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1. OP17 IBD ulcers are characterized by bioactive interleukin-1 and transcriptomic hallmarks of stromal cell state reprogramming

Author

Mitsialis, V, primary, Losa, M, additional, Field, M, additional, Collen, L, additional, Barends, J, additional, Ringel, A, additional, Bresnahan, M, additional, Yang, J, additional, Tumminkatti, R, additional, Sveen, M, additional, Bearup, R, additional, Kotlarz, D, additional, Klein, C, additional, Argmann, C, additional, Schadt, E, additional, Muise, A, additional, Thiagarajah, J, additional, Eran, A, additional, Horwitz, B, additional, and Snapper, S, additional

Published
2024
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3. Clinical genomics for the diagnosis of monogenic forms of inflammatory bowel disease

Author

Uhlig, H, Charbit-Henrion, F, Kotlarz, D, Shouval, D, Schwerd, T, Strisciuglio, C, de Ridder, L, van Limbergen, J, Macchia, L, Snapper, SB, Rummele, FM, Wilson, DC, Travis, SPL, Griffiths, AM, Turner, D, Klein, C, Muise, AM, Russell, RK, and ESPGHAN, Paediatric IBD Porto Group of

Abstract

Background: It is important to identify patients with monogenic IBD since management may differ from classical IBD. In this position statement we formulate recommendations for the use of genomics in evaluating potential monogenic causes of IBD across age groups. Methods: The consensus included paediatric IBD specialists from the Paediatric IBD Porto group of the European Society of Paediatric Gastroenterology, Hepatology and Nutrition (ESPGHAN) and specialists from several monogenic IBD research consortia. We defined key topics and performed a systematic literature review to cover indications, technologies (targeted panel, exome and genome sequencing), gene panel setup, cost-effectiveness of genetic screening, and requirements for the clinical care setting. We developed recommendations that were voted upon by all authors and Porto group members (32 voting specialists). Results: We recommend next-generation DNA sequencing technologies to diagnose monogenic causes of IBD in routine clinical practice embedded in a setting of multidisciplinary patient care. Routine genetic screening is not recommended for all IBD patients. Genetic testing should be considered depending on age of IBD onset (infantile IBD, very early onset IBD, paediatric or young adult IBD) and further criteria such as family history, relevant comorbidities and extraintestinal manifestations. Genetic testing is also recommended in advance of hematopoietic stem cell transplantation. We develop a diagnostic algorithm that includes a gene panel of seventy-five monogenic IBD genes. Considerations are provided also for low resource countries. Summary: Genomic technologies should be considered an integral part of patient care to investigate patients at risk for monogenic forms of IBD.

Published
2021

4. Congenital disorders of glycosylation with defective fucosylation

Author

Hüllen, A., Falkenstein, K., Weigel, C., Huidekoper, H., Naumann-Bartsch, N., Spenger, J., Feichtinger, R.G., Schaefers, J., Frenz, S., Kotlarz, D., Momen, T., Khoshnevisan, R., Riedhammer, K.M., Santer, R., Herget, T., Rennings, A.J., Lefeber, D.J., Mayr, J.A., Thiel, C, Wortmann, S.B., Hüllen, A., Falkenstein, K., Weigel, C., Huidekoper, H., Naumann-Bartsch, N., Spenger, J., Feichtinger, R.G., Schaefers, J., Frenz, S., Kotlarz, D., Momen, T., Khoshnevisan, R., Riedhammer, K.M., Santer, R., Herget, T., Rennings, A.J., Lefeber, D.J., Mayr, J.A., Thiel, C, and Wortmann, S.B.

Abstract

Item does not contain fulltext, Fucosylation is essential for intercellular and intracellular recognition, cell-cell interaction, fertilization, and inflammatory processes. Only five types of congenital disorders of glycosylation (CDG) related to an impaired fucosylation have been described to date: FUT8-CDG, FCSK-CDG, POFUT1-CDG SLC35C1-CDG, and the only recently described GFUS-CDG. This review summarizes the clinical findings of all hitherto known 25 patients affected with those defects with regard to their pathophysiology and genotype. In addition, we describe five new patients with novel variants in the SLC35C1 gene. Furthermore, we discuss the efficacy of fucose therapy approaches within the different defects.

Published
2021

7. Early-onset inflammatory bowel disease caused by mutant IL10 receptor

Author

Segal A W, Shah N, Koletzko S, Salzer U, Baumann U, Woellner C, Nustede R, Lacher M, Kreipe H, Sauer M, Sykora K W, Pfeifer D, Hätscher N, Murugan D, Allroth A, Diestelhorst J, Perro M, Noyan F, Schäffer A A, Gertz E M, Boztug K, Kotlarz D, Glocker E O, Sauerbrey A, Buderus S, Snapper S B, Grimbacher B, and Klein C

Subjects
Medicine
Published
2010
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8. Mutations in tetratricopeptide repeat domain 7A result in a severe form of very early onset inflammatory bowel disease

Author

Avitzur, Y, Guo, C, Mastropaolo, LA, Bahrami, E, Chen, H, Zhao, Z, Elkadri, A, Dhillon, S, Murchie, R, Fattouh, R, Huynh, H, Walker, JL, Wales, PW, Cutz, E, Kakuta, Y, Dudley, J, Kammermeier, J, Powrie, F, Shah, N, Walz, C, Nathrath, M, Kotlarz, D, Puchaka, J, Krieger, JR, Racek, T, Kirchner, T, Walters, TD, Brumell, JH, Griffiths, AM, Rezaei, N, Rashtian, P, Najafi, M, Monajemzadeh, M, Pelsue, S, McGovern, DPB, Uhlig, HH, Schadt, E, Klein, C, Snapper, SB, and Muise, AM

Subjects
Male, Candidate gene, DNA Mutational Analysis, Apoptosis, medicine.disease_cause, Compound heterozygosity, Severity of Illness Index, chemistry.chemical_compound, Exome, Lymphocytes, Age of Onset, 1-Phosphatidylinositol 4-Kinase, Exome sequencing, Enterocolitis, Mutation, Gastroenterology, Prognosis, Pedigree, Phenotype, Child, Preschool, Female, RNA Interference, medicine.symptom, Protein Binding, Signal Transduction, Heterozygote, Intestinal Atresia, Biology, Transfection, Article, Cell Line, medicine, Cell Adhesion, Humans, Genetic Predisposition to Disease, Phosphatidylinositol, Genetic Association Studies, Severe combined immunodeficiency, Hepatology, Infant, Newborn, Infant, Proteins, medicine.disease, Inflammatory Bowel Diseases, Enterocytes, chemistry, Immunology
Abstract

Background and Aims Very early onset inflammatory bowel diseases (VEOIBD), including infant disorders, are a diverse group of diseases found in children younger than 6 years of age. They have been associated with several gene variants. Our aim was to identify the genes that cause VEOIBD. Methods We performed whole exome sequencing of DNA from 1 infant with severe enterocolitis and her parents. Candidate gene mutations were validated in 40 pediatric patients and functional studies were carried out using intestinal samples and human intestinal cell lines. Results We identified compound heterozygote mutations in the Tetratricopeptide repeat domain 7 (TTC7A) gene in an infant from non-consanguineous parents with severe exfoliative apoptotic enterocolitis; we also detected TTC7A mutations in 2 unrelated families, each with 2 affected siblings. TTC7A interacts with EFR3 homolog B to regulate phosphatidylinositol 4-kinase at the plasma membrane. Functional studies demonstrated that TTC7A is expressed in human enterocytes. The mutations we identified in TTC7A result in either mislocalization or reduced expression of TTC7A. Phosphatidylinositol 4-kinase was found to co-immunoprecipitate with TTC7A; the identified TTC7A mutations reduced this binding. Knockdown of TTC7A in human intestinal-like cell lines reduced their adhesion, increased apoptosis, and decreased production of phosphatidylinositol 4-phosphate. Conclusions In a genetic analysis, we identified loss of function mutations in TTC7A in 5 infants with VEOIBD. Functional studies demonstrated that the mutations cause defects in enterocytes and T cells that lead to severe apoptotic enterocolitis. Defects in the phosphatidylinositol 4-kinase-TTC7A-EFR3 homolog B pathway are involved in the pathogenesis of VEOIBD. © 2014 by the AGA Institute.

Published
2016

10. Il-10 Receptor deficiency – discovery of novel mutations and rescue by allogeneic hematopoietic stem cell transplantation

Author

Kotlarz, D, Beier, R, Murugan, D, Diestelhorst, J, Jensen, O, Boztug, K, Kreipe, H, Pfister, Ed, Baumann, U, Sauerbrey, A, Buderus, S, Güngör, T, Enninger, A, Koda, Ykl, Guariso, Graziella, Weiss, B, Corbacioglu, S, Socha, P, Uslu, N, Metin, A, Wahbeh, Gt, Husain, K, Ramadan, D, AI HERZ, W, Grimbacher, B, Sauer, M, Sykora, Kw, Koletzko, S, and Klein, C.

Published
2012

11. Inherited biallelic CSF3R mutations in severe congenital neutropenia

Author

Triot, A. (Alexa), Järvinen, P.M. (Päivi), Arostegui, J.I. (Juan), Murugan, D. (Dhaarini), Kohistani, N. (Naschla), Díaz, J.A. (José Ángel), Racek, T. (Tomas), Puchałka, J. (Jacek), Gertz, M. (Morie), Schäffer, A.A. (Alejandro), Kotlarz, D. (Daniel), Pfeifer, D. (Dietmar), De Heredia Rubio, C.D. (Cristina Díaz), Ozdemir, M.A. (Mehmet Akif), Patiroglu, T. (Turkan), Karakukcu, M. (Musa), De Toledo Codina, J.S. (José Sánchez), Yagüe, J. (Jordi), Touw, I.P. (Ivo), Unal, E. (Ekrem), Klein, C. (Christoph), Triot, A. (Alexa), Järvinen, P.M. (Päivi), Arostegui, J.I. (Juan), Murugan, D. (Dhaarini), Kohistani, N. (Naschla), Díaz, J.A. (José Ángel), Racek, T. (Tomas), Puchałka, J. (Jacek), Gertz, M. (Morie), Schäffer, A.A. (Alejandro), Kotlarz, D. (Daniel), Pfeifer, D. (Dietmar), De Heredia Rubio, C.D. (Cristina Díaz), Ozdemir, M.A. (Mehmet Akif), Patiroglu, T. (Turkan), Karakukcu, M. (Musa), De Toledo Codina, J.S. (José Sánchez), Yagüe, J. (Jordi), Touw, I.P. (Ivo), Unal, E. (Ekrem), and Klein, C. (Christoph)

Abstract

Severe congenital neutropenia (SCN) is characterized by low numbers of peripheral neutrophil granulocytes and a predisposition to life-threatening bacterial infections. We describe a novel genetic SCN type in 2 unrelated families associated with recessively inherited loss-of-function mutations in CSF3R, encoding the granulocyte colony-stimulating factor (G-CSF) receptor. Family A, with 3 affected children, carried a homozygous missense mutation (NM-000760.3:c.922C>T, NP-000751.1:p.Arg308Cys), which resulted in perturbed N-glycosylation and aberrant localization to the cell surface. Family B, with 1 affected infant, carried compound heterozygous deletions provoking frameshifts and premature stop codons (NM-000760.3:c.948-963del, NP-000751.1:p. Gly316fsTer322 and NM-000760.3:c.1245del, NP-000751.1:p.Gly415fsTer432). Despite peripheral SCN, all patients had morphologic evidence of full myeloid cell maturation in bone marrow. None of the patients responded to treatment with recombinant human G-CSF. Our study highlights the genetic and morphologic SCN variability and provides evidence both for functional importance and redundancy of G-CSF receptor-mediated signaling in human granulopoiesis.

Published
2014
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15. Ex vivo expanded hematopoietic progenitor cells improve cardiac function after myocardial infarction: role of beta-catenin transduction and cell dose

Author

Templin, C, Kotlarz, D, Faulhaber, J, Schnabel, S, Grote, K, Salguero, G, Luchtefeld, M, Hiller, K H, Jakob, P, Naim, H Y, Schieffer, B, Hilfiker-Kleiner, D, Landmesser, U, Limbourg, F P, Drexler, H, Templin, C, Kotlarz, D, Faulhaber, J, Schnabel, S, Grote, K, Salguero, G, Luchtefeld, M, Hiller, K H, Jakob, P, Naim, H Y, Schieffer, B, Hilfiker-Kleiner, D, Landmesser, U, Limbourg, F P, and Drexler, H

Abstract

Cell-based therapy after myocardial infarction (MI) is a promising therapeutic option but the relevant cell subsets and dosage requirements are poorly defined. We hypothesized that cell therapy for myocardial infarction is improved by ex vivo expansion and high-dose transplantation of defined hematopoietic progenitor cells (HPCs). Since beta-catenin promotes self-renewal of stem cells we evaluated the therapeutic efficacy of beta-catenin-mediated ex vivo expansion of mouse HPCs in a mouse model of myocardial ischemia/reperfusion followed by intraarterial cell delivery. The impact of cell dose was determined by comparing a low-dose (LD, 5 x 10(5) cells) vs. a high-dose (HD, 1 x 10(7) cells) cell transplantation regimen of beta-catenin-HPCs. The impact of beta-catenin modification of HPCs was determined by comparing control-transduced HPCs (GFP-HPCs) vs. transgenic beta-catenin-HPCs. HD beta-catenin-HPCs significantly improved LV function and end-systolic and end-diastolic dimensions as compared to saline and LD beta-catenin-HPCs. Furthermore, while treatment with HD GFP-HPC resulted in a modest cardiac improvement the application of beta-catenin-HPCs was superior, resulting in a significant improvement in EF, FS and LVESD over saline and control GFP-HPC treatment. Although myocardial engraftment of HPCs was only transient, as determined by cell quantification after dye labeling, beta-catenin-HPC treatment significantly decreased infarct size, reduced cardiomyocyte apoptosis and increased capillary angiogenesis in vitro and in vivo. Ex vivo expanded HPCs improve cardiac function and remodeling post MI in a cell number- and beta-catenin-dependent manner.

Published
2008

16. Early-onset inflammatory bowel disease caused by mutant IL10 receptor

Author

Glocker, E O, primary, Kotlarz, D, additional, Boztug, K, additional, Gertz, E M, additional, Schäffer, A A, additional, Noyan, F, additional, Perro, M, additional, Diestelhorst, J, additional, Allroth, A, additional, Murugan, D, additional, Hätscher, N, additional, Pfeifer, D, additional, Sykora, K W, additional, Sauer, M, additional, Kreipe, H, additional, Lacher, M, additional, Nustede, R, additional, Woellner, C, additional, Baumann, U, additional, Salzer, U, additional, Koletzko, S, additional, Shah, N, additional, Segal, A W, additional, Sauerbrey, A, additional, Buderus, S, additional, Snapper, S B, additional, Grimbacher, B, additional, and Klein, C, additional

Published
2010
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20. Modulated expression of promoters containing upstream curved DNA sequences by the <em>Escherichia coli</em> nucleoid protein H-NS.

Author

Zuber, F., Kotlarz, D., Rimsky, S., and Buc, H.

Subjects
GENES, DNA, HEREDITY, MOLECULAR genetics, NUCLEIC acids
Abstract

Replacement of the CRP-binding site of the gal control region by curved sequences can lead to the restoration of promoter strength in vivo. One curved sequence called 5A6A, however, failed to do so. The gene hns exerts a strong negative control on the resulting 5A6A gal promoter as well as on the distant bla promoter, specifically in a 5A6A gal context. The product of this gene, H-NS, displays a better affinity for this particular insert compared to other curved sequences. Mechanisms by which H-NS may repress promoters both at short and long distances from a favoured binding site are discussed. [ABSTRACT FROM AUTHOR]

Published
1994
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21. Synthetic curved DNA sequences can act as transcriptional activators in Escherichia coli.

Author

Bracco, L., Kotlarz, D., Kolb, A., Diekmann, S., and Buc, H.

Abstract

Can a transcriptional activator known to bend DNA be functionally replaced by a sequence‐directed bend in Escherichia coli? To investigate this question, a partially truncated promoter was used, deleted of its ‐35 region and of its CRP binding site, leaving only two Pribnow boxes as functional elements. Synthetic and naturally occurring curved DNA sequences introduced upstream from these elements could restore transcription at either one of the two natural starts. Some of these hybrid promoters turned out to be more efficient than the CRP activated wild‐type gal promoter in vivo. Control experiments performed with very similar sequences devoid of any curvature produced weak promoters only. Minimal changes in the location of the centre of curvature or perturbation in the amount of curvature strongly affected the level of expression. No significant stimulation of transcription could be detected in vitro. Furthermore, both gal P1 and P2 starts could be activated in vivo but also in vitro via a properly positioned CRP binding site. This partial analogy suggests that bending induced by the cAMP‐CRP complex upon binding to its site may be biologically relevant to the mechanism of transcriptional activation.

Published
1989
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22. Variations of intramolecular ligation rates allow the detection of protein‐induced bends in DNA.

Author

Kotlarz, D., Fritsch, A., and Buc, H.

Abstract

A method requiring minute amounts of DNA and protein is proposed for the detection of DNA bending in solution. Local bending, induced by the binding of a protein at its stereospecific site, must increase the probability of circularization of short DNA fragments and hence the rate of formation of the corresponding minicircles. This effect should be highly sensitive to the location of the protein‐binding site on the DNA fragment. Simple controls allow other possible interpretations to be ruled out. The deformation due to the cyclic AMP receptor protein when it interacts with its stereospecific site at the lactose control region is studied by this method. It is shown in this case that untwisting is negligible and bending significant. Further measurements are required to assess the actual value of the radius of curvature of the DNA double helix in this complex.

Published
1986
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23. Comparison of the binding sites for the Escherichia coli cAMP receptor protein at the lactose and galactose promoters.

Author

Kolb, A., Busby, S., Herbert, M., Kotlarz, D., and Buc, H.

Abstract

Polyacrylamide gel electrophoresis has been used to visualise and quantitate complexes between the Escherichia coli cyclic AMP receptor protein (CRP) and DNA fragments containing the promoter region of either the E. coli galactose or lactose operons. We show that, although CRP binding to the gal fragment is weaker than binding to the lac fragment, in each case, stable complexes are formed between one dimer of CRP and one molecule of DNA. We have examined the effects of a series of deletions and point mutations in the gal promoter region on CRP binding. From the position of deletions and mutations which prevent the formation of stable complexes, we deduce the location and extent of the sequence at the CRP binding site. We show that it covers approximately the same length of sequence as the binding site at the lac promoter. Unlike the lac site, the gal site contains no palindromic sequence. We discuss the importance of symmetry in the sequence at CRP binding sites and the validity of CRP binding consensus sequences which have been proposed.

Published
1983
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24. Regulation of the amount and of the activity of phosphofructokinases and pyruvate kinases in Escherichia coli

Author

Kotlarz, D., Garreau, H., and Buc, H.

Abstract

Two isozymes of fructose-6-phosphate kinase and two isozymes of pyruvate kinase have been detected in Escherichia coliunder a wide variety of growth conditions. Their kinetic behavior has been characterized with respect to different effectors and substrates. The conclusions reached on one hand by Malcovati and Kornberg (Biochim. Biophys. Acta (1969) 178, 420–423), on the other hand by Fraenkel, Kotlarz and Buc (J. Biol. Chem. (1973) 248, 4865–4866) have been found to be true in aerobiosis as well as in anaerobiosis. The biosynthesis of the four proteins is sensitive to the nature of the carbon sources as well as to the shift from aerobic to anaerobic conditions. Kinetics of depression after a shift to anaerobiosis have been followed and found to be of the order of the doubling time.

Published
1975
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28. Clinical Genomics for the Diagnosis of Monogenic Forms of Inflammatory Bowel Disease: A Position Paper From the Paediatric IBD Porto Group of European Society of Paediatric Gastroenterology, Hepatology and Nutrition

Author

Simon Travis, Scott B. Snapper, Tobias Schwerd, Aleixo M. Muise, Dan Turner, Christoph Klein, Fabienne Charbit-Henrion, Caterina Strisciuglio, Frank M. Ruemmele, Richard K Russell, Marina Macchi, Johan L van Limbergen, David C. Wilson, Anne M. Griffiths, Dror S. Shouval, Lissy de Ridder, Daniel Kotlarz, Holm H. Uhlig, Paediatric Gastroenterology, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, APH - Digital Health, APH - Health Behaviors & Chronic Diseases, Pediatrics, Uhlig, H. H., Charbit-Henrion, F., Kotlarz, D., Shouval, D. S., Schwerd, T., Strisciuglio, C., de Ridder, L., van Limbergen, J., Macchi, M., Snapper, S. B., Ruemmele, F. M., Wilson, D. C., Travis, S. P. L., Griffiths, A. M., Turner, D., Klein, C., Muise, A. M., and Russell, R. K.

Subjects
medicine.medical_specialty, very early-onset inflammatory bowel disease, MEDLINE, primary immunodeficiency, digestive system, Article, ulcerative coliti, 03 medical and health sciences, 0302 clinical medicine, 030225 pediatrics, Internal medicine, Medicine, Humans, Family history, Young adult, Intensive care medicine, Child, Exome, Genetic testing, medicine.diagnostic_test, business.industry, Gastroenterology, Genomics, Hepatology, Colitis, Inflammatory Bowel Diseases, digestive system diseases, Crohn's disease, Systematic review, Pediatrics, Perinatology and Child Health, Genomic, Position paper, 030211 gastroenterology & hepatology, genetic, business, Child Nutritional Physiological Phenomena, exome sequencing, Coliti, Human
Abstract

BACKGROUND: It is important to identify patients with monogenic IBD as management may differ from classical IBD. In this position statement we formulate recommendations for the use of genomics in evaluating potential monogenic causes of IBD across age groups. METHODS: The consensus included paediatric IBD specialists from the Paediatric IBD Porto group of the European Society of Paediatric Gastroenterology, Hepatology and Nutrition (ESPGHAN) and specialists from several monogenic IBD research consortia. We defined key topics and performed a systematic literature review to cover indications, technologies (targeted panel, exome and genome sequencing), gene panel setup, cost-effectiveness of genetic screening, and requirements for the clinical care setting. We developed recommendations that were voted upon by all authors and Porto group members (32 voting specialists). RESULTS: We recommend next-generation DNA-sequencing technologies to diagnose monogenic causes of IBD in routine clinical practice embedded in a setting of multidisciplinary patient care. Routine genetic screening is not recommended for all IBD patients. Genetic testing should be considered depending on age of IBD-onset (infantile IBD, very early-onset IBD, paediatric or young adult IBD), and further criteria, such as family history, relevant comorbidities, and extraintestinal manifestations. Genetic testing is also recommended in advance of hematopoietic stem cell transplantation. We developed a diagnostic algorithm that includes a gene panel of 75 monogenic IBD genes. Considerations are provided also for low resource countries. CONCLUSIONS: Genomic technologies should be considered an integral part of patient care to investigate patients at risk for monogenic forms of IBD.

Published
2021

29. The E3 ubiquitin ligase UBR5 interacts with TTC7A and may be associated with very early onset inflammatory bowel disease

Author

Scott B. Snapper, Qi Li, Christoph Klein, Neil Warner, Neel Dhingani, Sasha Jardine, Claudia Gonzaga-Jauregui, Daniel Kotlarz, Aleixo M. Muise, Conghui Guo, Jie Pan, Gabriella Leung, Víctor Manuel Navas-López, [Dhingani,N, Jardine,S, Muise,AM] Department of Biochemistry, Faculty of Medicine, University of Toronto, Toronto, ON, Canada. [Dhingani,N, Guo,C, Pan,J, Li,Q, Warner,N, Leung,G, Muise,AM] SickKids Infammatory Bowel Disease Centre, Research Institute, Hospital for Sick Children, Toronto, ON, Canada. [Kotlarz,D, Klein,C] Department of Pediatrics, Dr. Von Hauner Children’s Hospital, University Hospital, LMU Munich, Munich, Germany. [Gonzaga-Jauregui,C] Regeneron Genetics Center, Regeneron Pharmaceuticals Inc., Tarrytown, NY, USA. [Snapper,SB] Division of Gastroenterology, Hepatology and Nutrition, Boston Children’s Hospital, Harvard Medical School, Boston, MA, USA. [Navas-López,VM] Pediatric Gastroenterology and Nutrition Unit, IBIMA, Hospital Regional Universitario de Málaga, Málaga, Spain. [Muise,AM] Cell Biology Program, Research Institute, The Hospital for Sick Children, Toronto, ON, Canada. [Muise,AM] Department of Pediatrics, Institute of Medical Science, University of Toronto, Toronto, Canada. [Snapper,SB] Division of Gastroenterology, Brigham and Women’s Hospital, Boston, MA, USA., and AMM is funded by a Canada Research Chair (Tier 1) in Pediatric IBD, CIHR Foundation Grant and NIDDK (RC2DK118640) Grant. AMM, SBS, CK, DK are supported by the Leona M. and Harry B. Helmsley Charitable Trust. CK and DK are supported by the Collaborative Research Consortium SFB1054 project A05.

Subjects
0301 basic medicine, Male, Enfermedades inflamatorias del intestino, lcsh:Medicine, Compound heterozygosity, Inflammatory bowel disease, Diseases::Digestive System Diseases::Gastrointestinal Diseases::Intestinal Diseases::Inflammatory Bowel Diseases [Medical Subject Headings], Unión proteica, Organisms::Eukaryota::Animals::Chordata::Vertebrates::Mammals::Primates::Haplorhini::Catarrhini::Hominidae::Humans [Medical Subject Headings], 0302 clinical medicine, Age of Onset, lcsh:Science, Child, Immunodeficiency, Exome sequencing, Multidisciplinary, biology, Intestinal atresia, Gastroenterology, Phenomena and Processes::Chemical Phenomena::Biochemical Phenomena::Biochemical Processes::Signal Transduction [Medical Subject Headings], Chemicals and Drugs::Amino Acids, Peptides, and Proteins::Proteins [Medical Subject Headings], Colitis, 3. Good health, Ubiquitin ligase, Ubiquitin-protein ligases, Tetratricopeptide, 030220 oncology & carcinogenesis, Niño, Child, Preschool, Protein Binding, Signal Transduction, Cell biology, Ubiquitin-Protein Ligases, Check Tags::Male [Medical Subject Headings], Inflammatory bowel diseases, Article, Amino acid sequence, 03 medical and health sciences, Ubiquitina-proteína ligasas, Phenomena and Processes::Chemical Phenomena::Biochemical Phenomena::Biochemical Processes::Protein Binding [Medical Subject Headings], medicine, Chemicals and Drugs::Enzymes and Coenzymes::Enzymes::Ligases::Ubiquitin-Protein Ligase Complexes::Ubiquitin-Protein Ligases [Medical Subject Headings], Protein binding, Humans, Secuencia de aminoácidos, Amino Acid Sequence, Health Care::Health Care Quality, Access, and Evaluation::Quality of Health Care::Epidemiologic Factors::Age Factors::Age of Onset [Medical Subject Headings], Diseases::Digestive System Diseases::Gastrointestinal Diseases::Intestinal Diseases::Colonic Diseases::Colitis [Medical Subject Headings], Sequence Homology, Amino Acid, business.industry, lcsh:R, Proteins, medicine.disease, Inflammatory Bowel Diseases, 030104 developmental biology, Immunology, biology.protein, Phenomena and Processes::Chemical Phenomena::Biochemical Phenomena::Molecular Structure::Amino Acid Sequence [Medical Subject Headings], lcsh:Q, business, Persons::Persons::Age Groups::Child::Child, Preschool [Medical Subject Headings]
Abstract

Very early onset inflammatory bowel disease (VEOIBD) denotes children with onset of IBD before six years of age. A number of monogenic disorders are associated with VEOIBD including tetratricopeptide repeat domain 7A (TTC7A) deficiency. TTC7A-deficiency is characterized by apoptotic colitis in milder cases with severe intestinal atresia and immunodeficiency in cases with complete loss of protein. We used whole exome sequencing in a VEOIBD patient presenting with colitis characterized by colonic apoptosis and no identified known VEOIBD variants, to identify compound heterozygous deleterious variants in the Ubiquitin protein ligase E3 component N-recognin 5 (UBR5) gene. Functional studies demonstrated that UBR5 co-immunoprecipitates with the TTC7A and the UBR5 variants had reduced interaction between UBR5 and TTC7A. Together this implicates UBR5 in regulating TTC7A signaling in VEOIBD patients with apoptotic colitis.

Published
2019

32. Human ITGAV variants are associated with immune dysregulation, brain abnormalities, and colitis.

Author

Ghasempour S, Warner N, Guan R, Rodari MM, Ivanochko D, Whittaker Hawkins R, Marwaha A, Nowak JK, Liang Y, Mulder DJ, Stallard L, Li M, Yu DD, Pluthero FG, Batura V, Zhao M, Siddiqui I, Upton JEM, Hulst JM, Kahr WHA, Mendoza-Londono R, Charbit-Henrion F, Hoefsloot LH, Khiat A, Moreira D, Trindade E, Espinheira MDC, Pinto Pais I, Weerts MJA, Douben H, Kotlarz D, Snapper SB, Klein C, Dowling JJ, Julien JP, Joosten M, Cerf-Bensussan N, Freeman SA, Parlato M, van Ham TJ, and Muise AM

Subjects
Humans, Animals, Female, Male, Pedigree, Signal Transduction genetics, Transforming Growth Factor beta metabolism, Transforming Growth Factor beta genetics, Zebrafish genetics, Brain metabolism, Brain pathology, Colitis genetics, Colitis pathology, Colitis immunology
Abstract

Integrin heterodimers containing an Integrin alpha V subunit are essential for development and play critical roles in cell adhesion and signaling. We identified biallelic variants in the gene coding for Integrin alpha V (ITGAV) in three independent families (two patients and four fetuses) that either caused abnormal mRNA and the loss of functional protein or caused mistargeting of the integrin. This led to eye and brain abnormalities, inflammatory bowel disease, immune dysregulation, and other developmental issues. Mechanistically, the reduction of functional Integrin αV resulted in the dysregulation of several pathways including TGF-β-dependent signaling and αVβ3-regulated immune signaling. These effects were confirmed using immunostaining, RNA sequencing, and functional studies in patient-derived cells. The genetic deletion of itgav in zebrafish recapitulated patient phenotypes including retinal and brain defects and the loss of microglia in early development as well as colitis in juvenile zebrafish with reduced SMAD3 expression and transcriptional regulation. Taken together, the ITGAV variants identified in this report caused a previously unknown human disease characterized by brain and developmental defects in the case of complete loss-of-function and atopy, neurodevelopmental defects, and colitis in cases of incomplete loss-of-function., (© 2024 Ghasempour et al.)

Published
2024
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33. Generation of complex bone marrow organoids from human induced pluripotent stem cells.

Author

Frenz-Wiessner S, Fairley SD, Buser M, Goek I, Salewskij K, Jonsson G, Illig D, Zu Putlitz B, Petersheim D, Li Y, Chen PH, Kalauz M, Conca R, Sterr M, Geuder J, Mizoguchi Y, Megens RTA, Linder MI, Kotlarz D, Rudelius M, Penninger JM, Marr C, and Klein C

Subjects
Humans, Animals, Mice, Hematopoietic Stem Cells cytology, Bone Marrow metabolism, Bone Marrow Cells cytology, Bone Marrow Cells metabolism, Cell Culture Techniques methods, Mesenchymal Stem Cells cytology, Mesenchymal Stem Cells metabolism, Organoids cytology, Organoids metabolism, Induced Pluripotent Stem Cells cytology, Induced Pluripotent Stem Cells metabolism, Cell Differentiation, Hematopoiesis
Abstract

The human bone marrow (BM) niche sustains hematopoiesis throughout life. We present a method for generating complex BM-like organoids (BMOs) from human induced pluripotent stem cells (iPSCs). BMOs consist of key cell types that self-organize into spatially defined three-dimensional structures mimicking cellular, structural and molecular characteristics of the hematopoietic microenvironment. Functional properties of BMOs include the presence of an in vivo-like vascular network, the presence of multipotent mesenchymal stem/progenitor cells, the support of neutrophil differentiation and responsiveness to inflammatory stimuli. Single-cell RNA sequencing revealed a heterocellular composition including the presence of a hematopoietic stem/progenitor (HSPC) cluster expressing genes of fetal HSCs. BMO-derived HSPCs also exhibited lymphoid potential and a subset demonstrated transient engraftment potential upon xenotransplantation in mice. We show that the BMOs could enable the modeling of hematopoietic developmental aspects and inborn errors of hematopoiesis, as shown for human VPS45 deficiency. Thus, iPSC-derived BMOs serve as a physiologically relevant in vitro model of the human BM microenvironment to study hematopoietic development and BM diseases., (© 2024. The Author(s).)

Published
2024
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35. Precision medicine in monogenic inflammatory bowel disease: proposed mIBD REPORT standards.

Author

Uhlig HH, Booth C, Cho J, Dubinsky M, Griffiths AM, Grimbacher B, Hambleton S, Huang Y, Jones K, Kammermeier J, Kanegane H, Koletzko S, Kotlarz D, Klein C, Lenardo MJ, Lo B, McGovern DPB, Özen A, de Ridder L, Ruemmele F, Shouval DS, Snapper SB, Travis SP, Turner D, Wilson DC, and Muise AM

Subjects
Humans, Prospective Studies, Retrospective Studies, Precision Medicine
Abstract

Owing to advances in genomics that enable differentiation of molecular aetiologies, patients with monogenic inflammatory bowel disease (mIBD) potentially have access to genotype-guided precision medicine. In this Expert Recommendation, we review the therapeutic research landscape of mIBD, the reported response to therapies, the medication-related risks and systematic bias in reporting. The mIBD field is characterized by the absence of randomized controlled trials and is dominated by retrospective observational data based on case series and case reports. More than 25 off-label therapeutics (including small-molecule inhibitors and biologics) as well as cellular therapies (including haematopoietic stem cell transplantation and gene therapy) have been reported. Heterogeneous reporting of outcomes impedes the generation of robust therapeutic evidence as the basis for clinical decision making in mIBD. We discuss therapeutic goals in mIBD and recommend standardized reporting (mIBD REPORT (monogenic Inflammatory Bowel Disease Report Extended Phenotype and Outcome of Treatments) standards) to stratify patients according to a genetic diagnosis and phenotype, to assess treatment effects and to record safety signals. Implementation of these pragmatic standards should help clinicians to assess the therapy responses of individual patients in clinical practice and improve comparability between observational retrospective studies and controlled prospective trials, supporting future meta-analysis., (© 2023. Springer Nature Limited.)

Published
2023
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36. Identification of the γδ IEL-secreted Paneth Cell Protective Factor API5 as a Promising Therapeutic Target for ATG16L1-associated Crohn's Disease.

Author

Kotlarz D

Subjects
Humans, Paneth Cells metabolism, Protective Factors, Autophagy, Biological Transport, Autophagy-Related Proteins genetics, Autophagy-Related Proteins metabolism, Nuclear Proteins metabolism, Apoptosis Regulatory Proteins metabolism, Crohn Disease diagnosis, Crohn Disease drug therapy, Crohn Disease metabolism
Published
2023
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37. Human MD2 deficiency-an inborn error of immunity with pleiotropic features.

Author

Li Y, Yu Z, Schenk M, Lagovsky I, Illig D, Walz C, Rohlfs M, Conca R, Muise AM, Snapper SB, Uhlig HH, Garty BZ, Klein C, and Kotlarz D

Subjects
Humans, Cytokines metabolism, Lymphocyte Antigen 96 metabolism, Signal Transduction, Toll-Like Receptors metabolism, Lipopolysaccharides pharmacology, Toll-Like Receptor 4 genetics
Abstract

Background: Toll-like receptors (TLRs) are important pattern recognition receptors that sense microbes and control host defense. Myeloid differentiation protein 2 (MD2) is the indispensable coreceptor for TLR4, facilitating the binding to the gram-negative bacterial cell wall component LPS and activation of downstream signaling., Objective: We sought to provide phenotypic and mechanistic insights into human MD2 deficiency., Methods: To elucidate the genetic cause in a patient with very early onset inflammatory bowel disease, we performed whole-exome sequencing and studied the functional consequences of the identified mutation in LY96 (encoding for MD2) in genetically engineered induced pluripotent stem cell-derived macrophages with knockout of MD2 or knockin of the patient-specific mutation, including TLR4-mediated signaling, cytokine production, and bacterial handling., Results: Whole-exome sequencing identified a homozygous in-frame deletion in the LY96 gene (c.347&#95;349delCAA; p.Thr116del) in a patient with very early onset inflammatory bowel disease and a sibling presenting with pneumonia and otitis media. Induced pluripotent stem cell-derived macrophages with knockout of MD2 or expression of the Thr116del mutation showed impaired activation of nuclear factor kappa B and mitogen-activated protein kinase signaling as well as TLR4 endocytosis on challenge with LPS or bacteria. In addition, MD2-deficient macrophages showed decreased cytokine expression (eg, IL-6, TNF, and IL-10) in response to LPS or gram-negative but not gram-positive bacteria., Conclusions: Human MD2 deficiency causes defective TLR4 signaling in response to LPS or gram-negative bacteria. The clinical manifestations and expressivity might be variable due to unknown secondary risk factors. Because TLR4 represents a therapeutic target for multiple inflammatory conditions, our study may provide insights into potential side effects of pharmacological TLR4 targeting., (Copyright © 2022 American Academy of Allergy, Asthma & Immunology. Published by Elsevier Inc. All rights reserved.)

Published
2023
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38. Biallelic TLR4 deficiency in humans.

Author

Capitani M, Al-Shaibi AA, Pandey S, Gartner L, Taylor H, Hubrack SZ, Agrebi N, Al-Mohannadi MJ, Al Kaabi S, Vogl T, Roth J, Kotlarz D, Klein C, Charles AK, Vijayakumar V, Karim MY, George B, Travis SP, Elawad M, Lo B, and Uhlig HH

Subjects
Humans, Lipopolysaccharides pharmacology, Toll-Like Receptors metabolism, Cytokines metabolism, Myeloid Differentiation Factor 88 genetics, Toll-Like Receptor 4 genetics, Toll-Like Receptor 2 genetics
Abstract

Background: Toll-like receptors (TLRs) mediate functions for host defense and inflammatory responses. TLR4 recognizes LPS, a component of gram-negative bacteria as well as host-derived endogenous ligands such as S100A8 and S100A9 proteins., Objective: We sought to report phenotype and cellular function of individuals with complete TLR4 deficiency., Methods: We performed genome sequencing and investigated exome and genome sequencing databases. Cellular responses were studied on primary monocytes, macrophages, and neutrophils, as well as cell lines using flow cytometry, reporter, and cytokine assays., Results: We identified 2 individuals in a family of Qatari origin carrying a homozygous stop codon variant p.Q188X in TLR4 presenting with a variable phenotype (asymptomatic and inflammatory bowel disease consistent with severe perianal Crohn disease). A third individual with homozygous p.Y794X was identified in a population database. In contrast to hypomorphic polymorphisms p.D299G and p.T399I, the variants p.Q188X and p.Y794X completely abrogated LPS-induced cytokine responses whereas TLR2 response was normal. TLR4 deficiency causes a neutrophil CD62L shedding defect, whereas antimicrobial activity toward intracellular Salmonella was intact., Conclusions: Biallelic TLR4 deficiency in humans causes an inborn error of immunity in responding to LPS. This complements the spectrum of known primary immunodeficiencies, in particular myeloid differentiation primary response 88 (MYD88) or the IL-1 receptor-associated kinase 4 (IRAK4) deficiency that are downstream of TLR4 and TLR2 signaling., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2023
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39. Pathogenic Interleukin-10 Receptor Alpha Variants in Humans - Balancing Natural Selection and Clinical Implications.

Author

Aschenbrenner D, Ye Z, Zhou Y, Hu W, Brooks I, Williams I, Capitani M, Gartner L, Kotlarz D, Snapper SB, Klein C, Muise AM, Marsden BD, Huang Y, and Uhlig HH

Subjects
Humans, Receptors, Interleukin-10 genetics, Interleukin-10 Receptor alpha Subunit genetics, Selection, Genetic, Interleukin-10 genetics, Leukocytes, Mononuclear
Abstract

Balancing natural selection is a process by which genetic variants arise in populations that are beneficial to heterozygous carriers, but pathogenic when homozygous. We systematically investigated the prevalence, structural, and functional consequences of pathogenic IL10RA variants that are associated with monogenic inflammatory bowel disease. We identify 36 non-synonymous and non-sense variants in the IL10RA gene. Since the majority of these IL10RA variants have not been functionally characterized, we performed a systematic screening of their impact on STAT3 phosphorylation upon IL-10 stimulation. Based on the geographic accumulation of confirmed pathogenic IL10RA variants in East Asia and in Northeast China, the distribution of infectious disorders worldwide, and the functional evidence of IL-10 signaling in the pathogenesis, we identify Schistosoma japonicum infection as plausible selection pressure driving variation in IL10RA. Consistent with this is a partially augmented IL-10 response in peripheral blood mononuclear cells from heterozygous variant carriers. A parasite-driven heterozygote advantage through reduced IL-10 signaling has implications for health care utilization in regions with high allele frequencies and potentially indicates pathogen eradication strategies that target IL-10 signaling., (© 2022. The Author(s).)

Published
2023
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41. Dysregulated inflammasome activity in intestinal inflammation - Insights from patients with very early onset IBD.

Author

Illig D and Kotlarz D

Subjects
Humans, Mice, Animals, Genome-Wide Association Study, Genetic Predisposition to Disease, Inflammation, Inflammasomes, Inflammatory Bowel Diseases
Abstract

Inflammatory bowel disease (IBD) is a multifactorial disorder triggered by imbalances of the microbiome and immune dysregulations in genetically susceptible individuals. Several mouse and human studies have demonstrated that multimeric inflammasomes are critical regulators of host defense and gut homeostasis by modulating immune responses to pathogen- or damage-associated molecular patterns. In the context of IBD, excessive production of pro-inflammatory Interleukin-1β has been detected in patient-derived intestinal tissues and correlated with the disease severity or failure to respond to anti-tumor necrosis factor therapy. Correspondingly, genome-wide association studies have suggested that single nucleotide polymorphisms in inflammasome components might be associated with risk of IBD development. The relevance of inflammasomes in controlling human intestinal homeostasis has been further exemplified by the discovery of very early onset IBD (VEO-IBD) patients with monogenic defects affecting different molecules in the complex regulatory network of inflammasome activity. This review provides an overview of known causative monogenic entities of VEO-IBD associated with altered inflammasome activity. A better understanding of the molecular mechanisms controlling inflammasomes in monogenic VEO-IBD may open novel therapeutic avenues for rare and common inflammatory diseases., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Illig and Kotlarz.)

Published
2022
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42. Novel CD55 Mutation Associated With Severe Small Bowel Ulceration Mimicking Inflammatory Bowel Disease in a Pair of Siblings.

Author

Chongsrisawat V, Suratannon N, Chatchatee P, Ittiwut R, Ittiwut C, Weerapakorn W, Theamboonlers A, Rohlfs M, Klein C, Kotlarz D, and Suphapeetiporn K

Subjects
Humans, Intestine, Small pathology, Mutation, Siblings, CD55 Antigens genetics, Inflammatory Bowel Diseases complications, Inflammatory Bowel Diseases diagnosis, Inflammatory Bowel Diseases genetics
Published
2022
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44. A Systematic Review of Monogenic Inflammatory Bowel Disease.

Author

Nambu R, Warner N, Mulder DJ, Kotlarz D, McGovern DPB, Cho J, Klein C, Snapper SB, Griffiths AM, Iwama I, and Muise AM

Subjects
Adaptor Proteins, Signal Transducing, Adolescent, Age of Onset, Humans, Proteins, Colitis, Inflammatory Bowel Diseases genetics, Inflammatory Bowel Diseases therapy
Abstract

Background & Aims: Advances in genomic technologies have led to increasing reports of monogenic inflammatory bowel disease (IBD). Here, we systematically review the literature to determine the clinical features, genetic profile, and previously used treatment strategies in monogenic IBD., Methods: A systematic review of MEDLINE articles published between January 2000 and December 2020 was conducted. A total of 750 individual monogenic IBD cases were identified from 303 eligible articles., Results: The most frequently reported monogenic IBD genes were IL10RA/B, XIAP, CYBB, LRBA, and TTC7A. In total, 63.4% of patients developed IBD before 6 years of age, 17.4% developed IBD between ages 10 and 17.9 years, and 10.9% developed IBD after age 18. There was a substantial difference between these age groups and the underlying monogenic disorders. Only 31.7% had any history of extraintestinal comorbidity (EIC) before IBD onset, but 76.0% developed at least 1 EIC during their clinical course. The most common EICs were atypical infection (44.7%), dermatologic abnormality (38.4%), and autoimmunity (21.9%). Bowel surgery, biologic therapy, and hematopoietic stem cell transplantation were performed in 27.1%, 32.9%, and 23.1% of patients, respectively., Conclusions: Monogenic IBD cases, although rare, have varied extraintestinal comorbidities and limited treatment options including surgery and transplant. Early identification and improved understanding of the characteristics of the genes and underlying disease processes in monogenic IBD is important for effective management., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2022
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45. Valosin-containing protein-regulated endoplasmic reticulum stress causes NOD2-dependent inflammatory responses.

Author

Ghalandary M, Li Y, Fröhlich T, Magg T, Liu Y, Rohlfs M, Hollizeck S, Conca R, Schwerd T, Uhlig HH, Bufler P, Koletzko S, Muise AM, Snapper SB, Hauck F, Klein C, and Kotlarz D

Subjects
Acetylmuramyl-Alanyl-Isoglutamine pharmacology, Humans, Nod2 Signaling Adaptor Protein genetics, Nod2 Signaling Adaptor Protein metabolism, Valosin Containing Protein genetics, Valosin Containing Protein metabolism, Endoplasmic Reticulum Stress, Interleukin-8 metabolism
Abstract

NOD2 polymorphisms may affect sensing of the bacterial muramyl dipeptide (MDP) and trigger perturbed inflammatory responses. Genetic screening of a patient with immunodeficiency and enteropathy revealed a rare homozygous missense mutation in the first CARD domain of NOD2 (ENST00000300589; c.160G > A, p.E54K). Biochemical assays confirmed impaired NOD2-dependent signaling and proinflammatory cytokine production in patient's cells and heterologous cellular models with overexpression of the NOD2 mutant. Immunoprecipitation-coupled mass spectrometry unveiled the ATPase valosin-containing protein (VCP) as novel interaction partner of wildtype NOD2, while the binding to the NOD2 variant p.E54K was abrogated. Knockdown of VCP in coloncarcinoma cells led to impaired NF-κB activity and IL8 expression upon MDP stimulation. In contrast, tunicamycin-induced ER stress resulted in increased IL8, CXCL1, and CXCL2 production in cells with knockdown of VCP, while enhanced expression of these proinflammatory molecules was abolished upon knockout of NOD2. Taken together, these data suggest that VCP-mediated inflammatory responses upon ER stress are NOD2-dependent., (© 2022. The Author(s).)

Published
2022
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46. Author Correction: Gain-of-function variants in SYK cause immune dysregulation and systemic inflammation in humans and mice.

Author

Wang L, Aschenbrenner D, Zeng Z, Cao X, Mayr D, Mehta M, Capitani M, Warner N, Pan J, Wang L, Li Q, Zuo T, Cohen-Kedar S, Lu J, Ardy RC, Mulder DJ, Dissanayake D, Peng K, Huang Z, Li X, Wang Y, Wang X, Li S, Bullers S, Gammage AN, Warnatz K, Schiefer AI, Krivan G, Goda V, Kahr WHA, Lemaire M, Lu CY, Siddiqui I, Surette MG, Kotlarz D, Engelhardt KR, Griffin HR, Rottapel R, Decaluwe H, Laxer RM, Proietti M, Hambleton S, Elcombe S, Guo CH, Grimbacher B, Dotan I, Ng SC, Freeman SA, Snapper SB, Klein C, Boztug K, Huang Y, Li D, Uhlig HH, and Muise AM

Published
2022
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47. Variants in STXBP3 are Associated with Very Early Onset Inflammatory Bowel Disease, Bilateral Sensorineural Hearing Loss and Immune Dysregulation.

Author

Ouahed J, Kelsen JR, Spessott WA, Kooshesh K, Sanmillan ML, Dawany N, Sullivan KE, Hamilton KE, Slowik V, Nejentsev S, Neves JF, Flores H, Chung WK, Wilson A, Anyane-Yeboa K, Wou K, Jain P, Field M, Tollefson S, Dent MH, Li D, Naito T, McGovern DPB, Kwong AC, Taliaferro F, Ordovas-Montanes J, Horwitz BH, Kotlarz D, Klein C, Evans J, Dorsey J, Warner N, Elkadri A, Muise AM, Goldsmith J, Thompson B, Engelhardt KR, Cant AJ, Hambleton S, Barclay A, Toth-Petroczy A, Vuzman D, Carmichael N, Bodea C, Cassa CA, Devoto M, Maas RL, Behrens EM, Giraudo CG, and Snapper SB

Subjects
Age of Onset, Female, Genetic Variation genetics, Hearing Loss, Sensorineural epidemiology, Humans, Immune System Diseases epidemiology, Infant, Newborn, Inflammatory Bowel Diseases epidemiology, Male, Qa-SNARE Proteins genetics, Exome Sequencing, Hearing Loss, Sensorineural genetics, Immune System Diseases genetics, Inflammatory Bowel Diseases genetics, Qa-SNARE Proteins analysis
Abstract

Background and Aims: Very early onset inflammatory bowel disease [VEOIBD] is characterized by intestinal inflammation affecting infants and children less than 6 years of age. To date, over 60 monogenic aetiologies of VEOIBD have been identified, many characterized by highly penetrant recessive or dominant variants in underlying immune and/or epithelial pathways. We sought to identify the genetic cause of VEOIBD in a subset of patients with a unique clinical presentation., Methods: Whole exome sequencing was performed on five families with ten patients who presented with a similar constellation of symptoms including medically refractory infantile-onset IBD, bilateral sensorineural hearing loss and, in the majority, recurrent infections. Genetic aetiologies of VEOIBD were assessed and Sanger sequencing was performed to confirm novel genetic findings. Western analysis on peripheral blood mononuclear cells and functional studies with epithelial cell lines were employed., Results: In each of the ten patients, we identified damaging heterozygous or biallelic variants in the Syntaxin-Binding Protein 3 gene [STXBP3], a protein known to regulate intracellular vesicular trafficking in the syntaxin-binding protein family of molecules, but not associated to date with either VEOIBD or sensorineural hearing loss. These mutations interfere with either intron splicing or protein stability and lead to reduced STXBP3 protein expression. Knock-down of STXBP3 in CaCo2 cells resulted in defects in cell polarity., Conclusion: Overall, we describe a novel genetic syndrome and identify a critical role for STXBP3 in VEOIBD, sensorineural hearing loss and immune dysregulation., (© The Author(s) 2021. Published by Oxford University Press on behalf of European Crohn’s and Colitis Organisation. All rights reserved. For permissions, please email: journals.permissions@oup.com.)

Published
2021
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48. Congenital disorders of glycosylation with defective fucosylation.

Author

Hüllen A, Falkenstein K, Weigel C, Huidekoper H, Naumann-Bartsch N, Spenger J, Feichtinger RG, Schaefers J, Frenz S, Kotlarz D, Momen T, Khoshnevisan R, Riedhammer KM, Santer R, Herget T, Rennings A, Lefeber DJ, Mayr JA, Thiel C, and Wortmann SB

Subjects
Adolescent, Adult, Child, Child, Preschool, Female, Fibroblasts metabolism, Fibroblasts pathology, Glycoproteins, Glycosylation, Humans, Infant, Male, Treatment Outcome, Young Adult, Congenital Disorders of Glycosylation drug therapy, Congenital Disorders of Glycosylation genetics, Fucose therapeutic use, Monosaccharide Transport Proteins genetics
Abstract

Fucosylation is essential for intercellular and intracellular recognition, cell-cell interaction, fertilization, and inflammatory processes. Only five types of congenital disorders of glycosylation (CDG) related to an impaired fucosylation have been described to date: FUT8-CDG, FCSK-CDG, POFUT1-CDG SLC35C1-CDG, and the only recently described GFUS-CDG. This review summarizes the clinical findings of all hitherto known 25 patients affected with those defects with regard to their pathophysiology and genotype. In addition, we describe five new patients with novel variants in the SLC35C1 gene. Furthermore, we discuss the efficacy of fucose therapy approaches within the different defects., (© 2021 SSIEM.)

Published
2021
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49. Abatacept for treatment-refractory pediatric CTLA4-haploinsufficiency.

Author

Lanz AL, Riester M, Peters P, Schwerd T, Lurz E, Hajji MS, Rohlfs M, Ley-Zaporozhan J, Walz C, Kotlarz D, Klein C, Albert MH, and Hauck F

Subjects
Adolescent, CTLA-4 Antigen genetics, CTLA-4 Antigen immunology, Female, Haploinsufficiency genetics, Haploinsufficiency immunology, Hematopoietic Stem Cell Transplantation, Humans, Immune System Diseases genetics, Immune System Diseases immunology, Immune System Diseases therapy, Male, Mutation, Missense, T-Lymphocytes, Regulatory immunology, Abatacept therapeutic use, CTLA-4 Antigen deficiency, Immunosuppressive Agents therapeutic use
Abstract

CTLA4-haploinsufficiency is a complex disease of immune dysregulation presenting with a broad spectrum of clinical manifestations. CTLA4-Fc fusion proteins such as abatacept have been described to alleviate immune dysregulation in several adult cases of CTLA4-haploinsufficiency. However, until now only few cases of pediatric CTLA4-haploinsufficiency treated with abatacept have been described. Here we present two pediatric cases of severe CTLA4-haploinsufficiency refractory to conventional immunosuppressive therapies that responded rapidly to treatment with abatacept. No side effects were observed during a follow-up period of 7-15 months. While one patient has successfully undergone HSCT the second patient continues to receive abatacept. Our cases demonstrate safe medium-term use of abatacept in the pediatric population., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published
2021
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50. Clinical and Mutation Description of the First Iranian Cohort of Infantile Inflammatory Bowel Disease: The Iranian Primary Immunodeficiency Registry (IPIDR).

Author

Rahmani F, Rayzan E, Rahmani MR, Shahkarami S, Zoghi S, Rezaei A, Aryan Z, Najafi M, Rohlfs M, Jeske T, Aflatoonian M, Chavoshzadeh Z, Farahmand F, Motamed F, Rohani P, Alimadadi H, Mahdaviani A, Mansouri M, Tavakol M, Vanderberg M, Kotlarz D, Klein C, and Rezaei N

Subjects
Child, Preschool, Cohort Studies, Diarrhea genetics, Female, Humans, Infant, Infant, Newborn, Iran, Male, Mutation, Receptors, Interleukin-10 genetics, Registries, Exome Sequencing, Inflammatory Bowel Diseases genetics, Primary Immunodeficiency Diseases genetics
Abstract

We describe a cohort of 25 Iranian patients with infantile inflammatory bowel disease (IBD), 14 (56%) of whom had monogenic defects. After proper screening, patients were referred for whole exome sequencing (WES). Four patients had missense mutations in the IL10 RA , and one had a large deletion in the IL10 RB . Four patients had mutations in genes implicated in host:microbiome homeostasis, including TTC7A deficiency, and two patients with novel mutations in the TTC37 and NOX1 . We found a novel homozygous mutation in the SRP54 in a deceased patient and the heterozygous variant in his sibling with a milder phenotype. Three patients had combined immunodeficiency: one with ZAP-70 deficiency (T + B + NK - ), and two with atypical SCID due to mutations in RAG1 and LIG4 . One patient had a G6PC3 mutation without neutropenia. Eleven of the 14 patients with monogenic defects were results of consanguinity and only 4 of them were alive to this date.

Published
2021
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