Your search keyword '"Kettwig M"' showing total 19 results

1. Tazarotene and Bexarotene Show Efficacy as In Vitro Therapeutic Agents in Multiple Sulfatase Deficiency.

Author

Schlotawa, L., Matysiak, K., Kettwig, M., Ahrens-Nicklas, R. C., Baud, M., Berulava, T., Brunetti-Pierri, N., Gagne, A., Herbst, Z. M., Maguire, J. A., Monfregola, J., Pena, T., Radhakrishnan, K., Schröder, S., Waxman, E. A., Ballabio, A., Dierks, T., Fischer, A., French, D. L., and Gelb, M. H.

Subjects

SULFATASES, LYSOSOMAL storage diseases, HIGH throughput screening (Drug development), NEURODEGENERATION, RESEARCH personnel, GLYCOGEN storage disease type II

Abstract

The article discusses the potential use of tazarotene and bexarotene as therapeutic agents for multiple sulfatase deficiency (MSD), an ultra-rare neurodegenerative lysosomal disorder. MSD is caused by mutations in the SUMF1 gene, resulting in impaired function of the formylglycine-generating enzyme (FGE) and reduced activity of cellular sulfatases. The researchers conducted a high-throughput screening assay and found that tazarotene and bexarotene increased sulfatase activities, improved cellular markers of disease, and normalized lysosomal size and position in MSD patient-derived cells. These findings suggest that these drugs could be repurposed as a therapy for MSD patients. [Extracted from the article]

Published

2023

2. Roifman Syndrome Is a Rare but Important Differential Diagnosis in Patients Suspected to Have CDG Syndrome.

Author

Borgmann, I., Johnsen, C., Hoffmann, J., Schlotawa, L., and Kettwig, M.

Subjects

DIFFERENTIAL diagnosis, ECZEMA, CONGENITAL disorders, FAILURE to thrive syndrome, SYNDROMES, GENETIC testing, SURVIVAL rate

Abstract

This article discusses a case study of a boy with symptoms of hypothermia, hypoglycemia, failure to thrive, hypotonia, seizures, facial dysmorphia, inverted nipple, and eczema. The boy was suspected to have congenital disorder of glycosylation (CDG) syndrome, and genetic testing confirmed a deletion on chromosome 2 and a pathogenic variant in the RNU4ATAC gene. The specific mutation in RNU4ATAC led to a diagnosis of Roifman syndrome (RS), which is a rare condition associated with CDG syndrome. RS is characterized by a range of symptoms, including immunodeficiency. Early diagnosis and treatment are important for the survival and outcome of patients with RS. [Extracted from the article]

Published

2023

3. Mitochondrial encephalomyopathy presenting with deafness, mutism, ataxia and late onset external ophthalmoplegia caused by a mutation in the X-linked gene AIFM1

Author

Kettwig, M, primary, Biskup, S, additional, Klinge, L, additional, Gärtner, J, additional, and Huppke, P, additional

Published

2013

4. Late-onset Krabbe disease presenting as spastic paraplegia - implications of GCase and CTSB/D.

Author

Mächtel R, Dobert JP, Hehr U, Weiss A, Kettwig M, Laugwitz L, Groeschel S, Schmidt M, Arnold P, Regensburger M, and Zunke F

Subjects

Humans, Male, Adult, Paraplegia genetics, Age of Onset, Glucosylceramidase genetics, Lysosomes, Fibroblasts metabolism, Fibroblasts pathology, Leukodystrophy, Globoid Cell genetics, Leukodystrophy, Globoid Cell pathology, Leukodystrophy, Globoid Cell diagnosis, Cathepsin D genetics, Cathepsin D metabolism, Galactosylceramidase genetics, Cathepsin B genetics, Cathepsin B metabolism

Abstract

Objective: Krabbe disease (KD) is a multisystem neurodegenerative disorder with severe disability and premature death, mostly with an infancy/childhood onset. In rare cases of late-onset phenotypes, symptoms are often milder and difficult to diagnose. We here present a translational approach combining diagnostic and biochemical analyses of a male patient with a progressive gait disorder starting at the age of 44 years, with a final diagnosis of late-onset KD (LOKD)., Methods: Additionally to cerebral MRI, protein structural analyses of the β-galactocerebrosidase protein (GALC) were performed. Moreover, expression, lysosomal localization, and activities of β-glucocerebrosidase (GCase), cathepsin B (CTSB), and cathepsin D (CTSD) were analyzed in leukocytes, fibroblasts, and lysosomes of fibroblasts., Results: Exome sequencing revealed biallelic likely pathogenic variants: GALC exons 11-17: 33 kb deletion; exon 4: missense variant (c.334A>G, p.Thr112Ala). We detected a reduced GALC activity in leukocytes and fibroblasts. While histological KD phenotypes were absent in fibroblasts, they showed a significantly decreased activities of GCase, CTSB, and CTSD in lysosomal fractions, while expression levels were unaffected., Interpretation: The presented LOKD case underlines the age-dependent appearance of a mildly pathogenic GALC variant and its interplay with other lysosomal proteins. As GALC malfunction results in reduced ceramide levels, we assume this to be causative for the here described decrease in CTSB and CTSD activity, potentially leading to diminished GCase activity. Hence, we emphasize the importance of a functional interplay between the lysosomal enzymes GALC, CTSB, CTSD, and GCase, as well as between their substrates, and propose their conjoined contribution in KD pathology., (© 2024 The Authors. Annals of Clinical and Translational Neurology published by Wiley Periodicals LLC on behalf of American Neurological Association.)

Published

2024

5. Ratio of Urinary Proteins to Albumin Excretion Shifts Substantially during Progression of the Podocytopathy Alport Syndrome, and Spot Urine Is a Reliable Method to Detect These Pathologic Changes.

Author

Boeckhaus J, Mohr L, Dihazi H, Tönshoff B, Weber LT, Pape L, Latta K, Fehrenbach H, Lange-Sperandio B, Kettwig M, Staude H, König S, John-Kroegel U, Gellermann J, Hoppe B, Galiano M, Haffner D, Rhode H, and Gross O

Subjects

Adolescent, Child, Humans, Albumins metabolism, Albuminuria, Creatinine, Prospective Studies, Nephritis, Hereditary diagnosis, Renal Insufficiency, Chronic

Abstract

The urinary albumin- and protein-to-creatinine ratios (UACR and UPCR, respectively) are key endpoints in most clinical trials assessing risk of progression of chronic kidney disease (CKD). For the first time, the current study compares the UACR versus the UPCR head-to-head at early stages of CKD, taking use of the hereditary podocytopathy Alport syndrome (AS) as a model disease for any CKD. Urine samples originated from the prospective randomized, controlled EARLY PRO-TECT Alport trial (NCT01485978). Urine samples from 47 children with confirmed diagnoses of AS at very early stages of CKD were divided according to the current stage of AS: stage 0 (UACR < 30 mg/g), stage 1 (30-300 mg/g) or stage 2 (>300 mg/g). The range of estimated glomerular filtration rate was 75-187.6 mL/min. The mean age was 10.4 ± 4.5 years. In children at stage 0, proteinuria in spot urine, confirmed in 24 h urine, was almost ten times higher than albuminuria (106.4 ± 42.2 vs. 12.5 ± 9.7; p < 0.05); it was "only" about three times higher in stage 1 (328.5 ± 210.1 vs. 132.3 ± 80.5; p < 0.05) and almost equal in stage 2 (1481.9 ± 983.4 vs. 1109.7 ± 873.6; p = 0.36). In 17 children, UACRs and UPCRs were measured simultaneously in 24 h urine and spot urine in the same study visit. Interestingly, the UACR (and UPCR) in 24 h urine vs. in spot urine varied by less than 10% (266.8 ± 426.4 vs. 291.2 ± 530.2). In conclusion, our study provides the first evidence that in patients with normal glomerular filtration rate (GFR) and low amounts of albuminuria, especially in children with podocytopathies such as AS, measuring the UACR and UPCR in spot urine is a reliable and convenient alternative to 24 h urine collection. Our study advocates both the UACR and the UPCR as relevant diagnostic biomarkers in future clinical trials in children with glomerular diseases because the UPCR seems to be a very significant parameter at very early stages of podocytopathies. The German Federal Ministry of Education and Research funded this trial (01KG1104).

Published

2023

6. Drug screening identifies tazarotene and bexarotene as therapeutic agents in multiple sulfatase deficiency.

Author

Schlotawa L, Tyka K, Kettwig M, Ahrens-Nicklas RC, Baud M, Berulava T, Brunetti-Pierri N, Gagne A, Herbst ZM, Maguire JA, Monfregola J, Pena T, Radhakrishnan K, Schröder S, Waxman EA, Ballabio A, Dierks T, Fischer A, French DL, Gelb MH, and Gärtner J

Subjects

Humans, Bexarotene, Drug Evaluation, Preclinical, Sulfatases genetics, Oxidoreductases Acting on Sulfur Group Donors, Multiple Sulfatase Deficiency Disease diagnosis, Multiple Sulfatase Deficiency Disease genetics, Multiple Sulfatase Deficiency Disease pathology

Abstract

Multiple sulfatase deficiency (MSD, MIM #272200) results from pathogenic variants in the SUMF1 gene that impair proper function of the formylglycine-generating enzyme (FGE). FGE is essential for the posttranslational activation of cellular sulfatases. MSD patients display reduced or absent sulfatase activities and, as a result, clinical signs of single sulfatase disorders in a unique combination. Up to date therapeutic options for MSD are limited and mostly palliative. We performed a screen of FDA-approved drugs using immortalized MSD patient fibroblasts. Recovery of arylsulfatase A activity served as the primary readout. Subsequent analysis confirmed that treatment of primary MSD fibroblasts with tazarotene and bexarotene, two retinoids, led to a correction of MSD pathophysiology. Upon treatment, sulfatase activities increased in a dose- and time-dependent manner, reduced glycosaminoglycan content decreased and lysosomal position and size normalized. Treatment of MSD patient derived induced pluripotent stem cells (iPSC) differentiated into neuronal progenitor cells (NPC) resulted in a positive treatment response. Tazarotene and bexarotene act to ultimately increase the stability of FGE variants. The results lay the basis for future research on the development of a first therapeutic option for MSD patients., (© 2023 The Authors. Published under the terms of the CC BY 4.0 license.)

Published

2023

7. Relationship between age at initiation of cysteamine treatment, adherence with therapy, and glomerular kidney function in infantile nephropathic cystinosis.

Author

Nießl C, Boulesteix AL, Oh J, Palm K, Schlingmann P, Wygoda S, Haffner D, Wühl E, Tönshoff B, Buescher A, Billing H, Hoppe B, Zirngibl M, Kettwig M, Moeller K, Acham-Roschitz B, Arbeiter K, Bald M, Benz M, Galiano M, John-Kroegel U, Klaus G, Marx-Berger D, Moser K, Mueller D, Patzer L, Pohl M, Seitz B, Treikauskas U, von Vigier RO, Gahl WA, and Hohenfellner K

Subjects

Child, Cysteamine therapeutic use, Humans, Infant, Infant, Newborn, Kidney, Cystinosis complications, Cystinosis drug therapy, Fanconi Syndrome chemically induced, Fanconi Syndrome diagnosis, Fanconi Syndrome drug therapy

Abstract

Infantile nephropathic cystinosis, due to impaired transport of cystine out of lysosomes, occurs with an incidence of 1 in 100-200,000 live births. It is characterized by renal Fanconi syndrome in the first year of life and glomerular dysfunction progression to end-stage kidney disease by approximately 10 years of age. Treatment with oral cysteamine therapy helps preserve glomerular function, but affected individuals eventually require kidney replacement therapy. This is because glomerular damage had already occurred by the time a child is diagnosed with cystinosis, typically in the second year of life. We performed a retrospective multicenter study to investigate the impact of initiating cysteamine treatment within the first 2 months of life in some infants and comparing two different levels of adherence in patients diagnosed at the typical age. We collected 3983 data points from 55 patients born between 1997 and 2020; 52 patients with 1592 data points could be further evaluated. These data were first analyzed by dividing the patient cohort into three groups: (i) standard treatment start with good adherence, (ii) standard treatment start with less good adherence, and (iii) early treatment start. At every age, mean estimated glomerular filtration rate (eGFR) was higher in early-treated patients than in later-treated patients. Second, a generalized additive mixed model (GAMM) was applied showing that patients with initiation of treatment before 2 months of age are expected to have a 34 ml/min/1.73 m 2 higher eGFR than patients with later treatment start while controlling for adherence and patients' age. These data strongly suggest that oral cysteamine treatment initiated within 2 months of birth preserves kidney function in infantile nephropathic cystinosis and provide evidence of the utility of newborn screening for this disease., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2022

8. Interferon-driven brain phenotype in a mouse model of RNaseT2 deficient leukoencephalopathy.

Author

Kettwig M, Ternka K, Wendland K, Krüger DM, Zampar S, Schob C, Franz J, Aich A, Winkler A, Sakib MS, Kaurani L, Epple R, Werner HB, Hakroush S, Kitz J, Prinz M, Bartok E, Hartmann G, Schröder S, Rehling P, Henneke M, Boretius S, Alia A, Wirths O, Fischer A, Stadelmann C, Nessler S, and Gärtner J

Subjects

Animals, CD8-Positive T-Lymphocytes metabolism, Cognitive Dysfunction genetics, Cognitive Dysfunction metabolism, Disease Models, Animal, Endoribonucleases genetics, Female, Flow Cytometry, Genotype, Humans, Immunohistochemistry, Leukoencephalopathies genetics, Magnetic Resonance Imaging, Male, Memory T Cells metabolism, Mice, Mice, Knockout, Neuroglia metabolism, Real-Time Polymerase Chain Reaction, Endoribonucleases metabolism, Leukoencephalopathies metabolism, Leukoencephalopathies pathology

Abstract

Infantile-onset RNaseT2 deficient leukoencephalopathy is characterised by cystic brain lesions, multifocal white matter alterations, cerebral atrophy, and severe psychomotor impairment. The phenotype is similar to congenital cytomegalovirus brain infection and overlaps with type I interferonopathies, suggesting a role for innate immunity in its pathophysiology. To date, pathophysiological studies have been hindered by the lack of mouse models recapitulating the neuroinflammatory encephalopathy found in patients. In this study, we generated Rnaset2 -/- mice using CRISPR/Cas9-mediated genome editing. Rnaset2 -/- mice demonstrate upregulation of interferon-stimulated genes and concurrent IFNAR1-dependent neuroinflammation, with infiltration of CD8 + effector memory T cells and inflammatory monocytes into the grey and white matter. Single nuclei RNA sequencing reveals homeostatic dysfunctions in glial cells and neurons and provide important insights into the mechanisms of hippocampal-accentuated brain atrophy and cognitive impairment. The Rnaset2 -/- mice may allow the study of CNS damage associated with RNaseT2 deficiency and may be used for the investigation of potential therapies., (© 2021. The Author(s).)

Published

2021

9. Targeted metabolomics revealed changes in phospholipids during the development of neuroinflammation in Abcd1 tm1Kds mice and X-linked adrenoleukodystrophy patients.

Author

Kettwig M, Klemp H, Nessler S, Streit F, Krätzner R, Rosewich H, and Gärtner J

Subjects

ATP Binding Cassette Transporter, Subfamily D, Member 1 genetics, Adrenoleukodystrophy complications, Adrenoleukodystrophy physiopathology, Animals, Biomarkers blood, Dried Blood Spot Testing, Encephalomyelitis, Autoimmune, Experimental blood, Female, Humans, Infant, Newborn, Male, Mice, Mice, Inbred C57BL, Neuroinflammatory Diseases blood, Phospholipids, Adrenoleukodystrophy diagnosis, Lysophosphatidylcholines analysis, Metabolomics methods, Neonatal Screening methods, Neuroinflammatory Diseases etiology

Abstract

X-linked adrenoleukodystrophy (X-ALD) is the most common leukodystrophy. Despite intensive research in recent years, it remains unclear, what drives the different clinical disease courses. Due to this missing pathophysiological link, therapy for the childhood cerebral disease course of X-ALD (CCALD) remains symptomatic; the allogenic hematopoietic stem cell transplantation or hematopoietic stem-cell gene therapy is an option for early disease stages. The inclusion of dried blood spot (DBS) C26:0-lysophosphatidylcholine to newborn screening in an increasing number of countries is leading to an increasing number of X-ALD patients diagnosed at risk for CCALD. Current follow-up in asymptomatic boys with X-ALD requires repetitive cerebral MRIs under sedation. A reliable and easily accessible biomarker that predicts CCALD would therefore be of great value. Here we report the application of targeted metabolomics by AbsoluteIDQ p180-Kit from Biocrates to search for suitable biomarkers in X-ALD. LysoPC a C20:3 and lysoPC a C20:4 were identified as metabolites that indicate neuroinflammation after induction of experimental autoimmune encephalitis in the serum of Abcd1 tm1Kds mice. Analysis of serum from X-ALD patients also revealed different concentrations of these lipids at different disease stages. Further studies in a larger cohort of X-ALD patient sera are needed to prove the diagnostic value of these lipids for use as early biomarkers for neuroinflammation in CCALD patients., (© 2021 The Authors. Journal of Inherited Metabolic Disease published by John Wiley & Sons Ltd on behalf of SSIEM.)

Published

2021

10. LC-MS Based Platform Simplifies Access to Metabolomics for Peroxisomal Disorders.

Author

Klemp HG, Kettwig M, Streit F, Gärtner J, Rosewich H, and Krätzner R

Abstract

Peroxisomes are central hubs for cell metabolism and their dysfunction is linked to devastating human disorders, such as peroxisomal biogenesis disorders and single peroxisomal enzyme/protein deficiencies. For decades, biochemical diagnostics have been carried out using classical markers such as very long-chain fatty acids (VLCFA), which can be inconspicuous in milder and atypical cases. Holistic metabolomics studies revealed several potentially new biomarkers for peroxisomal disorders for advanced laboratory diagnostics including atypical cases. However, establishing these new markers is a major challenge in routine diagnostic laboratories. We therefore investigated whether the commercially available AbsoluteIDQ p180 kit (Biocrates Lifesciences), which utilizes flow injection and liquid chromatography mass spectrometry, may be used to reproduce some key results from previous global metabolomics studies. We applied it to serum samples from patients with mutations in peroxisomal target genes PEX1 , ABCD1 , and the HSD17B4 gene. Here we found various changes in sphingomyelins and lysophosphatidylcholines. In conclusion, this kit can be used to carry out extended diagnostics for peroxisomal disorders in routine laboratories, even without access to a metabolomics unit.

Published

2021

11. Precise variant interpretation, phenotype ascertainment, and genotype-phenotype correlation of children in the EARLY PRO-TECT Alport trial.

Author

Boeckhaus J, Hoefele J, Riedhammer KM, Tönshoff B, Ehren R, Pape L, Latta K, Fehrenbach H, Lange-Sperandio B, Kettwig M, Hoyer P, Staude H, Konrad M, John U, Gellermann J, Hoppe B, Galiano M, Gessner M, Pohl M, Bergmann C, Friede T, and Gross O

Subjects

Adolescent, Child, Child, Preschool, Early Diagnosis, Female, Genes, X-Linked genetics, Genetic Testing, Humans, Infant, Kidney pathology, Male, Nephritis, Hereditary diagnosis, Nephritis, Hereditary pathology, Nephritis, Hereditary therapy, Renal Insufficiency diagnosis, Renal Insufficiency pathology, Renal Insufficiency therapy, Collagen Type IV genetics, Genetic Association Studies, Nephritis, Hereditary genetics, Renal Insufficiency genetics

Abstract

Early initiation of therapy in patients with Alport syndrome (AS) slows down renal failure by many years. Genotype-phenotype correlations propose that the location and character of the individual's variant correlate with the renal outcome and any extra renal manifestations. In-depth clinical and genetic data of 60/62 children who participated in the EARLY PRO-TECT Alport trial were analyzed. Genetic variants were interpreted according to current guidelines and criteria. Genetically solved patients with X-linked inheritance were then classified according to the severity of their COL4A5 variant into less-severe, intermediate, and severe groups and disease progress was compared. Almost 90% of patients were found to carry (likely) pathogenic variants and classified as genetically solved cases. Patients in the less-severe group demonstrated a borderline significant difference in disease progress compared to those in the severe group (p = 0.05). While having only limited power according to its sample size, an obvious strength is the precise clinical and genetic data of this well ascertained cohort. As in published data differences in clinical progress were shown between patients with COL4A5 less-severe and severe variants. Therefore, clinical and segregational data are important for variant (re)classification. Genetic testing should be mandatory allowing early diagnosis and therapy of AS., (© 2020 The Authors. Clinical Genetics published by John Wiley & Sons Ltd.)

Published

2021

12. Novel Biallelic CTSD Gene Variants Cause Late-Onset Ataxia and Retinitis Pigmentosa.

Author

Regensburger M, Minakaki G, Kettwig M, Huchzermeyer C, Eisenhut F, Haack TB, Kohl Z, and Winkler J

Subjects

Ataxia genetics, Cathepsin D, Humans, Pedigree, Retinitis Pigmentosa genetics

Published

2020

13. Immune Sensing of Synthetic, Bacterial, and Protozoan RNA by Toll-like Receptor 8 Requires Coordinated Processing by RNase T2 and RNase 2.

Author

Ostendorf T, Zillinger T, Andryka K, Schlee-Guimaraes TM, Schmitz S, Marx S, Bayrak K, Linke R, Salgert S, Wegner J, Grasser T, Bauersachs S, Soltesz L, Hübner MP, Nastaly M, Coch C, Kettwig M, Roehl I, Henneke M, Hoerauf A, Barchet W, Gärtner J, Schlee M, Hartmann G, and Bartok E

Subjects

CRISPR-Cas Systems, Cell Line, Endoribonucleases immunology, Erythrocytes immunology, Erythrocytes parasitology, Escherichia coli chemistry, Escherichia coli immunology, Gene Editing methods, Humans, Listeria monocytogenes chemistry, Listeria monocytogenes immunology, Monocytes microbiology, Monocytes parasitology, Neutrophils microbiology, Neutrophils parasitology, Plasmodium falciparum chemistry, Plasmodium falciparum immunology, Primary Cell Culture, RNA Stability, RNA, Bacterial immunology, RNA, Protozoan immunology, Serratia marcescens chemistry, Serratia marcescens immunology, Staphylococcus aureus chemistry, Staphylococcus aureus immunology, Streptococcus chemistry, Streptococcus immunology, THP-1 Cells, Toll-Like Receptor 8 immunology, Endoribonucleases metabolism, Monocytes immunology, Neutrophils immunology, RNA, Bacterial metabolism, RNA, Protozoan metabolism, Toll-Like Receptor 8 metabolism

Abstract

Human toll-like receptor 8 (TLR8) activation induces a potent T helper-1 (Th1) cell response critical for defense against intracellular pathogens, including protozoa. The receptor harbors two distinct binding sites, uridine and di- and/or trinucleotides, but the RNases upstream of TLR8 remain poorly characterized. We identified two endolysosomal endoribonucleases, RNase T2 and RNase 2, that act synergistically to release uridine from oligoribonucleotides. RNase T2 cleaves preferentially before, and RNase 2 after, uridines. Live bacteria, P. falciparum-infected red blood cells, purified pathogen RNA, and synthetic oligoribonucleotides all required RNase 2 and T2 processing to activate TLR8. Uridine supplementation restored RNA recognition in RNASE2 -/- or RNASET2 -/- but not RNASE2 -/- RNASET2 -/- cells. Primary immune cells from RNase T2-hypomorphic patients lacked a response to bacterial RNA but responded robustly to small-molecule TLR8 ligands. Our data identify an essential function of RNase T2 and RNase 2 upstream of TLR8 and provide insight into TLR8 activation., Competing Interests: Declaration of Interests W.B. is an employee of IFM Therapeutics. The other authors declare no competing interests., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

14. Mesenchymal Hamartoma of the Liver and DICER1 Syndrome.

Author

Apellaniz-Ruiz M, Segni M, Kettwig M, Glüer S, Pelletier D, Nguyen VH, Wagener R, López C, Muchantef K, Bouron-Dal Soglio D, Sabbaghian N, Wu MK, Zannella S, Fabian MR, Siebert R, Menke J, Priest JR, and Foulkes WD

Subjects

Child, Preschool, Female, Genetic Predisposition to Disease, Hamartoma diagnostic imaging, Hamartoma pathology, Humans, Liver diagnostic imaging, Liver pathology, Liver Diseases diagnostic imaging, Liver Diseases pathology, Male, Mesoderm, Pedigree, Phenotype, Chromosomes, Human, Pair 19, DEAD-box RNA Helicases genetics, Germ-Line Mutation, Hamartoma genetics, Liver Diseases genetics, MicroRNAs metabolism, Neoplastic Syndromes, Hereditary genetics, Ribonuclease III genetics

Abstract

Mesenchymal hamartoma of the liver (MHL) is a benign tumor affecting children that is characterized by a primitive myxoid stroma with cystically dilated bile ducts. Alterations involving chromosome 19q13 are a recurrent underlying cause of MHL; these alterations activate the chromosome 19 microRNA cluster (C19MC). Other cases remain unexplained. We describe two children with MHLs that harbored germline DICER1 pathogenic variants. Analysis of tumor tissue from one of the children revealed two DICER1 "hits." Mutations in DICER1 dysregulate microRNAs, mimicking the effect of the activation of C19MC. Our data suggest that MHL is a new phenotype of DICER1 syndrome. (Funded by the Canadian Institutes of Health Research and others.)., (Copyright © 2019 Massachusetts Medical Society.)

Published

2019

15. Kidney Injury by Variants in the COL4A5 Gene Aggravated by Polymorphisms in Slit Diaphragm Genes Causes Focal Segmental Glomerulosclerosis.

Author

Frese J, Kettwig M, Zappel H, Hofer J, Gröne HJ, Nagel M, Sunder-Plassmann G, Kain R, Neuweiler J, and Gross O

Subjects

Acute Kidney Injury genetics, Adult, Child, Child, Preschool, Female, Genetic Predisposition to Disease, Glomerulosclerosis, Focal Segmental complications, Hemizygote, Heterozygote, Humans, Infant, Male, Mutation, Pedigree, Acute Kidney Injury etiology, Collagen Type IV genetics, Glomerulosclerosis, Focal Segmental genetics, Intracellular Signaling Peptides and Proteins genetics, Membrane Proteins genetics, Nephritis, Hereditary genetics, Polymorphism, Single Nucleotide

Abstract

Kidney injury due to focal segmental glomerulosclerosis (FSGS) is the most common primary glomerular disorder causing end-stage renal disease. Homozygous mutations in either glomerular basement membrane or slit diaphragm genes cause early renal failure. Heterozygous carriers develop renal symptoms late, if at all. In contrast to mutations in slit diaphragm genes, hetero- or hemizygous mutations in the X-chromosomal COL4A5 Alport gene have not yet been recognized as a major cause of kidney injury by FSGS. We identified cases of FSGS that were unexpectedly diagnosed: In addition to mutations in the X-chromosomal COL4A5 type IV collagen gene, nephrin and podocin polymorphisms aggravated kidney damage, leading to FSGS with ruptures of the basement membrane in a toddler and early renal failure in heterozygous girls. The results of our case series study suggest a synergistic role for genes encoding basement membrane and slit diaphragm proteins as a cause of kidney injury due to FSGS. Our results demonstrate that the molecular genetics of different players in the glomerular filtration barrier can be used to evaluate causes of kidney injury. Given the high frequency of X-chromosomal carriers of Alport genes, the analysis of genes involved in the organization of podocyte architecture, the glomerular basement membrane, and the slit diaphragm will further improve our understanding of the pathogenesis of FSGS and guide prognosis of and therapy for hereditary glomerular kidney diseases.

Published

2019

16. Cathepsin D Polymorphism C224T in Childhood-Onset Neurodegenerative Disorders: No Impact for Childhood Dementia.

Author

Kettwig M, Ohlenbusch A, Jung K, Steinfeld R, and Gärtner J

Abstract

Compromised lysosomal functioning has been identified as a major risk factor for neurodegenerative disorders such as Alzheimer's and Parkinson's diseases. Furthermore, the association between a defined cathepsin D ( CTSD ) polymorphism and a higher risk of sporadic Alzheimer's disease has been established for particular populations. Here, we analyzed 189 children with rare neurodegenerative disease for carrying the T-allele by polymerase chain reaction-restriction fragment length polymorphism. We found no statistical differences in genotype and allele frequencies between the neurodegenerative group and European descent participants of genetic studies using the Cochran-Armitage's trend test. In contrast to adult-onset neurodegenerative diseases, analysis of clinical datasets of children carrying the T-allele did not demonstrate differences to the general disease group.

Published

2018

17. Compound heterozygous variants in PGAP1 causing severe psychomotor retardation, brain atrophy, recurrent apneas and delayed myelination: a case report and literature review.

Author

Kettwig M, Elpeleg O, Wegener E, Dreha-Kulaczewski S, Henneke M, Gärtner J, and Huppke P

Subjects

Atrophy diagnostic imaging, Brain diagnostic imaging, Brain Diseases pathology, Brain Diseases physiopathology, Child, Preschool, Developmental Disabilities physiopathology, Humans, Magnetic Resonance Imaging, Male, Mutation, Neuroimaging, Twins, Dizygotic genetics, Twins, Dizygotic psychology, Apnea genetics, Atrophy pathology, Brain pathology, Brain Diseases genetics, Developmental Disabilities genetics, Membrane Proteins genetics, Myelin Sheath pathology, Phosphoric Monoester Hydrolases genetics

Abstract

Background: Mutations in proteins involved in the glycosylphosphatidylinositol anchor biosynthesis and remodeling pathway are associated with autosomal recessive forms of intellectual disability. Recently mutations in the PGAP1 gene that codes for PGAP1, a protein localized in the endoplasmic reticulum responsible for the first step of the remodeling of glycosylphosphatidylinositol was linked to a disorder characterized by psychomotor retardation and facial dysmorphism. Whole exome sequencing (WES) was performed in siblings with severely delayed myelination and psychomotor retardation. Mutations in PGAP1 were confirmed by Sanger sequencing and RNA analysis. A literature search was performed to describe the emerging phenotype of PGAP1 related disease., Case Presentation: WES resulted in the detection of two novel compound heterozygous mutations in PGAP1, one base pair insertion leading to a frame shift c.334&#95;335InsA (p.A112fs) and a splice site mutation leading to exon skipping c.G1173C (p.L391L). A symptom not described in PGAP1 related disorder before but prominent in the siblings were recurrent apnea especially during sleep that persisted at least until age 2 years. Sequential cerebral MRI at age one and two year(s) respectively revealed frontal accentuated brain atrophy and significantly delayed myelination., Conclusion: We report siblings with two novel mutations in PGAP1. Other that the common symptoms related to PGAP1 mutations including non-progressive psychomotor retardation, neonatal feeding problems, microcephaly and brain atrophy these patients displayed severely delayed myelination and recurrent apneas thereby widing the clinical spectrum associated with such mutations.

Published

2016

18. From ventriculomegaly to severe muscular atrophy: expansion of the clinical spectrum related to mutations in AIFM1.

Author

Kettwig M, Schubach M, Zimmermann FA, Klinge L, Mayr JA, Biskup S, Sperl W, Gärtner J, and Huppke P

Subjects

Adolescent, Adult, Ataxia genetics, Ataxia pathology, Child, Child, Preschool, Family Health, Humans, Infant, Infant, Newborn, Male, Muscular Diseases genetics, Muscular Diseases pathology, Mutant Proteins genetics, Mutant Proteins metabolism, Mutation, Missense, Neurodegenerative Diseases genetics, Neurodegenerative Diseases pathology, Young Adult, Apoptosis Inducing Factor genetics, Apoptosis Inducing Factor metabolism, Genetic Diseases, Inborn genetics, Genetic Diseases, Inborn pathology, Mitochondrial Diseases genetics, Mitochondrial Diseases pathology

Abstract

The apoptosis-inducing factor (AIF) functions as a FAD-dependent NADH oxidase in mitochondria. Upon apoptotic stimulation it is released from mitochondria and migrates to the nucleus where it induces chromatin condensation and DNA fragmentation. So far mutations in AIFM1, a X-chromosomal gene coding for AIF, have been described in three families with 11 affected males. We report here on a further patient thereby expanding the clinical and mutation spectrum. In addition, we review the known phenotypes related to AIFM1 mutations. The clinical course in the male patient described here was characterized by phases with rapid deterioration and long phases without obvious progression of disease. At age 2.5 years he developed hearing loss and severe ataxia and at age 10 years muscle wasting, swallowing difficulties, respiratory insufficiency and external opthamoplegia. By next generation sequencing of whole exome we identified a hemizygous missense mutation in the AIFM1 gene, c.727G>T (p.Val243Leu) affecting a highly conserved residue in the FAD-binding domain. Summarizing what is known today, mutations in AIFM1 are associated with a progressive disorder with myopathy, ataxia and neuropathy. Severity varies greatly even within one family with onset of symptoms between birth and adolescence. 3 of 12 patients died before age 5 years while others were still able to walk during young adulthood. Less frequent symptoms were hearing loss, seizures and psychomotor regression. Results from clinical chemistry, brain imaging and muscle biopsy were unspecific and inconsistent., (Copyright © 2015. Published by Elsevier B.V.)

Published

2015

19. Initial insight into the function of the lysosomal 66.3 kDa protein from mouse by means of X-ray crystallography.

Author

Lakomek K, Dickmanns A, Kettwig M, Urlaub H, Ficner R, and Lübke T

Subjects

Animals, Bacterial Proteins chemistry, Catalytic Domain, Cell Line, Tumor, Crystallography, X-Ray, Glycosylation, Humans, Mice, Models, Molecular, Penicillin Amidase chemistry, Protein Structure, Secondary, Protein Structure, Tertiary, Structural Homology, Protein, Glycoproteins chemistry, Glycoproteins metabolism, Protein Processing, Post-Translational, Proteins chemistry, Proteins metabolism

Abstract

Background: The lysosomal 66.3 kDa protein from mouse is a soluble, mannose 6-phosphate containing protein of so far unknown function. It is synthesized as a glycosylated 75 kDa precursor that undergoes limited proteolysis leading to a 28 kDa N- and a 40 kDa C-terminal fragment., Results: In order to gain insight into the function and the post-translational maturation process of the glycosylated 66.3 kDa protein, three crystal structures were determined that represent different maturation states. These structures demonstrate that the 28 kDa and 40 kDa fragment which have been derived by a proteolytic cleavage remain associated. Mass spectrometric analysis confirmed the subsequent trimming of the C-terminus of the 28 kDa fragment making a large pocket accessible, at the bottom of which the putative active site is located. The crystal structures reveal a significant similarity of the 66.3 kDa protein to several bacterial hydrolases. The core alphabetabetaalpha sandwich fold and a cysteine residue at the N-terminus of the 40 kDa fragment (C249) classify the 66.3 kDa protein as a member of the structurally defined N-terminal nucleophile (Ntn) hydrolase superfamily., Conclusion: Due to the close resemblance of the 66.3 kDa protein to members of the Ntn hydrolase superfamily a hydrolytic activity on substrates containing a non-peptide amide bond seems reasonable. The structural homology which comprises both the overall fold and essential active site residues also implies an autocatalytic maturation process of the lysosomal 66.3 kDa protein. Upon the proteolytic cleavage between S248 and C249, a deep pocket becomes solvent accessible, which harbors the putative active site of the 66.3 kDa protein.

Published

2009