Your search keyword '"Enns GM"' showing total 158 results

1. Triheptanoin treatment in patients with pediatric cardiomyopathy associated with long chain-fatty acid oxidation disorders

Author

Vockley, J, Charrow, J, Ganesh, J, Eswara, M, Diaz, GA, McCracken, E, Conway, R, Enns, GM, Starr, J, Wang, R, Abdenur, JE, Sanchez-de-Toledo, J, and Marsden, DL

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Heart Disease, Pediatric, Cardiovascular, Rare Diseases, Clinical Research, Adolescent, Cardiomyopathies, Child, Child, Preschool, Clinical Trials as Topic, Energy Metabolism, Fatty Acids, Female, Humans, Infant, Infant, Newborn, Lipid Metabolism, Inborn Errors, Male, Oxidation-Reduction, Triglycerides, Cardiomyopathy, Fatty acid oxidation disorders, Metabolic disorders, Triheptanoin, Genetics & Heredity, Genetics, Clinical sciences

Abstract

Long-chain fatty acid oxidation disorders (LC-FAOD) can cause cardiac hypertrophy and cardiomyopathy, often presenting in infancy, typically leading to death or heart transplant despite ongoing treatment. Previous data on triheptanoin treatment of cardiomyopathy in LC-FAOD suggested a clinical benefit on heart function during acute failure. An additional series of LC-FAOD patients with critical emergencies associated with cardiomyopathy was treated with triheptanoin under emergency treatment or compassionate use protocols. Case reports from 10 patients (8 infants) with moderate or severe cardiomyopathy associated with LC-FAOD are summarized. The majority of these patients were detected by newborn screening, with follow up confirmatory testing, including mutation analysis; all patients were managed with standard treatment, including medium chain triglyceride (MCT) oil. While on this regimen, they presented with acute heart failure requiring hospitalization and cardiac support (ventilation, ECMO, vasopressors) and, in some cases, resuscitation. The patients discontinued MCT oil and began treatment with triheptanoin, an investigational drug. Triheptanoin is expected to provide anaplerotic metabolites, to replace deficient TCA cycle intermediates and improve effective energy metabolism. Cardiac function was measured by echocardiography and ejection fraction (EF) was assessed. EF was moderately to severely impaired prior to triheptanoin treatment, ranging from 12-45%. Improvements in EF began between 2 and 21days following initiation of triheptanoin, and peaked at 33-71%, with 9 of 10 patients achieving EF in the normal range. Continued treatment was associated with longer-term stabilization of clinical signs of cardiomyopathy. The most common adverse event observed was gastrointestinal distress. Of the 10 patients, 7 have continued on treatment, 1 elected to discontinue due to tolerability issues, and 2 patients died from other causes. Two of the case histories illustrate that cardiomyopathy may also develop later in childhood and/or persist into adulthood. Overall, the presented cases suggest a therapeutic effect of triheptanoin in the management of acute cardiomyopathy associated with LC-FAOD.

Published

2016

2. Clinical Spectrum and Functional Consequences Associated with Bi-Allelic Pathogenic PNPT1 Variants

Author

Rius, R, Van Bergen, NJ, Compton, AG, Riley, LG, Kava, MP, Balasubramaniam, S, Amor, DJ, Fanjul-Fernandez, M, Cowley, MJ, Fahey, MC, Koenig, MK, Enns, GM, Sadedin, S, Wilson, MJ, Tan, TY, Thorburn, DR, Christodoulou, J, Rius, R, Van Bergen, NJ, Compton, AG, Riley, LG, Kava, MP, Balasubramaniam, S, Amor, DJ, Fanjul-Fernandez, M, Cowley, MJ, Fahey, MC, Koenig, MK, Enns, GM, Sadedin, S, Wilson, MJ, Tan, TY, Thorburn, DR, and Christodoulou, J

Abstract

PNPT1 (PNPase-polynucleotide phosphorylase) is involved in multiple RNA processing functions in the mitochondria. Bi-allelic pathogenic PNPT1 variants cause heterogeneous clinical phenotypes affecting multiple organs without any established genotype-phenotype correlations. Defects in PNPase can cause variable combined respiratory chain complex defects. Recently, it has been suggested that PNPase can lead to activation of an innate immune response. To better understand the clinical and molecular spectrum of patients with bi-allelic PNPT1 variants, we captured detailed clinical and molecular phenotypes of all 17 patients reported in the literature, plus seven new patients, including a 78-year-old male with the longest reported survival. A functional follow-up of genomic sequencing by cDNA studies confirmed a splicing defect in a novel, apparently synonymous, variant. Patient fibroblasts showed an accumulation of mitochondrial unprocessed PNPT1 transcripts, while blood showed an increased interferon response. Our findings suggest that functional analyses of the RNA processing function of PNPase are more sensitive than testing downstream defects in oxidative phosphorylation (OXPHPOS) enzyme activities. This research extends our knowledge of the clinical and functional consequences of bi-allelic pathogenic PNPT1 variants that may guide management and further efforts into understanding the pathophysiological mechanisms for therapeutic development.

Published

2019

3. Relationship of primary mitochondrial respiratory chain dysfunction to fiber type abnormalities in skeletal muscle

Author

Enns, GM, primary, Hoppel, CL, additional, DeArmond, SJ, additional, Schelley, S, additional, Bass, N, additional, Weisiger, K, additional, Horoupian, D, additional, and Packman, S, additional

Published

2005

4. Survival after treatment with phenylacetate and benzoate for urea-cycle disorders.

Author

Enns GM, Berry SA, Berry GT, Rhead WJ, Brusilow SW, and Hamosh A

Published

2007

5. Novel deoxyguanosine kinase gene mutations and viral infection predispose apparently healthy children to fulminant liver failure.

Author

Shieh JT, Berquist WE, Zhang Q, Chou PC, Wong LJ, and Enns GM

Published

2009

6. Postpartum 'psychosis' in mild argininosuccinate sythetase deficiency.

Author

Enns GM, O'Brien WE, Kobayashi K, Shinzawa H, and Pellegrino JE

Published

2005

7. Systemic hyalinosis: a distinctive early childhood-onset disorder characterized by mutations in the anthrax toxin receptor 2 gene (ANTRX2)

Author

Shieh JTC, Swidler P, Martignetti JA, Ramirez MCM, Balboni I, Kaplan J, Kennedy J, Abdul-Rahman O, Enns GM, Sandborg C, Slavotinek A, and Hoyme HE

Published

2006

8. Newborn Screening for X-Linked Adrenoleukodystrophy (X-ALD): Biochemical, Molecular, and Clinical Characteristics of Other Genetic Conditions.

Author

Mares Beltran CF, Tise CG, Barrick R, Niehaus AD, Sponberg R, Chang R, Enns GM, and Abdenur JE

Subjects

Humans, Male, Female, Infant, Newborn, Zellweger Syndrome genetics, Zellweger Syndrome diagnosis, California, Genetic Testing methods, Adrenoleukodystrophy genetics, Adrenoleukodystrophy diagnosis, Neonatal Screening, ATP Binding Cassette Transporter, Subfamily D, Member 1 genetics

Abstract

The state of California (CA) added X-linked adrenoleukodystrophy (X-ALD) to newborn screening (NBS) in 2016 via the measurement of C26:0-lysophosphatidylcholine (C26:0-LPC) in a two-tier fashion, followed by sequencing of the ABCD1 gene. This has resulted in the identification of individuals with genetic conditions beyond X-ALD that can also result in elevated C26:0-LPC by NBS. We describe the biochemical, molecular, and clinical characteristics of nine patients from two metabolic centers in California who screened positive by NBS for elevated C26:0-LPC between 2016 and 2022 and were ultimately diagnosed with a genetic condition other than X-ALD. Seven individuals were diagnosed with Zellweger spectrum disorder (ZSD) due to biallelic variants in PEX genes. One male was diagnosed with Klinefelter syndrome and one female was found to have an X chromosome contiguous gene deletion syndrome after the identification of a heterozygous VUS and hemizygous VUS variant in ABCD1, respectively. Patients with ZSD had significantly higher first- and second-tier C26:0-LPC levels compared to the two non-ZSD cases. Identification of children with ZSD and atypical patterns of ABCD1 variants is a secondary benefit of NBS for X-ALD, leading to earlier diagnosis, prompt therapeutic initiation, and more accurate genetic counseling. As screening for X-ALD continues via the measurement of C26:0-LPC, our knowledge of additional genetic conditions associated with elevated C26:0-LPC will continue to advance, allowing for increased recognition of other genetic disorders for which early intervention is warranted.

Published

2024

9. Efficacy and safety of pegzilarginase in arginase 1 deficiency (PEACE): a phase 3, randomized, double-blind, placebo-controlled, multi-centre trial.

Author

Russo RS, Gasperini S, Bubb G, Neuman L, Sloan LS, Diaz GA, and Enns GM

Abstract

Background: Arginase 1 Deficiency (ARG1-D) is a rare debilitating, progressive, inherited, metabolic disease characterized by marked increases in plasma arginine (pArg) and its metabolites, with increased morbidity, substantial reductions in quality of life, and premature mortality. Effective treatments that can lower arginine and improve clinical outcomes is currently lacking. Pegzilarginase is a novel human arginase 1 enzyme therapy. The present trial aimed to demonstrate efficacy of pegzilarginase on pArg and key mobility outcomes., Methods: This Phase 3 randomized, double-blind, placebo-controlled, parallel-group clinical trial (clinicaltrials.govNCT03921541, EudraCT 2018-004837-34), randomized patients with ARG1-D 2:1 to intravenously/subcutaneously once-weekly pegzilarginase or placebo in conjunction with their individualized disease management. It was conducted in 7 countries; United States, United Kingdom, Canada, Austria, France, Germany, Italy. Primary endpoint was change from baseline in pArg after 24 weeks; key secondary endpoints were change from baseline at Week 24 in Gross Motor Function Measure part E (GMFM-E) and 2-min walk test (2MWT). Full Analysis Set was used for the analyses., Findings: From 01 May 2019 to 29 March 2021, 32 patients were enrolled and randomized (pegzilarginase, n = 21; placebo, n = 11). Pegzilarginase lowered geometric mean pArg from 354.0 μmol/L to 86.4 μmol/L at Week 24 vs 464.7 to 426.6 μmol/L for placebo (95% CI: -67.1%, -83.5%; p  < 0.0001) and normalized levels in 90.5% of patients (vs 0% with placebo). In addition, clinically relevant functional mobility improvements were demonstrated with pegzilarginase treatment. These effects were sustained long-term through additional 24 weeks of subsequent exposure. Pegzilarginase was well-tolerated, with adverse events being mostly transient and mild/moderate in severity., Interpretation: These results support pegzilarginase as the first potential treatment to normalize pArg in ARG1-D and achieve clinically meaningful improvements in functional mobility., Funding: Aeglea BioTherapeutics., Competing Interests: Dr Sanchez Russo has received travel support from Aeglea BioTherapeutics. Dr Gasperini has served on advisory boards for Aeglea BioTherapeutics and Immedica Pharma AB. Dr Neuman and Dr Bubb are former employees of Aeglea BioTherapeutics and owns stocks or equity in the company. Dr Sloan is former employee of Aeglea BioTherapeutics. Dr Diaz has received travel support from and served on advisory boards and speakers bureaus for Aeglea BioTherapeutics. Dr Enns has served on advisory boards for Aeglea BioTherapeutics, and performed consulting services for Horizon Therapeutics. Aeglea BioTherapeutics funded the trial and provided medical writing support. Immedica Pharma provided scientific editing and medical writing support., (© 2023 Immedica Pharma AB.)

Published

2024

10. Specifications of the ACMG/AMP guidelines for ACADVL variant interpretation.

Author

Flowers M, Dickson A, Miller MJ, Spector E, Enns GM, Baudet H, Pasquali M, Racacho L, Sadre-Bazzaz K, Wen T, Fogarty M, Fernandez R, Weaver MA, Feigenbaum A, Graham BH, and Mao R

Subjects

Humans, Infant, Newborn, Acyl-CoA Dehydrogenase, Long-Chain genetics, Congenital Bone Marrow Failure Syndromes genetics, Genetic Testing, Genetic Variation, Lipid Metabolism, Inborn Errors diagnosis, Lipid Metabolism, Inborn Errors genetics, Mitochondrial Diseases genetics, Muscular Diseases genetics

Abstract

Very long-chain acyl-CoA dehydrogenase (VLCAD) deficiency (VLCADD) is a relatively common inborn error of metabolism, but due to difficulty in accurately predicting affected status through newborn screening, molecular confirmation of the causative variants by sequencing of the ACADVL gene is necessary. Although the ACMG/AMP guidelines have helped standardize variant classification, ACADVL variant classification remains disparate due to a phenotype that can be nonspecific, the possibility of variants that produce late-onset disease, and relatively high carrier frequency, amongst other challenges. Therefore, an ACADVL-specific variant curation expert panel (VCEP) was created to facilitate the specification of the ACMG/AMP guidelines for VLCADD. We expect these guidelines to help streamline, increase concordance, and expedite the classification of ACADVL variants., Competing Interests: Declaration of Competing Interest None., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published

2023

11. Efficacy and Safety of Elamipretide in Individuals With Primary Mitochondrial Myopathy: The MMPOWER-3 Randomized Clinical Trial.

Author

Karaa A, Bertini E, Carelli V, Cohen BH, Enns GM, Falk MJ, Goldstein A, Gorman GS, Haas R, Hirano M, Klopstock T, Koenig MK, Kornblum C, Lamperti C, Lehman A, Longo N, Molnar MJ, Parikh S, Phan H, Pitceathly RDS, Saneto R, Scaglia F, Servidei S, Tarnopolsky M, Toscano A, Van Hove JLK, Vissing J, Vockley J, Finman JS, Brown DA, Shiffer JA, and Mancuso M

Subjects

Humans, Female, Middle Aged, Male, Merozoite Surface Protein 1 therapeutic use, Fatigue, Double-Blind Method, Treatment Outcome, Quality of Life, Mitochondrial Myopathies drug therapy

Abstract

Background and Objectives: Primary mitochondrial myopathies (PMMs) encompass a group of genetic disorders that impair mitochondrial oxidative phosphorylation, adversely affecting physical function, exercise capacity, and quality of life (QoL). Current PMM standards of care address symptoms, with limited clinical impact, constituting a significant therapeutic unmet need. We present data from MMPOWER-3, a pivotal, phase-3, randomized, double-blind, placebo-controlled clinical trial that evaluated the efficacy and safety of elamipretide in participants with genetically confirmed PMM., Methods: After screening, eligible participants were randomized 1:1 to receive either 24 weeks of elamipretide at a dose of 40 mg/d or placebo subcutaneously. Primary efficacy endpoints included change from baseline to week 24 on the distance walked on the 6-minute walk test (6MWT) and total fatigue on the Primary Mitochondrial Myopathy Symptom Assessment (PMMSA). Secondary endpoints included most bothersome symptom score on the PMMSA, NeuroQoL Fatigue Short-Form scores, and the patient global impression and clinician global impression of PMM symptoms., Results: Participants (N = 218) were randomized (n = 109 elamipretide; n = 109 placebo). The m0ean age was 45.6 years (64% women; 94% White). Most of the participants (n = 162 [74%]) had mitochondrial DNA (mtDNA) alteration, with the remainder having nuclear DNA (nDNA) defects. At screening, the most frequent bothersome PMM symptom on the PMMSA was tiredness during activities (28.9%). At baseline, the mean distance walked on the 6MWT was 336.7 ± 81.2 meters, the mean score for total fatigue on the PMMSA was 10.6 ± 2.5, and the mean T score for the Neuro-QoL Fatigue Short-Form was 54.7 ± 7.5. The study did not meet its primary endpoints assessing changes in the 6MWT and PMMSA total fatigue score (TFS). Between the participants receiving elamipretide and those receiving placebo, the difference in the least squares mean (SE) from baseline to week 24 on distance walked on the 6MWT was -3.2 (95% CI -18.7 to 12.3; p = 0.69) meters, and on the PMMSA, the total fatigue score was -0.07 (95% CI -0.10 to 0.26; p = 0.37). Elamipretide treatment was well-tolerated with most adverse events being mild to moderate in severity., Discussion: Subcutaneous elamipretide treatment did not improve outcomes in the 6MWT and PMMSA TFS in patients with PMM. However, this phase-3 study demonstrated that subcutaneous elamipretide is well-tolerated., Trial Registration Information: Trial registered with clinicaltrials.gov, Clinical Trials Identifier: NCT03323749; submitted on October 12, 2017; first patient enrolled October 9, 2017., Clinicaltrials: gov/ct2/show/NCT03323749?term = elamipretide&draw = 2&rank = 9., Classification of Evidence: This study provides Class I evidence that elamipretide does not improve the 6MWT or fatigue at 24 weeks compared with placebo in patients with primary mitochondrial myopathy., (Copyright © 2023 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the American Academy of Neurology.)

Published

2023

12. Contributions from medical geneticists in clinical trials of genetic therapies: A points to consider statement of the American College of Medical Genetics and Genomics (ACMG).

Author

Peña LDM, Burrage LC, Enns GM, Esplin ED, Harding C, Mendell JR, Niu ZN, Scharfe C, Yu T, and Koeberl DD

Subjects

Humans, United States, Genomics, Genetic Testing, Genetic Therapy, Genetics, Medical

Abstract

Competing Interests: Conflict of Interest Funding and support listed here did not support the development of this document unless included in the acknowledgments section. L.D.M.P. has received compensation for sponsored travel (Sanofi US), advisory board participation (ModernaTx; Sanofi US; Ultragenyx Pharmaceutical Inc; AveXis, Inc; Orphazyme; BioMarin Pharmaceutical Inc), and research support (ModernaTx; Cyclo Therapeutics, Inc; Takeda; Mallinckrodt Pharmaceuticals; Orphazyme) in the past 4 years. G.M.E. has served as a consultant to AllStripes; Codexis, Inc; Glycomine, Inc; Hemoshear Therapeutics; Homology Medicines, Inc; Horizon Therapeutics; M6P Therapeutics; Moderna, Inc; Travere Therapeutics, Inc; and Ultragenyx Pharmaceutical Inc; is the cofounder of Evvia Therapeutics; and serves on the Data Monitoring Committees for clinical trials for Abliva, Amicus Therapeutics, Audentes Therapeutics, BioMarin Pharmaceutical Inc, Modis Therapeutics, Paradigm Biopharma Ltd, Passage Bio, and RegenxBio. E.D.E. is a stockholder of Invitae Corporation and a scientific advisory board member and stockholder at Taproot Health. T.Y. has served as a consultant for BioMarin Pharmaceutical Inc. D.D.K. has served as a consultant for Sangamo Therapeutics, Inc; Sanofi; Amicus Therapeutics; Takeda; and Vertex Pharmaceuticals; has received grant support from Viking Therapeutics, Genzyme Sanofi, Roivant Rare Diseases, and Amicus Therapeutics; and has equity in Askbio, which is developing gene therapy for Pompe disease. All other authors declare no conflicts of interest.

Published

2023

13. MT-ATP6 mitochondrial disease identified by newborn screening reveals a distinct biochemical phenotype.

Author

Tise CG, Verscaj CP, Mendelsohn BA, Woods J, Lee CU, Enns GM, Stander Z, Hall PL, Cowan TM, and Cusmano-Ozog KP

Subjects

Humans, Infant, Newborn, Citrulline blood, Pedigree, Urea Cycle Disorders, Inborn diagnosis, Neonatal Screening, Mitochondrial Proton-Translocating ATPases genetics, Mitochondrial Diseases blood, Mitochondrial Diseases diagnosis, Mitochondrial Diseases genetics

Abstract

Although decreased citrulline is used as a newborn screening (NBS) marker to identify proximal urea cycle disorders (UCDs), it is also a feature of some mitochondrial diseases, including MT-ATP6 mitochondrial disease. Here we describe biochemical and clinical features of 11 children born to eight mothers from seven separate families who were identified with low citrulline by NBS (range 3-5 μM; screening cutoff >5) and ultimately diagnosed with MT-ATP6 mitochondrial disease. Follow-up testing revealed a pattern of hypocitrullinemia together with elevated propionyl-(C3) and 3-hydroxyisovaleryl-(C5-OH) acylcarnitines, and a homoplasmic pathogenic variant in MT-ATP6 in all cases. Single and multivariate analysis of NBS data from the 11 cases using Collaborative Laboratory Integrated Reports (CLIR; https://clir.mayo.edu) demonstrated citrulline <1st percentile, C3 > 50th percentile, and C5-OH >90th percentile when compared with reference data, as well as unequivocal separation from proximal UCD cases and false-positive low citrulline cases using dual scatter plots. Five of the eight mothers were symptomatic at the time of their child(ren)'s diagnosis, and all mothers and maternal grandmothers evaluated molecularly and biochemically had a homoplasmic pathogenic variant in MT-ATP6, low citrulline, elevated C3, and/or elevated C5-OH. All molecularly confirmed individuals (n = 17) with either no symptoms (n = 12), migraines (n = 1), or a neurogenic muscle weakness, ataxia, and retinitis pigmentosa (NARP) phenotype (n = 3) were found to have an A or U mitochondrial haplogroup, while one child with infantile-lethal Leigh syndrome had a B haplogroup., (© 2023 Wiley Periodicals LLC.)

Published

2023

14. Outcomes after liver transplantation in MPV17 deficiency: A rebuttal.

Author

Huang AC, Ebel NH, Romero D, Enns GM, Esquivel CO, and Bonham C

Subjects

Humans, Liver, Membrane Proteins, Mitochondrial Proteins, Liver Transplantation, Mitochondrial Diseases

Published

2023

15. A Phase 1 Study of Oral Vitamin D 3 in Boys and Young Men With X-Linked Adrenoleukodystrophy.

Author

Van Haren KP, Cunanan K, Awani A, Gu M, Peña D, Chromik LC, Považan M, Rossi NC, Goodman J, Sundaram V, Winterbottom J, Raymond GV, Cowan T, Enns GM, Waubant E, Steinman L, Barker PB, Spielman D, and Fatemi A

Abstract

Background and Objectives: There are no therapies for preventing cerebral demyelination in X-linked adrenoleukodystrophy (ALD). Higher plasma vitamin D levels have been linked to lower risk of inflammatory brain lesions. We assessed the safety and pharmacokinetics of oral vitamin D dosing regimens in boys and young men with ALD., Methods: In this open-label, multicenter, phase 1 study, we recruited boys and young men with ALD without brain lesions to a 12-month study of daily oral vitamin D 3 supplementation. Our primary outcome was attainment of plasma 25-hydroxyvitamin D levels in target range (40-80 ng/mL) at 6 and 12 months. Secondary outcomes included safety and glutathione levels in the brain, measured with magnetic resonance spectroscopy, and blood, measured via mass spectrometry. Participants were initially assigned to a fixed dosing regimen starting at 2,000 IU daily, regardless of weight. After a midstudy safety assessment, we modified the dosing regimen, so all subsequent participants were assigned to a weight-stratified dosing regimen starting as low as 1,000 IU daily., Results: Between October 2016 and June 2019, we enrolled 21 participants (n = 12, fixed-dose regimen; n = 9, weight-stratified regimen) with a median age of 6.7 years (range: 1.9-22 years) and median weight of 20 kg (range: 11.7-85.5 kg). The number of participants achieving target vitamin D levels was similar in both groups at 6 months (fixed dose: 92%; weight stratified: 78%) and 12 months (fixed dose: 67%; weight stratified: 67%). Among the 12 participants in the fixed-dose regimen, half had asymptomatic elevations in either urine calcium:creatinine or plasma 25-hydroxyvitamin D; no laboratory deviations occurred with the weight-stratified regimen. Glutathione levels in the brain, but not the blood, increased significantly between baseline and 12 months., Discussion: Our vitamin D dosing regimens were well tolerated and achieved target 25-hydroxyvitamin D levels in most participants. Brain glutathione levels warrant further study as a biomarker for vitamin D and ALD., Classification of Evidence: This study provides Class IV evidence that fixed or weight-stratified vitamin D supplementation achieved target levels of 25-hydroxyvitamin D in boys and young men with X-ALD without brain lesions., Competing Interests: K. Van Haren has received consulting fees from Bluebird bio, Minoryx, Viking Therapeutics, Poxel, and Orpheris and participated in advisory boards for Poxel, Viking, ALD Connect, and the United Leukodystrophy Foundations all outside the submitted work; G.V. Raymond has received consulting fees from Bluebird bio, Viking Therapeutics, and Minoryx for therapy development outside the submitted work; A. Fatemi has received consulting fees from Minoryx, Viking, Autobahn, Vertex, Poxel, Aevi, and Calico for scientific advising outside the submitted work, has participated in a DSMB for Bluebird Bio, and is a board member at ALD Connect. K. Cunanan, A. Avni, M. Gu, D. Pena, L.C. Chromik, M. Povazan, N.C. Rossi, J. Winterbottom, J. Goodman, V. Sundaram, T. Cowan, G.M. Enns, E. Waubant, L. Steinman, P.B. Barker, and D. Spielman have no disclosures. Full disclosure form information provided by the authors is available with the full text of this article at Neurology.org/NG., (Copyright © 2023 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the American Academy of Neurology.)

Published

2023

16. Fractionated plasma N-glycan profiling of novel cohort of ATP6AP1-CDG subjects identifies phenotypic association.

Author

Alharbi H, Daniel EJP, Thies J, Chang I, Goldner DL, Ng BG, Witters P, Aqul A, Velez-Bartolomei F, Enns GM, Hsu E, Kichula E, Lee E, Lourenco C, Poskanzer SA, Rasmussen S, Saarela K, Wang YM, Raymond KM, Schultz MJ, Freeze HH, Lam C, Edmondson AC, and He M

Subjects

Humans, Glycoproteins metabolism, Transferrin metabolism, Phenotype, Polysaccharides, Hydrolases genetics, Immunoglobulins genetics, Immunoglobulins metabolism, Congenital Disorders of Glycosylation genetics, Vacuolar Proton-Translocating ATPases genetics

Abstract

ATP6AP1-CDG is an X-linked disorder typically characterized by hepatopathy, immunodeficiency, and an abnormal type II transferrin glycosylation pattern. Here, we present 11 new patients and clinical updates with biochemical characterization on one previously reported patient. We also document intrafamilial phenotypic variability and atypical presentations, expanding the symptomatology of ATP6AP1-CDG to include dystonia, hepatocellular carcinoma, and lysosomal abnormalities on hepatic histology. Three of our subjects received successful liver transplantation. We performed N-glycan profiling of total and fractionated plasma proteins for six patients and show associations with varying phenotypes, demonstrating potential diagnostic and prognostic value of fractionated N-glycan profiles. The aberrant N-linked glycosylation in purified transferrin and remaining plasma glycoprotein fractions normalized in one patient post hepatic transplant, while the increases of Man4GlcNAc2 and Man5GlcNAc2 in purified immunoglobulins persisted. Interestingly, in the single patient with isolated immune deficiency phenotype, elevated high-mannose glycans were detected on purified immunoglobulins without glycosylation abnormalities on transferrin or the remaining plasma glycoprotein fractions. Given the diverse and often tissue specific clinical presentations and the need of clinical management post hepatic transplant in ATP6AP1-CDG patients, these results demonstrate that fractionated plasma N-glycan profiling could be a valuable tool in diagnosis and disease monitoring., (© 2023 SSIEM.)

Published

2023

17. Validation of a targeted metabolomics panel for improved second-tier newborn screening.

Author

Mak J, Peng G, Le A, Gandotra N, Enns GM, Scharfe C, and Cowan TM

Subjects

Humans, Infant, Newborn, Chromatography, Liquid, Tandem Mass Spectrometry, Neonatal Screening methods, Ornithine Carbamoyltransferase Deficiency Disease

Abstract

Improved second-tier assays are needed to reduce the number of false positives in newborn screening (NBS) for inherited metabolic disorders including those on the Recommended Uniform Screening Panel (RUSP). We developed an expanded metabolite panel for second-tier testing of dried blood spot (DBS) samples from screen-positive cases reported by the California NBS program, consisting of true- and false-positives from four disorders: glutaric acidemia type I (GA1), methylmalonic acidemia (MMA), ornithine transcarbamylase deficiency (OTCD), and very long-chain acyl-CoA dehydrogenase deficiency (VLCADD). This panel was assembled from known disease markers and new features discovered by untargeted metabolomics and applied to second-tier analysis of single DBS punches using liquid chromatography-tandem mass spectrometry (LC-MS/MS) in a 3-min run. Additionally, we trained a Random Forest (RF) machine learning classifier to improve separation of true- and false positive cases. Targeted metabolomic analysis of 121 analytes from DBS extracts in combination with RF classification at a sensitivity of 100% reduced false positives for GA1 by 83%, MMA by 84%, OTCD by 100%, and VLCADD by 51%. This performance was driven by a combination of known disease markers (3-hydroxyglutaric acid, methylmalonic acid, citrulline, and C14:1), other amino acids and acylcarnitines, and novel metabolites identified to be isobaric to several long-chain acylcarnitine and hydroxy-acylcarnitine species. These findings establish the effectiveness of this second-tier test to improve screening for these four conditions and demonstrate the utility of supervised machine learning in reducing false-positives for conditions lacking clearly discriminating markers, with future studies aimed at optimizing and expanding the panel to additional disease targets., (© 2023 The Authors. Journal of Inherited Metabolic Disease published by John Wiley & Sons Ltd on behalf of SSIEM.)

Published

2023

18. Outcomes after liver transplantation in MPV17 deficiency (Navajo neurohepatopathy): A single-center case series.

Author

Huang AC, Ebel NH, Romero D, Martin B, Jhun I, Brown M, Enns GM, Esquivel C, and Bonham C

Subjects

Child, Child, Preschool, DNA, Mitochondrial genetics, Heredodegenerative Disorders, Nervous System, Humans, Infant, Liver Diseases, Membrane Proteins genetics, Mitochondrial Diseases, Mitochondrial Proteins genetics, Peripheral Nervous System Diseases, Acute-On-Chronic Liver Failure, Liver Transplantation

Abstract

Background: MPV17-related mitochondrial DNA maintenance defect (MPV17 deficiency) is a rare, autosomal recessive mitochondrial DNA depletion syndrome with a high mortality rate in infancy and early childhood due to progression to liver failure. Liver transplantation for children with MPV17 deficiency has been considered controversial due to uncertainty about the potential progression of extrahepatic manifestations following liver transplantation., Methods: We describe our institution's experience for two infants diagnosed with infantile MPV17 deficiency who presented in acute on chronic liver failure, but with normal development and normal neurological status who successfully underwent liver transplantation., Results: Both patients underwent successful liver transplantation with normal development and neurological status at 3 years and 16 months post-transplant, respectively., Conclusions: In this rare disease population, we describe two infants with MPV17 deficiency who underwent liver transplantation for acute on chronic liver failure who continue to have normal development, without progression of neurological disease. MPV17 deficiency should not be considered a contraindication to liver transplantation., (© 2022 Wiley Periodicals LLC.)

Published

2022

19. Response to triheptanoin therapy in critically ill patients with LC-FAOD: Report of patients treated through an expanded access program.

Author

Vockley J, Enns GM, Ramirez AN, Bedrosian CL, Reineking B, Lu X, Ray K, Rahman S, and Marsden D

Subjects

Critical Illness therapy, Fatty Acids metabolism, Fatty Acids therapeutic use, Humans, Infant, Oxidation-Reduction, Retrospective Studies, Stroke Volume, Triglycerides therapeutic use, Ventricular Function, Left, Cardiomyopathies drug therapy, Cardiomyopathies metabolism, Lipid Metabolism, Inborn Errors

Abstract

Long-chain fatty acid oxidation disorders (LC-FAOD) are a group of inborn errors of metabolism wherein patients are unable to process long-chain fatty acids into useable energy in the mitochondria. LC-FAOD commonly affects organ systems with high energy demand, manifesting as hypoketotic hypoglycemia, liver dysfunction, cardiomyopathy, rhabdomyolysis, and skeletal myopathy, as well as peripheral neuropathy and retinopathy in some subtypes. Collectively, LC-FAOD have a high mortality rate, especially in cases of early onset disease, and in the presence of cardiomyopathy. Triheptanoin is a synthetic medium-odd chain triglyceride, produced using a GMP-compliant process, which was designed to replenish mitochondrial metabolic deficits and restore energy homeostasis. Prior to its approval, triheptanoin was only available through clinical trials or to seriously ill patients as part of an expanded access program (EAP) following physician request. This retrospective study examined the impact of triheptanoin on cardiovascular parameters, in critically ill patients who participated in the EAP from February 2013 to January 2018. These patients persisted in critical condition despite receiving standard treatment in highly qualified centers by expert metabolic physicians and dietitians. Physician-completed questionnaires and narrative summaries were used to evaluate the disease presentation and management prior to the trigger event leading to triheptanoin request and use, and the response to triheptanoin treatment. Following triheptanoin initiation, most patients survived the initial trigger event (e.g., severe urinary tract infection, pneumonia) and demonstrated improvements in both short-term and long-term LC-FAOD manifestations. In patients with cardiomyopathy, stabilization or improvement from pretreatment levels was reported in left ventricular ejection fraction and left ventricular mass, in particular, all infants with cardiomyopathy showed improvement in cardiac function during triheptanoin therapy. Triheptanoin therapy was generally well tolerated. The study results are consistent with the existing positive benefit/risk profile of triheptanoin and reflect the effect of triheptanoin improving cardiac function in patients experiencing severe episodes of metabolic decompensation despite standard therapy., (Copyright © 2022 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2022

20. Variable clinical severity in TANGO2 deficiency: Case series and literature review.

Author

Schymick J, Leahy P, Cowan T, Ruzhnikov MRZ, Gates R, Fernandez L, Pramanik G, Yarlagadda V, Wheeler M, Bernstein JA, Enns GM, and Lee C

Subjects

Exons, Humans, Phenotype, Exome Sequencing, Intellectual Disability genetics, Rhabdomyolysis diagnosis, Rhabdomyolysis genetics

Abstract

Biallelic pathogenic variants in the TANGO2 (transport and Golgi organization 2 homolog) gene have been identified as causing a rare metabolic disorder characterized by susceptibility to recurrent rhabdomyolysis, lactic acidosis, encephalopathy, and life-threatening tachyarrhythmias. Recently published reports suggest variable clinical severity and phenotypes. This study details five new patients from two families with biallelic pathogenic variants in the TANGO2 gene identified by whole exome sequencing and includes the largest number of affected individuals from a single family reported to date. We document significant intrafamilial variability and highlight that milder phenotypes may be underrecognized. We present biochemical and clinical data to help highlight the features that aid in consideration of this condition in the differential with disorders of fatty acid oxidation. We also present a comprehensive literature review summarizing the molecular, clinical, and biochemical findings for 92 individuals across 13 publications. Of the 27 pathogenic variants reported to date, the recurrent exons 3-9 deletion represents the most common variant seen in 42% of individuals with TANGO2 deficiency. Common clinical features seen in >70% of all individuals include acute metabolic crisis, rhabdomyolysis, neurologic abnormalities, developmental delay, and intellectual disability. Findings such as elevated creatine kinase, hypothyroidism, ketotic hypoglycemia, QT prolongation, or abnormalities of long-chain acylcarnitines and urine dicarboxylic acids should raise clinical suspicion for this life-threatening condition., (© 2021 Wiley Periodicals LLC.)

Published

2022

21. Diagnostic challenges and disease management in patients with a mild Zellweger spectrum disorder phenotype.

Author

Enns GM, Ammous Z, Himes RW, Nogueira J, Palle S, Sullivan M, and Ramirez C

Subjects

Adult, Clinical Trials as Topic, Humans, Longitudinal Studies, Zellweger Syndrome classification, Zellweger Syndrome drug therapy, Zellweger Syndrome physiopathology, Disease Management, Phenotype, Zellweger Syndrome diagnosis

Abstract

Peroxisome Biogenesis Disorders-Zellweger spectrum disorder (PBD-ZSD) is a rare, autosomal recessive peroxisome biogenesis disorder that presents with variable symptoms. In patients with PBD-ZSD, pathogenic variants in the PEX family of genes disrupt normal peroxisomal function, impairing α- and β-oxidation of very-long-chain fatty acids and synthesis of bile acids, resulting in increased levels of toxic bile acid intermediates and multisystem organ damage. The spectrum of severity in PBD-ZSD is variable, with some patients dying in the first year of life, while others live into adulthood. Symptoms of mild PBD-ZSD include various combinations of developmental delay, craniofacial dysmorphic features, visual impairment, sensorineural hearing loss, liver disease, and adrenal insufficiency. Disease progression in mild PBD-ZSD is generally slow, and may include extended periods of stability in some cases. The presence and extent to which symptoms occur in mild PBD-ZSD represents a diagnostic challenge that can cause delays in diagnosis with potential significant implications related to disease monitoring and treatment. There is some support for the pharmacologic therapies of Lorenzo's oil, docosohexanoic acid, and batyl alcohol in altering symptoms; however, systematic long-term studies are lacking. Cholic acid (CA) therapy has demonstrated treatment efficacy in patients with PBD-ZSD, including decreased toxic bile acid intermediates, transaminase levels, and liver inflammation, with improvement in growth parameters. However, these responses are most apparent in patients diagnosed and treated at a young age. Advanced liver disease may limit the efficacy of CA, underscoring the need to diagnose and treat these patients before significant liver damage and other related complications occur. Here we discuss the signs and symptoms of PBD-ZSD in patients with mild disease, standard diagnostic tools, factors affecting disease management, and available pharmacological interventions., Competing Interests: Declaration of Competing Interest Drs. Enns, Himes, and Ramirez are consultants for Travere Therapeutics, Inc., the sponsor of this research, and did not receive payment for their contributions to this work. Their participation in the research fulfill all authorship criteria as outlined by the International Committee of Medical Journal Editors (ICMJE). Zineb Ammous, MD: Consulting and speaking for Travere Therapeutics, Inc. (2018–2019); advisory board for BioMarin (2018) and Travere Therapeutics, Inc. (2017). Janaina Nogueira, MD: Consulting for Travere Therapeutics, Inc. Sirish Palle, MD: Consulting for Travere Therapeutics, Inc. Meghan Sullivan, PhD is an employee of MedVal Scientific Information Services, which was contracted by Travere Therapeutics, Inc., Inc. for medical writing support., (Copyright © 2021. Published by Elsevier Inc.)

Published

2021

22. Clinical effect and safety profile of pegzilarginase in patients with arginase 1 deficiency.

Author

Diaz GA, Schulze A, McNutt MC, Leão-Teles E, Merritt JL 2nd, Enns GM, Batzios S, Bannick A, Zori RT, Sloan LS, Potts SL, Bubb G, and Quinn AG

Subjects

Adolescent, Adult, Arginase adverse effects, Arginase blood, Arginine metabolism, Child, Child, Preschool, Disease Management, Female, Humans, Hyperammonemia etiology, Hyperargininemia blood, Hyperargininemia genetics, Hyperargininemia metabolism, Male, Recombinant Proteins adverse effects, Recombinant Proteins therapeutic use, United States, Vomiting etiology, Young Adult, Arginase genetics, Arginase therapeutic use, Arginine blood, Hyperargininemia drug therapy

Abstract

Hyperargininemia in patients with arginase 1 deficiency (ARG1-D) is considered a key driver of disease manifestations, including spasticity, developmental delay, and seizures. Pegzilarginase (AEB1102) is an investigational enzyme therapy which is being developed as a novel arginine lowering approach. We report the safety and efficacy of intravenously (IV) administered pegzilarginase in pediatric and adult ARG1-D patients (n = 16) from a Phase 1/2 study (101A) and the first 12 weeks of an open-label extension study (102A). Substantial disease burden at baseline included lower-limb spasticity, developmental delay, and previous hyperammonemic episodes in 75%, 56%, and 44% of patients, respectively. Baseline plasma arginine (pArg) was elevated (median 389 μM, range 238-566) on standard disease management. Once weekly repeat dosing resulted in a median decrease of pArg of 277 μM after 20 cumulative doses (n = 14) with pArg in the normal range (40 to 115 μM) in 50% of patients at 168 hours post dose (mean pegzilarginase dose 0.10 mg/kg). Lowering pArg was accompanied by improvements in one or more key mobility assessments (6MWT, GMFM-D & E) in 79% of patients. In 101A, seven hypersensitivity reactions occurred in four patients (out of 162 infusions administered). Other common treatment-related adverse events (AEs) included vomiting, hyperammonemia, pruritus, and abdominal pain. Treatment-related serious AEs that occurred in five patients were all observed in 101A. Pegzilarginase was effective in lowering pArg levels with an accompanying clinical response in patients with ARG1-D. The improvements with pegzilarginase occurred in patients receiving standard treatment approaches, which suggests that pegzilarginase could offer benefit over existing disease management., (© 2020 The Authors. Journal of Inherited Metabolic Disease published by John Wiley & Sons Ltd on behalf of SSIEM.)

Published

2021

23. The Present and Future of Mitochondrial-Based Therapeutics for Eye Disease.

Author

Ji MH, Kreymerman A, Belle K, Ghiam BK, Muscat SR, Mahajan VB, Enns GM, Mercola M, and Wood EH

Subjects

Humans, Eye Diseases drug therapy, Mitochondria

Abstract

Translational Relevance: Mitochondria are viable therapeutic targets for a broad spectrum of ocular diseases.

Published

2021

24. Aicardi-Goutières syndrome may present with positive newborn screen for X-linked adrenoleukodystrophy.

Author

Tise CG, Morales JA, Lee AS, Velez-Bartolomei F, Floyd BJ, Levy RJ, Cusmano-Ozog KP, Feigenbaum AS, Ruzhnikov MRZ, Lee CU, and Enns GM

Subjects

Adrenoleukodystrophy complications, Adrenoleukodystrophy genetics, Adrenoleukodystrophy pathology, Autoimmune Diseases of the Nervous System complications, Autoimmune Diseases of the Nervous System genetics, Autoimmune Diseases of the Nervous System pathology, Dried Blood Spot Testing, Female, Genetic Diseases, X-Linked complications, Genetic Diseases, X-Linked genetics, Genetic Diseases, X-Linked pathology, Humans, Infant, Infant, Newborn, Lysophosphatidylcholines blood, Male, Nervous System Malformations complications, Nervous System Malformations genetics, Nervous System Malformations pathology, Tandem Mass Spectrometry, Adrenoleukodystrophy blood, Autoimmune Diseases of the Nervous System blood, Genetic Diseases, X-Linked blood, Neonatal Screening, Nervous System Malformations blood

Abstract

We report three unrelated probands, two male and one female, diagnosed with Aicardi-Goutières syndrome (AGS) after screening positive on California newborn screening (CA NBS) for X-linked adrenoleukodystrophy (X-ALD) due to elevated C26:0 lysophosphatidylcholine (C26:0-LPC). Follow-up evaluation was notable for elevated C26:0, C26:1, and C26:0/C22:0 ratio, and normal red blood cell plasmalogens levels in all three probands. Diagnoses were confirmed by molecular sequencing prior to 12 months of age after clinical evaluation was inconsistent with X-ALD or suggestive of AGS. For at least one proband, the early diagnosis of AGS enabled candidacy for enrollment into a therapeutic clinical trial. This report demonstrates the importance of including AGS on the differential diagnosis for individuals who screen positive for X-ALD, particularly infants with abnormal neurological features, as this age of onset would be highly unusual for X-ALD. While AGS is not included on the Recommended Universal Screening Panel, affected individuals can be identified early through state NBS programs so long as providers are aware of a broader differential that includes AGS. This report is timely, as state NBS algorithms for X-ALD are actively being established, implemented, and refined., (© 2021 Wiley Periodicals LLC.)

Published

2021

25. Profound neonatal lactic acidosis and renal tubulopathy in a patient with glycogen storage disease type IXɑ2 secondary to a de novo pathogenic variant in PHKA2 .

Author

Morales JA, Tise CG, Narang A, Grimm PC, Enns GM, and Lee CU

Abstract

The phenotype of individuals with glycogen storage disease (GSD) IX appears to be highly variable, even within subtypes. Features include short stature, fasting hypoglycemia with ketosis, hepatomegaly, and transaminitis. GSD IXɑ2 is caused by hemizygous pathogenic variants in PHKA2 , and results in deficiency of the phosphorylase kinase enzyme, particularly in the liver. Like other GSDs, GSD IXɑ2 can present with hypoglycemia and post-prandial lactic acidosis, but has never been reported in a newborn, nor with lactic acidosis as the presenting feature. Here we describe the clinical presentation and course of a newborn boy with profound neonatal lactic and metabolic acidosis, renal tubulopathy, and sensorineural hearing loss (SNHL) diagnosed with GSD IXɑ2 through exome sequencing. Review of the literature suggests this case represents an atypical and severe presentation of GSD IXɑ2 and proposes expansion of the phenotype to include neonatal lactic acidosis and renal tubulopathy., Competing Interests: Dr. Enns reports grants from PTC Therapeutics, Astellas, Stealth Biotherapeutics, and University of Florida (outside the submitted work)., (© 2021 The Authors.)

Published

2021

26. Compound heterozygous KCTD7 variants in progressive myoclonus epilepsy.

Author

Burke EA, Sturgeon M, Zastrow DB, Fernandez L, Prybol C, Marwaha S, Frothingham EP, Ward PA, Eng CM, Fresard L, Montgomery SB, Enns GM, Fisher PG, Wolfe LA, Harding B, Carrington B, Bishop K, Sood R, Huang Y, Elkahloun A, Toro C, Bassuk AG, Wheeler MT, Markello TC, Gahl WA, and Malicdan MCV

Subjects

Animals, Child, Child, Preschool, Female, Humans, Infant, Male, Mutation, Myoclonic Epilepsies, Progressive physiopathology, Pedigree, Phenotype, Zebrafish, Myoclonic Epilepsies, Progressive genetics, Potassium Channels genetics

Abstract

KCTD7 is a member of the potassium channel tetramerization domain-containing protein family and has been associated with progressive myoclonic epilepsy (PME), characterized by myoclonus, epilepsy, and neurological deterioration. Here we report four affected individuals from two unrelated families in which we identified KCTD7 compound heterozygous single nucleotide variants through exome sequencing. RNAseq was used to detect a non-annotated splicing junction created by a synonymous variant in the second family. Whole-cell patch-clamp analysis of neuroblastoma cells overexpressing the patients' variant alleles demonstrated aberrant potassium regulation. While all four patients experienced many of the common clinical features of PME, they also showed variable phenotypes not previously reported, including dysautonomia, brain pathology findings including a significantly reduced thalamus, and the lack of myoclonic seizures. To gain further insight into the pathogenesis of the disorder, zinc finger nucleases were used to generate kctd7 knockout zebrafish. Kctd7 homozygous mutants showed global dysregulation of gene expression and increased transcription of c-fos , which has previously been correlated with seizure activity in animal models. Together these findings expand the known phenotypic spectrum of KCTD7 -associated PME, report a new animal model for future studies, and contribute valuable insights into the disease.

Published

2021

27. AMP-independent activator of AMPK for treatment of mitochondrial disorders.

Author

Moore T, Yanes RE, Calton MA, Vollrath D, Enns GM, and Cowan TM

Subjects

Allosteric Regulation drug effects, Animals, Biphenyl Compounds, Cell Respiration drug effects, Cell Survival, Cells, Cultured, Disease Models, Animal, Enzyme Activation drug effects, Fibroblasts cytology, Fibroblasts drug effects, Fibroblasts metabolism, Humans, Mice, Mitochondrial Diseases genetics, Mitochondrial Diseases metabolism, Oxidative Stress drug effects, Oxygen Consumption drug effects, Pyrimidines administration & dosage, Pyrimidines pharmacology, Pyrones administration & dosage, Pyrones pharmacology, Thiazoles pharmacology, Thiophenes administration & dosage, Thiophenes pharmacology, meta-Aminobenzoates pharmacology, AMP-Activated Protein Kinases genetics, AMP-Activated Protein Kinases metabolism, Mitochondrial Diseases drug therapy, Thiazoles administration & dosage, meta-Aminobenzoates administration & dosage

Abstract

Mitochondrial diseases are a clinically heterogenous group of disorders caused by respiratory chain dysfunction and associated with progressive, multi-systemic phenotype. There is no effective treatment or cure, and no FDA-approved drug for treating mitochondrial disease. To identify and characterize potential therapeutic compounds, we developed an in vitro screening assay and identified a group of direct AMP-activated protein kinase (AMPK) activators originally developed for the treatment of diabetes and metabolic syndrome. Unlike previously investigated AMPK agonists such as AICAR, these compounds allosterically activate AMPK in an AMP-independent manner, thereby increasing specificity and decreasing pleiotropic effects. The direct AMPK activator PT1 significantly improved mitochondrial function in assays of cellular respiration, energy status, and cellular redox. PT1 also protected against retinal degeneration in a mouse model of photoreceptor degeneration associated with mitochondrial dysfunction and oxidative stress, further supporting the therapeutic potential of AMP-independent AMPK agonists in the treatment of mitochondrial disease., Competing Interests: Part of this work was supported by a grant awarded from Raptor Pharmaceuticals. They had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. Raptor Pharmaceuticals is also not associated in anyway to the editorial board or committee of PLOS ONE nor have they acted as expert witness in any relevant legal proceedings. Our financial support from Raptor Pharmaceuticals does not alter our adherence to PLOS ONE policies on sharing data and materials.

Published

2020

28. Ethnic variability in newborn metabolic screening markers associated with false-positive outcomes.

Author

Peng G, Tang Y, Gandotra N, Enns GM, Cowan TM, Zhao H, and Scharfe C

Subjects

Acyl-CoA Dehydrogenase, Long-Chain blood, Amino Acid Metabolism, Inborn Errors blood, Biomarkers blood, Brain Diseases, Metabolic blood, California, Congenital Bone Marrow Failure Syndromes blood, False Positive Reactions, Female, Gestational Age, Glutaryl-CoA Dehydrogenase blood, Glutaryl-CoA Dehydrogenase deficiency, Humans, Infant, Newborn, Lipid Metabolism, Inborn Errors blood, Male, Mitochondrial Diseases blood, Muscular Diseases blood, Ornithine Carbamoyltransferase Deficiency Disease blood, Tandem Mass Spectrometry, Amino Acid Metabolism, Inborn Errors diagnosis, Congenital Bone Marrow Failure Syndromes diagnosis, Ethnicity statistics & numerical data, Lipid Metabolism, Inborn Errors diagnosis, Mitochondrial Diseases diagnosis, Muscular Diseases diagnosis, Neonatal Screening methods, Ornithine Carbamoyltransferase Deficiency Disease diagnosis

Abstract

Newborn screening (NBS) programmes utilise information on a variety of clinical variables such as gestational age, sex, and birth weight to reduce false-positive screens for inborn metabolic disorders. Here we study the influence of ethnicity on metabolic marker levels in a diverse newborn population. NBS data from screen-negative singleton babies (n = 100 000) were analysed, which included blood metabolic markers measured by tandem mass spectrometry and ethnicity status reported by the parents. Metabolic marker levels were compared between major ethnic groups (Asian, Black, Hispanic, White) using effect size analysis, which controlled for group size differences and influence from clinical variables. Marker level differences found between ethnic groups were correlated to NBS data from 2532 false-positive cases for four metabolic diseases: glutaric acidemia type 1 (GA-1), methylmalonic acidemia (MMA), ornithine transcarbamylase deficiency (OTCD), and very long-chain acyl-CoA dehydrogenase deficiency (VLCADD). In the result, 79% of the metabolic markers (34 of 43) had ethnicity-related differences. Compared to the other groups, Black infants had elevated GA-1 markers (C5DC, Cohen's d = .37, P < .001), Hispanics had elevated MMA markers (C3, Cohen's d = .13, P < .001, and C3/C2, Cohen's d = .27, P < .001); and Whites had elevated VLCADD markers (C14, Cohen's d = .28, P < .001, and C14:1, Cohen's d = .22, P < .001) and decreased OTCD markers (citrulline, Cohen's d = -.26, P < .001). These findings correlated with the higher false-positive rates in Black infants for GA-1, in Hispanics for MMA, and in Whites for OTCD and for VLCADD. Web-based tools are available to analyse ethnicity-related changes in newborn metabolism and to support developing methods to identify false-positives in metabolic screening., (© 2020 The Authors. Journal of Inherited Metabolic Disease published by John Wiley & Sons Ltd on behalf of SSIEM.)

Published

2020

29. Successful liver transplantation in mitochondrial neurogastrointestinal encephalomyopathy (MNGIE).

Author

Kripps K, Nakayuenyongsuk W, Shayota BJ, Berquist W, Gomez-Ospina N, Esquivel CO, Concepcion W, Sampson JB, Cristin DJ, Jackson WE, Gilliland S, Pomfret EA, Kueht ML, Pettit RW, Sherif YA, Emrick LT, Elsea SH, Himes R, Hirano M, Van Hove JLK, Scaglia F, Enns GM, and Larson AA

Subjects

Adolescent, Adult, Esophageal Motility Disorders genetics, Female, Hematopoietic Stem Cell Transplantation mortality, Humans, Infant, Liver Transplantation mortality, Magnetic Resonance Imaging, Male, Mitochondria enzymology, Mitochondria pathology, Mitochondrial Encephalomyopathies diagnostic imaging, Mitochondrial Encephalomyopathies genetics, Mitochondrial Encephalomyopathies physiopathology, Peripheral Nervous System Diseases genetics, Thymidine blood, Exome Sequencing, Liver Transplantation methods, Mitochondria metabolism, Mitochondrial Encephalomyopathies therapy, Thymidine Phosphorylase genetics

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is a fatal disorder characterized by progressive gastrointestinal dysmotility, peripheral neuropathy, leukoencephalopathy, skeletal myopathy, ophthalmoparesis, and ptosis. MNGIE stems from deficient thymidine phosphorylase activity (TP) leading to toxic elevations of plasma thymidine. Hematopoietic stem cell transplant (HSCT) restores TP activity and halts disease progression but has high transplant-related morbidity and mortality. Liver transplant (LT) was reported to restore TP activity in two adult MNGIE patients. We report successful LT in four additional MNGIE patients, including a pediatric patient. Our patients were diagnosed between ages 14 months and 36 years with elevated thymidine levels and biallelic pathogenic variants in TYMP. Two patients presented with progressive gastrointestinal dysmotility, and three demonstrated progressive peripheral neuropathy with two suffering limitations in ambulation. Two patients, including the child, had liver dysfunction and cirrhosis. Following LT, thymidine levels nearly normalized in all four patients and remained low for the duration of follow-up. Disease symptoms stabilized in all patients, with some manifesting improvements, including intestinal function. No patient died, and LT appeared to have a more favorable safety profile than HSCT, especially when liver disease is present. Follow-up studies will need to document the long-term impact of this new approach on disease outcome. Take Home Message: Liver transplantation is effective in stabilizing symptoms and nearly normalizing thymidine levels in patients with mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) and may have an improved safety profile over hematopoietic stem cell transplant., Competing Interests: Declaration of Competing Interest Austin Larson, MD and Johan Van Hove, MD, PhD participate in a clinical trial from Stealth Therapeutics. Fernando Scaglia, MD and Gregory Enns, MB, ChB receive research support from Stealth BioTherapeutics, Inc. and BioElectron Technology Corporation and are investigators in the North American Mitochondrial Disease Consortium. Brian J. Shayota receives funding through the NIH T32 (GM07526–41) Medical Genetics Trainee Grant., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

30. Mitochondrial diseases in North America: An analysis of the NAMDC Registry.

Author

Barca E, Long Y, Cooley V, Schoenaker R, Emmanuele V, DiMauro S, Cohen BH, Karaa A, Vladutiu GD, Haas R, Van Hove JLK, Scaglia F, Parikh S, Bedoyan JK, DeBrosse SD, Gavrilova RH, Saneto RP, Enns GM, Stacpoole PW, Ganesh J, Larson A, Zolkipli-Cunningham Z, Falk MJ, Goldstein AC, Tarnopolsky M, Gropman A, Camp K, Krotoski D, Engelstad K, Rosales XQ, Kriger J, Grier J, Buchsbaum R, Thompson JLP, and Hirano M

Abstract

Objective: To describe clinical, biochemical, and genetic features of participants with mitochondrial diseases (MtDs) enrolled in the North American Mitochondrial Disease Consortium (NAMDC) Registry., Methods: This cross-sectional, multicenter, retrospective database analysis evaluates the phenotypic and molecular characteristics of participants enrolled in the NAMDC Registry from September 2011 to December 2018. The NAMDC is a network of 17 centers with expertise in MtDs and includes both adult and pediatric specialists., Results: One thousand four hundred ten of 1,553 participants had sufficient clinical data for analysis. For this study, we included only participants with molecular genetic diagnoses (n = 666). Age at onset ranged from infancy to adulthood. The most common diagnosis was multisystemic disorder (113 participants), and only a minority of participants were diagnosed with a classical mitochondrial syndrome. The most frequent classical syndromes were Leigh syndrome (97 individuals) and mitochondrial encephalomyopathy, lactic acidosis, and stroke-like episodes (71 individuals). Pathogenic variants in the mitochondrial DNA were more frequently observed (414 participants) than pathogenic nuclear gene variants (252 participants). Pathogenic variants in 65 nuclear genes were identified, with POLG1 and PDHA1 being the most commonly affected. Pathogenic variants in 38 genes were reported only in single participants., Conclusions: The NAMDC Registry data confirm the high variability of clinical, biochemical, and genetic features of participants with MtDs. This study serves as an important resource for future enhancement of MtD research and clinical care by providing the first comprehensive description of participant with MtD in North America., (Copyright © 2020 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the American Academy of Neurology.)

Published

2020

31. Reducing False-Positive Results in Newborn Screening Using Machine Learning.

Author

Peng G, Tang Y, Cowan TM, Enns GM, Zhao H, and Scharfe C

Abstract

Newborn screening (NBS) for inborn metabolic disorders is a highly successful public health program that by design is accompanied by false-positive results. Here we trained a Random Forest machine learning classifier on screening data to improve prediction of true and false positives. Data included 39 metabolic analytes detected by tandem mass spectrometry and clinical variables such as gestational age and birth weight. Analytical performance was evaluated for a cohort of 2777 screen positives reported by the California NBS program, which consisted of 235 confirmed cases and 2542 false positives for one of four disorders: glutaric acidemia type 1 (GA-1), methylmalonic acidemia (MMA), ornithine transcarbamylase deficiency (OTCD), and very long-chain acyl-CoA dehydrogenase deficiency (VLCADD). Without changing the sensitivity to detect these disorders in screening, Random Forest-based analysis of all metabolites reduced the number of false positives for GA-1 by 89%, for MMA by 45%, for OTCD by 98%, and for VLCADD by 2%. All primary disease markers and previously reported analytes such as methionine for MMA and OTCD were among the top-ranked analytes. Random Forest's ability to classify GA-1 false positives was found similar to results obtained using Clinical Laboratory Integrated Reports (CLIR). We developed an online Random Forest tool for interpretive analysis of increasingly complex data from newborn screening., Competing Interests: Conflicts of Interest: The authors declare no conflict of interest.

Published

2020

32. De novo and inherited variants in ZNF292 underlie a neurodevelopmental disorder with features of autism spectrum disorder.

Author

Mirzaa GM, Chong JX, Piton A, Popp B, Foss K, Guo H, Harripaul R, Xia K, Scheck J, Aldinger KA, Sajan SA, Tang S, Bonneau D, Beck A, White J, Mahida S, Harris J, Smith-Hicks C, Hoyer J, Zweier C, Reis A, Thiel CT, Jamra RA, Zeid N, Yang A, Farach LS, Walsh L, Payne K, Rohena L, Velinov M, Ziegler A, Schaefer E, Gatinois V, Geneviève D, Simon MEH, Kohler J, Rotenberg J, Wheeler P, Larson A, Ernst ME, Akman CI, Westman R, Blanchet P, Schillaci LA, Vincent-Delorme C, Gripp KW, Mattioli F, Guyader GL, Gerard B, Mathieu-Dramard M, Morin G, Sasanfar R, Ayub M, Vasli N, Yang S, Person R, Monaghan KG, Nickerson DA, van Binsbergen E, Enns GM, Dries AM, Rowe LJ, Tsai ACH, Svihovec S, Friedman J, Agha Z, Qamar R, Rodan LH, Martinez-Agosto J, Ockeloen CW, Vincent M, Sunderland WJ, Bernstein JA, Eichler EE, Vincent JB, and Bamshad MJ

Subjects

Adolescent, Autism Spectrum Disorder diagnosis, Autism Spectrum Disorder diagnostic imaging, Autism Spectrum Disorder pathology, Child, Child, Preschool, Female, High-Throughput Nucleotide Sequencing methods, Humans, Male, Neurodevelopmental Disorders diagnosis, Neurodevelopmental Disorders diagnostic imaging, Neurodevelopmental Disorders pathology, Neuroimaging methods, Exome Sequencing methods, Autism Spectrum Disorder genetics, Carrier Proteins genetics, Genetic Predisposition to Disease, Nerve Tissue Proteins genetics, Neurodevelopmental Disorders genetics

Abstract

Purpose: Intellectual disability (ID) and autism spectrum disorder (ASD) are genetically heterogeneous neurodevelopmental disorders. We sought to delineate the clinical, molecular, and neuroimaging spectrum of a novel neurodevelopmental disorder caused by variants in the zinc finger protein 292 gene (ZNF292)., Methods: We ascertained a cohort of 28 families with ID due to putatively pathogenic ZNF292 variants that were identified via targeted and exome sequencing. Available data were analyzed to characterize the canonical phenotype and examine genotype-phenotype relationships., Results: Probands presented with ID as well as a spectrum of neurodevelopmental features including ASD, among others. All ZNF292 variants were de novo, except in one family with dominant inheritance. ZNF292 encodes a highly conserved zinc finger protein that acts as a transcription factor and is highly expressed in the developing human brain supporting its critical role in neurodevelopment., Conclusion: De novo and dominantly inherited variants in ZNF292 are associated with a range of neurodevelopmental features including ID and ASD. The clinical spectrum is broad, and most individuals present with mild to moderate ID with or without other syndromic features. Our results suggest that variants in ZNF292 are likely a recurrent cause of a neurodevelopmental disorder manifesting as ID with or without ASD.

Published

2020

33. Hypoglycemia in CDG patients due to PMM2 mutations: Follow up on hyperinsulinemic patients.

Author

Moravej H, Altassan R, Jaeken J, Enns GM, Ellaway C, Balasubramaniam S, De Lonlay P, Coman D, Mercimek-Andrews S, Witters P, and Morava E

Abstract

Background: Phosphomannomutase 2 deficiency (PMM2-CDG) is the most common congenital disorder of glycosylation (CDG). Hypoglycemia has been reported in various CDG including PMM2-CDG. The frequency and etiology of hypoglycemia in PMM2-CDG are not well studied., Methods: We conducted a systematic review of the literature on genetically and/or biochemically confirmed PMM2-CDG patients who developed hypoglycemia. Prospective follow-up information on the patients who received diazoxide therapy was collected and evaluated., Results: A total of 165 peer-reviewed articles reporting on 933 PMM2-CDG patients were assessed. Hypoglycemia was specifically mentioned only in 23 of these patients (2.5%). Hyperinsulinism was identified in 10 patients (43% of all hypoglycemic patients). Among these 10 patients, seven were successfully treated with diazoxide. However, most patients remained on therapy longer than a year to stay free of hypoglycemia., Conclusion: Hypoglycemia is a rarely reported finding in patients with PMM2-CDG. Diazoxide-responsive hyperinsulinism was found to have a good prognosis on medication in our PMM2-CDG patients with hypoglycemia. No genotype-phenotype correlation was observed with respect to hyperinsulinism. A prospective study should be undertaken to explore the hypothesis that hypoglycemia is underdiagnosed in PMM2-CDG and to evaluate whether hyperinsulinism is always associated with hypoglycemia., Competing Interests: The authors declare no potential conflict of interest., (© 2019 The Authors. Journal of Inherited Metabolic Disease published by John Wiley & Sons Ltd on behalf of SSIEM.)

Published

2019

34. Clinical Spectrum and Functional Consequences Associated with Bi-Allelic Pathogenic PNPT1 Variants.

Author

Rius R, Van Bergen NJ, Compton AG, Riley LG, Kava MP, Balasubramaniam S, Amor DJ, Fanjul-Fernandez M, Cowley MJ, Fahey MC, Koenig MK, Enns GM, Sadedin S, Wilson MJ, Tan TY, Thorburn DR, and Christodoulou J

Abstract

PNPT1 (PNPase-polynucleotide phosphorylase) is involved in multiple RNA processing functions in the mitochondria. Bi-allelic pathogenic PNPT1 variants cause heterogeneous clinical phenotypes affecting multiple organs without any established genotype-phenotype correlations. Defects in PNPase can cause variable combined respiratory chain complex defects. Recently, it has been suggested that PNPase can lead to activation of an innate immune response. To better understand the clinical and molecular spectrum of patients with bi-allelic PNPT1 variants, we captured detailed clinical and molecular phenotypes of all 17 patients reported in the literature, plus seven new patients, including a 78-year-old male with the longest reported survival. A functional follow-up of genomic sequencing by cDNA studies confirmed a splicing defect in a novel, apparently synonymous, variant. Patient fibroblasts showed an accumulation of mitochondrial unprocessed PNPT1 transcripts, while blood showed an increased interferon response. Our findings suggest that functional analyses of the RNA processing function of PNPase are more sensitive than testing downstream defects in oxidative phosphorylation (OXPHPOS) enzyme activities. This research extends our knowledge of the clinical and functional consequences of bi-allelic pathogenic PNPT1 variants that may guide management and further efforts into understanding the pathophysiological mechanisms for therapeutic development.

Published

2019

35. Assessing the strength of evidence for genes implicated in fatty acid oxidation disorders using the ClinGen clinical validity framework.

Author

McGlaughon JL, Pasquali M, Wallace K, Ross J, Senol-Cosar O, Shen W, Weaver MA, Feigenbaum A, Lyon E, Enns GM, Mao R, and Baudet HG

Subjects

Genetic Predisposition to Disease, Humans, Infant, Newborn, Neonatal Screening, Oxidation-Reduction, Reproducibility of Results, Fatty Acids metabolism, Genetic Testing, Lipid Metabolism, Inborn Errors diagnosis, Lipid Metabolism, Inborn Errors genetics

Abstract

Newborn screening is an incredibly useful tool for the early identification of many metabolic disorders, including fatty acid oxidation (FAO) disorders. In many cases, molecular tests are necessary to reach a final diagnosis, highlighting the need for a thorough evaluation of genes implicated in FAO disorders. Using the ClinGen (Clinical Genome Resource) clinical validity framework, thirty genes were analyzed for the strength of evidence supporting their association with FAO disorders. Evidence was gathered from the literature by biocurators and presented to disease experts for review in order to assign a clinical validity classification of Definitive, Strong, Moderate, Limited, Disputed, Refuted, or No Reported Evidence. Of the gene-disease relationships evaluated, 22/30 were classified as Definitive, three as Moderate, one as Limited, three as No Reported Evidence and one as Disputed. Gene-disease relationships with a Limited, Disputed, and No Reported Evidence were found on two, six, and up to four panels out of 30 FAO disorder-specific panels, respectively, in the National Institute of Health Genetic Testing Registry, while over 70% of the genes on panels are definitively associated with an FAO disorder. These results highlight the need to systematically assess the clinical relevance of genes implicated in fatty acid oxidation disorders in order to improve the interpretation of genetic testing results and diagnosis of patients with these disorders., (Copyright © 2019. Published by Elsevier Inc.)

Published

2019

36. Perspectives on urea cycle disorder management: Results of a clinician survey.

Author

Enns GM, Porter MH, Francis-Sedlak M, Burdett A, and Vockley J

Subjects

Humans, Hyperammonemia diagnosis, Longitudinal Studies, Quality of Life, Urea metabolism, Urea Cycle Disorders, Inborn diagnosis, Disease Management, Physicians, Surveys and Questionnaires, Urea Cycle Disorders, Inborn drug therapy

Abstract

Background/aims: Urea cycle disorders (UCDs) are rare inborn errors of urea synthesis. US and European consensus statements on the diagnosis and treatment of UCDs were last published in 2001 and 2019, respectively. Recommendations are based primarily on case reports and expert opinion and there is limited agreement or consistency related to long-term management approaches. A clinician survey was conducted to assess current real-world practices and perspectives on challenges and unmet needs., Methods: A 14-item multiple-choice survey was administered to physicians in 2017. Clinicians who reported actively managing at least 1 patient with UCD were eligible to participate. Descriptive statistics were calculated for each survey item (frequencies for categorical variables; means, standard deviations, medians, and ranges for continuous variables)., Results: Sixty-six US clinicians completed the survey (65 geneticists; 1 pediatric neurologist). Over 90% of responders agreed or strongly agreed that even modest elevations in ammonia could cause physiological and functional brain damage; >80% of respondents agreed that asymptomatic UCD patients are at risk of brain damage over time due to mild/subclinical elevations in ammonia. Eighty-six percent of clinicians agreed or strongly agreed with recommending genetic testing for female relatives when a patient is diagnosed with ornithine transcarbamylase deficiency. Ninety-four percent of respondents agreed that patients have better disease control when they are more adherent to their UCD therapy. Nearly 90% indicated that clinicians and patients would benefit from updated UCD management guidance. More than half (53%) of respondents rated the symptoms of UCDs as extremely or very burdensome to the everyday lives of patients and their families; only 8% rated UCD symptoms as slightly or not at all burdensome. The majority of clinicians agreed (48%) or strongly agreed (32%) that caring for a child or family member with a UCD has a negative impact on the quality of life and/or health of family members/guardians (e.g. stress, relationships, ability to work)., Conclusions: This self-reported survey suggests a need for updated and expanded clinical guidance on the long-term treatment and management of UCD patients., (Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2019

37. Case series of sebelipase alfa hypersensitivity reactions and successful sebelipase alfa rapid desensitization.

Author

Huffaker MF, Liu AY, Enns GM, Vijay S, Amor AJ, and Adkinson NF Jr

Abstract

Allergic immune-mediated hypersensitivity reactions are known potential complications of enzyme replacement therapy. Sebelipase alfa, recombinant lysosomal acid lipase (LAL), is a potentially life-altering treatment for patients with LAL deficiency. There is very little information on the diagnosis and management of immediate hypersensitivity reactions to this drug. Here we present three unique cases of hypersensitivity reactions to sebelipase alfa, spanning a broad age spectrum from infancy to adulthood, each managed with successful rapid desensitization., Competing Interests: M.F.H., A.Y.L., and A.J.A. declare that they have no conflict of interest. G.M.E. received funding for the conduct of clinical studies from Alexion Pharmaceuticals, Inc. S.V. has been a consultant for Alexion Pharmaceuticals, Inc., received honoraria and travel grants from Alexion Pharmaceuticals, Inc. N.F.A. has been a consultant for Alexion Pharmaceuticals, Inc.

Published

2019

38. Combining newborn metabolic and DNA analysis for second-tier testing of methylmalonic acidemia.

Author

Peng G, Shen P, Gandotra N, Le A, Fung E, Jelliffe-Pawlowski L, Davis RW, Enns GM, Zhao H, Cowan TM, and Scharfe C

Subjects

Amino Acid Metabolism, Inborn Errors genetics, Amino Acid Metabolism, Inborn Errors pathology, Dried Blood Spot Testing, Female, Humans, Infant, Newborn, Machine Learning, Male, Metabolism, Inborn Errors genetics, Metabolism, Inborn Errors pathology, Amino Acid Metabolism, Inborn Errors blood, Genetic Variation, Metabolism, Inborn Errors blood, Neonatal Screening

Abstract

Purpose: Improved second-tier tools are needed to reduce false-positive outcomes in newborn screening (NBS) for inborn metabolic disorders on the Recommended Universal Screening Panel (RUSP)., Methods: We designed an assay for multiplex sequencing of 72 metabolic genes (RUSPseq) from newborn dried blood spots. Analytical and clinical performance was evaluated in 60 screen-positive newborns for methylmalonic acidemia (MMA) reported by the California Department of Public Health NBS program. Additionally, we trained a Random Forest machine learning classifier on NBS data to improve prediction of true and false-positive MMA cases., Results: Of 28 MMA patients sequenced, we found two pathogenic or likely pathogenic (P/LP) variants in a MMA-related gene in 24 patients, and one pathogenic variant and a variant of unknown significance (VUS) in 1 patient. No such variant combinations were detected in MMA false positives and healthy controls. Random Forest-based analysis of the entire NBS metabolic profile correctly identified the MMA patients and reduced MMA false-positive cases by 51%. MMA screen-positive newborns were more likely of Hispanic ethnicity., Conclusion: Our two-pronged approach reduced false positives by half and provided a reportable molecular finding for 89% of MMA patients. Challenges remain in newborn metabolic screening and DNA variant interpretation in diverse multiethnic populations.

Published

2019

39. Targeting ferroptosis: A novel therapeutic strategy for the treatment of mitochondrial disease-related epilepsy.

Author

Kahn-Kirby AH, Amagata A, Maeder CI, Mei JJ, Sideris S, Kosaka Y, Hinman A, Malone SA, Bruegger JJ, Wang L, Kim V, Shrader WD, Hoff KG, Latham JC, Ashley EA, Wheeler MT, Bertini E, Carrozzo R, Martinelli D, Dionisi-Vici C, Chapman KA, Enns GM, Gahl W, Wolfe L, Saneto RP, Johnson SC, Trimmer JK, Klein MB, and Holst CR

Subjects

Arachidonate 15-Lipoxygenase metabolism, Cell Line, Epilepsy metabolism, Epilepsy pathology, Humans, Hydroxyeicosatetraenoic Acids metabolism, Mitochondrial Diseases metabolism, Mitochondrial Diseases pathology, Phospholipid Hydroperoxide Glutathione Peroxidase metabolism, Ubiquinone pharmacology, Carbolines pharmacology, Epilepsy drug therapy, Ferroptosis drug effects, Mitochondrial Diseases drug therapy, Phospholipid Hydroperoxide Glutathione Peroxidase antagonists & inhibitors, Ubiquinone analogs & derivatives

Abstract

Background: Mitochondrial disease is a family of genetic disorders characterized by defects in the generation and regulation of energy. Epilepsy is a common symptom of mitochondrial disease, and in the vast majority of cases, refractory to commonly used antiepileptic drugs. Ferroptosis is a recently-described form of iron- and lipid-dependent regulated cell death associated with glutathione depletion and production of lipid peroxides by lipoxygenase enzymes. Activation of the ferroptosis pathway has been implicated in a growing number of disorders, including epilepsy. Given that ferroptosis is regulated by balancing the activities of glutathione peroxidase-4 (GPX4) and 15-lipoxygenase (15-LO), targeting these enzymes may provide a rational therapeutic strategy to modulate seizure. The clinical-stage therapeutic vatiquinone (EPI-743, α-tocotrienol quinone) was reported to reduce seizure frequency and associated morbidity in children with the mitochondrial disorder pontocerebellar hypoplasia type 6. We sought to elucidate the molecular mechanism of EPI-743 and explore the potential of targeting 15-LO to treat additional mitochondrial disease-associated epilepsies., Methods: Primary fibroblasts and B-lymphocytes derived from patients with mitochondrial disease-associated epilepsy were cultured under standardized conditions. Ferroptosis was induced by treatment with the irreversible GPX4 inhibitor RSL3 or a combination of pharmacological glutathione depletion and excess iron. EPI-743 was co-administered and endpoints, including cell viability and 15-LO-dependent lipid oxidation, were measured., Results: EPI-743 potently prevented ferroptosis in patient cells representing five distinct pediatric disease syndromes with associated epilepsy. Cytoprotection was preceded by a dose-dependent decrease in general lipid oxidation and the specific 15-LO product 15-hydroxyeicosatetraenoic acid (15-HETE)., Conclusions: These findings support the continued clinical evaluation of EPI-743 as a therapeutic agent for PCH6 and other mitochondrial diseases with associated epilepsy., Competing Interests: The authors have read the journal’s policy and the authors of this manuscript have the following competing interests: The following authors declare financial competing interests as paid current or former employees and/or equity holders of BioElectron Technology Corporation, Inc.: AA, JJB, AH, KGH, CRH, AHKK, VK, MBK, YK, JCL, CIM, SAM, JJM, WDS, SS, JKT, LWang. EPI-743 is a commercial product in development by BioElectron Technology Corporation, Inc., from which employees may benefit. The following authors declare patent applications (pending or actual) belonging to BioElectron Technology Corporation, from which they may benefit: JJB, AH, CRH, AHKK, JCL, SAM, WDS, JKT. The following authors declare grant support from BioElectron Technology Corporation pertaining to the work under consideration forpublication: GME, CD-V, DM. WG declares a cooperative research agreement between NHGRI and BioElectron pertaining to the scope of the work under consideration, as well as to activities outside the submitted work. RPS is a site principal investigator for two studies sponsored by BioElectron Technology Corporation. GME is a site principal investigator for an emergency protocol sponsored by BioElectron Technology Corporation. Outside the scope of the submitted work, EAA declares he is a Co-Founder of Personalis Inc., and DeepCell, Inc. CD-V declares grant support from Actelion and Sanofi Genzyme, as well as personal fees from Actelion, CureVac, Moderna Therapeutics, Logic- Biotherapeutics, Nutricia, Orphan Europe, Medifood, Promethera, Sanofi Genzyme, and SOBI. GME declares grant support and serving as site principal investigator for a clinical trial sponsored by Stealth Therapeutics. DM declares personal fees from SOBI. Thefollowing authors declared no competing interests: EB, RC, KAC, SCJ, MTW, LWolfe. This does not alter our adherence to PLOS ONE policies on sharing data and materials.

Published

2019

40. Elevated methylmalonic acidemia (MMA) screening markers in Hispanic and preterm newborns.

Author

Peng G, de Fontnouvelle CA, Enns GM, Cowan TM, Zhao H, and Scharfe C

Subjects

Black or African American statistics & numerical data, Biomarkers blood, Birth Weight, California epidemiology, False Positive Reactions, Female, Gestational Age, Humans, Infant, Newborn, Male, Methylmalonic Acid blood, Neonatal Screening, Public Health, Amino Acid Metabolism, Inborn Errors diagnosis, Amino Acid Metabolism, Inborn Errors ethnology, Hispanic or Latino statistics & numerical data, Premature Birth ethnology

Abstract

Analysis of California newborn screening (NBS) data revealed a high prevalence of Hispanic infants testing positive for methylmalonic acidemia (MMA), a trend seen for both true- and false-positive cases. Here we show that Hispanic infants have significantly higher levels of MMA screening markers than non-Hispanics. Preterm birth and increased birth weight were found to be associated with elevated MMA marker levels but could not entirely explain these differences. While the preterm birth rate was higher in Blacks than Hispanics, Black infants had on average the lowest MMA marker levels. Preterm birth was associated with lower birth weight and increased MMA marker levels suggesting that gestational age is the stronger predictive covariate compared to birth weight. These findings could help explain why MMA false-positive results are more likely in Hispanic than in Black infants, which could inform screening and diagnostic procedures for MMA and potentially other disorders in newborns., (Copyright © 2018 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2019

41. Conducting an investigator-initiated randomized double-blinded intervention trial in acute decompensation of inborn errors of metabolism: Lessons from the N-Carbamylglutamate Consortium.

Author

Ah Mew N, Cnaan A, McCarter R, Choi H, Glass P, Rice K, Scavo L, Gillespie CW, Diaz GA, Berry GT, Wong D, Konczal L, McCandless SE, Coughlin Ii CR, Weisfeld-Adams JD, Ficicioglu C, Yudkoff M, Enns GM, Lichter-Konecki U, Gallagher R, and Tuchman M

Abstract

Organic acidemias and urea cycle disorders are ultra-rare inborn errors of metabolism characterized by episodic acute decompensation, often associated with hyperammonemia, resulting in brain edema and encephalopathy. Retrospective reports and translational studies suggest that N-carbamylglutamate (NCG) may be effective in reducing ammonia levels during acute decompensation in two organic acidemias, propionic and methylmalonic acidemia (PA and MMA), and in two urea cycle disorders, carbamylphosphate synthetase 1 and ornithine transcarbamylase deficiency (CPSD and OTCD). We established the 9-site N-carbamylglutamate Consortium (NCGC) in order to conduct two randomized double-blind, placebo-controlled trials of NCG in acute hyperammonemia of PA, MMA, CPSD and OTCD. Conducting clinical trials is challenging in any disease, but poses unique barriers and risks in the ultra-rare disorders. As the number of clinical trials in orphan diseases increases, evaluating the successes and opportunities for improvement in such trials is essential. We summarize herein the design, methods, experiences, challenges and lessons from the NCGC-conducted trials.

Published

2018

42. FGF21 underlies a hormetic response to metabolic stress in methylmalonic acidemia.

Author

Manoli I, Sysol JR, Epping MW, Li L, Wang C, Sloan JL, Pass A, Gagné J, Ktena YP, Li L, Trivedi NS, Ouattara B, Zerfas PM, Hoffmann V, Abu-Asab M, Tsokos MG, Kleiner DE, Garone C, Cusmano-Ozog K, Enns GM, Vernon HJ, Andersson HC, Grunewald S, Elkahloun AG, Girard CL, Schnermann J, DiMauro S, Andres-Mateos E, Vandenberghe LH, Chandler RJ, and Venditti CP

Subjects

Amino Acid Metabolism, Inborn Errors genetics, Amino Acid Metabolism, Inborn Errors pathology, Animals, Biomarkers blood, Disease Models, Animal, Female, Fibroblast Growth Factors blood, Genetic Therapy, Humans, Kidney Diseases metabolism, Liver metabolism, Liver pathology, Liver Transplantation, Male, Methylmalonyl-CoA Mutase genetics, Mice, Mice, Knockout, Mice, Transgenic, Mitochondria metabolism, Mitochondria pathology, Phenotype, Transcriptome, Amino Acid Metabolism, Inborn Errors metabolism, Fibroblast Growth Factors metabolism, Hormesis, Methylmalonyl-CoA Mutase metabolism, Stress, Physiological

Abstract

Methylmalonic acidemia (MMA), an organic acidemia characterized by metabolic instability and multiorgan complications, is most frequently caused by mutations in methylmalonyl-CoA mutase (MUT). To define the metabolic adaptations in MMA in acute and chronic settings, we studied a mouse model generated by transgenic expression of Mut in the muscle. Mut-/-;TgINS-MCK-Mut mice accurately replicate the hepatorenal mitochondriopathy and growth failure seen in severely affected patients and were used to characterize the response to fasting. The hepatic transcriptome in MMA mice was characterized by the chronic activation of stress-related pathways and an aberrant fasting response when compared with controls. A key metabolic regulator, Fgf21, emerged as a significantly dysregulated transcript in mice and was subsequently studied in a large patient cohort. The concentration of plasma FGF21 in MMA patients correlated with disease subtype, growth indices, and markers of mitochondrial dysfunction but was not affected by renal disease. Restoration of liver Mut activity, by transgenesis and liver-directed gene therapy in mice or liver transplantation in patients, drastically reduced plasma FGF21 and was associated with improved outcomes. Our studies identify mitocellular hormesis as a hepatic adaptation to metabolic stress in MMA and define FGF21 as a highly predictive disease biomarker.

Published

2018

43. Unique aspects of sequence variant interpretation for inborn errors of metabolism (IEM): The ClinGen IEM Working Group and the Phenylalanine Hydroxylase Gene.

Author

Zastrow DB, Baudet H, Shen W, Thomas A, Si Y, Weaver MA, Lager AM, Liu J, Mangels R, Dwight SS, Wright MW, Dobrowolski SF, Eilbeck K, Enns GM, Feigenbaum A, Lichter-Konecki U, Lyon E, Pasquali M, Watson M, Blau N, Steiner RD, Craigen WJ, and Mao R

Subjects

Databases, Genetic, Gene Frequency genetics, Genetic Testing, Genetic Variation genetics, Humans, Genome, Human genetics, Metabolism, Inborn Errors genetics, Phenylalanine Hydroxylase genetics

Abstract

The ClinGen Inborn Errors of Metabolism Working Group was tasked with creating a comprehensive, standardized knowledge base of genes and variants for metabolic diseases. Phenylalanine hydroxylase (PAH) deficiency was chosen to pilot development of the Working Group's standards and guidelines. A PAH variant curation expert panel (VCEP) was created to facilitate this process. Following ACMG-AMP variant interpretation guidelines, we present the development of these standards in the context of PAH variant curation and interpretation. Existing ACMG-AMP rules were adjusted based on disease (6) or strength (5) or both (2). Disease adjustments include allele frequency thresholds, functional assay thresholds, and phenotype-specific guidelines. Our validation of PAH-specific variant interpretation guidelines is presented using 85 variants. The PAH VCEP interpretations were concordant with existing interpretations in ClinVar for 69 variants (81%). Development of biocurator tools and standards are also described. Using the PAH-specific ACMG-AMP guidelines, 714 PAH variants have been curated and will be submitted to ClinVar. We also discuss strategies and challenges in applying ACMG-AMP guidelines to autosomal recessive metabolic disease, and the curation of variants in these genes., (© 2018 Wiley Periodicals, Inc.)

Published

2018

44. Current clinical evidence does not support a link between TBL1XR1 and Rett syndrome: Description of one patient with Rett features and a novel mutation in TBL1XR1, and a review of TBL1XR1 phenotypes.

Author

Zaghlula M, Glaze DG, Enns GM, Potocki L, Schwabe AL, and Suter B

Subjects

Child, Female, Humans, Phenotype, Mutation, Nuclear Proteins genetics, Receptors, Cytoplasmic and Nuclear genetics, Repressor Proteins genetics, Rett Syndrome genetics, Rett Syndrome pathology

Published

2018

45. A New Approach to Rare Diseases of Children: The Undiagnosed Diseases Network.

Author

Reuter CM, Brimble E, DeFilippo C, Dries AM, Enns GM, Ashley EA, Bernstein JA, Fisher PG, and Wheeler MT

Subjects

Child, Preschool, Forkhead Transcription Factors genetics, Genotype, Government Programs methods, Humans, Male, Mutation, NAV1.5 Voltage-Gated Sodium Channel genetics, National Institutes of Health (U.S.) organization & administration, Nerve Tissue Proteins genetics, Phenotype, Rare Diseases genetics, United States, Genetic Testing methods, Rare Diseases diagnosis

Published

2018

46. Biallelic Mutations in ATP5F1D, which Encodes a Subunit of ATP Synthase, Cause a Metabolic Disorder.

Author

Oláhová M, Yoon WH, Thompson K, Jangam S, Fernandez L, Davidson JM, Kyle JE, Grove ME, Fisk DG, Kohler JN, Holmes M, Dries AM, Huang Y, Zhao C, Contrepois K, Zappala Z, Frésard L, Waggott D, Zink EM, Kim YM, Heyman HM, Stratton KG, Webb-Robertson BM, Snyder M, Merker JD, Montgomery SB, Fisher PG, Feichtinger RG, Mayr JA, Hall J, Barbosa IA, Simpson MA, Deshpande C, Waters KM, Koeller DM, Metz TO, Morris AA, Schelley S, Cowan T, Friederich MW, McFarland R, Van Hove JLK, Enns GM, Yamamoto S, Ashley EA, Wangler MF, Taylor RW, Bellen HJ, Bernstein JA, and Wheeler MT

Subjects

Amino Acid Sequence, Base Sequence, Child, Child, Preschool, Female, Humans, Infant, Infant, Newborn, Loss of Function Mutation genetics, Male, Mitochondria metabolism, Mitochondria ultrastructure, Mitochondrial Proton-Translocating ATPases chemistry, Protein Subunits chemistry, Alleles, Metabolic Diseases genetics, Mitochondrial Proton-Translocating ATPases genetics, Mutation genetics, Protein Subunits genetics

Abstract

ATP synthase, H + transporting, mitochondrial F1 complex, δ subunit (ATP5F1D; formerly ATP5D) is a subunit of mitochondrial ATP synthase and plays an important role in coupling proton translocation and ATP production. Here, we describe two individuals, each with homozygous missense variants in ATP5F1D, who presented with episodic lethargy, metabolic acidosis, 3-methylglutaconic aciduria, and hyperammonemia. Subject 1, homozygous for c.245C>T (p.Pro82Leu), presented with recurrent metabolic decompensation starting in the neonatal period, and subject 2, homozygous for c.317T>G (p.Val106Gly), presented with acute encephalopathy in childhood. Cultured skin fibroblasts from these individuals exhibited impaired assembly of F 1 F O ATP synthase and subsequent reduced complex V activity. Cells from subject 1 also exhibited a significant decrease in mitochondrial cristae. Knockdown of Drosophila ATPsynδ, the ATP5F1D homolog, in developing eyes and brains caused a near complete loss of the fly head, a phenotype that was fully rescued by wild-type human ATP5F1D. In contrast, expression of the ATP5F1D c.245C>T and c.317T>G variants rescued the head-size phenotype but recapitulated the eye and antennae defects seen in other genetic models of mitochondrial oxidative phosphorylation deficiency. Our data establish c.245C>T (p.Pro82Leu) and c.317T>G (p.Val106Gly) in ATP5F1D as pathogenic variants leading to a Mendelian mitochondrial disease featuring episodic metabolic decompensation., (Copyright © 2018 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2018

47. Prenatal treatment of ornithine transcarbamylase deficiency.

Author

Wilnai Y, Blumenfeld YJ, Cusmano K, Hintz SR, Alcorn D, Benitz WE, Berquist WE, Bernstein JA, Castillo RO, Concepcion W, Cowan TM, Cox KL, Lyell DJ, Esquivel CO, Homeyer M, Hudgins L, Hurwitz M, Palma JP, Schelley S, Akula VP, Summar ML, and Enns GM

Subjects

Ammonia blood, Ammonia toxicity, Drug Combinations, Female, Glutamine blood, Humans, Hyperammonemia blood, Hyperammonemia diagnosis, Hyperammonemia genetics, Infant, Newborn, Male, Mutation, Ornithine Carbamoyltransferase genetics, Ornithine Carbamoyltransferase Deficiency Disease blood, Ornithine Carbamoyltransferase Deficiency Disease diagnosis, Ornithine Carbamoyltransferase Deficiency Disease genetics, Pregnancy, Prenatal Diagnosis, Treatment Outcome, Urea metabolism, Hyperammonemia drug therapy, Ornithine Carbamoyltransferase Deficiency Disease drug therapy, Phenylacetates therapeutic use, Prenatal Care methods, Sodium Benzoate therapeutic use

Abstract

Purpose of Study: Patients with neonatal urea cycle defects (UCDs) typically experience severe hyperammonemia during the first days of life, which results in serious neurological injury or death. Long-term prognosis despite optimal pharmacological and dietary therapy is still poor. The combination of intravenous sodium phenylacetate and sodium benzoate (Ammonul®) can eliminate nitrogen waste independent of the urea cycle. We report attempts to improve outcomes for males with severe ornithine transcarbamylase deficiency (OTCD), a severe X-linked condition, via prenatal intravenous administration of Ammonul and arginine to heterozygous carrier females of OTCD during labor., Methods Used: Two heterozygote OTCD mothers carrying male fetuses with a prenatal diagnosis of OTCD received intravenous Ammonul, arginine and dextrose-containing fluids shortly before birth. Maintenance Ammonul and arginine infusions and high-caloric enteral nutrition were started immediately after birth. Ammonul metabolites were measured in umbilical cord blood and the blood of the newborn immediately after delivery. Serial ammonia and biochemical analyses were performed following delivery., Summary of Results: Therapeutic concentrations of Ammonul metabolites were detected in umbilical cord and neonatal blood samples. Plasma ammonia and glutamine levels in the postnatal period were within the normal range. Peak ammonia levels in the first 24-48h were 53mcmol/l and 62mcmol/l respectively. The boys did not experience neurological sequelae secondary to hyperammonemia and received liver transplantation at ages 3months and 5months. The patients show normal development at ages 7 and 3years., Conclusion: Prenatal treatment of mothers who harbor severe OTCD mutations and carry affected male fetuses with intravenous Ammonul and arginine, followed by immediate institution of maintenance infusions after delivery, results in therapeutic levels of benzoate and phenylacetate in the newborn at delivery and, in conjunction with high-caloric enteral nutrition, prevents acute hyperammonemia and neurological decompensation. Following initial medical management, early liver transplantation may improve developmental outcome., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

48. Triheptanoin: A Rescue Therapy for Cardiogenic Shock in Carnitine-acylcarnitine Translocase Deficiency.

Author

Mahapatra S, Ananth A, Baugh N, Damian M, and Enns GM

Abstract

Carnitine-acylcarnitine translocase (CACT) deficiency is a rare long-chain fatty acid oxidation disorder (LC-FAOD) with high mortality due to cardiomyopathy or lethal arrhythmia. Triheptanoin (UX007), an investigational drug composed of synthetic medium odd-chain triglycerides, is a novel therapy in development for LC-FAOD patients. However, cases of its safe and efficacious use to reverse severe heart failure in CACT deficiency are limited. Here, we present a detailed report of an infant with CACT deficiency admitted in metabolic crisis that progressed into severe cardiogenic shock who was successfully treated by triheptanoin. The child was managed, thereafter, on triheptanoin until her death at 3 years of age from a cardiopulmonary arrest in the setting of acute respiratory illness superimposed on chronic hypercarbic respiratory failure.

Published

2018

49. Correction of hyperleucinemia in MSUD patients on leucine-free dietary therapy.

Author

Scott AI, Cusmano-Ozog K, Enns GM, and Cowan TM

Subjects

Acidosis complications, Adolescent, Child, Child, Preschool, Female, Humans, Infant, Infant, Newborn, Male, Maple Syrup Urine Disease blood, Retrospective Studies, Treatment Outcome, Diet, Leucine blood, Leucine metabolism, Maple Syrup Urine Disease diet therapy

Abstract

Purpose: Maple Syrup Urine Disease (MSUD) is a rare disorder of branched-chain amino acid catabolism associated with encephalopathy from accumulation of leucine. Leucine is closely monitored during normal growth and particularly during acute illness. As most hospitals do not have access to rapid plasma amino acid quantification, the initial management is often empirical. A model describing the reduction of plasma leucine in hyperleucinemic patients on leucine-free formula would help to guide management and optimize testing frequency., Methods: We retrospectively reviewed charts from 15 MSUD patients comprising 29 episodes of hyperleucinemia that were managed with leucine-free formula. Episodes were categorized by clinical presentation., Results: Upon leucine restriction, plasma leucine concentrations fell exponentially at a rate proportional to approximately 50% of the starting value over each 24-hour period. Recovery appears to be sensitive to clinical status and triggering event of the hyperleucinemic episode. Patients with upper respiratory infections generally recovered slowly, while cases of dietary non-adherence resolved more quickly., Conclusion: This general model may help anticipate leucine levels during clinical management of MSUD patients when using nutritional support and leucine-free formula. The response of individual patients may vary depending on clinical status and triggering factors., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

50. Response to Newman et al.

Author

Parikh S, Goldstein A, Karaa A, Koenig MK, Anselm I, Brunel-Guitton C, Christodoulou J, Cohen BH, Dimmock D, Enns GM, Falk MJ, Feigenbaum A, Frye RE, Ganesh J, Griesemer D, Haas R, Horvath R, Korson M, Kruer MC, Mancuso M, McCormack S, Josee Raboisson M, Reimschisel T, Salvarinova R, Saneto RP, Scaglia F, Shoffner J, Stacpoole PW, Sue CM, Tarnopolsky M, Van Karnebeek C, Wolfe LA, Zolkipli Cunningham Z, Rahman S, and Chinnery PF

Published

2017