentrations were measured using a validated liquid chromatography/mass spectrometry method. Intracellular antioxidant enzyme activity and plasma markers for inflammation and lipid and protein modifications were measured using colorimetric and immunoassays. Interim analysis of data from 10 patients revealed that NAC at this dose did not significantly alter any of the neurochemical markers. However, validated MRS markers related to neuronal health such as N-acetyl aspartate (NAA) and glutamate showed trends toward improvement. Similar trends were also observed in blood antioxidant and inflammatory biomarkers. Pharmacokinetic analysis using serial samples collected 90-days after NAC regimen is underway to determine if a dose increase is warranted. If these favorable trends subsequently are shown to be significant, NAC could be a new adjunctive therapeutic option.

Published

2019

26. Cardiopulmonary findings with enzyme replacement therapy after hematopoietic cell transplantation for MPS VI

Author

Elizabeth A. Braunlin, Paul J. Orchard, Chester B. Whitley, Jeanine R. Jarnes-Utz, and Nathaniel Gaeckle

Subjects

Transplantation, Endocrinology, Hematopoietic cell, business.industry, Endocrinology, Diabetes and Metabolism, Genetics, Cancer research, Medicine, Enzyme replacement therapy, business, Molecular Biology, Biochemistry

Published

2019