Your search keyword '"Arif, B."' showing total 107 results

1. Genetics of serum urate concentrations and gout in a high-risk population, patients with chronic kidney disease.

Author

Jing, Jiaojiao, Ekici, Arif B., Sitter, Thomas, Eckardt, Kai-Uwe, Schaeffner, Elke, Li, Yong, Kronenberg, Florian, Köttgen, Anna, and Schultheiss, Ulla T.

Published

2018

2. Analyses of association of psoriatic arthritis and psoriasis vulgaris with functional NCF1 variants.

Author

Löhr, Sabine, Ekici, Arif B, Uebe, Steffen, Büttner, Christian, Köhm, Michaela, Behrens, Frank, Böhm, Beate, Sticherling, Michael, Schett, Georg, Simon, David, Mössner, Rotraut, Nimeh, Ali, Oji, Vinzenz, Assmann, Gunter, Rech, Jürgen, Holmdahl, Rikard, Burkhardt, Harald, Reis, André, and Hüffmeier, Ulrike

Subjects

*AUTOIMMUNE diseases, *PSORIASIS & genetics, *PSORIASIS, *REACTIVE oxygen species, *AGE distribution, *AGE factors in disease, *BLOOD donors, *GENETIC polymorphisms, *MOLECULAR biology, *PSORIATIC arthritis, *GENOMICS, *DESCRIPTIVE statistics, *DISEASE risk factors

Abstract

The article discusses a study which showed the absence of evidence for associating psoriatic arthritis (PsA) and psoriasis vulgaris (PsV) in a combined analysis. It states that neither NCF1 reduced copy numbers nor missense variants leading to decreased oxidative burst are linked to PsA or PsV. Also noted is an indicated difference in contributing genetic factors between autoimmune diseases.

Published

2019

3. Conceptual Design of Fuel Transfer Cask for Reactor TRIGA PUSPATI (RTP).

Author

Shalina Sheik Muhamad and Mohd Arif B. Hamzah

Subjects

*SPENT reactor fuels, *NUCLEAR reactors, *RADIATION shielding, *STEEL, *NEUTRON flux, *FINITE element method, *LEAD pipe

Abstract

Spent fuel transfer cask is used to transfer a spent fuel from the reactor tank to the spent fuel storage or for spent fuel inspection. Typically, the cask made from steel cylinders that are either welded or bolted closed. The cylinder is enclosed with additional steel, concrete, or other material to provide radiation shielding and containment of the spent fuel. This paper will discuss the Conceptual Design of fuel transfer cask for Reactor TRIGA Puspati (RTP). [ABSTRACT FROM AUTHOR]

Published

2014

4. Chromatin-Remodeling-Factor ARID1B Represses Wnt/β-Catenin Signaling.

Author

Vasileiou, Georgia, Ekici, Arif B., Uebe, Steffen, Zweier, Christiane, Hoyer, Juliane, Engels, Hartmut, Behrens, Jürgen, Reis, André, and Hadjihannas, Michel V.

Subjects

*CHROMATIN-remodeling complexes, *CATENINS, *GENETIC mutation, *NEURAL development, *WNT proteins, *CANCER patients, *LABORATORY mice, *CELLULAR signal transduction

Abstract

The link of chromatin remodeling to both neurodevelopment and cancer has recently been highlighted by the identification of mutations affecting BAF chromatin-remodeling components, such as ARID1B, in individuals with intellectual disability and cancer. However, the underlying molecular mechanism(s) remains unknown. Here, we show that ARID1B is a repressor of Wnt/β-catenin signaling. Through whole-transcriptome analysis, we find that in individuals with intellectual disability and ARID1B loss-of-function mutations, Wnt/β-catenin target genes are upregulated. Using cellular models of low and high Wnt/β-catenin activity, we demonstrate that knockdown of ARID1B activates Wnt/β-catenin target genes and Wnt/β-catenin-dependent transcriptional reporters in a β-catenin-dependent manner. Reciprocally, forced expression of ARID1B inhibits Wnt/β-catenin signaling downstream of the β-catenin destruction complex. Both endogenous and exogenous ARID1B associate with β-catenin and repress Wnt/β-catenin-mediated transcription through the BAF core subunit BRG1. Accordingly, mutations in ARID1B leading to partial or complete deletion of its BRG1-binding domain, as is often observed in intellectual disability and cancers, compromise association with β-catenin, and the resultant ARID1B mutant proteins fail to suppress Wnt/β-catenin signaling. Finally, knockdown of ARID1B in mouse neuroblastoma cells leads to neurite outgrowth through β-catenin. The data suggest that aberrations in chromatin-remodeling factors, such as ARID1B, might contribute to neurodevelopmental abnormalities and cancer through deregulation of developmental and oncogenic pathways, such as the Wnt/β-catenin signaling pathway. [ABSTRACT FROM AUTHOR]

Published

2015

5. Renal fibrosis is the common feature of autosomal dominant tubulointerstitial kidney diseases caused by mutations in mucin 1 or uromodulin.

Author

Ekici, Arif B, Hackenbeck, Thomas, Morinière, Vincent, Pannes, Andrea, Buettner, Maike, Uebe, Steffen, Janka, Rolf, Wiesener, Antje, Hermann, Ingo, Grupp, Sina, Hornberger, Martin, Huber, Tobias B, Isbel, Nikky, Mangos, George, McGinn, Stella, Soreth-Rieke, Daniela, Beck, Bodo B, Uder, Michael, Amann, Kerstin, and Antignac, Corinne

Subjects

*RENAL fibrosis, *KIDNEY diseases, *KIDNEY failure, *CYTOSINE, *GENETIC counseling, *PATHOLOGICAL physiology

Abstract

For decades, ill-defined autosomal dominant renal diseases have been reported, which originate from tubular cells and lead to tubular atrophy and interstitial fibrosis. These diseases are clinically indistinguishable, but caused by mutations in at least four different genes: UMOD, HNF1B, REN, and, as recently described, MUC1. Affected family members show renal fibrosis in the biopsy and gradually declining renal function, with renal failure usually occurring between the third and sixth decade of life. Here we describe 10 families and define eligibility criteria to consider this type of inherited disease, as well as propose a practicable approach for diagnosis. In contrast to what the frequently used term 'Medullary Cystic Kidney Disease' implies, development of (medullary) cysts is neither an early nor a typical feature, as determined by MRI. In addition to Sanger and gene panel sequencing of the four genes, we established SNaPshot minisequencing for the predescribed cytosine duplication within a distinct repeat region of MUC1 causing a frameshift. A mutation was found in 7 of 9 families (3 in UMOD and 4 in MUC1), with one indeterminate (UMOD p.T62P). On the basis of clinical and pathological characteristics we propose the term 'Autosomal Dominant Tubulointerstitial Kidney Disease' as an improved terminology. This should enhance recognition and correct diagnosis of affected individuals, facilitate genetic counseling, and stimulate research into the underlying pathophysiology. [ABSTRACT FROM AUTHOR]

Published

2014

6. The proinflammatory effect of C-reactive protein on human endothelial cells depends on the FcγRIIa genotype.

Author

Raaz-Schrauder, Dorette, Ekici, Arif B., Klinghammer, Lutz, Stumpf, Christian, Achenbach, Stephan, Herrmann, Martin, Reis, André, and Garlichs, Christoph D.

Subjects

*INFLAMMATION, *C-reactive protein, *ENDOTHELIAL cells, *FC receptors, *IMMUNOGLOBULIN allotypes, *ARGININE, *HISTIDINE, *CELL adhesion molecules

Abstract

Abstract: Introduction: The stimulatory effects of CRP (C-reactive protein) on endothelial cells are mainly mediated via FcγRIIa. This receptor exists in two different allotypes bearing either arginine (R131) or histidine (H131) at the extracellular amino acid position 131 of the mature protein, but only FcγRIIa-R131 displays high avidity for CRP. This study investigated the role of the FcγRIIa genotype in CRP-stimulated endothelial cells. Materials and Methods: We tested the effects of CRP on expression of the adhesion molecules ICAM-1, VCAM-1, and E-selectin, as well as the endothelial release of pro-inflammatory molecules as a function of the FcγRIIa-genotype (FcγRIIa-H/H131, FcγRIIa-H/R131, FcγRIIa-R/R131) in HUVEC (Human Umbilical Vein Endothelial Cells). HUVEC were grouped according to their FcγRIIa status by genotyping with an allele specific nested-PCR. The expression of ICAM-1, VCAM-1, and E-selectin on HUVEC was detected by flow cytometry. The release of soluble markers (sCD40L, IL-6, IL-8, MCP-1, tPA, sP-selectin, and sVCAM-1) was measured using a multiplex assay for flow cytometry. Results and Conclusions: CRP-stimulated expression of ICAM-1 and E-selectin was dependent on the specific FcγRIIa-genotype, with most pronounced induction in HUVEC with the FcγRIIa-R/R genotype, followed by H/R and H/H. In accordance with this finding, the supernatants of stimulated HUVEC with the R/R genotype showed significantly higher levels of tPA, MCP-1, and IL-6. Our data show that CRP stimulates the expression of adhesion molecules and the release of soluble markers by HUVEC as a function of the FcγRIIa-genotype. These findings could be relevant in the context of risk stratification in patients with cardiovascular disease. [Copyright &y& Elsevier]

Published

2014

7. HOXA10 and HOXA13 sequence variations in human female genital malformations including congenital absence of the uterus and vagina

Author

Ekici, Arif B., Strissel, Pamela L., Oppelt, Patricia G., Renner, Stefan P., Brucker, Sara, Beckmann, Matthias W., and Strick, Reiner

Subjects

*HOMEOBOX genes, *NUCLEOTIDE sequence, *FEMALE reproductive organs abnormalities, *GENETIC disorders, *VAGINA abnormalities, *UTERUS abnormalities, *GENITALIA development

Abstract

Abstract: Congenital genital malformations occurring in the female population are estimated to be 5 per 1000 and associate with infertility, abortion, stillbirth, preterm delivery and other organ abnormalities. Complete aplasia of the uterus, cervix and upper vagina (Mayer–Rokitansky–Küster–Hauser (MRKH) syndrome) has an incidence of 1 per 4000 female live births. The molecular etiology of congenital genital malformations including MRKH is unknown up to date. The homeobox (HOX) genes HOXA10 and HOXA13 are involved in the development of human genitalia. In this investigation, HOXA10 and HOXA13 genes of 20 patients with the MRKH syndrome, 7 non-MRKH patients with genital malformations and 53 control women were sequenced to assess for DNA variations. A total of 14 DNA sequence variations (10 novel and 4 known) within exonic and untranslated regions were detected in HOXA10 and HOXA13 among our cohorts. Four HOXA10 and two HOXA13 DNA sequence variations were found solely in patients with genital malformations. In addition to mutations resulting in synonymous amino acid substitutions, in the HOXA10 gene a missense mutation was identified and predicted by computer analysis as probably damaging to protein function in two non-MRKH patients, one with a bicornate and the other patient with a septated uterus. A novel exonic HOXA10 cytosine deletion was also identified in a non-MRKH patient with a septate uterus and renal malformations resulting in a premature stop codon and loss of the homeodomain helix 3/4. This cytosine deletion and the missense mutation in HOXA10 were analysed by real time PCR and sequencing, respectively, in two additional larger cohorts of 103 patients with MRKH and 109 non-MRKH patients with genital malformations. No other patients were found with the cytosine deletion however one additional patient was identified regarding the missense mutation. Rare DNA sequence variations in the HOXA10 gene could contribute to the misdevelopment of female internal genitalia. [Copyright &y& Elsevier]

Published

2013

8. A defect of CD16-positive monocytes can occur without disease

Author

Frankenberger, Marion, Ekici, Arif B., Angstwurm, Matthias W., Hoffmann, Harald, Hofer, Thomas P.J., Heimbeck, Irene, Meyer, Peter, Lohse, Peter, Wjst, Matthias, Häussinger, Karl, Reis, André, and Ziegler-Heitbrock, Loems

Subjects

*CD antigens, *MONOCYTES, *LEUCOCYTES, *PLEURAL effusions, *AUTOIMMUNITY, *INFLAMMATION, *MACROPHAGE colony-stimulating factor, *TUMOR necrosis factors

Abstract

Abstract: The CD16-positive monocytes have been first described in 1988 but to date no selective defect in the number of these cells in blood has been reported. We now describe a family in which three of four siblings lack both CD16-positive monocyte subsets, i.e. the nonclassical and the intermediate monocytes. All three had CD16-positive monocytes of 2cells/μl or less as compared to 52±18cells/μl in healthy controls. The index case was affected by recurrent pleural effusion and infections and had evidence of an auto-inflammatory condition but no mutation of any of the relevant candidate genes. The other two siblings without CD16-positive monocytes were apparently healthy. There was no defect in serum M-CSF levels and no mutation in the M-CSF and M-CSFR genes. The data indicate that the absence of CD16-positive monocytes in blood does not lead to disease. [Copyright &y& Elsevier]

Published

2013

9. Patients with unstable angina pectoris show an increased frequency of the Fc gamma RIIa R131 allele.

Author

Raaz-Schrauder, Dorette, Ekici, Arif B., Munoz, Luis E., Klinghammer, Lutz, Voll, Reinhard E., Leusen, Jeanette H.W., van de Winkel, Jan G.J., Reis, André, Schett, Georg, Garlichs, Christoph D., and Herrmann, Martin

Abstract

Patients with Systemic Lupus Erythematosus (SLE) carry an increased risk for the development of coronary artery disease (CAD). The R131 allele of the Fc gamma receptor IIa (FcγRIIa) is associated with SLE incidence and disease severity but also with CAD. Compared to stable angina pectoris (SAP) the unstable angina (UAP), as a manifestation of destabilizing CAD, is associated with increased risk of persistent instability, myocardial infarction, and death. Identification of clinically relevant determinants for unstable angina promises reduction of UAP-associated mortality in patients with SLE. We conducted a clinical study among 553 consecutive patients with stable angina pectoris ( n = 330) and unstable angina pectoris ( n = 223). All patients were genotyped for a frequent functional variant at position 131 of the mature FcγRIIa. UAP, but not SAP was significantly associated with the R/R131 genotype ( P < 0.001). In troponin-negative patients with angina carrying the R/R131 genotype the odds ratio for suffering from UAP was 4.02 (95% confidence interval, 2.52-6.41) compared to those with non-R/R131 genotypes. In a multivariable analysis, the R/R131 genotype independently predicted the risk for development of UAP in a model adjusted for classical atherogenic risk factors. Our data imply that risk stratification of SLE- and other high risk patients with troponin-negative angina could be significantly improved by FcγRIIa genotyping. [ABSTRACT FROM AUTHOR]

Published

2012

10. Haploinsufficiency of ARID1B, a Member of the SWI/SNF-A Chromatin-Remodeling Complex, Is a Frequent Cause of Intellectual Disability

Author

Hoyer, Juliane, Ekici, Arif B., Endele, Sabine, Popp, Bernt, Zweier, Christiane, Wiesener, Antje, Wohlleber, Eva, Dufke, Andreas, Rossier, Eva, Petsch, Corinna, Zweier, Markus, Göhring, Ina, Zink, Alexander M., Rappold, Gudrun, Schröck, Evelin, Wieczorek, Dagmar, Riess, Olaf, Engels, Hartmut, Rauch, Anita, and Reis, André

Subjects

*CHROMATIN-remodeling complexes, *NEUROLOGICAL disorders, *ETIOLOGY of diseases, *FRAMESHIFT mutation, *COHORT analysis, *PERFORMANCE evaluation

Abstract

Intellectual disability (ID) is a clinically and genetically heterogeneous common condition that remains etiologically unresolved in the majority of cases. Although several hundred diseased genes have been identified in X-linked, autosomal-recessive, or syndromic types of ID, the establishment of an etiological basis remains a difficult task in unspecific, sporadic cases. Just recently, de novo mutations in SYNGAP1, STXBP1, MEF2C, and GRIN2B were reported as relatively common causes of ID in such individuals. On the basis of a patient with severe ID and a 2.5 Mb microdeletion including ARID1B in chromosomal region 6q25, we performed mutational analysis in 887 unselected patients with unexplained ID. In this cohort, we found eight (0.9%) additional de novo nonsense or frameshift mutations predicted to cause haploinsufficiency. Our findings indicate that haploinsufficiency of ARID1B, a member of the SWI/SNF-A chromatin-remodeling complex, is a common cause of ID, and they add to the growing evidence that chromatin-remodeling defects are an important contributor to neurodevelopmental disorders. [ABSTRACT FROM AUTHOR]

Published

2012

11. A method of concurrent thermographic–photographic visualization of flow boiling in a minichannel

Author

Ozer, Arif B., Oncel, Ahmet F., Hollingsworth, D. Keith, and Witte, Larry C.

Subjects

*FLOW visualization, *THERMOGRAPHY, *PHOTOGRAPHY, *EBULLITION, *TEMPERATURE effect, *BUBBLE dynamics, *DENSITY, *NUCLEATION, *WORKING fluids, *HEAT flux

Abstract

Abstract: A method is developed to capture the distribution of surface temperature while simultaneously imaging the bubble motions in diabatic flow boiling in a horizontal minichannel. Liquid crystal thermography is used to obtain highly resolved surface temperature measurements on the uniformly heated upper surface of the channel. High-speed images of the flow field are acquired simultaneously and are overlaid with the thermal images. The local surface temperature and heat transfer coefficient can be analyzed with the knowledge of the nucleation site density and location, and bubble motion and size evolution. The horizontal channel is 1.2mm high×23mm wide×357mm long, and the working fluids are Novec 649 and R-11. Optical access is through a machined glass plate which forms the bottom of the channel. The top surface is an electrically heated 76μm-thick Hastelloy foil held in place by a water-cooled aluminum and glass frame. The heat loss resulting from this construction is computed using a conduction model in Fluent. The model is driven by temperature measurements on the foil, glass plate and aluminum frame. This model produces a corrected value for the local surface heat flux and enables the computation of the bulk fluid temperature and heat transfer coefficient along the channel. The streamwise evolution of the heat transfer coefficient for single-phase laminar flow is compared to theoretical values for a uniform-flux boundary condition. Examples of the use of the facility for visualizing subcooled two-phase flows are presented. These examples include measurements of the surface temperature distribution around active nucleation sites and the construction of boiling curves for locations along the test surface. Points on the curve can be associated with specific image sequences so that the role of mechanisms such as nucleation and the sliding of confined bubbles may be discerned. [Copyright &y& Elsevier]

Published

2011

12. The effect of sliding bubbles on nucleate boiling of a subcooled liquid flowing in a narrow channel

Author

Ozer, Arif B., Oncel, Ahmet F., Hollingsworth, D. Keith, and Witte, Larry C.

Subjects

*BUBBLE dynamics, *NUCLEATE boiling, *HEAT transfer, *SURFACE coatings, *LIQUID crystals, *VIDEO recording, *LAMINAR flow, *NUCLEATION

Abstract

Abstract: An apparatus that produces flow and heat transfer in horizontal narrow channels was used to explore the physics of the onset of subcooled nucleate boiling for R-11 and Novec 649. The apparatus uses a downward-facing electrically-heated thin foil as a heater, with the outside of the heater coated with a liquid crystal to display full-field temperature distributions for the heater surface. Video recordings were made of the temperature fields for a given set of operating conditions, accompanied by video recordings of the boiling behavior of the fluids in the channel itself. These two recordings were superimposed spatially so that the influence of various bubble dynamics could be directly correlated to the temperature response of the heater. Data have been obtained in a series of experiments performed in a horizontal channel, approximately 1.2mm high×20mm wide×357mm long at mass fluxes indicative of laminar single phase flow in the channel. These data show that the enhancement of heat transfer behind the “boiling front”, i.e., the point in the channel where bubbles are observed to first nucleate, is caused primarily by sliding bubbles rather than the activation of additional nucleation sites. These results tend to confirm the speculation made with an apparatus that did not allow visual observation of the boiling phenomena that surface temperatures near the boiling front can be depressed even though active bubble nucleation is not occurring there. This leads to boiling curves that involve a “turning angle” type of behavior that connects single-phase convection heat transfer to nucleate boiling heat transfer. The results reported in this paper provide a much clearer physical description of the controlling features of the transition from convection to boiling than has been available in the past. [Copyright &y& Elsevier]

Published

2011

13. Two naturally occurring variants of the serotonin receptor gene HTR3C are associated with nausea in pregnancy.

Author

GOECKE, TAMME W., EKICI, ARIF B., NIESLER, BEATE, LOEHBERG, CHRISTIAN R., HAMMER, CHRISTIAN, RAPPOLD, GUDRUN, SCHANZE, DENNY, STRAUB, VERICA, ALTMANN, HANS-HARALD, STRISSEL, PAMELA, STRICK, REINER, BECKMANN, MATTHIAS W., and FASCHING, PETER A.

Subjects

*SINGLE nucleotide polymorphisms, *NAUSEA, *VOMITING, *SEROTONIN, *PREGNANCY complications

Abstract

Objective. To assess the association between pregnancy-associated symptoms and common single nucleotide polymorphisms (SNPs) in genes known to be involved in the pathogenesis of nausea and vomiting. Design. In a standardized, questionnaire-based interview, women selected from a control cohort for association studies were asked retrospectively about nausea and vomiting during their first pregnancy. Population. A total of 593 women who had completed at least one pregnancy and for whom germline DNA was available were selected. Methods. Eight SNPs in the serotonin receptor genes HTR3A, HTR3B, HTR3C, HTR3D, HTR3E, and NK1R (TACR1) were tested using polymerase chain reaction. The occurrence of nausea and vomiting was correlated with the patients' genotyping results and medical history parameters. Results. Both young age at first pregnancy and positive smoking status were significantly associated with vomiting and nausea during pregnancy. After adjustment for these two parameters, the two SNPs rs6806362 (odds ratio (OR) 1.38 per allele; 95% confidence interval (CI) 1.06-1.79; p = 0.017) and rs6807670 (OR 1.37; 95% CI 1.05-1.79 per allele; p = 0.023) were marginally associated with pregnancy-related nausea. None of the other polymorphisms showed any association. Conclusion. Polymorphisms in the subunit gene HTR3C of the serotonin receptor may be involved in the pathogenesis of pregnancy-associated nausea. [ABSTRACT FROM AUTHOR]

Published

2010

14. Neurokinin 1 receptor gene polymorphism might be correlated with recurrence rates in endometriosis.

Author

Renner, Stefan P., Ekici, Arif B., Maihöfner, Christian, Oppelt, Peter, Thiel, Falk C., Schrauder, Michael, Uenluehan, Nesrin, Bani, Mayada R., Strissel, Pamela L., Strick, Reiner, Beckmann, Matthias W., and Fasching, Peter A.

Subjects

*TACHYKININS, *GENETIC polymorphisms, *ENDOMETRIOSIS, *DISEASE relapse, *PAIN management, *DYSMENORRHEA, *GERMFREE life, *CASE-control method

Abstract

Introduction. Dysmenorrhoea is the major symptom in women with endometriosis. Recently, pain modulation through Neurokinin-1-receptor (NK1R) pathways have been investigated in neuropathic pain patients. Aim of this study was, therefore, to examine the effect of a single nucleotide polymorphism (SNP) of the NK1R gene on the susceptibility for endometriosis and the disease free survival (DFS) after surgery for endometriosis. Material and methods. A case-control study was conducted and germline DNA was isolated. Patients were followed up for a recurrence of the disease up to 4 years. Case-control analyses were performed for parameters of the medical history and the genotype of the NK1R-SNP rs881. Furthermore, DFS probabilities were calculated. Results. Concerning the DFS preoperative pain levels and the NK1R genotype were independent predictors for a recurrence with hazard ratios of 2.55 (95% CI: 1.32-4.95) for patients with a high preoperative pain level and 0.44 for patients with a heterozygous or homozygous variant genotype in rs881 (95% CI: 0.21-0.88). Conclusion. The polymorphism rs811 seems to be associated with a lower recurrence risk in endometriosis patients. Thus, there might be a clinical relevant role of the NK1 pathway in the pain perception of endometriosis patients. [ABSTRACT FROM AUTHOR]

Published

2009

15. Tracing Myelin Protein Zero (P0) in vivo by construction of P0-GFP fusion proteins.

Author

Ekici, Arif B., Oezbey, Sevinc, Fuchs, Christina, Nelis, Eva, Van Broeckhoven, Christine, Schachner, Melitta, and Rautenstrauss, Bernd

Subjects

*MYELIN proteins, *GENETIC mutation, *CHARCOT-Marie-Tooth disease, *AMINO acids, *MUTAGENESIS

Abstract

Background: Mutations in P0, the major protein of the myelin sheath in peripheral nerves, cause the inherited peripheral neuropathies Charcot-Marie-Tooth disease type 1B (CMT1B), Dejerine- Sottas syndrome (DSS) and congenital hypomyelination (CH). We reported earlier a de novo insertional mutation c.662_663GC (Ala221fs) in a DSS patient. The c.662_663GC insertion results in a frame shift mutation Ala221fs altering the C-terminal amino acid sequence. The adhesion-relevant intracellular RSTK domain is replaced by a sequence similar to Na+/K+ ATPase. To further clarify the molecular disease mechanisms in this sporadic patient we constructed wild type P0 and the c.662_663GC mutant expression cassettes by site-specific mutagenesis and transfected the constructs into insect cells (S2, High5). To trace the effects in live cells, green fluorescent protein (GFP) has been added to the carboxyterminus of the wild type and mutated P0 protein. Results: In contrast to the membrane-localized wild type P0-GFP the Ala221fs P0-GFP protein was detectable almost only in the cytoplasm of the cells, and a complete loss of adhesion function was observed. Conclusions: The present study provides evidence that GFP is a versatile tool to trace in vivo effects of P0 and its mutations. Not only a loss of adhesion function as a result of the loss of the RSTK domain, but also altered intracellular trafficking indicated by a loss of membrane insertion are possible consequences of the Ala221fs mutation. [ABSTRACT FROM AUTHOR]

Published

2002

16. Mutual Amplification of GLI2/Hedgehog and Transcription Factor JUN/AP‐1 Signaling in Fibroblasts in Systemic Sclerosis: Potential Implications for Combined Therapies.

Author

Bergmann, Christina, Chenguiti Fakhouri, Sara, Trinh‐Minh, Thuong, Filla, Tim, Rius Rigau, Aleix, Ekici, Arif B., Merlevede, Benita, Hallenberger, Ludwig, Zhu, Honglin, Dees, Clara, Matei, Alexandru‐Emil, Auth, Janina, Györfi, Andrea‐Hermina, Zhou, Xiang, Rauber, Simon, Bozec, Aline, Dickel, Nicholas, Liang, Chunguang, Kunz, Meik, and Schett, Georg

Abstract

Objective Methods Results Conclusion Deregulation of the cJUN/AP‐1 and hedgehog/GLI2 signaling pathways has been implicated in fibroblast activation in systemic sclerosis (SSc). However, the consequences of their concomitant up‐regulation are unknown. Here, we tested the hypothesis that mutual amplification of both pathways might drive persistent fibroblast activation.Cultured fibroblasts and skin sections of patients with diffuse SSc and healthy volunteers were analyzed. cJUN/AP‐1 signaling and hedgehog/GLI2 signaling were inhibited using knockdown and pharmacologic approaches. Hedgehog signaling was activated in mice by fibroblast‐specific overexpression of constitutively active Smoothened.cJUN and GLI2 are concomitantly up‐regulated and colocalize in fibroblasts of patients with SSc compared to healthy controls. Activation of hedgehog/GLI2 signaling induces the expression of cJUN in vitro and in vivo, whereas inactivation of GLI2 inhibits cJUN expression. Likewise, inactivation of cJUN impairs the expression of GLI2. This mutual regulation occurs at the level of transcription with binding of cJUN and GLI2 to specific binding motifs. Interference with this mutual amplification of cJUN signaling and GLI2 signaling inhibits fibroblast activation and collagen release: Inhibition of cJUN/AP‐1 signaling ameliorates hedgehog‐induced fibroblast activation and skin fibrosis in SmoACT mice with a reduction of skin thickness of 103% (P = 0.0043) in the treatment group compared to the fibrotic control group. Moreover, combined pharmacologic inhibition of cJUN/AP‐1 and hedgehog/GLI2 exerts additive antifibrotic effects in a model of TGFβ‐driven experimental fibrosis (TBRACT mice).The transcription factors cJUN and GLI2 reinforce each other's activity to promote fibroblast activation in SSc. Interruption of this crosstalk by combined inhibition of both pathways exerts additive antifibrotic effects at well‐tolerated doses. [ABSTRACT FROM AUTHOR]

Published

2024

17. The missing link: ARID1B non-truncating variants causing Coffin-Siris syndrome due to protein aggregation.

Author

Bosch, Elisabeth, Güse, Esther, Kirchner, Philipp, Winterpacht, Andreas, Walther, Mona, Alders, Marielle, Kerkhof, Jennifer, Ekici, Arif B., Sticht, Heinrich, Sadikovic, Bekim, Reis, André, and Vasileiou, Georgia

Subjects

*WESTERN immunoblotting, *GENETIC disorder diagnosis, *VIMENTIN, *CELL lines, *AMINO acids

Abstract

ARID1B is the most frequently mutated gene in Coffin-Siris syndrome (CSS). To date, the vast majority of causative variants reported in ARID1B are truncating, leading to nonsense-mediated mRNA decay. In the absence of experimental data, only few ARID1B amino acid substitutions have been classified as pathogenic, mainly based on clinical data and their de novo occurrence, while most others are currently interpreted as variants of unknown significance. The present study substantiates the pathogenesis of ARID1B non-truncating/NMD-escaping variants located in the SMARCA4-interacting EHD2 and DNA-binding ARID domains. Overexpression assays in cell lines revealed that the majority of EHD2 variants lead to protein misfolding and formation of cytoplasmic aggresomes surrounded by vimentin cage-like structures and co-localizing with the microtubule organisation center. ARID domain variants exhibited not only aggresomes, but also nuclear aggregates, demonstrating robust pathological effects. Protein levels were not compromised, as shown by quantitative western blot analysis. In silico structural analysis predicted the exposure of amylogenic segments in both domains due to the nearby variants, likely causing this aggregation. Genome-wide transcriptome and methylation analysis in affected individuals revealed expression and methylome patterns consistent with those of the pathogenic haploinsufficiency ARID1B alterations in CSS cases. These results further support pathogenicity and indicate two approaches for disambiguation of such variants in everyday practice. The few affected individuals harbouring EHD2 non-truncating variants described to date exhibit mild CSS clinical traits. In summary, this study paves the way for the re-evaluation of previously unclear ARID1B non-truncating variants and opens a new era in CSS genetic diagnosis. [ABSTRACT FROM AUTHOR]

Published

2024

18. 4,5-Dihydro-1H-pyrazolo[3,4-d]pyrimidine containing phenothiazines as antitubercular agents.

Author

Siddiqui, Arif B., Trivedi, Amit R., Kataria, Vipul B., and Shah, Viresh H.

Subjects

*PHENOTHIAZINE, *ANTITUBERCULAR agents, *PHARMACEUTICAL chemistry, *NUCLEAR magnetic resonance, *MYCOBACTERIUM tuberculosis, *DRUG development, *THERAPEUTICS

Abstract

Abstract: A series of novel dihydropyrazolo[3,4-d]pyrimidine derivatives bearing a phenothiazine nucleus were synthesized in excellent yields via a modified Biginelli multicomponent reaction. The newly synthesized compounds were characterized by IR, 1H NMR, 13C NMR, Mass spectra and elemental analysis followed by antimycobacterial screening. Among all the screened compounds, compound 4g showed most pronounced activity against Mycobacterium tuberculosis (Mtb) with minimum inhibitory concentration (MIC) of 0.02μg/mL, making it more potent than first line antitubercular drug isoniazid. [Copyright &y& Elsevier]

Published

2014

19. Apolipoprotein A-IV concentrations and cancer in a large cohort of chronic kidney disease patients: results from the GCKD study.

Author

Kollerits, Barbara, Gruber, Simon, Steinbrenner, Inga, Schwaiger, Johannes P., Weissensteiner, Hansi, Schönherr, Sebastian, Forer, Lukas, Kotsis, Fruzsina, Schultheiss, Ulla T., Meiselbach, Heike, Wanner, Christoph, Eckardt, Kai-Uwe, Kronenberg, Florian, Schneider, Markus P., Schiffer, Mario, Prokosch, Hans-Ulrich, Bärthlein, Barbara, Beck, Andreas, Reis, André, and Ekici, Arif B.

Subjects

*CHRONIC kidney failure, *CHRONICALLY ill, *KIDNEY physiology, *DISEASE risk factors

Abstract

Background: Chronic kidney disease (CKD) is highly connected to inflammation and oxidative stress. Both favour the development of cancer in CKD patients. Serum apolipoprotein A-IV (apoA-IV) concentrations are influenced by kidney function and are an early marker of kidney impairment. Besides others, it has antioxidant and anti-inflammatory properties. Proteomic studies and small case–control studies identified low apoA-IV as a biomarker for various forms of cancer; however, prospective studies are lacking. We therefore investigated whether serum apoA-IV is associated with cancer in the German Chronic Kidney Disease (GCKD) study. Methods: These analyses include 5039 Caucasian patients from the prospective GCKD cohort study followed for 6.5 years. Main inclusion criteria were an eGFR of 30–60 mL/min/1.73m2 or an eGFR > 60 mL/min/1.73m2 in the presence of overt proteinuria. Results: Mean apoA-IV concentrations of the entire cohort were 28.9 ± 9.8 mg/dL (median 27.6 mg/dL). 615 patients had a history of cancer before the enrolment into the study. ApoA-IV concentrations above the median were associated with a lower odds for a history of cancer (OR = 0.79, p = 0.02 when adjusted age, sex, smoking, diabetes, BMI, albuminuria, statin intake, and eGFRcreatinine). During follow-up 368 patients developed an incident cancer event and those with apoA-IV above the median had a lower risk (HR = 0.72, 95%CI 0.57–0.90, P = 0.004). Finally, 62 patients died from such an incident cancer event and each 10 mg/dL higher apoA-IV concentrations were associated with a lower risk for fatal cancer (HR = 0.62, 95%CI 0.44–0.88, P = 0.007). Conclusions: Our data indicate an association of high apoA-IV concentrations with reduced frequencies of a history of cancer as well as incident fatal and non-fatal cancer events in a large cohort of patients with CKD. [ABSTRACT FROM AUTHOR]

Published

2024

20. Genetic variations in estrogen and progesterone pathway genes in preeclampsia patients and controls in Bavaria.

Author

Pretscher, Jutta, Ruebner, Matthias, Ekici, Arif B., Rödl, Melanie, Huebner, Hanna, Schwitulla, Judith, Titzmann, Adriana, Hartwig, Charlotte, Beckmann, Matthias W., Fasching, Peter A., Schneider, Michael O., and Schwenke, Eva

Subjects

*GENES, *PREECLAMPSIA, *SINGLE nucleotide polymorphisms, *PROGESTERONE, *PROGESTERONE receptors

Abstract

Purpose: Hypertensive pregnancy disorders and preeclampsia are major causes of maternal and fetal morbidity and mortality worldwide. Many different organs are involved in the diseases' clinical phenotype. The underlying mechanism is still unknown, with a possible genetic component. This case–control study investigated effects on the risk of preeclampsia of genetic variations (single nucleotide polymorphisms, SNPs) in the estrogen and progesterone pathway genes. Methods: The study included 167 patients with preeclampsia and 115 healthy controls from the "Franconian Maternal Health Evaluation Studies" (FRAMES). All patients completed an epidemiological questionnaire, data from which were correlated with prospective data on pregnancy and labor. DNA was isolated from blood samples and genotyping was done by PCR. Variants in the aromatase gene CYP19A1 (rs10046, rs4646), progesterone receptor gene (rs1042838, rs10895068), and estrogen receptor-α gene (rs488133) were examined, and the genotype distribution in the two groups was analyzed statistically. Results: A significant difference in the distribution frequency of genotypes between preeclampsia patients and controls was identified in one of the five SNPs. For rs10895068 in the progesterone receptor gene, genotype G/A was significantly more frequent among cases than controls (P = 0.023). No significant differences between the two cohorts were found in the other SNPs. Conclusions: This study showed a significant association between only one SNP in the progesterone receptor and preeclampsia. Other studies have also noted genetic aspects of preeclampsia. The underlying mechanism and causal relationship are not yet known, and further research is needed to explain the extent of genetic variations and the causal relationship in preeclampsia. [ABSTRACT FROM AUTHOR]

Published

2021

21. Tobacco Smoke Exposure in Mice is Associated with Changes in the Expression of MMP-9 and MMP-2 in Infra-Renal Aortic Vascular Smooth Muscle Cells.

Author

Airhart, N., Arif, B., Ennis, T., and Curci, J.

Published

2014

22. ID: 167: The anti-viral properties of IL-17A in allergic asthma.

Author

Graser, Anna, Ekici, Arif B., Melichar, Volker O., Zimmermann, Theodor, Papadopoulos, Nikolaos G., Taka, Stella, Ferrazzi, Fulvia, Vuorinen, Tytti, and Finotto, Susetta

Subjects

*ASTHMA, *INTERLEUKIN-17, *CYTOKINES, *TYPE I interferons, *GENOMES

Abstract

In the latter part of the 20th century the prevalence of the chronic inflammatory disease Athma bronchiale increased especially in developed countries and affects children and adults. Besides a pathological expansion of Th2 cells, it has been also suggested that Th17 cells and their key cytokine IL17A play a relevant role during the development of asthma, although their particular role is not completely understood. Besides allergens, recurrent infections with Rhinovirus (RV), especially in early life, could increase the risk of asthma. Th17 cells and IL17A seem to modulate immune pathophysiology of viral infections, but their precise role during anti-viral immune responses is not yet clear. Therefore, we addressed the role of IL17A during allergic asthma and anti-viral immune responses. In a cohort of pre-school children with and without asthma, we found out that children with asthma suffer more often from lower respiratory tract infections than control children. Furthermore, we analysed a nasal–pharyngeal specimen for RV infection and isolated PBMCs from the whole blood of these children. We observed that the PBMCs of children with asthma and a RV infection in their upper airways express more IFNB and TBX21 but less OAS1 and IL17A than asthmatic children without a viral infection. In addition, we could show that rIL17A induces OAS1 gene expression and reduces viral replication in lung epithelial A549 cells. Thus, IL17A might be a promising anti-viral therapy for RV infection in asthma, because it would activate the cellular components to initiate OAS1 mediated anti-viral immune responses. [ABSTRACT FROM AUTHOR]

Published

2015

23. High resolution chromosomal microarray analysis in paediatric obsessive-compulsive disorder.

Author

Grünblatt, Edna, Oneda, Beatrice, Ekici, Arif B., Ball, Juliane, Geissler, Julia, Uebe, Steffen, Romanos, Marcel, Rauch, Anita, and Walitza, Susanne

Subjects

*MENTAL health services, *OBSESSIVE-compulsive disorder, *GENETICS of schizophrenia, *NEURODEVELOPMENTAL treatment, *DNA copy number variations, *GENETICS

Abstract

Background: Obsessive-Compulsive Disorder (OCD) is a common and chronic disorder in which a person has uncontrollable, reoccurring thoughts and behaviours. It is a complex genetic condition and, in case of early onset (EO), the patients manifest a more severe phenotype, and an increased heritability. Large (>500 kb) copy number variations (CNVs) previously associated with autism and schizophrenia have been reported in OCD. Recently, rare CNVs smaller than 500 kb overlapping risk loci for other neurodevelopmental conditions have also been reported in OCD, stressing the importance of examining CNVs of any size range. The aim of this study was to further investigate the role of rare and small CNVs in the aetiology of EO-OCD. Methods: We performed high-resolution chromosomal microarray analysis in 121 paediatric OCD patients and in 124 random controls to identify rare CNVs (>50 kb) which might contribute to EO-OCD. Results: The frequencies and the size of the observed rare CNVs in the patients did not differ from the controls. However, we observed a significantly higher frequency of rare CNVs affecting brain related genes, especially deletions, in the patients (OR = 1.98, 95% CI 1.02-3.84; OR = 3.61, 95% CI 1.14-11.41, respectively). Similarly, enrichment-analysis of CNVs gene content, performed with three independent methods, confirmed significant clustering of predefined genes involved in synaptic/brain related functional pathways in the patients but not in the controls. In two patients we detected de-novo CNVs encompassing genes previously associated with different neurodevelopmental disorders (NRXN1, ANKS1B, UHRF1BP1). Conclusions: Our results further strengthen the role of small rare CNVs, particularly deletions, as susceptibility factors for paediatric OCD. [ABSTRACT FROM AUTHOR]

Published

2017

24. ChemInform Abstract: 4,5-Dihydro-1H-pyrazolo[3,4-d]pyrimidine Containing Phenothiazines as Antitubercular Agents.

Author

Siddiqui, Arif B., Trivedi, Amit R., Kataria, Vipul B., and Shah, Viresh H.

Subjects

*PHENOTHIAZINE derivatives, *PYRIMIDINES, *ANTITUBERCULAR agents, *DRUG therapy for tuberculosis, *MYCOBACTERIUM tuberculosis, *THERAPEUTICS

Abstract

Novel pyrazolopyrimidine derivatives (IV) (11 examples) are synthesized in high yield via a modified Biginelli multicomponent reaction and screened for their antimycobacterial activities. [ABSTRACT FROM AUTHOR]

Published

2014

25. Impaired ATF3 signaling involves SNAP25 in SOD1 mutant ALS patients.

Author

Yazar, Volkan, Kühlwein, Julia K., Knehr, Antje, Grozdanov, Veselin, Ekici, Arif B., Ludolph, Albert C., and Danzer, Karin M.

Subjects

*MONONUCLEAR leukocytes, *AMYOTROPHIC lateral sclerosis, *GENE expression, *SUPEROXIDE dismutase, *CHROMOSOMES

Abstract

Epigenetic remodeling is emerging as a critical process for several neurodegenerative diseases, including amyotrophic lateral sclerosis (ALS). Genetics alone fails to explain the etiology of ALS, the investigation of the epigenome might therefore provide novel insights into the molecular mechanisms of the disease. In this study, we interrogated the epigenetic landscape in peripheral blood mononuclear cells (PBMCs) of familial ALS (fALS) patients with either chromosome 9 open reading frame 72 (C9orf72) or superoxide dismutase 1 (SOD1) mutation and aimed to identify key epigenetic footprints of the disease. To this end, we used an integrative approach that combines chromatin immunoprecipitation targeting H3K27me3 (ChIP-Seq) with the matching gene expression data to gain new insights into the likely impact of blood-specific chromatin remodeling on ALS-related molecular mechanisms. We demonstrated that one of the hub molecules that modulates changes in PBMC transcriptome in SOD1-mutant ALS patients is ATF3, which has been previously reported in an SOD1G93A mouse model. We also identified potential suppression of SNAP25, with impaired ATF3 signaling in SOD1-mutant ALS blood. Together, our study shed light on the mechanistic underpinnings of SOD1 mutations in ALS. [ABSTRACT FROM AUTHOR]

Published

2023

26. Genetic variants in the genes of the sex steroid hormone metabolism and depressive symptoms during and after pregnancy.

Author

Schneider, Michael O., Pretscher, Jutta, Goecke, Tamme W., Häberle, Lothar, Engel, Anne, Kornhuber, Johannes, Eichler, Anna, Ekici, Arif B., Beckmann, Matthias W., Fasching, Peter A., and Schwenke, Eva

Subjects

*GENETIC variation, *CATECHOL-O-methyltransferase gene, *SEX hormones, *SINGLE nucleotide polymorphisms, *EDINBURGH Postnatal Depression Scale, *RECURRENT miscarriage, *FETAL movement

Abstract

Purpose: The aim of this study was to conduct an association analysis of depressive symptoms and polymorphisms in the ESR1, PGR, CYP19A1, and COMT genes in pregnant and postpartum women. Methods: The Franconian Maternal Health Evaluation Study (FRAMES) recruited healthy pregnant women prospectively for assessment of maternal and fetal health. The German version of the 10-item Edinburgh Postnatal Depression Scale (EPDS) was completed at three time points in this prospective cohort study. Visit 1 was at study entry in the third trimester of pregnancy, visit 2 was shortly after birth, and visit 3 was 6–8 months after birth. Germline DNA and depression measurements from 361 pregnant women were available for analysis. Six single nucleotide polymorphisms (SNPs) in the above-mentioned genes were genotyped. After reconstruction of haplotypes for PGR (rs1042838 and rs10895068) and CYP19A1 (rs10046 and rs4646), a multifactorial linear mixed model was applied to the data to describe the association between haplotypes and depression values. The single SNPs for ESR1 (rs488133) and COMT (rs4680) were analyzed separately using linear mixed models analogously. Results: The mean antepartum EPDS measurement was 5.1, the mean postpartal measurement after 48–72 h was 3.5, and the mean value 6–8 months postpartum was 4.2. The SNPs in PGR were reconstructed into three haplotypes. The most common haplotype was GG, with 63.43% of patients carrying two copies and 33.52% carrying one copy. For haplotype GA, the group of carriers of two copies (0.28%) was combined with the carriers of one copy (9.70%). Haplotype reconstruction using CYP19A1 SNPs resulted in three haplotypes. The most common haplotype was TC, with 25.48% of patients carrying two copies and 51.52% one copy. None of the haplotype blocks and neither of the two single SNPs showed any significant associations with EPDS values. Conclusions: The candidate haplotypes analyzed in PGR and CYP19A1 and single SNPs in ESR1 and COMT did not show any association with depression scores as assessed by EPDS in this cohort of healthy unselected pregnant women. [ABSTRACT FROM AUTHOR]

Published

2023

27. Lifetime ovulatory years and risk of epithelial ovarian cancer: a multinational pooled analysis.

Author

Fu, Zhuxuan, Brooks, Maria Mori, Irvin, Sarah, Jordan, Susan, Aben, Katja K H, Anton-Culver, Hoda, Bandera, Elisa V, Beckmann, Matthias W, Berchuck, Andrew, Brooks-Wilson, Angela, Chang-Claude, Jenny, Cook, Linda S, Cramer, Daniel W, Cushing-Haugen, Kara L, Doherty, Jennifer A, Ekici, Arif B, Fasching, Peter A, Fortner, Renée T, Gayther, Simon A, and Gentry-Maharaj, Aleksandra

Subjects

*CONTRACEPTION, *OVARIAN epithelial cancer, *ORAL contraceptives, *BETA (Finance), *OVULATION, *ANOVULATION

Abstract

Background The role of ovulation in epithelial ovarian cancer (EOC) is supported by the consistent protective effects of parity and oral contraceptive use. Whether these factors protect through anovulation alone remains unclear. We explored the association between lifetime ovulatory years (LOY) and EOC. Methods LOY was calculated using 12 algorithms. Odds ratios (ORs) and 95% confidence intervals (CIs) estimated the association between LOY or LOY components and EOC among 26 204 control participants and 21 267 case patients from 25 studies. To assess whether LOY components act through ovulation suppression alone, we compared beta coefficients obtained from regression models with expected estimates assuming 1 year of ovulation suppression has the same effect regardless of source. Results LOY was associated with increased EOC risk (OR per year increase = 1.014, 95% CI = 1.009 to 1.020 to OR per year increase = 1.044, 95% CI = 1.041 to 1.048). Individual LOY components, except age at menarche, also associated with EOC. The estimated model coefficient for oral contraceptive use and pregnancies were 4.45 times and 12- to 15-fold greater than expected, respectively. LOY was associated with high-grade serous, low-grade serous, endometrioid, and clear cell histotypes (ORs per year increase = 1.054, 1.040, 1.065, and 1.098, respectively) but not mucinous tumors. Estimated coefficients of LOY components were close to expected estimates for high-grade serous but larger than expected for low-grade serous, endometrioid, and clear cell histotypes. Conclusions LOY is positively associated with nonmucinous EOC. Differences between estimated and expected model coefficients for LOY components suggest factors beyond ovulation underlie the associations between LOY components and EOC in general and for non-HGSOC. [ABSTRACT FROM AUTHOR]

Published

2023

28. ALS is imprinted in the chromatin accessibility of blood cells.

Author

Kühlwein, Julia K., Ruf, Wolfgang P., Kandler, Katharina, Witzel, Simon, Lang, Christina, Mulaw, Medhanie A., Ekici, Arif B., Weishaupt, Jochen H., Ludolph, Albert C., Grozdanov, Veselin, and Danzer, Karin M.

Abstract

Amyotrophic Lateral Sclerosis (ALS) is a complex and incurable neurodegenerative disorder in which genetic and epigenetic factors contribute to the pathogenesis of all forms of ALS. The interplay of genetic predisposition and environmental footprints generates epigenetic signatures in the cells of affected tissues, which then alter transcriptional programs. Epigenetic modifications that arise from genetic predisposition and systemic environmental footprints should in theory be detectable not only in affected CNS tissue but also in the periphery. Here, we identify an ALS-associated epigenetic signature (‘epiChromALS’) by chromatin accessibility analysis of blood cells of ALS patients. In contrast to the blood transcriptome signature, epiChromALS includes also genes that are not expressed in blood cells; it is enriched in CNS neuronal pathways and it is present in the ALS motor cortex. By combining simultaneous ATAC-seq and RNA-seq with single-cell sequencing in PBMCs and motor cortex from ALS patients, we demonstrate that epigenetic changes associated with the neurodegenerative disease can be found in the periphery, thus strongly suggesting a mechanistic link between the epigenetic regulation and disease pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2023

29. Vascular Smooth Muscle Cells From Abdominal Aortic Aneurysms Have Uniquely High Elastolytic Potential Associated With Activation of MMP-2

Author

Airhart, N.D., Arif, B., and Curci, J.

Published

2013

30. Reset of Inflammatory Priming of Joint Tissue and Reduction of the Severity of Arthritis Flares by Bromodomain Inhibition.

Author

Friščić, Jasna, Reinwald, Christiane, Böttcher, Martin, Houtman, Miranda, Euler, Maximilien, Chen, Xi, Walker, Kellie I., Kirchner, Philipp, Zhu, Honglin, Wirth, Benjamin, Weidner, Daniela, Krüger, René, Trajkovic, Vladimir, Ekici, Arif B., Klein, Kerstin, Mougiakakos, Dimitrios, Ospelt, Caroline, Schett, Georg, and Hoffmann, Markus H.

Subjects

*DRUG therapy for arthritis, *BROMODOMAIN-containing proteins, *BIOLOGICAL models, *FIBROBLASTS, *ANIMAL experimentation, *SEVERITY of illness index, *MICE, *SYNOVIAL fluid, *CHEMICAL inhibitors

Abstract

Objective: We have recently shown that priming of synovial fibroblasts (SFs) drives arthritis flares. Pathogenic priming of SFs is essentially mediated by epigenetic reprogramming. Bromodomain and extraterminal motif (BET) proteins translate epigenetic changes into transcription. Here, we used a BET inhibitor (I‐BET151) to target inflammatory tissue priming and to reduce flare severity in a murine experimental arthritis model. Methods: BALB/c mice were treated by intraperitoneal injection or by local injection in the paw with I‐BET151, which blocks the interaction of BET proteins with acetylated histones. We assessed the effects of I‐BET151 on acute arthritis and/or inflammatory tissue priming in a model of repeated injections of monosodium urate crystals or zymosan into the mouse paw. I‐BET151 was given before arthritis induction, at peak inflammation, or after healing of the first arthritis bout. We performed transcriptomic (RNA‐Seq), epigenomic (ATAC‐Seq), and functional (invasion, cytokine production, migration, senescence, metabolic flux) analyses of murine and human SFs treated with I‐BET151 in vitro or in vivo. Results: Systemic I‐BET151 administration did not affect acute inflammation but abolished inflammatory tissue priming and diminished flare severity in both preventive and therapeutic treatment settings. I‐BET151 was also effective when applied locally in the joint. BET inhibition also inhibited osteoclast differentiation, while macrophage activation in the joint was not affected. Flare reduction after BET inhibition was mediated, at least in part, by rolling back the primed transcriptional, metabolic, and pathogenic phenotype of SFs. Conclusion: Inflammatory tissue priming is dependent on transcriptional regulation by BET proteins, making them promising therapeutic targets for prevention of arthritis flares in previously affected joints. [ABSTRACT FROM AUTHOR]

Published

2023

31. QS412. Effect of Tobacco Smoke on Arterial Cell Populations and Stimulated Cytokine Responses

Author

Kittel, J., Arif, B., Pagano, M., and Curci, J.A.

Published

2009

32. Improved Bladder Tumor RNA Isolation from Archived Tissues Using Methylene Blue for Normalization, Multiplex RNA Hybridization, Sequencing and Subtyping.

Author

Köhler, Stefanie A., Brandl, Lisa, Strissel, Pamela L., Gloßner, Laura, Ekici, Arif B., Angeloni, Miriam, Ferrazzi, Fulvia, Bahlinger, Veronika, Hartmann, Arndt, Beckmann, Matthias W., Eckstein, Markus, and Strick, Reiner

Subjects

*NUCLEIC acid hybridization, *METHYLENE blue, *NUCLEIC acid isolation methods, *BLADDER cancer, *RNA, *UROTHELIUM

Abstract

Methylene blue (MB) is a dye used for histology with clinical importance and intercalates into nucleic acids. After MB staining of formalin fixed paraffin embedded (FFPE) muscle invasive bladder cancer (MIBC) and normal urothelium, specific regions could be microdissected. It is not known if MB influences RNA used for gene expression studies. Therefore, we analyzed MIBC using five different RNA isolation methods comparing patient matched FFPE and fresh frozen (FF) tissues pre-stained with or without MB. We demonstrate a positive impact of MB on RNA integrity with FF tissues using real time PCR with no interference of its chemical properties. FFPE tissues showed no improvement of RNA integrity, which we propose is due to formalin induced nucleotide crosslinks. Using direct multiplex RNA hybridization the best genes for normalization of MIBC and control tissues were identified from 34 reference genes. In addition, 5SrRNA and 5.8SrRNA were distinctive reference genes detecting <200 bp fragments important for mRNA analyses. Using these normalized RNAs from MB stained MIBC and applying multiplex RNA hybridization and mRNA sequencing, a minimal gene expression panel precisely identified luminal and basal MIBC tumor subtypes, important for diagnosis, prognosis and chemotherapy response. [ABSTRACT FROM AUTHOR]

Published

2022

33. Th2 single-cell heterogeneity and clonal distribution at distant sites in helminth-infected mice.

Author

Radtke, Daniel, Thuma, Natalie, Schülein, Christine, Kirchner, Philipp, Ekici, Arif B., Schober, Kilian, and Voehringer, David

Subjects

*TH2 cells, *HELMINTHIASIS, *IMMUNE response, *LUNG infections, *CELL differentiation, *HETEROGENEITY

Abstract

Th2 cells provide effector functions in type 2 immune responses to helminths and allergens. Despite knowledge about molecular mechanisms of Th2 cell differentiation, there is little information on Th2 cell heterogeneity and clonal distribution between organs. To address this, we performed combined single-cell transcriptome and T-cell receptor (TCR) clonotype analysis on murine Th2 cells in mesenteric lymph nodes (MLNs) and lung after infection with Nippostrongylus brasiliensis (Nb) as a human hookworm infection model. We find organ-specific expression profiles, but also populations with conserved migration or effector/resident memory signatures that unexpectedly cluster with potentially regulatory Il10posFoxp3neg cells. A substantial MLN subpopulation with an interferon response signature suggests a role for interferon signaling in Th2 differentiation or diversification. Further RNA-inferred developmental directions indicate proliferation as a hub for differentiation decisions. Although the TCR repertoire is highly heterogeneous, we identified expanded clones and CDR3 motifs. Clonal relatedness between distant organs confirmed effective exchange of Th2 effector cells, although locally expanded clones dominated the response. We further cloned an Nb-specific TCR from an expanded clone in the lung effector cluster and describe surface markers that distinguish transcriptionally defined clusters. These results provide insights in Th2 cell subset diversity and clonal relatedness in distant organs. [ABSTRACT FROM AUTHOR]

Published

2022

34. Rare Copy Number Variants Are a Common Cause of Short Stature.

Author

Zahnleiter, Diana, Uebe, Steffen, Ekici, Arif B., Hoyer, Juliane, Wiesener, Antje, Wieczorek, Dagmar, Kunstmann, Erdmute, Reis, André, Doerr, Helmuth-Guenther, Rauch, Anita, and Thiel, Christian T.

Subjects

*SHORT stature, *BODY size, *DWARFISM, *NEURODEGENERATION, *GENE expression

Abstract

Human growth has an estimated heritability of about 80%-90%. Nevertheless, the underlying cause of shortness of stature remains unknown in the majority of individuals. Genome-wide association studies (GWAS) showed that both common single nucleotide polymorphisms and copy number variants (CNVs) contribute to height variation under a polygenic model, although explaining only a small fraction of overall genetic variability in the general population. Under the hypothesis that severe forms of growth retardation might also be caused by major gene effects, we searched for rare CNVs in 200 families, 92 sporadic and 108 familial, with idiopathic short stature compared to 820 control individuals. Although similar in number, patients had overall significantly larger CNVs (p-value<1 x 1027). In a gene-based analysis of all non-polymorphic CNVs>50 kb for gene function, tissue expression, and murine knock-out phenotypes, we identified 10 duplications and 10 deletions ranging in size from 109 kb to 14 Mb, of which 7 were de novo (p<0.03) and 13 inherited from the likewise affected parent but absent in controls. Patients with these likely disease causing 20 CNVs were smaller than the remaining group (p<0.01). Eleven (55%) of these CNVs either overlapped with known microaberration syndromes associated with short stature or contained GWAS loci for height. Haploinsufficiency (HI) score and further expression profiling suggested dosage sensitivity of major growth-related genes at these loci. Overall 10% of patients carried a disease-causing CNV indicating that, like in neurodevelopmental disorders, rare CNVs are a frequent cause of severe growth retardation. [ABSTRACT FROM AUTHOR]

Published

2013

35. Reduced Syncytin-1 Expression Levels in Placental Syndromes Correlates with Epigenetic Hypermethylation of the ERVW-1 Promoter Region.

Author

Ruebner, Matthias, Strissel, Pamela L., Ekici, Arif B., Stiegler, Elisabeth, Dammer, Ulf, Goecke, Tamme W., Faschingbauer, Florian, Fahlbusch, Fabian B., Beckmann, Matthias W., and Strick, Reiner

Subjects

*SYNCYTINS, *GENE expression, *PLACENTA, *EPIGENETICS, *METHYLATION, *FETAL development, *PROMOTERS (Genetics), *CELL differentiation

Abstract

Terminal differentiation of villous cytotrophoblasts (CT) ends in formation of the multinucleated syncytiotrophoblast representing the fetal-maternal interface. Aberrations during this cell-fusion process are associated with Intrauterine Growth Restriction (IUGR), Preeclampsia (PE) and High Elevated Liver and Low Platelets (HELLP) Syndrome. Syncytin-1, the envelope gene of the human Endogenous Retrovirus ERVW-1, is one of the most important genes involved in cell-fusion and showed decreased gene expression during these pathological pregnancies. The aim of this study was to determine the methylation pattern of the entire promoter of ERVW-1 and to correlate these findings with the expression profile of Syncytin-1 in the placental syndromes. 14 isolated villous cytotrophoblasts from control (n = 3), IUGR (n = 3), PE (n = 3), PE/IUGR (n = 3) and HELLP/IUGR (n = 2) placentae were used to determine the mean methylation level (ML) for the ERVW-1 promoter region. ML rose significantly from 29% in control CTs to 49% in IUGR, 53% in PE, 47% in PE/IUGR and 64% in HELLP/IUGR indicating an epigenetic down-regulation of Syncytin-1 by promoter hypermethylation. DNA demethylation of the trophoblast like cell lines BeWo, JEG-3 and JAR with 5-AZA-2′desoxycytidine (AZA) showed an increased Syncytin-1 expression and fusion ability in all cell lines. Promoter activity of the 5′LTR could be inhibited by hypermethylation 42-fold using a luciferase based reporter-gene assay. Finally overexpression of the methyltransferases DNMT3a and LSH could be responsible for a decreased Syncytin-1 expression by promoter hypermethylation of ERVW-1. Our study linked decreased Syncytin-1 expression to an epigenetic hypermethylation of the entire promoter of ERVW-1. Based on our findings we are predicting a broad aberrant epigenetic DNA-methylation pattern in pathological placentae affecting placentogenesis, but also the development of the fetus and the mother during pregnancy. [ABSTRACT FROM AUTHOR]

Published

2013

36. Common variants at TRAF3IP2 are associated with susceptibility to psoriatic arthritis and psoriasis.

Author

Hüffmeier, Ulrike, Uebe, Steffen, Ekici, Arif B., Bowes, John, Giardina, Emiliano, Korendowych, Eleanor, Juneblad, Kristina, Apel, Maria, McManus, Ross, Ho, Pauline, Bruce, Ian N., Ryan, Anthony W., Behrens, Frank, Lascorz, Jesús, Böhm, Beate, Traupe, Heiko, Lohmann, Jörg, Gieger, Christian, Wichmann, Heinz-Erich, and Herold, Christine

Subjects

*PSORIATIC arthritis, *PSORIASIS, *DISEASE susceptibility, *IMMUNOGENETICS, *SKIN diseases

Abstract

Psoriatic arthritis (PsA) is an inflammatory joint disease that is distinct from other chronic arthritides and which is frequently accompanied by psoriasis vulgaris (PsV) and seronegativity for rheumatoid factor. We conducted a genome-wide association study in 609 German individuals with PsA (cases) and 990 controls with replication in 6 European cohorts including a total of 5,488 individuals. We replicated PsA associations at HLA-C and IL12B and identified a new association at TRAF3IP2 (rs13190932, P = 8.56 × 10−17). TRAF3IP2 was also associated with PsV in a German cohort including 2,040 individuals (rs13190932, P = 1.95 × 10−3). Sequencing of the exons of TRAF3IP2 identified a coding variant (p.Asp10Asn, rs33980500) as the most significantly associated SNP (P = 1.13 × 10−20, odds ratio = 1.95). Functional assays showed reduced binding of this TRAF3IP2 variant to TRAF6, suggesting altered modulation of immunoregulatory signals through altered TRAF interactions as a new and shared pathway for PsA and PsV. [ABSTRACT FROM AUTHOR]

Published

2010

37. FcγRIIa genotype is associated with acute coronary syndromes as first manifestation of coronary artery disease

Author

Raaz, Dorette, Herrmann, Martin, Ekici, Arif B., Klinghammer, Lutz, Lausen, Berthold, Voll, Reinhard E., Leusen, Jeanette H.W., van de Winkel, Jan G.J., Daniel, Werner G., Reis, André, and Garlichs, Christoph D.

Subjects

*CELL receptors, *NEUTROPHILS, *CORONARY disease, *GENETIC polymorphisms, *C-reactive protein, *CARDIOVASCULAR diseases risk factors, *HEART disease related mortality

Abstract

Abstract: Objective: Identification of clinically relevant determinants for acute coronary syndromes (ACS) promises reduction of ACS-associated mortality. C-reactive protein (CRP) has proved to be useful identifying people at risk for cardiovascular events. However, it is unknown whether genetic variants at Fcγ receptor IIa (FcγRIIa), the main receptor for CRP, are involved in CRP-related cardiovascular risk. We evaluated the potential impact of FcγRIIa through a genetic association study in patients with ACS. Methods and results: We conducted a genetic association study among 701 consecutive patients with first event of ACS compared to 467 patients with stable angina pectoris. All patients were genotyped for a frequent functional variant at position 131 of the mature FcγRIIa, where the arginine (R) allele results in an increased signal transduction upon CRP binding. In our study, the R/R131 genotype was significantly associated with ACS as the first manifestation of coronary artery disease (P =1.2×10−9, odds ratio 2.86, 95% CI: 2.06–3.99) compared to the non-R/R131 genotype. Conclusions: Our data show a genetic association of the FcγRIIa R/R131 genotype with a more frequent occurrence of ACS as the first manifestation of coronary artery disease, probably mediated via its interaction with CRP. Genotyping of this FcγRIIa variant could help to improve risk stratification in the course of coronary disease in the future. [Copyright &y& Elsevier]

Published

2009

38. Receptor of activated C kinase 1 (RACK1) is necessary for the 20-hydroxyecdysone-induced expression of the transcription factor CHR3 in the spruce budworm Choristoneura fumiferana.

Author

Quan, G. X., Krell, P. J., Arif, B. M., and Feng, Q.

Subjects

*SPRUCE budworm, *CHORISTONEURA, *ECDYSIS, *ARTHROPODA physiology, *INSECT development, *TRANSCRIPTION factors, *MOLECULAR biology

Abstract

To initiate moulting and metamorphosis, 20-hydroxyecdysone (20E) binds to its nuclear receptors and the ligand–receptor complex then mediates changes in gene expression. Phosphorylation of the receptors is required for their function. The intracellular signal transduction pathway that is involved in receptor phosphorylation remains elusive. This study provides evidence that the receptor of activated C kinase 1 (RACK1) and protein kinase C (PKC) signal transduction cascade is involved in the 20E-induced expression of the moult-associated transcription factor CHR3. A cDNA clone encoding a receptor of activated C kinase 1 was isolated from Choristoneura fumiferana ( CfRACK1). This single copy gene coded a 36 kDa protein and was expressed ubiquitously in all of the developmental stages and the tissues tested, including the midgut, epidermis, fat body, head, Malpighian tubules, ovary and testis of larvae. High levels of the transcripts were also detected in a midgut-derived CF-203 cell line. We noticed that the green fluorescence protein-fused CfRACK1 protein was distributed in the cytosol surrounding the nuclei in stably transformed cells. Interference of CfRACK1 mRNA suppressed the 20E-induced expression of the transcription factor CHR3. Dequalinium-14; 1,1′-decamethylenebis-4-aminoquinaldinium diiodide (DECA), an inhibitor of RACK1 binding to protein kinase C, blocked the 20E-induced expression of CHR3 and accumulation of the ecdysone receptor (EcR) in the nuclei. All of these data together suggest that 20E-induced expression of CHR3 may involve phosphorylation of the ecdysone receptor component through the PKC/RACK1 signal transduction cascade, which facilitates the import of the receptor into the nuclei of cells. [ABSTRACT FROM AUTHOR]

Published

2006

39. RNA sequencing reveals induction of specific renal inflammatory pathways in a rat model of malignant hypertension.

Author

Menendez-Castro, Carlos, Cordasic, Nada, Fahlbusch, Fabian B., Ekici, Arif B., Kirchner, Philipp, Daniel, Christoph, Amann, Kerstin, Velkeen, Roland, Wölfle, Joachim, Schiffer, Mario, Hartner, Andrea, and Hilgers, Karl F.

Subjects

*ANIMAL disease models, *HYPERTENSION, *RNA sequencing, *RENOVASCULAR hypertension, *RENIN-angiotensin system, *KIDNEY cortex

Abstract

In malignant hypertension, far more severe kidney injury occurs than in the "benign" form of the disease. The role of high blood pressure and the renin–angiotensin–aldosterone system is well recognized, but the pathogenesis of the renal injury of malignant hypertension (MH) remains incompletely understood. Using the rat model of two-kidney, one-clip renovascular hypertension in which some but not all animals develop MH, we performed a transcriptomic analysis of gene expression by RNA sequencing to identify transcriptional changes in the kidney cortex specific for MH. Differential gene expression was assessed in three groups: MH, non-malignant hypertension (NMH), and normotensive, sham-operated controls. To distinguish MH from NMH, we considered two factors: weight loss and typical renovascular lesions. Mean blood pressure measured intraarterially was elevated in MH (220 ± 6.5 mmHg) as well as in NMH (192 ± 6.4 mmHg), compared to controls (119 ± 1.7 mmHg, p < 0.05). Eight hundred eighty-six genes were exclusively regulated in MH only. Principal component analysis revealed a separated clustering of the three groups. The data pointed to an upregulation of many inflammatory mechanisms in MH including pathways which previously attracted relatively little attention in the setting of hypertensive kidney injury: Transcripts from all three complement activation pathways were upregulated in MH compared to NMH but not in NMH compared with controls; immunohistochemistry confirmed complement deposition in MH exclusively. The expression of chemokines attracting neutrophil granulocytes (CXCL6) and infiltration of myeloperoxidase-positive cells were increased only in MH rats. The data suggest that these pathways, especially complement deposition, may contribute to kidney injury under MH. Key messages: The most severe hypertension-induced kidney injury occurs in malignant hypertension. In a rat model of malignant hypertension, we assessed transcriptional responses in the kidney exposed to high blood pressure. A broad stimulation of inflammatory mechanisms was observed, but a few specific pathways were activated only in the malignant form of the disease, notably activation of the complement cascades. Complement inhibitors may alleviate the thrombotic microangiopathy of malignant hypertension even in the absence of primary complement abnormalities. [ABSTRACT FROM AUTHOR]

Published

2021

40. Neonatal nephron loss during active nephrogenesis results in altered expression of renal developmental genes and markers of kidney injury.

Author

Raming, Roman, Cordasic, Nada, Kirchner, Philipp, Ekici, Arif B., Fahlbusch, Fabian B., Woelfle, Joachim, Hilgers, Karl F., Hartner, Andrea, and Menendez-Castro, Carlos

Subjects

*KIDNEY tubules, *KIDNEY injuries, *GENETIC regulation, *FUNCTIONAL groups, *GENES, *PROXIMAL kidney tubules

Abstract

Preterm neonates are at a high risk for nephron loss under adverse clinical conditions. Renal damage potentially collides with postnatal nephrogenesis. Recent animal studies suggest that nephron loss within this vulnerable phase leads to renal damage later in life. Nephrogenic pathways are commonly reactivated after kidney injury supporting renal regeneration. We hypothesized that nephron loss during nephrogenesis affects renal development, which, in turn, impairs tissue repair after secondary injury. Neonates prior to 36 wk of gestation show an active nephrogenesis. In rats, nephrogenesis is ongoing until day 10 after birth. Mimicking the situation of severe nephron loss during nephrogenesis, male pups were uninephrectomized at day 1 of life (UNXd1). A second group of males was uninephrectomized at postnatal day 14 (UNXd14), after terminated nephrogenesis. Age-matched controls were sham operated. Three days after uninephrectomy transcriptional changes in the right kidney were analyzed by RNA-sequencing, followed by functional pathway analysis. In UNXd1, 1,182 genes were differentially regulated, but only 143 genes showed a regulation both in UNXd1 and UNXd14. The functional groups "renal development" and "kidney injury" were among the most differentially regulated groups and revealed distinctive alterations. Reduced expression of candidate genes concerning renal development (Bmp7, Gdnf, Pdgf-B, Wt1) and injury (nephrin, podocin, Tgf-fiT) were detected. The down-regulation of Bmp7 and Gdnf persisted until day 28. In UNXd14, Six2 was upregulated and Pax2 was downregulated. We conclude that nephron loss during nephrogenesis affects renal development and induces a specific regulation of genes that might hinder tissue repair after secondary kidney injury. [ABSTRACT FROM AUTHOR]

Published

2021

41. scRNA sequencing uncovers a TCF4-dependent transcription factor network regulating commissure development in mouse.

Author

Wittmann, Marie-Theres, Sayako Katada, Sock, Elisabeth, Kirchner, Philipp, Ekici, Arif B., Wegner, Michael, Kinichi Nakashima, Lie, Dieter Chichung, and Reis, André

Subjects

*TRANSCRIPTION factors, *NEURAL development, *RNA sequencing, *MICE, *GENE regulatory networks

Abstract

Transcription factor 4 (TCF4) is a crucial regulator of neurodevelopment and has been linked to the pathogenesis of autism, intellectual disability and schizophrenia. As a class I bHLH transcription factor (TF), it is assumed that TCF4 exerts its neurodevelopmental functions through dimerization with proneural class II bHLH TFs. Here, we aim to identify TF partners of TCF4 in the control of interhemispheric connectivity formation. Using a new bioinformatic strategy integrating TF expression levels and regulon activities from single cell RNA-sequencing data, we find evidence that TCF4 interacts with non-bHLH TFs and modulates their transcriptional activity in Satb2+ intercortical projection neurons. Notably, this network comprises regulators linked to the pathogenesis of neurodevelopmental disorders, e.g. FOXG1, SOX11 and BRG1. In support of the functional interaction of TCF4 with non-bHLH TFs, we find that TCF4 and SOX11 biochemically interact and cooperatively control commissure formation in vivo, and regulate the transcription of genes implicated in this process. In addition to identifying new candidate interactors of TCF4 in neurodevelopment, this study illustrates how scRNA-Seq data can be leveraged to predict TF networks in neurodevelopmental processes. [ABSTRACT FROM AUTHOR]

Published

2021

42. Genetic variants in the glucocorticoid pathway genes and birth weight.

Author

Schneider, Michael O., Hübner, Theresa, Pretscher, Jutta, Goecke, Tamme W., Schwitulla, Judith, Häberle, Lothar, Kornhuber, Johannes, Ekici, Arif B, Beckmann, Matthias W., Fasching, Peter A., and Schwenke, Eva

Subjects

*BIRTH weight, *GENES, *FETAL movement, *PARITY (Obstetrics), *BODY mass index, *SINGLE nucleotide polymorphisms, *HYPOTHALAMIC-pituitary-adrenal axis

Abstract

Purpose: The aim of this study was to examine associations between single nucleotide polymorphisms (SNPs) that tag genetic variation in the glucocorticoid pathways (particularly in maternal genes FKBP5, NR3C1, and CRHR1) and birth weight. Methods: The Franconian Maternal Health Evaluation Study (FRAMES) recruited healthy pregnant women prospectively for the assessment of maternal and fetal health. Germline DNA was collected from 375 pregnant women. Nine SNPs in the above-mentioned genes were genotyped. After reconstruction of haplotypes for each gene, a linear regression model was applied to the data to describe the association between haplotypes and birth weight. Results: Female sex in the newborn (compared to male) was associated with lower birth weight, whereas a later week of gestation, higher body mass index pre-pregnancy, and higher parity were associated with higher birth weight. No association with birthweight was shown for the haplotypes of the selected SNPs. Conclusions: In this cohort of healthy unselected pregnant women, the analyzed candidate haplotypes in FKBP5, NR3C1, and CRHR1 did not show any association with birth weight. This might be in line with several other studies that have found no influence of fetal polymorphisms in the glucocorticoid receptor gene or triggers of the maternal HPA axis such as stress and psychosocial problems on birth weight. However, the small sample size in this study and the lack of consideration of individual risk factors and levels of stress in this cohort needs to be taken into account when interpreting the results. [ABSTRACT FROM AUTHOR]

Published

2021

43. Myeloperoxidase Modulates Inflammation in Generalized Pustular Psoriasis and Additional Rare Pustular Skin Diseases.

Author

Haskamp, Stefan, Bruns, Heiko, Hahn, Madelaine, Hoffmann, Markus, Gregor, Anne, Löhr, Sabine, Hahn, Jonas, Schauer, Christine, Ringer, Mark, Flamann, Cindy, Frey, Benjamin, Lesner, Adam, Thiel, Christian T., Ekici, Arif B., von Hörsten, Stephan, Aßmann, Gunter, Riepe, Claudia, Euler, Maximilien, Schäkel, Knut, and Philipp, Sandra

Subjects

*SKIN diseases, *ZYMOGENS, *PATHOLOGY, *PSORIASIS, *MYELOPEROXIDASE

Abstract

Generalized pustular psoriasis (GPP) is a severe multi-systemic inflammatory disease characterized by neutrophilic pustulosis and triggered by pro-inflammatory IL-36 cytokines in skin. While 19%–41% of affected individuals harbor bi-allelic mutations in IL36RN , the genetic cause is not known in most cases. To identify and characterize new pathways involved in the pathogenesis of GPP, we performed whole-exome sequencing in 31 individuals with GPP and demonstrated effects of mutations in MPO encoding the neutrophilic enzyme myeloperoxidase (MPO). We discovered eight MPO mutations resulting in MPO -deficiency in neutrophils and monocytes. MPO mutations, primarily those resulting in complete MPO deficiency, cumulatively associated with GPP (p = 1.85E−08; OR = 6.47). The number of mutant MPO alleles significantly differed between 82 affected individuals and >4,900 control subjects (p = 1.04E−09); this effect was stronger when including IL36RN mutations (1.48E−13) and correlated with a younger age of onset (p = 0.0018). The activity of four proteases, previously implicated as activating enzymes of IL-36 precursors, correlated with MPO deficiency. Phorbol-myristate-acetate-induced formation of neutrophil extracellular traps (NETs) was reduced in affected cells (p = 0.015), and phagocytosis assays in MPO-deficient mice and human cells revealed altered neutrophil function and impaired clearance of neutrophils by monocytes (efferocytosis) allowing prolonged neutrophil persistence in inflammatory skin. MPO mutations contribute significantly to GPP's pathogenesis. We implicate MPO as an inflammatory modulator in humans that regulates protease activity and NET formation and modifies efferocytosis. Our findings indicate possible implications for the application of MPO inhibitors in cardiovascular diseases. MPO and affected pathways represent attractive targets for inducing resolution of inflammation in neutrophil-mediated skin diseases. [ABSTRACT FROM AUTHOR]

Published

2020

44. Genetic interaction screen for severe neurodevelopmental disorders reveals a functional link between Ube3a and Mef2 in Drosophila melanogaster.

Author

Straub, Jonas, Gregor, Anne, Sauerer, Tatjana, Fliedner, Anna, Distel, Laila, Suchy, Christine, Ekici, Arif B., Ferrazzi, Fulvia, and Zweier, Christiane

Subjects

*GENES, *NEURODEVELOPMENTAL treatment, *DROSOPHILA melanogaster, *PHENOTYPES, *MYONEURAL junction

Abstract

Neurodevelopmental disorders (NDDs) are clinically and genetically extremely heterogeneous with shared phenotypes often associated with genes from the same networks. Mutations in TCF4, MEF2C, UBE3A, ZEB2 or ATRX cause phenotypically overlapping, syndromic forms of NDDs with severe intellectual disability, epilepsy and microcephaly. To characterize potential functional links between these genes/proteins, we screened for genetic interactions in Drosophila melanogaster. We induced ubiquitous or tissue specific knockdown or overexpression of each single orthologous gene (Da, Mef2, Ube3a, Zfh1, XNP) and in pairwise combinations. Subsequently, we assessed parameters such as lethality, wing and eye morphology, neuromuscular junction morphology, bang sensitivity and climbing behaviour in comparison between single and pairwise dosage manipulations. We found most stringent evidence for genetic interaction between Ube3a and Mef2 as simultaneous dosage manipulation in different tissues including glia, wing and eye resulted in multiple phenotype modifications. We subsequently found evidence for physical interaction between UBE3A and MEF2C also in human cells. Systematic pairwise assessment of the Drosophila orthologues of five genes implicated in clinically overlapping, severe NDDs and subsequent confirmation in a human cell line revealed interactions between UBE3A/Ube3a and MEF2C/Mef2, thus contributing to the characterization of the underlying molecular commonalities. [ABSTRACT FROM AUTHOR]

Published

2020

45. Dissecting TSC2-mutated renal and hepatic angiomyolipomas in an individual with ARID1B-associated intellectual disability.

Author

Popp, Bernt, Agaimy, Abbas, Kraus, Cornelia, Knaup, Karl X., Ekici, Arif B., Uebe, Steffen, Reis, André, Wiesener, Michael, and Zweier, Christiane

Subjects

*TUBEROUS sclerosis, *INTELLECTUAL disabilities, *THERAPEUTICS, *MOLECULAR diagnosis, TUMOR genetics

Abstract

Background: Several subunits of the SWI/SNF chromatin remodeling complex are implicated in both cancer and neurodevelopmental disorders (NDD). Though there is no clinical evidence for an increased tumor risk in individuals with NDDs due to germline mutations in most of these genes so far, this has been repeatedly proposed and discussed. A young woman with NDD due to a de novo mutation in ARID1B now presented with a large renal (> 19 cm in diameter) and multiple hepatic angiomyolipomas (AMLs) but no other signs of tuberous sclerosis complex.Methods: We analyzed tumor and healthy tissue samples with exome and panel sequencing.Results: Additionally to the previously known, germline ARID1B variant we identified a post-zygotic truncating TSC2 variant in both renal and hepatic AMLs but not in any of the healthy tissues. We did not detect any further, obvious tumor driver events. The identification of a passenger variant in SIPA1L3 in both AMLs points to a common clonal origin. Metastasis of the renal AML into the liver is unlikely on the basis of discordant histopathological features. Our findings therefore point to very low-grade mosaicism for the TSC2 variant, possibly in a yet unknown mesenchymal precursor cell that expanded clonally during tumor development. A possible contribution of the germline ARID1B variant to the tumorigenesis remains unclear but cannot be excluded given the absence of any other evident tumor drivers in the AMLs.Conclusion: This unique case highlights the blurred line between tumor genetics and post-zygotic events that can complicate exact molecular diagnoses in patients with rare manifestations. It also demonstrates the relevance of multiple disorders in a single individual, the challenges of detecting low-grade mosaicisms, and the importance of proper diagnosis for treatment and surveillance. [ABSTRACT FROM AUTHOR]

Published

2019

46. Biallelic intragenic deletion in MASP1 in an adult female with 3MC syndrome.

Author

Graul-Neumann, Luitgard M., Mensah, Martin A., Klopocki, Eva, Uebe, Steffen, Ekici, Arif B., Thiel, Christian T., Reis, André, and Zweier, Christiane

Subjects

*DELETION mutation, *MUSCLE dysmorphia, *INTELLECTUAL disabilities, *EXOMES, *PALATE

Abstract

3MC syndrome is a rare autosomal recessive disorder with characteristic craniofacial dysmorphism and multiple anomalies. It is caused by biallelic mutations in one of three genes, MASP1 , COLEC11 and COLEC10 , all encoding factors of the lectin complement pathway. In MASP1 , either truncating mutations or missense variants in exon 12 encoding the C-terminal serine protease domain specific for isoform MASP-3 are causative. By trio exome sequencing we now identified a novel, homozygous 2kb deletion, partially affecting exon 12 in an adult female with the typical facial gestalt of 3MC syndrome and hearing loss, but without the main feature cleft lip/palate, and without intellectual disability, or short stature. We therefore expand the MASP1 associated mutational and clinical spectrum and describe the development of her clinical presentation over a period of 21 years. As the homozygous deletion in our patient was only found by thorough and visual evaluation of the whole exome sequencing data, such deletions might escape detection in some routine diagnostic workflows and might explain a few of the so far molecularly unconfirmed cases of 3MC syndrome. [ABSTRACT FROM AUTHOR]

Published

2018

47. Prenatal androgen receptor activation determines adult alcohol and water drinking in a sex-specific way.

Author

Huber, Sabine E., Zoicas, Iulia, Reichel, Martin, Mühle, Christiane, Büttner, Christian, Ekici, Arif B., Eulenburg, Volker, Lenz, Bernd, Kornhuber, Johannes, and Müller, Christian P.

Subjects

*ALCOHOLISM, *ANDROGEN receptors, *SEX hormones, *MENTAL illness, *GENDER differences (Psychology), *EMBRYOLOGY

Abstract

Alcohol use disorders are major psychiatric disorders. Correlational studies in humans suggested organizational hormonal effects during embryonic development as a risk factor for adult alcohol dependence. Permanent changes can be induced by the activity of sex hormones, like testosterone. Here, we demonstrate a relationship between prenatal androgen receptor (AR)-activation and adult alcohol as well as water drinking in mice in a sex-dependent fashion. Prenatal AR inhibition using the antagonist flutamide decreased adult male alcohol consumption. In contrast, prenatal AR activation by dihydrotestosterone (DHT) led to an increase in adult alcohol consumption in females. These effects were different in adult water drinking, flutamide increased water consumption in females and DHT increased water consumption in males. Prenatal flutamide reduced locomotion and anxiety in adult males but was ineffective in females. We found that prenatal AR activation controls adult levels of monoaminergic modulatory transmitters in the brain and blood hormone levels in a sex-specific way. RNA-Seq analysis confirmed a prenatal AR mediated control of adult expression of alcohol drinking-related genes like Bdnf and Per2. These findings demonstrate that prenatal androgen activity is a risk factor for the establishment of alcohol consumption in adults by its organizational effects. [ABSTRACT FROM AUTHOR]

Published

2018

48. Genetic overlap between endometriosis and endometrial cancer: evidence from cross‐disease genetic correlation and GWAS meta‐analyses.

Author

Painter, Jodie N., O'Mara, Tracy A., Morris, Andrew P., Cheng, Timothy H. T., Gorman, Maggie, Martin, Lynn, Hodson, Shirley, Jones, Angela, Martin, Nicholas G., Gordon, Scott, Henders, Anjali K., Attia, John, McEvoy, Mark, Holliday, Elizabeth G., Scott, Rodney J., Webb, Penelope M., Fasching, Peter A., Beckmann, Matthias W., Ekici, Arif B., and Hein, Alexander

Subjects

*ENDOMETRIOSIS, *ENDOMETRIAL cancer, *GENETIC correlations, *EPIDEMIOLOGY, *GENOMES, *REGRESSION analysis, *GENETICS

Abstract

Abstract: Epidemiological, biological, and molecular data suggest links between endometriosis and endometrial cancer, with recent epidemiological studies providing evidence for an association between a previous diagnosis of endometriosis and risk of endometrial cancer. We used genetic data as an alternative approach to investigate shared biological etiology of these two diseases. Genetic correlation analysis of summary level statistics from genomewide association studies (GWAS) using LD Score regression revealed moderate but significant genetic correlation (rg = 0.23, P = 9.3 × 10−3), and SNP effect concordance analysis provided evidence for significant SNP pleiotropy (P = 6.0 × 10−3) and concordance in effect direction (P = 2.0 × 10−3) between the two diseases. Cross‐disease GWAS meta‐analysis highlighted 13 distinct loci associated at P ≤ 10−5 with both endometriosis and endometrial cancer, with one locus (SNP rs2475335) located within PTPRD associated at a genomewide significant level (P = 4.9 × 10−8, OR = 1.11, 95% CI = 1.07–1.15). PTPRD acts in the STAT3 pathway, which has been implicated in both endometriosis and endometrial cancer. This study demonstrates the value of cross‐disease genetic analysis to support epidemiological observations and to identify biological pathways of relevance to multiple diseases. [ABSTRACT FROM AUTHOR]

Published

2018

49. Mutations in the BAF-Complex Subunit DPF2 Are Associated with Coffin-Siris Syndrome.

Author

Vasileiou, Georgia, Vergarajauregui, Silvia, Endele, Sabine, Popp, Bernt, Büttner, Christian, Ekici, Arif B., Gerard, Marion, Bramswig, Nuria C., Albrecht, Beate, Clayton-Smith, Jill, Morton, Jenny, Tomkins, Susan, Karen Low, Weber, Astrid, Wenzel, Maren, Altmüller, Janine, Yun Li, Wollnik, Bernd, Hogansonc, George, and Plona, Maria-Renée

Subjects

*GENETIC mutation, *RECOMBINANT proteins, *HISTONES, *CELL lines, *SPEECH disorders

Abstract

Variants affecting the function of different subunits of the BAF chromatin-remodelling complex lead to various neurodevelopmental syndromes, including Coffin-Siris syndrome. Furthermore, variants in proteins containing PHD fingers, motifs recognizing specific histone tail modifications, have been associated with several neurological and developmental-delay disorders. Here, we report eight heterozygous de novo variants (one frameshift, two splice site, and five missense) in the gene encoding the BAF complex subunit double plant homeodomain finger 2 (DPF2). Affected individuals share common clinical features described in individuals with Coffin-Siris syndrome, including coarse facial features, global developmental delay, intellectual disability, speech impairment, and hypoplasia of fingernails and toenails. All variants occur within the highly conserved PHD1 and PHD2 motifs. Moreover, missense variants are situated close to zinc binding sites and are predicted to disrupt these sites. Pull-down assays of recombinant proteins and histone peptides revealed that a subset of the identified missense variants abolish or impaire DPF2 binding to unmodified and modified H3 histone tails. These results suggest an impairment of PHD finger structural integrity and cohesion and most likely an aberrant recognition of histone modifications. Furthermore, the overexpression of these variants in HEK293 and COS7 cell lines was associated with the formation of nuclear aggregates and the recruitment of both wild-type DPF2 and BRG1 to these aggregates. Expression analysis of truncating variants found in the affected individuals indicated that the aberrant transcripts escape nonsense-mediated decay. Altogether, we provide compelling evidence that de novo variants in DPF2 cause Coffin-Siris syndrome and propose a dominant-negative mechanism of pathogenicity. [ABSTRACT FROM AUTHOR]

Published

2018

50. Transcriptome sequencing reveals maelstrom as a novel target gene of the terminal system in the red flour beetle Tribolium castaneum.

Author

Pridohl, Fabian, Weißkopf, Matthias, Koniszewski, Nikolaus, Sulzmaier, Andreas, Uebe, Steffen, Ekici, Arif B., and Schoppmeier, Michael

Subjects

*RED flour beetle, *INSECT embryology, *DROSOPHILA

Abstract

Terminal regions of the Drosophila embryo are patterned by the localized activation of the Torso-RTK pathway, which promotes the downregulation of Capicua. In the short-germ beetle Tribolium, the function of the terminal system appears to be rather different, as the pathway promotes axis elongation and, in addition, is required for patterning the extra-embryonic serosa at the anterior. Here, we show that Torso signalling also induces gene expression by relieving Capicua-mediated repression in Tribolium. Given that the majority of Torso target genes remain to be identified, we established a differential gene-expression screen. A subset of 50 putative terminal target genes was screened for functions in early embryonic patterning. Of those, 13 genes show early terminal expression domains and also phenotypes were related to terminal patterning. Among others, we found the PIWI-interacting RNA factor Maelstrom to be crucial for early embryonic polarization. Tc-mael is required for proper serosal size regulation and head morphogenesis. Moreover, Tc-mael promotes growth-zone formation and axis elongation. Our results suggest that posterior patterning by Torso may be realized through Maelstrom-dependent activation of posterior Wnt domains. [ABSTRACT FROM AUTHOR]

Published

2017