Your search keyword '"NCF1"' showing total 72 results

51. Ncf1 (p47phox) polymorphism determines oxidative burst and the severity of arthritis in rats and mice

Author

Hultqvist, Malin and Holmdahl, Rikard

Subjects

*JOINT diseases, *AUTOIMMUNE diseases, *RHEUMATOID arthritis, *CONNECTIVE tissues, *EXTRACELLULAR matrix proteins

Abstract

Abstract: Identifying genes that regulate polygenic diseases influenced by the environment such as rheumatoid arthritis (RA), has so far proven to be difficult. By using an alternative approach, i.e., linkage analysis using relevant animal models we succeeded in finding the Ncf1 gene residing in the Pia4 quantitative trait locus to be responsible for the severity of pristane induced arthritis in rats. The influence of another mutation in the mouse Ncf1 gene showed the same association between decreased oxidative burst and enhanced arthritis. In this case the mutation affected a splice site giving a non-detectable oxidative burst response and enhanced collagen induced arthritis as well as myelin oligodendrocyte protein induced experimental autoimmune encephalomyelitis. These findings open up new possibilities for new treatments for autoimmune diseases, i.e., RA, targeting the NADPH oxidase pathway. [Copyright &y& Elsevier]

Published

2005

52. Inconsistent susceptibility to autoimmunity in inbred LEW rats is due to genetic crossbreeding involving segregation of the arthritis-regulating gene Ncf1

Author

Olofsson, Peter, Johansson, Åsa, Wedekind, Dirk, Klöting, Ingrid, Klinga-Levan, Karin, Lu, Shemin, and Holmdahl, Rikard

Subjects

*AUTOIMMUNITY, *LABORATORY mice, *ARTHRITIS, *LEUCOCYTES

Abstract

We recently identified a single-nucleotide polymorphism in the Ncf1 gene, a component of the NADPH oxidase complex, to be the cause of one of the strongest identified loci for arthritis severity in rats. This polymorphism was found to be naturally occurring in a collection of inbred rat strains as well as in wild rats. Among the inbred strains we found that different LEW substrains (LEW/Ztm and LEW/Mol), originating from different breeders, showed an allelic discrepancy in Ncf1, suggesting an impact on arthritis susceptibility between these substrains. In fact, the LEW/Mol strain was completely resistant to pristane-induced arthritis, in contrast to the LEW/Ztm strain, which was susceptible. Moreover, the LEW/Mol strain had higher production of radical oxygen species in peripheral blood leukocytes, a phenomenon most likely regulated by the polymorphisms in the Ncf1 gene. However, the phenotypic difference between LEW/Mol and LEW/Ztm is most likely a combination of several genes, of which Ncf1 is suggested to be the major regulating gene. This has also been confirmed by previous linkage analyses involving the LEW/Ztm strain which shows that a QTL on chromosome 12, most likely caused by polymorphism of Ncf1, is the major regulatory gene but that other loci are contributing. That more genes are likely to contribute was shown by a complete genome comparison of the LEW/Ztm and the LEW/Mol rat strains that uncovered an introduction of approximately 37% non-LEW genome into the LEW/Mol strain, which probably was caused by past crossbreeding. Therefore, the LEW/Mol should be regarded as a recombinant inbred strain. [Copyright &y& Elsevier]

Published

2004

53. Targeted Repair of p47-CGD in iPSCs by CRISPR/Cas9

Author

Klatt, Denise, Cheng, Erica, Philipp, Friederike, Selich, Anton, Dahlke, Julia, Schmidt, Reinhold E., Schott, Juliane W., Büning, Hildegard, Hoffmann, Dirk, Thrasher, Adrian J., Schambach, Axel, and Publica

Subjects

human induced pluripotent stem cells, NADPH oxidase, gene editing, CRISPR / Cas9, p47phox, chronic granulomatous disease (CGD), Pseudogenes, NCF1

Abstract

Mutations in the NADPH oxidase, which is crucial for the respiratory burst in phagocytes, result in chronic granulomatous disease (CGD). The only curative treatment option for CGD patients, who suffer from severe infections, is allogeneic bone marrow transplantation. Over 90% of patients with mutations in the p47phox subunit of the oxidase complex carry the deletion c.75_76delGT (DGT). This frequent mutation most likely originates via gene conversion from one of the two pseudogenes NCF1B or NCF1C, which are highly homologous to NCF1 (encodes p47phox) but carry the DGT mutation. We applied CRISPR/Cas9 to generate patient-like p47-DGT iPSCs for disease modeling. To avoid unpredictable chromosomal rearrangements by CRISPR/Cas9-mediated cleavage in the pseudogenes, we developed a gene-correction approach to specifically target NCF1 but leave the pseudogenes intact. Functional assays revealed restored NADPH oxidase activity and killing of bacteria in corrected phagocytes as well as the specificity of this approach.

Published

2019

54. p47phox deficiency improves cognitive impairment and attenuates tau hyperphosphorylation in mouse models of AD.

Author

Gong, Ping, Chen, Yan-qing, Lin, Ai-hua, Zhang, Hai-bo, Zhang, Yan, Ye, Richard D., and Yu, Yang

Subjects

TAU proteins, COGNITION disorders, NICOTINAMIDE adenine dinucleotide phosphate, DELETION mutation, AMYLOID plaque, NADPH oxidase

Abstract

Background: Alzheimer's disease (AD) is characterized by progressive memory loss and cognitive impairment. The aggregation of amyloid β (Aβ) and hyperphosphorylated tau protein are two major pathological features of AD. Nicotinamide adenine dinucleotide phosphate oxidase (NADPH oxidase, NOX) has been indicated in Aβ pathology; however, whether and how it affects tau pathology are not yet clear. Methods: The role of NOX2 in cognitive function, amyloid plaque formation, and tau hyperphosphorylation were examined in APP/PS1 transgenic mice mated with p47phox-deficient mice (with deletion of the gene of neutrophil cytosolic factor 1, Ncf1) and/or in p47phox-deficient mice receiving intracerebroventricular (ICV) injection of streptozotocin (STZ). The cognitive and non-cognitive functions in these mice were assessed by Morris water maze, Rotarod test, open field, and elevated plus maze. Aβ levels, amyloid plaques, p47phox expression, and astrocyte activation were evaluated using immunofluorescence staining, ELISA, and/or Western blotting. Cultured primary neuronal cells were treated with okadaic acid or conditioned media (CM) from high glucose-stimulated primary astrocytes. The alteration in tau pathology was determined using Western blotting and immunofluorescence staining. Results: Deletion of the gene coding for p47phox, the organizer subunit of NOX2, significantly attenuated cognitive impairment and tau pathology in these mice. p47phox deficiency decreased the activation of astrocytes but had no effect on Aβ levels and amyloid plaque formation in the brains of aged APP/PS1 mice, which displayed markedly increased expression of p47phox in neurons and astrocytes. Cell culture studies found that neuronal p47phox deletion attenuated okadaic acid-induced tau hyperphosphorylation at specific sites in primary cultures of neurons. CM from high glucose-treated WT astrocytes increased tau hyperphosphorylation in primary neurons, whereas this effect was absent from p47phox-deficient astrocytes. Conclusions: These results suggest that p47phox is associated with cognitive function and tau pathology in AD. p47phox expressed in neurons contributes to tau hyperphosphorylation directly, while p47phox in astrocytes affect tau hyperphosphorylation by activating astrocytes indirectly. Our results provide new insights into the role of NOX2 in AD and indicate that targeted inhibition of p47phox may be a new strategy for the treatment of AD. [ABSTRACT FROM AUTHOR]

Published

2020

55. Ncf1 affects osteoclast formation but is not critical for postmenopausal bone loss

Author

Alexandra, Stubelius, Annica, Andersson, Rikard, Holmdahl, Claes, Ohlsson, Ulrika, Islander, and Hans, Carlsten

Subjects

Genotype, Ovariectomy, Osteoclasts, Lymphocyte Activation, Mice, Bone Density, Bone mineral density, Animals, Humans, Point Mutation, Bone Resorption, Osteoporosis, Postmenopausal, Ncf1, Macrophages, NADPH Oxidases, Postmenopausal bone loss, Estrogens, Flow Cytometry, Disease Models, Animal, Osteoimmunology, Pre-osteoclasts, Female, Reactive Oxygen Species, NOX 2, Estrogen Deficiency, Research Article, Neutrophil cytosolic factor 1

Abstract

Background Increased reactive oxygen species and estrogen deficiency contribute to the pathophysiology of postmenopausal osteoporosis. Reactive oxygen species contribute to bone degradation and is necessary for RANKL-induced osteoclast differentiation. In postmenopausal bone loss, reactive oxygen species can also activate immune cells to further enhance bone resorption. Here, we investigated the role of reactive oxygen species in ovariectomy-induced osteoporosis in mice deficient in Ncf1, a subunit for the NADPH oxidase 2 and a well-known regulator of the immune system. Methods B10.Q wild-type (WT) mice and mice with a spontaneous point mutation in the Ncf1-gene (Ncf1*/*) were ovariectomized (ovx) or sham-operated. After 4 weeks, osteoclasts were generated ex vivo, and bone mineral density was measured using peripheral quantitative computed tomography. Lymphocyte populations, macrophages, pre-osteoclasts and intracellular reactive oxygen species were analyzed by flow cytometry. Results After ovx, Ncf1*/*-mice formed fewer osteoclasts ex vivo compared to WT mice. However, trabecular bone mineral density decreased similarly in both genotypes after ovx. Ncf1*/*-mice had a larger population of pre-osteoclasts, whereas lymphocytes were activated to the same extent in both genotypes. Conclusion Ncf1*/*-mice develop fewer osteoclasts after ovx than WT mice. However, irrespective of genotype, bone mineral density decreases after ovx, indicating that a compensatory mechanism retains bone degradation after ovx.

Published

2016

56. A single nucleotide polymorphism in the NCF1 gene leading to reduced oxidative burst is associated with systemic lupus erythematosus

Author

Olsson, Lina M, Johansson, Åsa C, Gullstrand, Birgitta, Jönsen, Andreas, Saevarsdottir, Saedis, Rönnblom, Lars, Leonard, Dag, Wetterö, Jonas, Sjöwall, Christopher, Svenungsson, Elisabet, Gunnarsson, Iva, Bengtsson, Anders A, Holmdahl, Rikard, Olsson, Lina M, Johansson, Åsa C, Gullstrand, Birgitta, Jönsen, Andreas, Saevarsdottir, Saedis, Rönnblom, Lars, Leonard, Dag, Wetterö, Jonas, Sjöwall, Christopher, Svenungsson, Elisabet, Gunnarsson, Iva, Bengtsson, Anders A, and Holmdahl, Rikard

Abstract

OBJECTIVES: Ncf1 polymorphisms leading to low production of reactive oxygen species (ROS) are strongly associated with autoimmune diseases in animal models. The human NCF1 gene is very complex with both functional and non-functional gene copies and genotyping requires assays specific for functional NCF1 genes. We aimed at investigating association and function of the missense single nucleotide polymorphism (SNP), rs201802880 (here denoted NCF1-339) in NCF1 with systemic lupus erythematosus (SLE). METHODS: We genotyped the NCF1-339 SNP in 973 Swedish patients with SLE and 1301 controls, using nested PCR and pyrosequencing. ROS production and gene expression of type 1 interferon-regulated genes were measured in isolated cells from subjects with different NCF1-339 genotypes. RESULTS: We found an increased frequency of the NCF1-339 T allele in patients with SLE, 11% compared with 4% in controls, OR 3.0, 95% CI 2.4 to 3.9, p=7.0×10(-20). The NCF1-339 T allele reduced extracellular ROS production in neutrophils (p=0.004) and led to an increase expression of type 1 interferon-regulated genes. In addition, the NCF1-339 T allele was associated with a younger age at diagnosis of SLE; mean age 30.3 compared with 35.9, p=2.0×1(-6). CONCLUSIONS: These results clearly demonstrate that a genetically controlled reduced production of ROS increases the risk of developing SLE and confirm the hypothesis that ROS regulate chronic autoimmune inflammatory diseases., Funding agencies: Knut and Alice Wallenberg Foundation; Swedish Rheumatism Association; Swedish Medical Research Council; Swedish Research Council; Swedish Foundation for Strategic Research; King Gustaf Vs 80-Year Fund; Alfred Osterlund, Greta and Johan Kock, Anna-Greta Cr

Published

2017

57. ATPR-induced differentiation and G0/G1 phase arrest in acute promyelocytic leukemia by repressing EBP50/NCF1 complex to promote the production of ROS.

Author

Feng, Yubin, Niu, Ruowen, Cheng, Xin, Wang, Ke, Du, Yan, Peng, Xiaoqing, and Chen, Feihu

Subjects

*ACUTE promyelocytic leukemia, *CELL differentiation

Abstract

Our previous study has demonstrated that 4-amino-2-trifluoromethyl-phenyl Retinate (ATPR) can induce human leukemia NB4 cells differentiation and G0/G1 phase arrest, but the underlying mechanism is still unclear. In this study, we used proteomics to screen differentially expressed protein profiles in NB4 cells before and after ATPR treatment in vitro. We analyzed the peptides digested from total cellular proteins by reverse phase LC-MS/MS and then performed label-free quantitative analysis. We found 27 significantly up-regulated proteins in the ATPR group compared to the control group. NCF1 was the most significantly changed protein. Immunoprecipitation and double immunofluorescent staining showed that EBP50 bind to NCF1. We further explored the potential molecular mechanism of EBP50/NCF1 complex in ATPR-induced differentiation and G0/G1 phase arrest. The results showed that ATPR remarkably reduced the expression of EBP50 in vivo and in vitro. Interestingly, the reduction of EBP50 contributed to ROS release by modulating the subcellular localization of NCF1. The reduction of EBP50 also contributed to G0/G1 phase arrest by inhibiting CyclinD1, CyclinA2 and CDK4, as well as promoting the differentiation of NB4 cells by increasing the expression of CD11b. Furthermore, we found that the overexpression of EBP50 restrained the effects of ATPR on differentiation and G0/G1 phase arrest in NB4 cells. These results suggest that ATPR-induced differentiation and G0/G1 phase arrest in acute promyelocytic leukemia (APL) by repressing EBP50/NCF1 complex to promote the production of ROS, and the results from in vivo experiments were consistent with those from in vitro studies. Therefore, our finding results suggest that EBP50 may be a new target for ATPR in the treatment of APL. • ATPR may be developed into a highly effective and low-toxic clinical first-line drug for the treatment of APL. • EBP50 was overexpressed in APL patients. • EBP50 may become a direct target protein for ATPR treatment of APL. • EBP50 may play a role in anti-tumor effect by regulating NCF1 subcellular localization to affect ROS release. • EBP50 plays an important role in ATPR-induced APL differentiation and G0/G1 phase arrest in vitro and in vivo. [ABSTRACT FROM AUTHOR]

Published

2019

58. First Report of Clinical, Functional, and Molecular Investigation of Chronic Granulomatous Disease in Nine Jordanian Families

Author

Bakri, Faris G., Martel, Cécile, Khuri-Bulos, Najwa, Mahafzah, Azmi, El-Khateeb, Mohammad S., Al-Wahadneh, Adel M., Hayajneh, Wail A., Hamamy, Hanan A., Maquet, Elisabeth, Molin, Michelle, and Stasia, Marie José

Published

2009

59. Targeted Repair of p47-CGD in iPSCs by CRISPR/Cas9: Functional Correction without Cleavage in the Highly Homologous Pseudogenes.

Author

Klatt D, Cheng E, Philipp F, Selich A, Dahlke J, Schmidt RE, Schott JW, Büning H, Hoffmann D, Thrasher AJ, and Schambach A

Subjects

Enzyme Activation, Gene Expression, Gene Targeting, Genetic Loci, Granulocytes immunology, Granulocytes metabolism, Granulomatous Disease, Chronic metabolism, Humans, Introns, Macrophages immunology, Macrophages metabolism, Macrophages microbiology, NADPH Oxidases metabolism, Phagocytosis immunology, Pseudogenes genetics, Sequence Homology, CRISPR-Cas Systems, Gene Editing, Granulomatous Disease, Chronic genetics, Induced Pluripotent Stem Cells metabolism, NADPH Oxidases genetics

Abstract

Mutations in the NADPH oxidase, which is crucial for the respiratory burst in phagocytes, result in chronic granulomatous disease (CGD). The only curative treatment option for CGD patients, who suffer from severe infections, is allogeneic bone marrow transplantation. Over 90% of patients with mutations in the p47 phox subunit of the oxidase complex carry the deletion c.75_76delGT (ΔGT). This frequent mutation most likely originates via gene conversion from one of the two pseudogenes NCF1B or NCF1C, which are highly homologous to NCF1 (encodes p47 phox ) but carry the ΔGT mutation. We applied CRISPR/Cas9 to generate patient-like p47-ΔGT iPSCs for disease modeling. To avoid unpredictable chromosomal rearrangements by CRISPR/Cas9-mediated cleavage in the pseudogenes, we developed a gene-correction approach to specifically target NCF1 but leave the pseudogenes intact. Functional assays revealed restored NADPH oxidase activity and killing of bacteria in corrected phagocytes as well as the specificity of this approach., (Copyright © 2019 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2019

60. Novel Diagnostic Tool for p47 phox -Deficient Chronic Granulomatous Disease Patient and Carrier Detection.

Author

Wrona D, Siler U, and Reichenbach J

Abstract

Chronic granulomatous disease (CGD) is a primary immunodeficiency caused by mutations of the phagocytic nicotinamide adenine dinucleotide phosphate (NADPH) oxidase. Autosomal recessive p47 phox -deficient CGD (p47 phox CGD) is the second most frequent form of the disease in western countries, and more than 94% of patients have a disease-causing dinucleotide deletion (ΔGT) in the neutrophil cytosolic factor 1 ( NCF1 ) gene. The ΔGT mutation is most likely transferred onto the NCF1 from one of its two pseudogenes co-localized on the same chromosome. The presence of NCF1 pseudogenes in healthy individuals makes the genetic diagnostics of ΔGT p47 phox CGD challenging, as it requires the distinction between ΔGT in NCF1 and in the two pseudogenes. We have developed a diagnostic tool for the identification of p47 phox CGD based on PCR co-amplification of NCF1 and its pseudogenes, followed by band intensity quantification of restriction fragment length polymorphism products. The single-day, reliable p47 phox CGD diagnostics allow for robust discrimination of homozygous ΔGT p47 phox CGD patients from heterozygous carriers and healthy individuals, as well as for monitoring gene therapy efficacy.

Published

2019

61. Preliminary study on chronic granulomatous disease in Sri Lanka.

Author

Fernando, Shalinda Jude Arjuna, Faiz, Noorul Mifra, Handunnetti, Shiroma Mangaika, De Silva, Aruna Dharshan, Dasanayake, Wasala Mudiyanselage Dhanushka Kumari, Wickramasinghe, Geethani Devika, Karunatilake, Rathnayake Mudiyanselage Chandima Hasanthi, and de Silva, Nilhan Rajiva

Subjects

CHRONIC granulomatous disease, IMMUNODEFICIENCY, REACTIVE oxygen species, NICOTINAMIDE adenine dinucleotide phosphate, CLINICAL trials

Abstract

Background: Chronic granulomatous disease (CGD) is a rare primary immunodeficiency of the phagocytic cells, which results in absent or diminished levels of microbicidal reactive oxygen species. The disease occurs due to germline mutations in the genes encoding the five subunits of NADPH oxidase complex. The present study is a pilot study to understand the clinical and genetic aspects of CGD in Sri Lanka. Methods: Clinical records of thirteen CGD patients were analysed and compared with similar studies performed in different countries and regions to identify patterns in demographics, clinical manifestations and infectious agents. Genomic DNA and cDNA were analysed in eight patients to identify mutations in CYBB and NCF1 genes, thereby to ascertain the potential X-linked and autosomal recessive (AR) CGD patients. Results: The onset of symptoms in the patient cohort was very early (mean 4.6 months) compared to 20 months in India and 23.9 months in Latin America. Similarly, the age at diagnosis was lower (mean 1.6 years after birth) compared to other studies; 4.5 years in India and 6.1 years in Europe. Pulmonary manifestations were the most common (85%), followed by skin/subcutaneous infections (77%) and lymphadenopathy (62%). The death rate of local patients (38%) was higher than other countries (India 35%, Europe 20%). Majority (77%) were treated for tuberculosis at some point in life. Genetic analysis confirmed six out of eight patients as X-linked CGD cases with mutations in CYBB gene. A novel splice site mutation was identified in P-07 at position c.141+6 which resulted in the deletion of entire exon 2. Two siblings (P-05 and P-06) from consanguineous parents, were identified with AR-CGD based on the homozygous GT deletion mutation in NCF1 gene. Conclusions: The clinical presentation, manifestations and genetic subtypes in the local cohort, appear to be comparable with global trends. Mycobacterial infections should be investigated and treated with more prominence. Effective treatment options are required to control the high mortality rate. [ABSTRACT FROM AUTHOR]

Published

2018

62. Clinical, functional, and genetic characterization of chronic granulomatous disease in 89 Turkish patients

Author

Ayse Metin, Hüseyin Avcılar, Mustafa Yavuz Köker, Mustafa Yilmaz, Isil Barlan, Yildiz Camcioglu, Alisan Yildiran, Sara Sebnem Kilic, Olcay Yegin, Ilhan Tezcan, Dirk Roos, Karin van Leeuwen, Ozden Sanal, Martin de Boer, Turkan Patiroglu, Uludağ Üniversitesi/Tıp Fakültesi/Pediatrik Alerji ve İmmünoloji Anabilim Dalı., Kılıç, Sara Şebnem, AAH-1658-2021, Çukurova Üniversitesi, Landsteiner Laboratory, and Ondokuz Mayıs Üniversitesi

Subjects

Male, Allergy, Survival rate, Turkey, Neutrophils, CYBB gene, Gene sequence, Granulomatous Disease, Chronic, Gene, CYBB, Turkey (republic), CYBA, Families, Chronic granulomatous disease, hemic and lymphatic diseases, Genotype, Autoimmune disease, Immunology and Allergy, Enzyme activity, NCF2, Child, Features, NCF1, Priority journal, Oxidase test, NADPH oxidase, biology, Incidence, Neutrophil, Sequence analysis, Stem cell transplantation, Term-follow-up, Phenotype, mean fluorescence intensity, Abscess, BCG vaccination, Dihydrorhodamine-1,2,3 assay, Child, Preschool, dihydrorhodamine-1,2,3 assay, Medical history, Female, Itraconazole, Tuberculostatic agent, Infection, Mutations, NCF2 gene, Human, Stimulation index, Adult, congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, Immunology, Cause of death, Major clinical study, Infections, Chronic Granulomatous Disease, Neutrophil cytosol Factor 40K, Mutation, Article, Lymphadenitis, medicine, Humans, Tuberculosis, Gene mutation, stimulation index, Disease severity, BCG vaccine, Gamma interferon, Autosomal recessive disorder, nicotinamide dinucleotide phosphate reduced oxidase, business.industry, NADPH Oxidases, Mean fluorescence intensity, CYBA gene, Sequence Analysis, DNA, medicine.disease, NCF1 gene, Nicotinamide dinucleotide phosphate reduced oxidase, Cotrimoxazole, Enzyme Activation, Clinical feature, Preschool child, Primary immunodeficiency, biology.protein, School child, Gene expression, business, Reduced nicotinamide adenine dinucleotide phosphate oxidase, Controlled study

Abstract

Background: Chronic granulomatous disease (CGD) is a rare primary immunodeficiency disorder of phagocytes resulting in impaired killing of bacteria and fungi. A mutation in one of the 4 genes encoding the components p22(phox), p47(phox), p67(phox), and p40(phox) of the leukocyte nicotinamide dinucleotide phosphate reduced (NADPH) oxidase leads to autosomal recessive (AR) CGD. A mutation in the CYBB gene encoding gp91(phox) leads to X-linked recessive CGD., Background Chronic granulomatous disease (CGD) is a rare primary immunodeficiency disorder of phagocytes resulting in impaired killing of bacteria and fungi. Amutation in one of the 4 genes encoding the components p22phox, p47phox, p67phox, and p40phox of the leukocyte nicotinamide dinucleotide phosphate reduced (NADPH) oxidase leads to autosomal recessive (AR) CGD. Amutation in the CYBB gene encoding gp91phox leads to X-linked recessive CGD. Objective The aim of this study is to show the correlation between clinical, functional, and genetic data of patients with CGD from Turkey. Methods We report here the results of 89 patients with CGD from 73 Turkish families in a multicenter study. Results Most of the families (55%) have an AR genotype, and 38% have an X-linked genotype; patients from 5 families with a suspected AR genotype (7%) were not fully characterized. We compared patients with CGD according to the severity of NADPH oxidase deficiency of neutrophils. Patients with A220, A670 or X910 phenotypes with a stimulation index of 1.5 or less have early clinical presentation and younger age at diagnosis (mean, 3.2 years). However, in p47phox-deficient cases and in 5 other AR cases with high residual oxidase activity (stimulation index≥ 3), later and less severe clinical presentation and older age at diagnosis (mean, 7.1 years) were found. Pulmonary involvement was the most common clinical feature, followed by lymphadenitis and abscesses. Conclusion Later and less severe clinical presentation and older age at diagnosis are related to the residual NADPH oxidase activity of neutrophils and not to the mode of inheritance. CGD caused by A220 and A670 subtypes manifests as severe as the X910 subtype.

Published

2013

63. Different unequal cross-over events between NCF1 and its pseudogenes in autosomal p47(Phox)-deficient chronic granulomatous disease

Author

Astghik Hayrapetyan, Paula C.D. Dencher, Martin de Boer, Karin van Leeuwen, Dirk Roos, and Landsteiner Laboratory

Subjects

DNA Copy Number Variations, Partial NCF1 deletion, Pseudogene, Genetic cross-over, Biology, NCF1 pseudogene, Granulomatous Disease, Chronic, medicine.disease_cause, Compound heterozygosity, Fusion gene, Exon, Chronic granulomatous disease, medicine, Humans, CYBB, Multiplex ligation-dependent probe amplification, Allele, Molecular Biology, Alleles, NCF1, Genetics, Mutation, NADPH Oxidases, Exons, medicine.disease, Molecular biology, Introns, Molecular Medicine, Pseudogenes

Abstract

Chronic granulomatous disease (CGD) is a rare congenital disorder in which phagocytes cannot generate superoxide (O-2(-)) and other microbicidal oxidants due to mutations in one of the five components of the O-2(-)-generating NADPH oxidase complex. The most common autosomal subtype of CGD is caused by mutations in NCF1, encoding the NADPH subunit p47(Phox). Usually, these mutations are the result of unequal exchange of chromatid between NCF1 and one of its two pseudogenes. We have now investigated in detail the breakpoints within or between these (pseudo) NCF1 genes in 43 families with p47(Phox)-deficient CGD by means of multiplex ligase-dependent probe amplification (MLPA). In 24 families the patients totally lacked NCF1 sequences, indicating that in these families the cross-over points are located between NCF1 and its pseudogenes. Six other families were compound heterozygous for a total NCF1 deletion and another mutation in NCF1 on the other allele. In 8 families, the patients lacked NCF1 exons 1-4 but had retained NCF1 exons 6-10, indicating that a cross-over point is located within NCF1 between exons 4 and 6. Similarly, in 4 families a cross-over point was located within NCF1 between exons 2 and 4. Similar cross-avers, in heterozygous form, were observed in family members of the patients. Several patients were compound heterozygous for total and partial NCF1 deletions. Thus, at least three different cross-over points exist within the NCF1 gene cluster, indicating that autosomal p47(Phox)-deficient CGD is genetically heterogeneous but can be dissected in detail by MLPA. (C) 2013 Elsevier B.V. All rights reserved

Published

2013

64. Mannan induces ROS-regulated, IL-17A-dependent psoriasis arthritis-like disease in mice

Author

Khmaladze, Ia, Kelkka, Tiina, Guerard, Simon, Wing, Kajsa, Pizzolla, Angela, Saxena, Amit, Lundqvist, Katarina, Holmdahl, Meirav, Nandakumar, Kutty Selva, Holmdahl, Rikard, Khmaladze, Ia, Kelkka, Tiina, Guerard, Simon, Wing, Kajsa, Pizzolla, Angela, Saxena, Amit, Lundqvist, Katarina, Holmdahl, Meirav, Nandakumar, Kutty Selva, and Holmdahl, Rikard

Abstract

Psoriasis (Ps) and psoriasis arthritis (PsA) are poorly understood common diseases, induced by unknown environmental factors, affecting skin and articular joints. A single i.p. exposure to mannan from Saccharomyces cerevisiae induced an acute inflammation in inbred mouse strains resembling human Ps and PsA-like disease, whereas multiple injections induced a relapsing disease. Exacerbation of disease severity was observed in mice deficient for generation of reactive oxygen species (ROS). Interestingly, restoration of ROS production, specifically in macrophages, ameliorated both skin and joint disease. Neutralization of IL-17A, mainly produced by gammadelta T cells, completely blocked disease symptoms. Furthermore, mice depleted of granulocytes were resistant to disease development. In contrast, certain acute inflammatory mediators (C5, Fcgamma receptor III, mast cells, and histamine) and adaptive immune players (alphabeta T and B cells) were redundant in disease induction. Hence, we propose that mannan-induced activation of macrophages leads to TNF-alpha secretion and stimulation of local gammadelta T cells secreting IL-17A. The combined action of activated macrophages and IL-17A produced in situ drives neutrophil infiltration in the epidermis and dermis of the skin, leading to disease manifestations. Thus, our finding suggests a new mechanism triggered by exposure to exogenous microbial components, such as mannan, that can induce and exacerbate Ps and PsA., Funding text: We thank Carlos and Kristina Palestro and Tomasz Klaczkowski for taking care of animals. This study was supported by the Swedish Strategic Science Foundation, the Knut and Alice Wallenberg Foundation, the Konung Gustaf V:s 80-ars fond, the Swedish Research Council, the Swedish Rheumatism Association, European Union Masterswitch (Grant HEALTH-F2-2008-223404), Neurinox, and BeTheCure.

Published

2014

65. Evolució molecular i estudi funcional de gens localitzats a les duplicacions segmentàries de la regió 7q11.23

Author

Antonell Boixader, Anna, Pérez Jurado, Luis Alberto, and Universitat Pompeu Fabra. Departament de Ciències Experimentals i de la Salut

Subjects

reordenament genòmic, hypertension, NAD(P)H oxidasa, síndrome de Williams-Beuren, NAD(P)H oxidase, hominoids, hipertensió, genomic rearrangement, Williams-Beuren syndrome, evolution, deleció, estrès oxidatiu, evolució, oxidative stress, duplicacions segmentàries, factor de transcripció, deletion, segmental duplications, transcription factor, GTF2IRD2, NCF1

Abstract

En aquest treball es presenta l'evolució molecular i estudi funcional de gens localitzats a les duplicacions segmentàries de la regió 7q11.23, implicada en la Síndrome de Williams-Beuren (SWB). S'ha datat l'aparició d'aquestes duplicacions en els últims 25 milions d'anys d'evolució i s'ha proposat un model evolutiu amb reordenaments específics i mecanismes de generació. Correlacions clínico-moleculars en els pacients amb la SWB han permès determinar que l'haploinsuficiència per NCF1, un gen localitzat a les duplicacions, és un factor protector per hipertensió. S'ha proposat un model patogènic per la hipertensió, implicant l'oxidasa NAD(P)H i estrès oxidatiu, suggerint que noves estratègies terapèutiques podrien ser utilitzades. A més, s'ha caracteritzat parcialment la funció de GTF2IRD2, un altre gen de les duplicacions. GTF2IRD2 interacciona amb altres factors de transcripció relacionats, té una localització subcel·lular variable i no s'uneix a ADN. Aquests resultats contribueixen a conèixer millor els mecanismes mutacionals i patogènics de la SWB., This work presents the molecular evolution along with the functional analysis of the genes located in the segmental duplications flanking the 7q11.23 region, involved in Williams-Beuren syndrome (WBS). The generation of the segmental duplications has been dated to the last 25 million years of evolution and an evolutionary model with specific rearrangements and mechanisms has been proposed. Clinical-molecular correlations in WBS patients have allowed to determine that haploinsufficiency at NCF1, a gene located in the duplications, is a protective factor for hypertension. A pathogenic model for hypertension has been proposed, implicating NAD(P)H oxidase and oxidative stress, and suggesting that novel therapeutic strategies could be used. In addition, the functional characterization of another gene of the duplications, GTF2IRD2, has been partially achieved. GTF2IRD2 has been shown to interact with other related transcription factors, to display variable subcellular localization and to lack DNA binding properties. These results contribute to a better knowledge of the mutational and pathogenic mechanisms of the WBS.

Published

2006

66. Chronic Granulomatous Disease.

Author

Roos D

Subjects

Biomarkers, Combined Modality Therapy, Disease Management, Enzyme Activation, Granulomatous Disease, Chronic diagnosis, Granulomatous Disease, Chronic therapy, Humans, Hydrogen Peroxide metabolism, Mutation, NADPH Oxidases chemistry, NADPH Oxidases genetics, NADPH Oxidases metabolism, Phagocytes immunology, Phagocytes metabolism, Phenotype, Protein Binding, Reactive Oxygen Species metabolism, Symptom Assessment, Treatment Outcome, Granulomatous Disease, Chronic etiology, Granulomatous Disease, Chronic metabolism

Abstract

Chronic granulomatous disease is a clinical condition that stems from inactivating mutations in NOX2 and its auxiliary proteins. Together, these proteins form the phagocyte NADPH oxidase enzyme that generates superoxide. Superoxide (O 2 ċ- ) and its reduced product hydrogen peroxide (H 2 O 2 ) give rise to several additional reactive oxygen species (ROS), which together are necessary for adequate killing of pathogens. Thus, CGD patients, with a phagocyte NADPH oxidase that is not properly functioning, suffer from recurrent, life-threatening infections with certain bacteria, fungi, and yeasts. Here, I give a short survey of the genetic mutations that underlie CGD, the effect of these mutations on the activity of the leukocyte NADPH oxidase, the clinical symptoms of CGD patients, and the treatment options for these patients.

Published

2019

67. A false-carrier state for the c.579G>A mutation in the NCF1 gene in Ashkenazi Jews.

Author

De Boer M, Gavrieli R, van Leeuwen K, Wolf HR, Dushnitzki M, Bar-Yosef Y, Bar-Ziv A, Behar D, Lipitz S, Miller TE, Tool ATJ, Kuijpers TW, van den Berg TK, Wolach B, Roos D, and Pras E

Subjects

Alleles, Exons genetics, Female, Genetic Carrier Screening, Genetic Testing, Granulomatous Disease, Chronic pathology, Humans, Male, Mutation, Pregnancy, Granulomatous Disease, Chronic genetics, Heterozygote, Jews genetics, NADPH Oxidases genetics

Abstract

Background: Mutations in the NCF1 gene that encodes p47 phox , a subunit of the NADPH oxidase complex, cause chronic granulomatous disease (CGD). In Kavkazi Jews, a c.579G>A (p.Trp193Ter) mutation in NCF1 is frequently found, leading to CGD. The same mutation is found in about 1% of Ashkenazi Jews, although Ashkenazi CGD patients with this mutation have never been described., Methods: We used Sanger sequencing, multiplex ligation-dependent probe amplification (MLPA), gene scan analysis and Ion Torrent Next Generation Sequencing for genetic analysis, and measured NADPH oxidase activity and p47 phox expression., Results: In an Ashkenazi couple expecting a baby, both parents were found to be heterozygotes for this mutation, as was the fetus. However, segregation analysis in the extended family was consistent with the fetus inheriting both carrier alleles from the parents. MLPA indicated four complete NCF1 genes in the fetus and three in each parent. Gene sequencing confirmed these results. Analysis of fetal leucocytes obtained by cordocentesis revealed substantial oxidase activity with three different assays, which was confirmed after birth. In six additional Ashkenazi carriers of the NCF1 c.579G>A mutation, we found five individuals with three complete NCF1 genes of which one was mutated (like the parents), and one individual with in addition a fusion gene of NCF1 with a pseudogene., Conclusion: These results point to the existence of a 'false-carrier' state in Ashkenazi Jews and have wide implications regarding pre-pregnancy screening in this and other population groups., Competing Interests: Competing interests: None declared., (© Article author(s) (or their employer(s) unless otherwise stated in the text of the article) 2018. All rights reserved. No commercial use is permitted unless otherwise expressly granted.)

Published

2018

68. A single nucleotide polymorphism in the NCF1 gene leading to reduced oxidative burst is associated with systemic lupus erythematosus.

Author

Olsson LM, Johansson ÅC, Gullstrand B, Jönsen A, Saevarsdottir S, Rönnblom L, Leonard D, Wetterö J, Sjöwall C, Svenungsson E, Gunnarsson I, Bengtsson AA, and Holmdahl R

Subjects

Adult, Case-Control Studies, Female, Gene Expression, Gene Expression Regulation, Genetic Predisposition to Disease, Humans, Lupus Erythematosus, Systemic immunology, Lupus Erythematosus, Systemic metabolism, Male, Neutrophils immunology, Polymorphism, Single Nucleotide, Reactive Oxygen Species metabolism, Sweden, White People genetics, Lupus Erythematosus, Systemic genetics, NADPH Oxidases genetics, Respiratory Burst genetics

Abstract

Objectives: Ncf1 polymorphisms leading to low production of reactive oxygen species (ROS) are strongly associated with autoimmune diseases in animal models. The human NCF1 gene is very complex with both functional and non-functional gene copies and genotyping requires assays specific for functional NCF1 genes. We aimed at investigating association and function of the missense single nucleotide polymorphism (SNP), rs201802880 (here denoted NCF1-339) in NCF1 with systemic lupus erythematosus (SLE)., Methods: We genotyped the NCF1-339 SNP in 973 Swedish patients with SLE and 1301 controls, using nested PCR and pyrosequencing. ROS production and gene expression of type 1 interferon-regulated genes were measured in isolated cells from subjects with different NCF1-339 genotypes., Results: We found an increased frequency of the NCF1-339 T allele in patients with SLE, 11% compared with 4% in controls, OR 3.0, 95% CI 2.4 to 3.9, p=7.0×10 -20 . The NCF1-339 T allele reduced extracellular ROS production in neutrophils (p=0.004) and led to an increase expression of type 1 interferon-regulated genes. In addition, the NCF1-339 T allele was associated with a younger age at diagnosis of SLE; mean age 30.3 compared with 35.9, p=2.0×1 -6 ., Conclusions: These results clearly demonstrate that a genetically controlled reduced production of ROS increases the risk of developing SLE and confirm the hypothesis that ROS regulate chronic autoimmune inflammatory diseases., Competing Interests: Competing interests: None declared., (© Article author(s) (or their employer(s) unless otherwise stated in the text of the article) 2017. All rights reserved. No commercial use is permitted unless otherwise expressly granted.)

Published

2017

69. Clinical, functional, and genetic characterization of chronic granulomatous disease in 89 Turkish patients.

Author

Köker, Mustafa Yavuz, Camc?o?lu, Y?ld?z, van Leeuwen, Karin, K?l?ç, Sara ?ebnem, Barlan, I??l, Y?lmaz, Mustafa, Metin, Ay?e, de Boer, Martin, Avc?lar, Hüseyin, Pat?ro?lu, Türkan, Y?ld?ran, Ali?an, Ye?in, Olcay, Tezcan, ?lhan, Sanal, Özden, and Roos, Dirk

Abstract

Background: Chronic granulomatous disease (CGD) is a rare primary immunodeficiency disorder of phagocytes resulting in impaired killing of bacteria and fungi. A mutation in one of the 4 genes encoding the components p22phox, p47phox, p67phox, and p40phox of the leukocyte nicotinamide dinucleotide phosphate reduced (NADPH) oxidase leads to autosomal recessive (AR) CGD. A mutation in the CYBB gene encoding gp91phox leads to X-linked recessive CGD. Objective: The aim of this study is to show the correlation between clinical, functional, and genetic data of patients with CGD from Turkey. Methods: We report here the results of 89 patients with CGD from 73 Turkish families in a multicenter study. Results: Most of the families (55%) have an AR genotype, and 38% have an X-linked genotype; patients from 5 families with a suspected AR genotype (7%) were not fully characterized. We compared patients with CGD according to the severity of NADPH oxidase deficiency of neutrophils. Patients with A220, A670 or X910 phenotypes with a stimulation index of 1.5 or less have early clinical presentation and younger age at diagnosis (mean, 3.2 years). However, in p47phox-deficient cases and in 5 other AR cases with high residual oxidase activity (stimulation index ? 3), later and less severe clinical presentation and older age at diagnosis (mean, 7.1 years) were found. Pulmonary involvement was the most common clinical feature, followed by lymphadenitis and abscesses. Conclusion: Later and less severe clinical presentation and older age at diagnosis are related to the residual NADPH oxidase activity of neutrophils and not to the mode of inheritance. CGD caused by A220 and A670 subtypes manifests as severe as the X910 subtype. [Copyright &y& Elsevier]

Published

2013

70. Mannan induces ROS-regulated, IL-17A-dependent psoriasis arthritis-like disease in mice.

Author

Khmaladze Ia, Kelkka T, Guerard S, Wing K, Pizzolla A, Saxena A, Lundqvist K, Holmdahl M, Nandakumar KS, and Holmdahl R

Subjects

Animals, Arthritis, Psoriatic metabolism, Dermatitis immunology, Dermatitis pathology, Disease Models, Animal, Humans, Interleukin-17 metabolism, Joints immunology, Joints pathology, Macrophages drug effects, Macrophages immunology, Macrophages metabolism, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Mice, Mutant Strains, Monocytes drug effects, Monocytes immunology, Monocytes metabolism, NADPH Oxidases genetics, NADPH Oxidases immunology, NADPH Oxidases metabolism, Neutrophils drug effects, Neutrophils immunology, Neutrophils metabolism, Reactive Oxygen Species metabolism, Receptors, Antigen, T-Cell, gamma-delta immunology, Receptors, Antigen, T-Cell, gamma-delta metabolism, Tumor Necrosis Factor-alpha immunology, Tumor Necrosis Factor-alpha metabolism, Arthritis, Psoriatic chemically induced, Arthritis, Psoriatic immunology, Interleukin-17 immunology, Mannans pharmacology

Abstract

Psoriasis (Ps) and psoriasis arthritis (PsA) are poorly understood common diseases, induced by unknown environmental factors, affecting skin and articular joints. A single i.p. exposure to mannan from Saccharomyces cerevisiae induced an acute inflammation in inbred mouse strains resembling human Ps and PsA-like disease, whereas multiple injections induced a relapsing disease. Exacerbation of disease severity was observed in mice deficient for generation of reactive oxygen species (ROS). Interestingly, restoration of ROS production, specifically in macrophages, ameliorated both skin and joint disease. Neutralization of IL-17A, mainly produced by γδ T cells, completely blocked disease symptoms. Furthermore, mice depleted of granulocytes were resistant to disease development. In contrast, certain acute inflammatory mediators (C5, Fcγ receptor III, mast cells, and histamine) and adaptive immune players (αβ T and B cells) were redundant in disease induction. Hence, we propose that mannan-induced activation of macrophages leads to TNF-α secretion and stimulation of local γδ T cells secreting IL-17A. The combined action of activated macrophages and IL-17A produced in situ drives neutrophil infiltration in the epidermis and dermis of the skin, leading to disease manifestations. Thus, our finding suggests a new mechanism triggered by exposure to exogenous microbial components, such as mannan, that can induce and exacerbate Ps and PsA.

Published

2014

71. Chronic Granulomatous Disease

Author

Leiding JW, Holland SM, Adam MP, Everman DB, Mirzaa GM, Pagon RA, Wallace SE, Bean LJH, Gripp KW, and Amemiya A

Abstract

Clinical Characteristics: Chronic granulomatous disease (CGD) is a primary immunodeficiency disorder of phagocytes (neutrophils, monocytes, macrophages, and eosinophils) resulting from impaired killing of bacteria and fungi. CGD is characterized by severe recurrent bacterial and fungal infections and dysregulated inflammatory responses resulting in granuloma formation and other inflammatory disorders such as colitis. Infections typically involve the lung (pneumonia), lymph nodes (lymphadenitis), liver (abscess), bone (osteomyelitis), and skin (abscesses or cellulitis). Granulomas typically involve the genitourinary system (bladder) and gastrointestinal tract (often the pylorus initially, and later the esophagus, jejunum, ileum, cecum, rectum, and perirectal area). Some males with X-linked CGD have McLeod neuroacanthocytosis syndrome as the result of a contiguous gene deletion. While CGD may present anytime from infancy to late adulthood, the vast majority of affected individuals are diagnosed before age five years. Use of antimicrobial prophylaxis and therapy has greatly improved overall survival., Diagnosis/testing: The diagnosis of CGD is established in a proband with suggestive findings by identification of pathogenic variant(s) in one of six genes that encode or permit assembly of the subunits of phagocyte NADPH oxidase: biallelic pathogenic variants in CYBA , CYBC1 , NCF1 , NCF2 , and NCF4 cause autosomal recessive CGD; pathogenic variants of CYBB cause X-linked CGD., Management: Treatment of manifestations: A definitive microbiologic diagnosis is essential to proper treatment of infections. Newer azole drugs (voriconazole, posaconazole, isovuconazole) have expanded therapeutic options for fungal infections. Long courses of antimicrobials are often needed for adequate treatment. Abscesses may require percutaneous drainage or excisional surgery. Simultaneous administration of antimicrobials and corticosteroids can help resolve the associated heightened inflammatory response, including colitis. Prevention of primary manifestations: Lifelong daily antibacterial and antifungal prophylaxis is recommended; immunomodulatory therapy with interferon gamma (IFN-gamma) is part of the prophylactic regimen in many centers. Allogeneic hematopoietic stem cell transplantation (HSCT) is the only known cure for CGD and is associated with excellent overall and event-free survival, especially when performed with matched donors at a younger age. Surveillance: Screening labs every 3-4 months in a healthy individual with CGD can aid in early detection and treatment of asymptomatic or minimally symptomatic infections and noninfectious complications such as colitis, pulmonary granulomas, and pulmonary fibrosis. Agents/circumstances to avoid: (1) Decayed organic matter (e.g., mulching, gardening, leaf raking, house demolition) as inhalation of fungal spores can result in fulminant pneumonitis; (2) live bacterial vaccines including bacille Calmette-Guérin (BCG) vaccination and Salmonella typhi vaccination; (3) persons with CGD and McLeod neuroacanthocytosis syndrome: blood transfusions that are Kell antigen positive. Evaluation of relatives at risk: Early diagnosis of relatives at risk allows for prompt initiation of antimicrobial prophylaxis and other treatment. Pregnancy management: The major concern during the pregnancy of a woman known to have CGD is use of prophylactic antimicrobials: trimethoprim, a folic acid antagonist, is discontinued during pregnancy because of the high risk for birth defects. Although sulfamethoxazole is not known to increase the risk of birth defects in humans, it is typically administered in conjunction with trimethoprim. Data regarding teratogenicity of itraconazole are limited., Genetic Counseling: CGD associated with a pathogenic variant in CYBB is inherited in an X-linked manner. CGD associated with biallelic pathogenic variants in CYBA , CYBC1 , NCF1 , NCF2 , or NCF4 is inherited in an autosomal recessive manner. X-linked CGD. If the mother of an affected male is heterozygous for a CYBB pathogenic variant, the chance of transmitting it in each pregnancy is 50%. Males who inherit the pathogenic variant will be affected. Females who inherit the pathogenic variant will be heterozygous. Heterozygous females are typically not affected with CGD but are at substantial risk for inflammatory conditions. Once the CYBB pathogenic variant has been identified in an affected family member, molecular genetic heterozygote detection for at-risk female relatives is possible. Autosomal recessive CGD. If both parents are known to be heterozygous for an autosomal recessive CGD-causing pathogenic variant, each sib of an affected individual has at conception a 25% chance of being affected, a 50% chance of being a carrier, and a 25% chance of inheriting neither of the familial pathogenic variants. Once the CGD-causing pathogenic variants have been identified in an affected family member, molecular genetic carrier testing for at-risk relatives is possible. Once the CGD-causing pathogenic variant(s) have been identified in an affected family member, prenatal and preimplantation genetic testing are possible. (Other prenatal testing options may be available if the pathogenic variant[s] in the family are not known.), (Copyright © 1993-2022, University of Washington, Seattle. GeneReviews is a registered trademark of the University of Washington, Seattle. All rights reserved.)

Published

1993

72. T cell Surface Redox Levels Determine T Cell Reactivity and Arthritis Susceptibility

Author

Gelderman, Kyra A., Hultqvist, Malin, Holmberg, Jens, Olofsson, Peter, and Holmdahl, Rikard

Published

2006