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3. Genotypic and phenotypic spectrum of infantile liver failure due to pathogenic TRMU variants.

Author

Vogel, G.F., Mozer-Glassberg, Y., Landau, Y.E., Schlieben, L.D., Prokisch, H., Feichtinger, R.G., Mayr, J.A., Brennenstuhl, H., Schröter, J., Pechlaner, A., Alkuraya, F.S., Baker, J.J., Barcia, G., Baric, I., Braverman, N., Burnyte, B., Christodoulou, J., Ciara, E., Coman, D., Das, A.M., Darin, N., Marina, A. Della, Distelmaier, F., Eklund, E.A., Ersoy, M., Fang, W., Gaignard, P., Ganetzky, R.D., Gonzales, E., Howard, C., Hughes, J., Konstantopoulou, V., Kose, M., Kerr, M., Khan, A., Lenz, D., McFarland, R., Margolis, M.G., Morrison, K., Müller, T., Murayama, K., Nicastro, E., Pennisi, A., Peters, Heidi, Piekutowska-Abramczuk, D., Rötig, A., Santer, R., Scaglia, F., Schiff, M., Shagrani, M., Sharrard, M., Soler-Alfonso, C., Staufner, C., Storey, I., Stormon, M., Taylor, R.W., Thorburn, D.R., Teles, E.L., Wang, J.S., Weghuber, D., Wortmann, S.B., Vogel, G.F., Mozer-Glassberg, Y., Landau, Y.E., Schlieben, L.D., Prokisch, H., Feichtinger, R.G., Mayr, J.A., Brennenstuhl, H., Schröter, J., Pechlaner, A., Alkuraya, F.S., Baker, J.J., Barcia, G., Baric, I., Braverman, N., Burnyte, B., Christodoulou, J., Ciara, E., Coman, D., Das, A.M., Darin, N., Marina, A. Della, Distelmaier, F., Eklund, E.A., Ersoy, M., Fang, W., Gaignard, P., Ganetzky, R.D., Gonzales, E., Howard, C., Hughes, J., Konstantopoulou, V., Kose, M., Kerr, M., Khan, A., Lenz, D., McFarland, R., Margolis, M.G., Morrison, K., Müller, T., Murayama, K., Nicastro, E., Pennisi, A., Peters, Heidi, Piekutowska-Abramczuk, D., Rötig, A., Santer, R., Scaglia, F., Schiff, M., Shagrani, M., Sharrard, M., Soler-Alfonso, C., Staufner, C., Storey, I., Stormon, M., Taylor, R.W., Thorburn, D.R., Teles, E.L., Wang, J.S., Weghuber, D., and Wortmann, S.B.

Abstract

01 juni 2023, Item does not contain fulltext, PURPOSE: This study aimed to define the genotypic and phenotypic spectrum of reversible acute liver failure (ALF) of infancy resulting from biallelic pathogenic TRMU variants and determine the role of cysteine supplementation in its treatment. METHODS: Individuals with biallelic (likely) pathogenic variants in TRMU were studied within an international retrospective collection of de-identified patient data. RESULTS: In 62 individuals, including 30 previously unreported cases, we described 47 (likely) pathogenic TRMU variants, of which 17 were novel, and 1 intragenic deletion. Of these 62 individuals, 42 were alive at a median age of 6.8 (0.6-22) years after a median follow-up of 3.6 (0.1-22) years. The most frequent finding, occurring in all but 2 individuals, was liver involvement. ALF occurred only in the first year of life and was reported in 43 of 62 individuals; 11 of whom received liver transplantation. Loss-of-function TRMU variants were associated with poor survival. Supplementation with at least 1 cysteine source, typically N-acetylcysteine, improved survival significantly. Neurodevelopmental delay was observed in 11 individuals and persisted in 4 of the survivors, but we were unable to determine whether this was a primary or a secondary consequence of TRMU deficiency. CONCLUSION: In most patients, TRMU-associated ALF was a transient, reversible disease and cysteine supplementation improved survival.

Published
2023

4. Phenotypic spectrum and clinical course of single large-scale mitochondrial DNA deletion disease in the paediatric population:a multicentre study

Author

Björkman, K. (Kristoffer), Vissing, J. (John), Østergaard, E. (Elsebet), Bindoff, L. A. (Laurence A.), de Coo, I. F. (Irenaeus F. M.), Engvall, M. (Martin), Hikmat, O. (Omar), Isohanni, P. (Pirjo), Kollberg, G. (Gittan), Lindberg, C. (Christopher), Majamaa, K. (Kari), Naess, K. (Karin), Uusimaa, J. (Johanna), Tulinius, M. (Mar), Darin, N. (Niklas), Björkman, K. (Kristoffer), Vissing, J. (John), Østergaard, E. (Elsebet), Bindoff, L. A. (Laurence A.), de Coo, I. F. (Irenaeus F. M.), Engvall, M. (Martin), Hikmat, O. (Omar), Isohanni, P. (Pirjo), Kollberg, G. (Gittan), Lindberg, C. (Christopher), Majamaa, K. (Kari), Naess, K. (Karin), Uusimaa, J. (Johanna), Tulinius, M. (Mar), and Darin, N. (Niklas)

Abstract

Background: Large-scale mitochondrial DNA deletions (LMD) are a common genetic cause of mitochondrial disease and give rise to a wide range of clinical features. Lack of longitudinal data means the natural history remains unclear. This study was undertaken to describe the clinical spectrum in a large cohort of patients with paediatric disease onset. Methods: A retrospective multicentre study was performed in patients with clinical onset <16 years of age, diagnosed and followed in seven European mitochondrial disease centres. Results: A total of 80 patients were included. The average age at disease onset and at last examination was 10 and 31 years, respectively. The median time from disease onset to death was 11.5 years. Pearson syndrome was present in 21%, Kearns-Sayre syndrome spectrum disorder in 50% and progressive external ophthalmoplegia in 29% of patients. Haematological abnormalities were the hallmark of the disease in preschool children, while the most common presentations in older patients were ptosis and external ophthalmoplegia. Skeletal muscle involvement was found in 65% and exercise intolerance in 25% of the patients. Central nervous system involvement was frequent, with variable presence of ataxia (40%), cognitive involvement (36%) and stroke-like episodes (9%). Other common features were pigmentary retinopathy (46%), short stature (42%), hearing impairment (39%), cardiac disease (39%), diabetes mellitus (25%) and renal disease (19%). Conclusion: Our study provides new insights into the phenotypic spectrum of childhood-onset, LMD-associated syndromes. We found a wider spectrum of more prevalent multisystem involvement compared with previous studies, most likely related to a longer time of follow-up.

Published
2023

8. Renal phenotype in mitochondrial diseases:a multicenter study

Author

Parasyri, M. (Maria), Brandström, P. (Per), Uusimaa, J. (Johanna), Ostergaard, E. (Elsebet), Hikmat, O. (Omar), Isohanni, P. (Pirjo), Naess, K. (Karin), de Coo, I. F. (I. F. M.), Osorio, A. N. (Andrés Nascimento), Nuutinen, M. (Matti), Lindberg, C. (Christopher), Bindoff, L. A. (Laurence A.), Tulinius, M. (Már), Darin, N. (Niklas), Sofou, K. (Kalliopi), Parasyri, M. (Maria), Brandström, P. (Per), Uusimaa, J. (Johanna), Ostergaard, E. (Elsebet), Hikmat, O. (Omar), Isohanni, P. (Pirjo), Naess, K. (Karin), de Coo, I. F. (I. F. M.), Osorio, A. N. (Andrés Nascimento), Nuutinen, M. (Matti), Lindberg, C. (Christopher), Bindoff, L. A. (Laurence A.), Tulinius, M. (Már), Darin, N. (Niklas), and Sofou, K. (Kalliopi)

Abstract

Aims: This study aimed to investigate associations between renal and extrarenal manifestations of mitochondrial diseases and their natural history as well as predictors of renal disease severity and overall disease outcome. The secondary aim was to generate a protocol of presymptomatic assessment and monitoring of renal function in patients with a defined mitochondrial disease. Methods: A multicenter, retrospective cohort study was performed by the Mitochondrial Clinical and Research Network (MCRN). Patients of any age with renal manifestations associated with a genetically verified mitochondrial disease were included from 8 expert European centers specializing in mitochondrial diseases: Gothenburg, Oulu, Copenhagen, Bergen, Helsinki, Stockholm, Rotterdam, and Barcelona. Results: Of the 36 patients included, two-thirds had mitochondrial DNA-associated disease. Renal manifestations were the first sign of mitochondrial disease in 19%, and renal involvement was first identified by laboratory tests in 57% of patients. Acute kidney injury occurred in 19% of patients and was the first sign of renal disease in the majority of these. The most common renal manifestation was chronic kidney disease (75% with stage 2 or greater), followed by tubulopathy (44.4%), the latter seen mostly among patients with single large-scale mitochondrial DNA deletions. Acute kidney injury and tubulopathy correlated with worse survival outcome. The most common findings on renal imaging were increased echogenicity and renal dysplasia/hypoplasia. Renal histology revealed focal segmental glomerulosclerosis, nephrocalcinosis, and nephronophthisis. Conclusion: Acute kidney injury is a distinct renal phenotype in patients with mitochondrial disease. Our results highlight the importance to recognize renal disease as a sign of an underlying mitochondrial disease. Acute kidney injury and tubulopathy are 2 distinct indicators of poor survival in patients with mitochondrial diseases.

Published
2022

9. Renal Phenotype in Mitochondrial Diseases : A Multicenter Study

Author

Parasyri, M. (Maria), Brandström, P. (Per), Uusimaa, J. (Johanna), Ostergaard, E. (Elsebet), Hikmat, O. (Omar), Isohanni, P. (Pirjo), Naess, K. (Karin), de Coo, I. F. (I. F. M.), Osorio, A. N. (Andrés Nascimento), Nuutinen, M. (Matti), Lindberg, C. (Christopher), Bindoff, L. A. (Laurence A.), Tulinius, M. (Már), Darin, N. (Niklas), Sofou, K. (Kalliopi), Research Programs Unit, Clinicum, Children's Hospital, Anu Wartiovaara / Principal Investigator, HUS Children and Adolescents, RS: MHeNs - R3 - Neuroscience, and Toxicogenomics

Subjects
KIDNEY, MUTATIONS, CHILDREN, urologic and male genital diseases, Renal manifestations, 3126 Surgery, anesthesiology, intensive care, radiology, Internal medicine, RC31-1245, Mitochondrial disease, Mitochondrial DNA, Research Article, Acute kidney injury
Abstract

Aims: This study aimed to investigate associations between renal and extrarenal manifestations of mitochondrial diseases and their natural history as well as predictors of renal disease severity and overall disease outcome. The secondary aim was to generate a protocol of presymptomatic assessment and monitoring of renal function in patients with a defined mitochondrial disease. Methods: A multicenter, retrospective cohort study was performed by the Mitochondrial Clinical and Research Network (MCRN). Patients of any age with renal manifestations associated with a genetically verified mitochondrial disease were included from 8 expert European centers specializing in mitochondrial diseases: Gothenburg, Oulu, Copenhagen, Bergen, Helsinki, Stockholm, Rotterdam, and Barcelona. Results: Of the 36 patients included, two-thirds had mitochondrial DNA-associated disease. Renal manifestations were the first sign of mitochondrial disease in 19%, and renal involvement was first identified by laboratory tests in 57% of patients. Acute kidney injury occurred in 19% of patients and was the first sign of renal disease in the majority of these. The most common renal manifestation was chronic kidney disease (75% with stage 2 or greater), followed by tubulopathy (44.4%), the latter seen mostly among patients with single large-scale mitochondrial DNA deletions. Acute kidney injury and tubulopathy correlated with worse survival outcome. The most common findings on renal imaging were increased echogenicity and renal dysplasia/hypoplasia. Renal histology revealed focal segmental glomerulosclerosis, nephrocalcinosis, and nephronophthisis. Conclusion: Acute kidney injury is a distinct renal phenotype in patients with mitochondrial disease. Our results highlight the importance to recognize renal disease as a sign of an underlying mitochondrial disease. Acute kidney injury and tubulopathy are 2 distinct indicators of poor survival in patients with mitochondrial diseases. Aims: This study aimed to investigate associations between renal and extrarenal manifestations of mitochondrial diseases and their natural history as well as predictors of renal disease severity and overall disease outcome. The secondary aim was to generate a protocol of presymptomatic assessment and monitoring of renal function in patients with a defined mitochondrial disease. Methods: A multicenter, retrospective cohort study was performed by the Mitochondrial Clinical and Research Network (MCRN). Patients of any age with renal manifestations associated with a genetically verified mitochondrial disease were included from 8 expert European centers specializing in mitochondrial diseases: Gothenburg, Oulu, Copenhagen, Bergen, Helsinki, Stockholm, Rotterdam, and Barcelona. Results: Of the 36 patients included, two-thirds had mitochondrial DNA-associated disease. Renal manifestations were the first sign of mitochondrial disease in 19%, and renal involvement was first identified by laboratory tests in 57% of patients. Acute kidney injury occurred in 19% of patients and was the first sign of renal disease in the majority of these. The most common renal manifestation was chronic kidney disease (75% with stage 2 or greater), followed by tubulopathy (44.4%), the latter seen mostly among patients with single large-scale mitochondrial DNA deletions. Acute kidney injury and tubulopathy correlated with worse survival outcome. The most common findings on renal imaging were increased echogenicity and renal dysplasia/hypoplasia. Renal histology revealed focal segmental glomerulosclerosis, nephrocalcinosis, and nephronophthisis. Conclusion: Acute kidney injury is a distinct renal phenotype in patients with mitochondrial disease. Our results highlight the importance to recognize renal disease as a sign of an underlying mitochondrial disease. Acute kidney injury and tubulopathy are 2 distinct indicators of poor survival in patients with mitochondrial diseases.

Published
2022
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10. Diagnostic value of serum biomarkers FGF21 and GDF15 compared to muscle sample in mitochondrial disease

Author

Keinänen-Kiukaanniemi, S. (Sirkka), Auranen, M. (Mari), Darin, N. (Niklas), Sofou, K. (Kalliopi), Bindoff, L. (Laurence), Hikmat, O. (Omar), Uusimaa, J. (Johanna), Vieira, P. (Päivi), Tulinius, M. (Már), Lönnqvist, T. (Tuula), de Coo, I. F. (Irenaeus F.), Suomalainen, A. (Anu), Isohanni, P. (Pirjo), Keinänen-Kiukaanniemi, S. (Sirkka), Auranen, M. (Mari), Darin, N. (Niklas), Sofou, K. (Kalliopi), Bindoff, L. (Laurence), Hikmat, O. (Omar), Uusimaa, J. (Johanna), Vieira, P. (Päivi), Tulinius, M. (Már), Lönnqvist, T. (Tuula), de Coo, I. F. (Irenaeus F.), Suomalainen, A. (Anu), and Isohanni, P. (Pirjo)

Abstract

The aim of this study was to compare the value of serum biomarkers, fibroblast growth factor 21 (FGF21) and growth differentiation factor 15 (GDF15), with histological analysis of muscle in the diagnosis of mitochondrial disease. We collected 194 serum samples from patients with a suspected or known mitochondrial disease. Biomarkers were analyzed blinded using enzyme-labeled immunosorbent assay. Clinical data were collected using a structured questionnaire. Only 39% of patients with genetically verified mitochondrial disease had mitochondrial pathology in their muscle histology. In contrast, biomarkers were elevated in 62% of patients with genetically verified mitochondrial disease. Those with both biomarkers elevated had a muscle manifesting disorder and a defect affecting mitochondrial DNA expression. If at least one of the biomarkers was induced and the patient had a myopathic disease, a mitochondrial DNA expression disease was the cause with 94% probability. Among patients with biomarker analysis and muscle biopsy taken <12 months apart, a mitochondrial disorder would have been identified in 70% with analysis of FGF21 and GDF15 compared to 50% of patients whom could have been identified with muscle biopsy alone. Muscle findings were nondiagnostic in 72% (children) and 45% (adults). Induction of FGF21 and GDF15 suggest a mitochondrial etiology as an underlying cause of a muscle manifesting disease. Normal biomarker values do not, however, rule out a mitochondrial disorder, especially if the disease does not manifest in muscle. We suggest that FGF21 and GDF15 together should be first-line diagnostic investigations in mitochondrial disease complementing muscle biopsy.

Published
2021

12. De novo variants in CAMTA1 cause a syndrome variably associated with spasticity, ataxia, and intellectual disability

Author

Wijnen, I.G.M., Veenstra-Knol, Hermine E., Vansenne, F., Gerkes, E.H., Koning, T. de, Vos, Y.J., Tijssen, Marina A. J., Sival, D., Darin, N., Vanhoutte, E.K., Oosterloo, M., Pennings, M., Warrenburg, B.P.C. van de, Kamsteeg, E.J., Wijnen, I.G.M., Veenstra-Knol, Hermine E., Vansenne, F., Gerkes, E.H., Koning, T. de, Vos, Y.J., Tijssen, Marina A. J., Sival, D., Darin, N., Vanhoutte, E.K., Oosterloo, M., Pennings, M., Warrenburg, B.P.C. van de, and Kamsteeg, E.J.

Abstract

Contains fulltext : 220425.pdf (Publisher’s version ) (Closed access), Previously, intragenic CAMTA1 copy number variants (CNVs) have been shown to cause non-progressive, congenital ataxia with or without intellectual disability (OMIM#614756). However, ataxia, intellectual disability, and dysmorphic features were all incompletely penetrant, even within families. Here, we describe four patients with de novo nonsense, frameshift or missense CAMTA1 variants. All four patients predominantly manifested features of ataxia and/or spasticity. Borderline intellectual disability and dysmorphic features were both present in one patient only, and other neurological and behavioural symptoms were variably present. Neurodevelopmental delay was found to be mild. Our findings indicate that also nonsense, frameshift and missense variants in CAMTA1 can cause a spastic ataxia syndrome as the main phenotype.

Published
2020

13. The impact of gender, puberty, and pregnancy in patients with POLG disease

Author

Hikmat, O. (Omar), Naess, K. (Karin), Engvall, M. (Martin), Klingenberg, C. (Claus), Rasmussen, M. (Magnhild), Tallaksen, C. M. (Chantal M. E.), Samsonsen, C. (Christian), Brodtkorb, E. (Eylert), Ostergaard, E. (Elsebet), de Coo, R. (Rene), Pias‐Peleteiro, L. (Leticia), Isohanni, P. (Pirjo), Uusimaa, J. (Johanna), Darin, N. (Niklas), Rahman, S. (Shamima), Bindoff, L. A. (Laurence A.), Hikmat, O. (Omar), Naess, K. (Karin), Engvall, M. (Martin), Klingenberg, C. (Claus), Rasmussen, M. (Magnhild), Tallaksen, C. M. (Chantal M. E.), Samsonsen, C. (Christian), Brodtkorb, E. (Eylert), Ostergaard, E. (Elsebet), de Coo, R. (Rene), Pias‐Peleteiro, L. (Leticia), Isohanni, P. (Pirjo), Uusimaa, J. (Johanna), Darin, N. (Niklas), Rahman, S. (Shamima), and Bindoff, L. A. (Laurence A.)

Abstract

Objective: To study the impact of gender, puberty, and pregnancy on the expression of POLG disease, one of the most common mitochondrial diseases known. Methods: Clinical, laboratory, and genetic data were collected retrospectively from 155 patients with genetically confirmed POLG disease recruited from seven European countries. We used the available data to study the impact of gender, puberty, and pregnancy on disease onset and deterioration. Results: We found that disease onset early in life was common in both sexes but there was also a second peak in females around the time of puberty. Further, pregnancy had a negative impact with 10 of 14 women (71%) experiencing disease onset or deterioration during pregnancy. Interpretation: Gender clearly influences the expression of POLG disease. While onset very early in life was common in both males and females, puberty in females appeared associated both with disease onset and increased disease activity. Further, both disease onset and deterioration, including seizure aggravation and status epilepticus, appeared to be associated with pregnancy. Thus, whereas disease activity appears maximal early in life with no subsequent peaks in males, both menarche and pregnancy appear associated with disease onset or worsening in females. This suggests that hormonal changes may be a modulating factor.

Published
2020

14. Simplifying the clinical classification of polymerase gamma (POLG) disease based on age of onset; studies using a cohort of 155 cases

Author

Hikmat, O. (Omar), Naess, K. (Karin), Engvall, M. (Martin), Klingenberg, C. (Claus), Rasmussen, M. (Magnhild), Tallaksen, C. M. (Chantal ME), Brodtkorb, E. (Eylert), Ostergaard, E. (Elsebet), de Coo, I. F. (I. F. M), Pias-Peleteiro, L. (Leticia), Isohanni, P. (Pirjo), Uusimaa, J. (Johanna), Darin, N. (Niklas), Rahman, S. (Shamima), Bindoff, L. A. (Laurence A.), Hikmat, O. (Omar), Naess, K. (Karin), Engvall, M. (Martin), Klingenberg, C. (Claus), Rasmussen, M. (Magnhild), Tallaksen, C. M. (Chantal ME), Brodtkorb, E. (Eylert), Ostergaard, E. (Elsebet), de Coo, I. F. (I. F. M), Pias-Peleteiro, L. (Leticia), Isohanni, P. (Pirjo), Uusimaa, J. (Johanna), Darin, N. (Niklas), Rahman, S. (Shamima), and Bindoff, L. A. (Laurence A.)

Abstract

Summary Background: Variants in POLG are one of the most common causes of inherited mitochondrial disease. Phenotypic classification of POLG disease has evolved haphazardly making it complicated and difficult to implement in everyday clinical practise. The aim of our study was to simplify the classification and facilitate better clinical recognition. Methods: A multinational, retrospective study using data from 155 patients with POLG variants recruited from seven European countries. Results: We describe the spectrum of clinical features associated with POLG variants in the largest known cohort of patients. While clinical features clearly form a continuum, stratifying patients simply according to age of onset—onset prior to age 12 years; onset between 12 and 40 years and onset after the age of 40 years, permitted us to identify clear phenotypic and prognostic differences. Prior to 12 years of age, liver involvement (87%), seizures (84%), and feeding difficulties (84%) were the major features. For those with onset between 12 and 40 years, ataxia (90%), peripheral neuropathy (84%), and seizures (71%) predominated, while for those with onset over 40 years, ptosis (95%), progressive external ophthalmoplegia (89%), and ataxia (58%) were the major clinical features. The earlier the onset the worse the prognosis. Patients with epilepsy and those with compound heterozygous variants carried significantly worse prognosis. Conclusions: Based on our data, we propose a simplified POLG disease classification, which can be used to guide diagnostic investigations and predict disease course.

Published
2020

15. The relationship between deficit in digit span and genotype in nonsense mutation Duchenne muscular dystrophy

Author

Thangarajh, M, Elfring, GL, Trifillis, P, McIntosh, J, Peitz, SW, Ryan, MM, Kornberg, AJ, RodriguezCasero, V, Wray, A, Jones, KJ, North, K, Goemans, N, Buyse, GM, Campbell, C, Mah, J, Sarnat, H, Selby, K, Voit, T, Doppler, V, De Castro, D, Chabrol, B, Levy, N, Halbert, C, Pereon, Y, Magot, A, Perrier, J, Mahe, JY, Schara, U, Lutz, S, Busse, M, Della Marina, A, Kirschner, J, Stanescu, A, Pohl, A, RensingZimmerman, C, Bertini, E, D'Amico, A, Kofler, A, Carlesi, A, Bonetti, AM, Santecchia, L, Emma, F, Bergami, G, Mercuri, EM, Vasco, G, Bianco, F, Mazzone, ES, De Sanctis, R, Alfieri, P, Pane, M, Messina, S, Comi, GP, Magri, F, Lucchini, V, Corti, SP, Moggio, MG, Sciacco, M, Bresolin, N, Prelle, AC, Magri, R, Virgilio, R, Lamperti, C, Nevo, Y, DorWollman, T, Vilchez, J, Muelas, N, Sevilla, T, Smeyers, P, de la Osa, A, Colomer, J, Ortez, CI, Nascimento, A, Febrer, A, Medina, J, Tulinus, M, Thorarinsdottir, B, Darin, N, Sejersen, T, Hovmoller, M, Bushby, K, Straub, V, Guglieri, M, Sarkozy, A, Willis, T, Eagle, M, Mayhew, A, Muntoni, F, Cirak, S, Manzur, AY, Robb, SA, Kinali, M, Quinlivan, RCM, Smith, MR, Pandey, R, Wong, B, Collins, J, Finkel, R, Bonnemann, C, Yang, M, Foley, AR, Yum, S, Sampson, J, Bromberg, M, Swoboda, K, Day, J, Karachunski, P, Mathews, K, Bonthius, D, Laubenthal, KS, Darras, B, Kang, P, Parson, J, Barohn, R, Dasouki, M, Anderson, H, Burns, J, Dimachkie, M, Pasnoor, M, Wang, YX, Ciafaloni, E, Heatwole, C, Connolly, A, Pestronk, A, Al-Lozi, M, Lopate, G, Golumbek, P, Sommerville, B, Wang, L, Wojcicka-Mitchell, A, Godbey, A, Harms, M, Varadachary, A, Iyadurai, S, Rojas, L, Iannacone, S, Khonghatithum, C, Sproule, D, De Vivo, D, Constantinescu, A, McDonald, C, Han, J, Ben Renfroe, Russman, B, Sussman, M, BurnsWechsler, S, Juel, V, Hobson-Webb, L, Smith, E, Ataluren Phase 2b Study Grp, Schara, Ulrike (Beitragende*r), and Marina, Adela Della (Beitragende*r)

Subjects
Male, 0301 basic medicine, Adolescent, Duchenne muscular dystrophy, Nonsense mutation, Medizin, Neuropsychological Tests, 030105 genetics & heredity, Article, Young Adult, 03 medical and health sciences, Exon, Settore MED/39 - NEUROPSICHIATRIA INFANTILE, 0302 clinical medicine, Genotype, Memory span, medicine, Humans, Child, Genetics, biology, Promoter, Duchenne, medicine.disease, Muscular Dystrophy, Duchenne, Cross-Sectional Studies, Memory, Short-Term, Codon, Nonsense, Child, Preschool, Mutation (genetic algorithm), biology.protein, Neurology (clinical), Dystrophin, 030217 neurology & neurosurgery
Abstract

ObjectiveTo evaluate the relationship between deficit in digit span and genotype in nonsense mutation (nm) Duchenne muscular dystrophy (DMD) (nmDMD).MethodsWe investigated the relationship between normalized digit-span forward (d-sf) and digit-span backward (d-sb) scores to the location of nmDMD mutations in 169 participants ≥5 to ≤20 years who participated in a phase 2b clinical trial. Because alternative promoters are found upstream of DMD exons 30, 45, and 63, we correlated d-sf and d-sb to the specific nmDMD mutation location.ResultsParticipants with nm downstream of exon 30, downstream of exon 45, and downstream of exon 63 had significantly lower normalized d-sf scores (p < 0.0001). Participants with nm downstream of exon 45 in addition had significantly lower normalized d-sb score (p < 0.04). There was no significant difference in the normalized d-sb score in participants with mutations upstream or downstream of DMD exon 30 or upstream or downstream of DMD exon 63.ConclusionOur data provide evidence that specific cognitive deficits correlate to genotype in individuals with nmDMD, highlighting the critical role of brain-specific dystrophin isoforms in the neurobiological manifestations of this disease.Clinicaltrials.gov identifierNCT02090959.

Published
2018
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23. What powers can a donor retain over transferred property?

Author

Digby, Darin N.

Subjects
Charitable contributions -- Laws, regulations and rules, Estate planning -- Methods, Gift tax -- Planning, Estate tax -- Planning, Trusts and trustees -- Laws, regulations and rules
Abstract

Donors can retain substantial control over donated property. Transfers to trusts and revocable transfers are not completed gifts and cannot therefore be claimed for tax purposes. The donor should not serve as a trustee for the property, although the donor can serve as trustee for an irrevocable trust. Income tax provisions will apply if the gift property is included in the donor's gross estate.

Published
1997

24. Finite Element Analysis of the Space Shuttle 2.5-Inch Frangible Nut

Author

Darin N. McKinnis

Subjects
Launch Vehicles And Space Vehicles
Abstract

Finite element analysis of the Space Shuttle 2.5-inch frangible nut was conducted to improve understanding of the current design and proposed design changes to this explosively-actuated nut. The 2.5-inch frangible nut is used in two places to attach the aft end of the Space Shuttle Orbiter to the External Tank. Both 2.5-inch frangible nuts must function to complete safe separation. The 2.5-inch frangible nut contains two explosive boosters containing RDX explosive each capable of splitting the nut in half, on command from the Orbiter computers. To ensure separation, the boosters are designed to be redundant. The detonation of one booster is sufficient to split the nut in half. However, beginning in 1987 some production lots of 2.5-inch frangible nuts have demonstrated an inability to separate using only a single booster. The cause of the failure has been attributed to differences in the material properties and response of the Inconel 718 from which the 2.5-inch frangible nut is manufactured. Subsequent tests have resulted in design modifications of the boosters and frangible nut. Model development and initial analysis was conducted by Sandia National Laboratories (SNL) under funding from NASA Lyndon B. Johnson Space Center (NASA-JSC) starting in 1992. Modeling codes previously developed by SNL were transferred to NASA-JSC for further analysis on this and other devices. An explosive bolt with NASA Standard Detonator (NSD) charge, a 3/4-inch frangible nut, and the Super*Zip linear separation system are being modeled by NASA-JSC.

Published
1994

25. Mutations in the histone methyltransferase gene KMT2B cause complex early-onset dystonia

Author

Meyer E, Carss KJ, Rankin J, Nichols JM, Grozeva D, Joseph AP, Mencacci NE, Papandreou A, Ng J, Barral S, Ngoh A, Ben-Pazi H, Willemsen MA, Arkadir D, Barnicoat A, Bergman H, Bhate S, Boys A, Darin N, Foulds N, Gutowski N, Hills A, Houlden H, Hurst JA, Israel Z, Kaminska M, Limousin P, Lumsden D, McKee S, Misra S, Mohammed SS, Nakou V, Nicolai J, Nilsson M, Pall H, Peall KJ, Peters GB, Prabhakar P, Reuter MS, Rump P, Segel R, Sinnema M, Smith M, Turnpenny P, White SM, Wieczorek D, Wiethoff S, Wilson BT, Winter G, Wragg C, Pope S, Heales SJ, Morrogh D, UK10K Consortium, Deciphering Developmental Disorders Study, NIHR BioResource Rare Diseases Consortium, Pittman A, Carr LJ, Pérez-Dueñas B, Lin JP, Reis A, Gahl WA, Toro C, Bhatia KP, Wood NW, Kamsteeg EJ, Chong WK, Gissen P, Topf M, Dale RC, Chubb JR, Raymond FL, Kurian MA, and Apollo - University of Cambridge Repository

Subjects
DNA-Binding Proteins, Histones, Male, Dystonia, Adolescent, Lysine, Mutation, Histone Methyltransferases, Humans, Nuclear Proteins, Female, Histone-Lysine N-Methyltransferase, Methylation
Abstract

Histone lysine methylation, mediated by mixed-lineage leukemia (MLL) proteins, is now known to be critical in the regulation of gene expression, genomic stability, cell cycle and nuclear architecture. Despite MLL proteins being postulated as essential for normal development, little is known about the specific functions of the different MLL lysine methyltransferases. Here we report heterozygous variants in the gene KMT2B (also known as MLL4) in 27 unrelated individuals with a complex progressive childhood-onset dystonia, often associated with a typical facial appearance and characteristic brain magnetic resonance imaging findings. Over time, the majority of affected individuals developed prominent cervical, cranial and laryngeal dystonia. Marked clinical benefit, including the restoration of independent ambulation in some cases, was observed following deep brain stimulation (DBS). These findings highlight a clinically recognizable and potentially treatable form of genetic dystonia, demonstrating the crucial role of KMT2B in the physiological control of voluntary movement.

Published
2017

26. Thiamine deficiency in childhood with attention to genetic causes: Survival and outcome predictors

Author

Ortigoza-Escobar JD, Alfadhel M, Molero M, Darin N, Spiegel R, de Coo IF, Gerards M, Taylor RW, Artuch-Iriberri R, Nashabat M, Rodríguez-Pombo P, Tabarki B, Pérez-Dueñas B, and Marti-Sanchez L

Subjects
food and beverages
Abstract

Primary and secondary conditions leading to thiamine deficiency have overlapping features in children, presenting with acute episodes of encephalopathy, bilateral symmetric brain lesions, and high excretion of organic acids that are specific of thiamine-dependent mitochondrial enzymes, mainly lactate, alpha-ketoglutarate, and branched chain keto-acids. Undiagnosed and untreated thiamine deficiencies are often fatal or lead to severe sequelae. Herein, we describe the clinical and genetic characterization of 79 patients with inherited thiamine defects causing encephalopathy in childhood, identifying outcome predictors in patients with pathogenic SLC19A3 variants, the most common genetic etiology. We propose diagnostic criteria that will aid clinicians to establish a faster and accurate diagnosis so that early vitamin supplementation is considered. Ann Neurol 2017;82:317-330.

Published
2017

27. Fastening apparatus having shape memory alloy actuator

Author

Mckinnis, Darin N

Subjects
Mechanical Engineering
Abstract

A releasable fastening apparatus is presented. The device includes a connecting member and a housing. The housing supports a gripping mechanism that is adapted to engage the connecting member. A triggering member is movable within the housing between a first position in which it constrains the gripping mechanism in locked engagement with the connecting member, and a second position in which the gripping mechanism is disengaged from the connecting member. A shaped memory alloy actuator is employed for translating the triggering member from its first to its second position. The actuator is designed to expand longitudinally when transitioned from a martensitic to an austenitic state.

Published
1992

28. Mutations in the histone methyltransferase gene KMT2B cause complex early-onset dystonia

Author

Meyer, E., Carss, K.J., Rankin, J., Nichols, J.M., Grozeva, D., Joseph, A.P., Mencacci, N.E., Papandreou, A., Ng, J., Barral, S., Ngoh, A., Ben-Pazi, H., Willemsen, M.A., Arkadir, D., Barnicoat, A., Bergman, H., Bhate, S., Boys, A., Darin, N., Foulds, N., Gutowski, N., Hills, A., Houlden, H., Hurst, J.A., Israel, Z., Kaminska, M., Limousin, P., Lumsden, D., McKee, S., Misra, S., Mohammed, S.S., Nakou, V., Nicolai, J., Nilsson, M., Pall, H., Peall, K.J., Peters, G.B., Prabhakar, P., Reuter, M.S., Rump, P., Segel, R., Sinnema, M., Smith, M., Turnpenny, P., White, S.M., Wieczorek, D., Wiethoff, S., Wilson, B.T., Winter, G., Wragg, C., Pope, S., Heales, S.J., Morrogh, D., Pittman, A., Carr, L.J., Perez-Duenas, B., Lin, J.P., Reis, A., Gahl, W.A., Toro, C., Bhatia, K.P., Wood, N.W., Kamsteeg, E.J., Chong, W.K., Gissen, P., Topf, M., Dale, R.C., Chubb, J.R., Raymond, F.L., Kurian, M.A., Meyer, E., Carss, K.J., Rankin, J., Nichols, J.M., Grozeva, D., Joseph, A.P., Mencacci, N.E., Papandreou, A., Ng, J., Barral, S., Ngoh, A., Ben-Pazi, H., Willemsen, M.A., Arkadir, D., Barnicoat, A., Bergman, H., Bhate, S., Boys, A., Darin, N., Foulds, N., Gutowski, N., Hills, A., Houlden, H., Hurst, J.A., Israel, Z., Kaminska, M., Limousin, P., Lumsden, D., McKee, S., Misra, S., Mohammed, S.S., Nakou, V., Nicolai, J., Nilsson, M., Pall, H., Peall, K.J., Peters, G.B., Prabhakar, P., Reuter, M.S., Rump, P., Segel, R., Sinnema, M., Smith, M., Turnpenny, P., White, S.M., Wieczorek, D., Wiethoff, S., Wilson, B.T., Winter, G., Wragg, C., Pope, S., Heales, S.J., Morrogh, D., Pittman, A., Carr, L.J., Perez-Duenas, B., Lin, J.P., Reis, A., Gahl, W.A., Toro, C., Bhatia, K.P., Wood, N.W., Kamsteeg, E.J., Chong, W.K., Gissen, P., Topf, M., Dale, R.C., Chubb, J.R., Raymond, F.L., and Kurian, M.A.

Abstract

Item does not contain fulltext, Histone lysine methylation, mediated by mixed-lineage leukemia (MLL) proteins, is now known to be critical in the regulation of gene expression, genomic stability, cell cycle and nuclear architecture. Despite MLL proteins being postulated as essential for normal development, little is known about the specific functions of the different MLL lysine methyltransferases. Here we report heterozygous variants in the gene KMT2B (also known as MLL4) in 27 unrelated individuals with a complex progressive childhood-onset dystonia, often associated with a typical facial appearance and characteristic brain magnetic resonance imaging findings. Over time, the majority of affected individuals developed prominent cervical, cranial and laryngeal dystonia. Marked clinical benefit, including the restoration of independent ambulation in some cases, was observed following deep brain stimulation (DBS). These findings highlight a clinically recognizable and potentially treatable form of genetic dystonia, demonstrating the crucial role of KMT2B in the physiological control of voluntary movement.

Published
2017

29. Identification of a large intronic transposal insertion in SLC17A5 causing sialic acid storage disease

Author

Tarailo-Graovac, M. (Maja), Drögemöller, B.I. (Britt I.), Wasserman, W.W. (Wyeth W.), Ross, C.J., Ouweland, A.M.W. (Ans) van den, Darin, N. (Niklas), Kollberg, G. (Gittan), Van Karnebeek, C.D.M. (Clara D. M.), Blomqvist, M. (Maria), Tarailo-Graovac, M. (Maja), Drögemöller, B.I. (Britt I.), Wasserman, W.W. (Wyeth W.), Ross, C.J., Ouweland, A.M.W. (Ans) van den, Darin, N. (Niklas), Kollberg, G. (Gittan), Van Karnebeek, C.D.M. (Clara D. M.), and Blomqvist, M. (Maria)

Abstract

Background: Sialic acid storage diseases are neurodegenerative disorders characterized by accumulation of sialic acid in the lysosome. These disorders are caused by mutations in SLC17A5, the gene encoding sialin, a sialic acid transporter located in the lysosomal membrane. The most common form of sialic acid storage disease is the slowly progressive Salla disease, presenting with hypotonia, ataxia, epilepsy, nystagmus and findings of cerebral and cerebellar atrophy. Hypomyelination and corpus callosum hypoplasia are typical as well. We report a 16 year-old boy with an atypically mild clinical phenotype of sialic acid storage disease characterized by psychomotor retardation and a mixture of spasticity and rigidity but no ataxia, and only weak features of hypomyelination and thinning of corpus callosum on MRI of the brain. Results: The thiobarbituric acid method showed elevated levels of free sialic acid in urine and fibroblasts, indicating sialic acid storage disease. Initial Sanger sequencing of SLC17A5 coding regions did not show any pathogenic variants, although exon 9 could not be sequenced. Whole exome sequencing followed by RNA and genomic DNA analysis identified a homozygous 6040 bp insertion in intron 9 of SLC17A5 corresponding to a long interspersed element-1 retrotransposon (KF425758.1). This insertion adds two splice sites, both resulting in a frameshift which in turn creates a premature stop codon 4 bp into intron 9. Conclusions: This study describes a novel pathogenic variant in SLC17A5, namely an intronic transposal insertion, in a patient with mild biochemical and clinical phenotypes. The presence of a small fraction of normal transcript may explain the mild phenotype. This case illustrates the importance of including lysosomal sialic acid storage disease in the differential diagnosis of developmental delay with postnatal onset and hypomyelination, as well as intronic regions in the genetic investigation of inborn errors of metabolism.

Published
2017
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30. Progressive deafness-dystonia due to SERAC1 mutations: A study of 67 cases

Author

Maas, RR, Iwanicka-Pronicka, K, Ucar, SK, Alhaddad, B, AlSayed, M, Al-Owain, MA, Al-Zaidan, HI, Balasubramaniam, S, Baric, I, Bubshait, DK, Burlina, A, Christodoulou, J, Chung, WK, Colombo, R, Darin, N, Freisinger, P, Garcia Silva, MT, Grunewald, S, Haack, TB, van Hasselt, PM, Hikmat, O, Hoerster, F, Isohanni, P, Ramzan, K, Kovacs-Nagy, R, Krumina, Z, Martin-Hernandez, E, Mayr, JA, McClean, P, De Meirleir, L, Naess, K, Ngu, LH, Pajdowska, M, Rahman, S, Riordan, G, Riley, L, Roeben, B, Rutsch, F, Santer, R, Schiff, M, Seders, M, Sequeira, S, Sperl, W, Staufner, C, Synofzik, M, Taylor, RW, Trubicka, J, Tsiakas, K, Unal, O, Wassmer, E, Wedatilake, Y, Wolff, T, Prokisch, H, Morava, E, Pronicka, E, Wevers, RA, de Brouwer, AP, Wortmann, SB, Maas, RR, Iwanicka-Pronicka, K, Ucar, SK, Alhaddad, B, AlSayed, M, Al-Owain, MA, Al-Zaidan, HI, Balasubramaniam, S, Baric, I, Bubshait, DK, Burlina, A, Christodoulou, J, Chung, WK, Colombo, R, Darin, N, Freisinger, P, Garcia Silva, MT, Grunewald, S, Haack, TB, van Hasselt, PM, Hikmat, O, Hoerster, F, Isohanni, P, Ramzan, K, Kovacs-Nagy, R, Krumina, Z, Martin-Hernandez, E, Mayr, JA, McClean, P, De Meirleir, L, Naess, K, Ngu, LH, Pajdowska, M, Rahman, S, Riordan, G, Riley, L, Roeben, B, Rutsch, F, Santer, R, Schiff, M, Seders, M, Sequeira, S, Sperl, W, Staufner, C, Synofzik, M, Taylor, RW, Trubicka, J, Tsiakas, K, Unal, O, Wassmer, E, Wedatilake, Y, Wolff, T, Prokisch, H, Morava, E, Pronicka, E, Wevers, RA, de Brouwer, AP, and Wortmann, SB

Abstract

OBJECTIVE: 3-Methylglutaconic aciduria, dystonia-deafness, hepatopathy, encephalopathy, Leigh-like syndrome (MEGDHEL) syndrome is caused by biallelic variants in SERAC1. METHODS: This multicenter study addressed the course of disease for each organ system. Metabolic, neuroradiological, and genetic findings are reported. RESULTS: Sixty-seven individuals (39 previously unreported) from 59 families were included (age range = 5 days-33.4 years, median age = 9 years). A total of 41 different SERAC1 variants were identified, including 20 that have not been reported before. With the exception of 2 families with a milder phenotype, all affected individuals showed a strikingly homogeneous phenotype and time course. Severe, reversible neonatal liver dysfunction and hypoglycemia were seen in >40% of all cases. Starting at a median age of 6 months, muscular hypotonia (91%) was seen, followed by progressive spasticity (82%, median onset = 15 months) and dystonia (82%, 18 months). The majority of affected individuals never learned to walk (68%). Seventy-nine percent suffered hearing loss, 58% never learned to speak, and nearly all had significant intellectual disability (88%). Magnetic resonance imaging features were accordingly homogenous, with bilateral basal ganglia involvement (98%); the characteristic "putaminal eye" was seen in 53%. The urinary marker 3-methylglutaconic aciduria was present in virtually all patients (98%). Supportive treatment focused on spasticity and drooling, and was effective in the individuals treated; hearing aids or cochlear implants did not improve communication skills. INTERPRETATION: MEGDHEL syndrome is a progressive deafness-dystonia syndrome with frequent and reversible neonatal liver involvement and a strikingly homogenous course of disease. Ann Neurol 2017;82:1004-1015.

Published
2017

32. A new early-onset myopathy associated with deficiency in kyphoscoliosis peptidase (KY)

Author

Hedberg-Oldfors, C, Darin, N, Olsson Engman, M, Orfanos, Z, van der Ven, PFM, and Oldfors, A

Subjects
ddc: 610, 610 Medical sciences, Medicine
Abstract

Introduction: A neuromuscular disorder caused by a homozygous variant in the kyphoscoliosis peptidase gene (Ky) was first described in a mouse model (ky/ky). In this model, kyphoscoliosis develops due to atrophy of postural muscles during postnatal growth. The muscle phenotype of the ky/ky[for full text, please go to the a.m. URL], Joint-Meeting of the German Society for Neuropathology and Neuroanatomy (DGNN) and the Scandinavian Neuropathological Society (SNS)

Published
2016
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37. Electron-withdrawing effects on metal-olefin bond strengths in Ni(PH3)(sub 2)(CO)(C2XnH4-n), X = F, Cl; n = 0-4: A DFT study

Author

Schlappi, Darin N. and Cedeno, David L.

Subjects
Dissociation -- Research, Nickel -- Research, Nickel -- Chemical properties, Density functionals -- Usage, Chemistry, Physical and theoretical -- Research, Chemicals, plastics and rubber industries
Abstract

Density functional theory (DFT) studies are performed in the title complexes to determine the effect of electron-withdrawing halogens around the C=C bond on the metal-olefin bond dissociation energy. Reorganizational effects in olefin and Ni(PH3)(sub 2)(CO) play a vital role in the overall bond dissociation energy trend.

Published
2003

39. Electron-Withdrawing Effects on Metal−Olefin Bond Strengths in Ni(PH3)2(CO)(C2XnH4-n), X = F, Cl; n = 0−4: A DFT Study

Author

David L. Cedeño and Darin N. Schlappi

Subjects
Bond length, Crystallography, Chemical bond, Computational chemistry, Chemistry, Sextuple bond, Single bond, Physical and Theoretical Chemistry, Bond energy, Triple bond, Bond order, Bent bond
Abstract

Density functional theory (DFT) studies have been performed in the title complexes to determine the effect of electron-withdrawing halogens around the CC bond on the metal−olefin bond dissociation energy. Calculations indicate that the nickel−olefin bond dissociation energy would be nearly independent of the number of electron-withdrawing elements around the double bond. The results are explained in terms of electronic, steric, and reorganizational effects that derive from the olefin−metal interaction and are compared to computational and experimental results for related complexes, which show similar metal−olefin bond strength behavior. It has been found that reorganizational effects in both the olefin and Ni(PH3)2(CO) play a determining role in the overall bond dissociation energy trend.

Published
2003
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42. Eyes on MEGDEL: Distinctive Basal Ganglia Involvement in Dystonia Deafness Syndrome

Author

Wortmann, S.B., Hasselt, P.M. van, Baric, I., Burlina, A., Darin, N., Horster, F., Coker, M., Ucar, S. Kalkan, Krumina, Z., Naess, K., Ngu, L.H., Pronicka, E., Riordan, G., Santer, R., Wassmer, E., Zschocke, J., Schiff, M., Meirleir, L. de, Alowain, M.A., Smeitink, J.A.M., Morava, E., Kozicz, L.T., Wevers, R.A., Wolf, N.I., Willemsen, M.A., Wortmann, S.B., Hasselt, P.M. van, Baric, I., Burlina, A., Darin, N., Horster, F., Coker, M., Ucar, S. Kalkan, Krumina, Z., Naess, K., Ngu, L.H., Pronicka, E., Riordan, G., Santer, R., Wassmer, E., Zschocke, J., Schiff, M., Meirleir, L. de, Alowain, M.A., Smeitink, J.A.M., Morava, E., Kozicz, L.T., Wevers, R.A., Wolf, N.I., and Willemsen, M.A.

Abstract

Contains fulltext : 155252.pdf (publisher's version ) (Closed access), Pediatric movement disorders are still a diagnostic challenge, as many patients remain without a (genetic) diagnosis. Magnetic resonance imaging (MRI) pattern recognition can lead to the diagnosis. MEGDEL syndrome (3-MethylGlutaconic aciduria, Deafness, Encephalopathy, Leigh-like syndrome MIM #614739) is a clinically and biochemically highly distinctive dystonia deafness syndrome accompanied by 3-methylglutaconic aciduria, severe developmental delay, and progressive spasticity. Mutations are found in SERAC1, encoding a phosphatidylglycerol remodeling enzyme essential for both mitochondrial function and intracellular cholesterol trafficking. Based on the homogenous phenotype, we hypothesized an accordingly characteristic MRI pattern. A total of 43 complete MRI studies of 30 patients were systematically reevaluated. All patients presented a distinctive brain MRI pattern with five characteristic disease stages affecting the basal ganglia, especially the putamen. In stage 1, T2 signal changes of the pallidum are present. In stage 2, swelling of the putamen and caudate nucleus is seen. The dorsal putamen contains an "eye" that shows no signal alteration and (thus) seems to be spared during this stage of the disease. It later increases, reflecting progressive putaminal involvement. This "eye" was found in all patients with MEGDEL syndrome during a specific age range, and has not been reported in other disorders, making it pathognomonic for MEDGEL and allowing diagnosis based on MRI findings.

Published
2015

43. Product Unbundling in the Travel Industry: The Economics of Airline Bag Fees

Author

Brueckner, Jan K., Lee, Darin N., Picard, Pierre M, Singer, Ethan, Brueckner, Jan K., Lee, Darin N., Picard, Pierre M, and Singer, Ethan

Abstract

This paper provides theory and evidence on airline bag fees, offering insights into a real-world case of product unbundling. The theory predicts that an airline’s fares should fall when it introduces a bag fee, but that the full-trip price (the bag fee plus the new fare) could either rise or fall. The empirical evidence presented in the paper provides strong confirmation of the first prediction. The data also suggest that the average fare falls by less than the bag fee itself so that the full price of a trip rises for passengers who choose to check bags.

Published
2015

44. Product Unbundling in the Travel Industry: The Economics of Airline Bag Fees

Author

Brueckner, Jan K., Lee, Darin N., Picard, Pierre M., and Singer, Ethan

Subjects
airlines, ddc:330, unbundling, bag fees, L90
Abstract

This paper provides theory and evidence on airline bag fees, offering insights into a real-world case of product unbundling. The theory predicts that an airline's fares should fall when it introduces a bag fee, but that the full trip price (the bag fee plus the new fare) could either rise or fall. The empirical evidence presented in the paper provides strong confirmation of this prediction. The data also suggest that the average fare falls by less than the bag fee itself, so that the full price of a trip rises for passengers who choose to check bags.

Published
2013

46. OP6 – 2631: Decreased free-thiamine in cerebro spinal fluid and fibroblasts is a sensitive marker of thiamine transporter 2 deficiency in Leigh syndrome patients

Author

Escobar, J.D. Ortigoza, primary, Molero-Luis, M., additional, Arias, A., additional, Darin, N., additional, Casado, M., additional, Serrano, M., additional, Tondo, M., additional, Mayr, J.A., additional, Ribes, A., additional, Artuch, R., additional, and Pérez-Dueñas, B., additional

Published
2015
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48. A multicenter study on Leigh syndrome: Disease course and predictors of survival

Author

Sofou, K. (Kalliopi), Coo, I.F.M. (René) de, Isohanni, M.K. (Matti), Ostergaard, M., Naess, K. (Karin), Meirleir, L. (Linda) de, Tzoulis, C. (Charalampos), Uusimaa, J. (Johanna), Angst, I.B. (Isabel) de, Lönnqvist, T. (Tuula), Pihko, H. (Helena), Mankinen, K. (Katariina), Bindoff, L.A. (Laurence Albert), Tulinius, M. (Már), Darin, N. (Niklas), Sofou, K. (Kalliopi), Coo, I.F.M. (René) de, Isohanni, M.K. (Matti), Ostergaard, M., Naess, K. (Karin), Meirleir, L. (Linda) de, Tzoulis, C. (Charalampos), Uusimaa, J. (Johanna), Angst, I.B. (Isabel) de, Lönnqvist, T. (Tuula), Pihko, H. (Helena), Mankinen, K. (Katariina), Bindoff, L.A. (Laurence Albert), Tulinius, M. (Már), and Darin, N. (Niklas)

Abstract

Background: Leigh syndrome is a progressive neurodegenerative disorder, associated with primary or secondary dysfunction of the mitochondrial oxidative phosphorylation. Despite the fact that Leigh syndrome is the most common phenotype of mitochondrial disorders in children, longitudinal natural history data is missing. This study was undertaken to assess the phenotypic and genotypic spectrum of patients with Leigh syndrome, characterise the clinical course and identify predictors of survival in a large cohort of patients. Methods. This is a retrospective study of patients with Leigh syndrome that have been followed at eight centers specialising in mitochondrial diseases in Europe; Gothenburg, Rotterdam, Helsinki, Copenhagen, Stockholm, Brussels, Bergen and Oulu. Results: A total of 130 patients were included (78 males; 52 females), of whom 77 patients had identified pathogenic mutations. The median age of disease onset was 7 months, wi

Published
2014
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49. A multicenter study on Leigh syndrome: disease course and predictors of survival

Author

Sofou, K, Coo, IFM, Isohanni, P, Ostergaard, E, Naess, K, de Meirleir, L, Tzoulis, C, Uusimaa, J, de Angst, Isabel, Lonnqvist, T, Pihko, H, Mankinen, K, Bindoff, LA, Tulinius, M, Darin, N, Sofou, K, Coo, IFM, Isohanni, P, Ostergaard, E, Naess, K, de Meirleir, L, Tzoulis, C, Uusimaa, J, de Angst, Isabel, Lonnqvist, T, Pihko, H, Mankinen, K, Bindoff, LA, Tulinius, M, and Darin, N

Abstract

Background: Leigh syndrome is a progressive neurodegenerative disorder, associated with primary or secondary dysfunction of the mitochondrial oxidative phosphorylation. Despite the fact that Leigh syndrome is the most common phenotype of mitochondrial disorders in children, longitudinal natural history data is missing. This study was undertaken to assess the phenotypic and genotypic spectrum of patients with Leigh syndrome, characterise the clinical course and identify predictors of survival in a large cohort of patients. Methods: This is a retrospective study of patients with Leigh syndrome that have been followed at eight centers specialising in mitochondrial diseases in Europe; Gothenburg, Rotterdam, Helsinki, Copenhagen, Stockholm, Brussels, Bergen and Oulu. Results: A total of 130 patients were included (78 males; 52 females), of whom 77 patients had identified pathogenic mutations. The median age of disease onset was 7 months, with 80.8% of patients presenting by the age of 2 years. The most common clinical features were abnormal motor findings, followed by abnormal ocular findings. Epileptic seizures were reported in 40% of patients. Approximately 44% of patients experienced acute exacerbations requiring hospitalisation during the previous year, mainly due to infections. The presence of pathological signs at birth and a history of epileptic seizures were associated with higher occurrence of acute exacerbations and/or relapses. Increased lactate in the cerebrospinal fluid was significantly correlated to a more severe disease course, characterised by early onset before 6 months of age, acute exacerbations and/or relapses, as well as brainstem involvement. 39% of patients had died by the age of 21 years, at a median age of 2.4 years. Disease onset before 6 months of age, failure to thrive, brainstem lesions on neuroimaging and intensive care treatment were significantly associated with poorer survival. Conclusions: This is a multicenter study performed in a larg

Published
2014

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