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51. Determinants of discordance in patients' and physicians' rating of rheumatoid arthritis disease activity

Author

Khan, Nasim A., primary, Spencer, Horace J., additional, Abda, Esam, additional, Aggarwal, Amita, additional, Alten, Rieke, additional, Ancuta, Codrina, additional, Andersone, Daina, additional, Bergman, Martin, additional, Craig‐Muller, Jurgen, additional, Detert, Jacqueline, additional, Georgescu, Lia, additional, Gossec, Laure, additional, Hamoud, Hisham, additional, Jacobs, Johannes W. G., additional, Laurindo, Ieda Maria Magalhaes, additional, Majdan, Maria, additional, Naranjo, Antonio, additional, Pandya, Sapan, additional, Pohl, Christof, additional, Schett, Georg, additional, Selim, Zahraa I., additional, Toloza, Sergio, additional, Yamanaka, Hisahi, additional, and Sokka, Tuulikki, additional

Published
2012
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52. The Impact of Porphyromonas gingivalis Lipids on Apoptosis of Primary Human Chondrocytes.

Author

Röhner, Eric, Hoff, Paula, Matziolis, Georg, Perka, Carsten, Riep, Birgit, Nichols, Frank C., Kielbassa, Andrej M., Detert, Jacqueline, Burmester, Gerd R., Buttgereit, Frank, Zahlten, Janine, and Pischon, Nicole

Subjects
PORPHYROMONAS gingivalis, LIPIDS, APOPTOSIS, CARTILAGE cells, PERIODONTAL disease, RHEUMATOID arthritis, ANNEXINS
Abstract

The role of oral bacterial infections including periodontal disease in the pathogenesis of rheumatoid arthritis (RA) has gained increasing interest. Among the major periodontal pathogens, Porphyromonas gingivalis has been mostly associated with RA pathogenesis. The aim of this study was to analyze the effect of P. gingivalis total lipid (TL) fraction and dihydroceramides, as potent virulence factors, on human primary chondrocytes. Primary chondrocyte cultures were incubated with P. gingivalis phosphoglycerol dihydroceramide (PG DHC) lipids, the TL fraction or phosphoethanolamine dihydroceramide. Cell morphology changes were determined by phase contrast light microscopy. Early and late apoptosis cell analysis was performed by Annexin-V, active caspases, and 7-Aminoactinomycin D staining, and examined by flow cytometry, and cell necrosis was evaluated by lactate dehydrogenase release. Procaspase-3 activation was determined by Western blot analysis. Microscopic analysis showed altered cell morphology and cell shrinkage following incubation with P. gingivalis TLs and PG DHC lipids. Flow cytometry demonstrated an increase of Annexin-V positive and active caspases positive chondrocytes after incubation with TL and PG DHC fractions but not after phosphoethanolamine dihydroceramide (control lipid) treatment or in untreated control cells. Furthermore, Western blot analysis showed an early cleavage of procaspase-3 after 1 hr. Significant lactate dehydrogenase release following incubation with P. gingivalis lipids was demonstrated. The present data demonstrate that P. gingivalis lipids promote apoptosis in primary human chondrocytes, and thereby may contribute to the joint damage seen in the pathogenesis of RA. [ABSTRACT FROM AUTHOR]

Published
2012
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55. Plant-derived pectin nanocoatings to prevent inflammatory cellular response of osteoblasts following Porphyromonas gingivalis infection

Author

Meresta, Anna, Folkert, Justyna, Gaber, Timo, Miksch, Korneliusz, Buttgereit, Frank, Detert, Jacqueline, Pischon, Nicole, and Gurzawska, Katarzyna

Subjects
nanocoatings, inflammation, osteoblasts, 600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit, Porphyromonas gingivalis, 3. Good health, Rhamnogalacturonan-I
Abstract

Background: Bioengineered plant-derived Rhamnogalacturonan-Is (RG-Is) from pectins are potential candidates for surface nanocoating of medical devices. It has recently been reported that RG-I nanocoatings may prevent bacterial infection and improve the biocompatibility of implants. The aim of the study was to evaluate in vitro impact of bioengineered RG-I nanocoatings on osteogenic capacity and proinflammatory cytokine response of murine osteoblasts following Porphyromonas gingivalis infection. Methods: Murine MC3T3-E1 osteoblasts and isolated primary calvarial osteoblasts from C57BL/6J (B6J osteoblasts) mice were infected with P. gingivalis and incubated on tissue culture polystyrene plates with or without nanocoatings of unmodified RG-Is isolated from potato pulps (PU) or dearabinanated RG-Is (PA). To investigate a behavior of infected osteoblasts cultured on RG-Is cell morphology, proliferation, metabolic activity, mineralization and osteogenic and pro-inflammatory gene expression were examined. Results: Following P. gingivalis infection, PA, but not PU, significantly promoted MC3T3-E1 and BJ6 osteoblasts proliferation, metabolic activity, and calcium deposition. Moreover, Il-1b, Il-6, TNF-α, and Rankl gene expressions were downregulated in cells cultured on PU and to a higher extent on PA as compared to the corresponding control, whereas Runx, Alpl, Col1a1, and Bglap gene expressions were upregulated vice versa. Conclusion: Our data clearly showed that pectin RG-Is nanocoating with high content of galactan (PA) reduces the osteoblastic response to P. gingivalis infection in vitro and may, therefore, reduce a risk of inflammation especially in immunocompromised patients with rheumatoid or periodontal disorders.

56. Rheumatoid arthritis - clinical aspects: 134. Predictors of Joint Damage in South Africans with Rheumatoid Arthritis

Author

Ickinger, Claudia, Musenge, Eustasius, Tikly, Mohammed, Barnes, Jonathan, Donnison, C., Scott, M., Bartholomew, Peter, Rynne, Martin, Hamilton, Jennifer, Saravanan, V., Heycock, Carol, Kelly, Clive, de la Torre, Inmaculada, Moura, Rita A., Leandro, Maria, Edwards, Jonathan, Cambridge, Geraldine, Edwards, Johnathan, Daniels, Louise E., Gullick, Nicola J., Rees, Jonathan D., Kirkham, Bruce W., Rees, Jonathan, Scott, Ian C., Johnson, Deborah, Scott, David L., Kingsley, Gabrielle, Ma, Margaret H., Cope, Andrew P., Brode, Sven, Nisar, Muhammad K., Östör, Andrew J., Oakley, Stephen P., Jones, Tim, Mistlin, Alan, Panayi, Gabriel S., El Miedany, Yasser, Palmer, Deborah, Porkodi, Ramanathan, Rajendran, Panchapakesa, Waller, Rosemary, Williamson, Lyn, Collins, David, Price, Elizabeth, Juarez, Maria J., El Gaafary, Maha, Youssef, sally, Cramp, Fiona, Hewlett, Sarah, Almeida, Celia, Kirwan, John, Choy, Ernest, Chalder, Trudie, Pollock, Jon, Christensen, Robin, Mirjafari, Hoda, Verstappen, Suzanne, Bunn, Diane, Edlin, Helena, Charlton-Menys, Valentine, Pemberton, Philip, Marshall, Tarnya, Wilson, Paddy, Lunt, Mark, Symmons, Deborah, Bruce, Ian N., Bell, Carolyn, Rowe, Ian F., Jayakumar, Keeranur, Norton, Sam J., Dixey, Josh, Williams, Peter, Young, Adam, Kurunadalingam, Hariney, Parwaiz, Iram, Kumar, Kanta, Howlett, Kath, Hands, Becki, Raza, Karim, Pitzalis, Costantino, Buckley, Chris, Kelly, Stephen, Filer, Andrew, Wheater, Gill, Hogan, Vanessa E., Onno Teng, YK, Tekstra, Janneke, Tuck, Stephen P., Lafeber, Floris P., Huizinga, Tom W., Bijlsma, Johannes W., Francis, Roger M., Datta, Harish K., van Laar, Jaap, Pratt, Arthur G., Charles, Peter J., Choudhury, Muslima, Wilson, Gill, Venables, Patrick J., Isaacs, John, Stack, Rebecca, Kwiatkowska, Brygida, Rantapaa-Dahlqvist, Solbritt, Saxne, Tore, Sidiropoulos, Prodromos, Kteniadaki, Eleni, Misirlaki, Chariklia, Mann, Herman, Vencovsky, Jiri, Ciurea, Adrian, Tamborrini, Giorgio, Kyburz, Diego, Bastian, Hans, Burmester, Gerd R., Detert, Jacqueline, Buckley, Christopher D., Sheehy, Claire, Shipman, Alexa, Stech, Irina, Mukhtyar, Chetan, Atzeni, Fabiola, Sitia, Simona, Tomasoni, Livio, Gianturco, Luigi, Ricci, Cristian, Sarzi-Puttini, Piercarlo, De Gennaro Colonna, Vito, Turiel, Maurizio, Galloway, James, Low, Audrey, Mercer, Louise K., Dixon, Will, Ustianowski, Andrew, Watson, Kath, Fisher, Benjamin, Plant, Darren, Lundberg, Karin, Barton, Anne, Venables, Patrick, Lorenzi, Alice R., Platt, Philip N., Ickinger, Claudia, Musenge, Eustasius, Tikly, Mohammed, Barnes, Jonathan, Donnison, C., Scott, M., Bartholomew, Peter, Rynne, Martin, Hamilton, Jennifer, Saravanan, V., Heycock, Carol, Kelly, Clive, de la Torre, Inmaculada, Moura, Rita A., Leandro, Maria, Edwards, Jonathan, Cambridge, Geraldine, Edwards, Johnathan, Daniels, Louise E., Gullick, Nicola J., Rees, Jonathan D., Kirkham, Bruce W., Rees, Jonathan, Scott, Ian C., Johnson, Deborah, Scott, David L., Kingsley, Gabrielle, Ma, Margaret H., Cope, Andrew P., Brode, Sven, Nisar, Muhammad K., Östör, Andrew J., Oakley, Stephen P., Jones, Tim, Mistlin, Alan, Panayi, Gabriel S., El Miedany, Yasser, Palmer, Deborah, Porkodi, Ramanathan, Rajendran, Panchapakesa, Waller, Rosemary, Williamson, Lyn, Collins, David, Price, Elizabeth, Juarez, Maria J., El Gaafary, Maha, Youssef, sally, Cramp, Fiona, Hewlett, Sarah, Almeida, Celia, Kirwan, John, Choy, Ernest, Chalder, Trudie, Pollock, Jon, Christensen, Robin, Mirjafari, Hoda, Verstappen, Suzanne, Bunn, Diane, Edlin, Helena, Charlton-Menys, Valentine, Pemberton, Philip, Marshall, Tarnya, Wilson, Paddy, Lunt, Mark, Symmons, Deborah, Bruce, Ian N., Bell, Carolyn, Rowe, Ian F., Jayakumar, Keeranur, Norton, Sam J., Dixey, Josh, Williams, Peter, Young, Adam, Kurunadalingam, Hariney, Parwaiz, Iram, Kumar, Kanta, Howlett, Kath, Hands, Becki, Raza, Karim, Pitzalis, Costantino, Buckley, Chris, Kelly, Stephen, Filer, Andrew, Wheater, Gill, Hogan, Vanessa E., Onno Teng, YK, Tekstra, Janneke, Tuck, Stephen P., Lafeber, Floris P., Huizinga, Tom W., Bijlsma, Johannes W., Francis, Roger M., Datta, Harish K., van Laar, Jaap, Pratt, Arthur G., Charles, Peter J., Choudhury, Muslima, Wilson, Gill, Venables, Patrick J., Isaacs, John, Stack, Rebecca, Kwiatkowska, Brygida, Rantapaa-Dahlqvist, Solbritt, Saxne, Tore, Sidiropoulos, Prodromos, Kteniadaki, Eleni, Misirlaki, Chariklia, Mann, Herman, Vencovsky, Jiri, Ciurea, Adrian, Tamborrini, Giorgio, Kyburz, Diego, Bastian, Hans, Burmester, Gerd R., Detert, Jacqueline, Buckley, Christopher D., Sheehy, Claire, Shipman, Alexa, Stech, Irina, Mukhtyar, Chetan, Atzeni, Fabiola, Sitia, Simona, Tomasoni, Livio, Gianturco, Luigi, Ricci, Cristian, Sarzi-Puttini, Piercarlo, De Gennaro Colonna, Vito, Turiel, Maurizio, Galloway, James, Low, Audrey, Mercer, Louise K., Dixon, Will, Ustianowski, Andrew, Watson, Kath, Fisher, Benjamin, Plant, Darren, Lundberg, Karin, Barton, Anne, Venables, Patrick, Lorenzi, Alice R., and Platt, Philip N.

Abstract

Background: Rheumatoid arthritis (RA) causes progressive joint damage and functional disability. Studies on factors affecting joint damage as clinical outcome are lacking in Africa. The aim of the present study was to identify predictors of joint damage in adult South Africans with established RA. Methods: A cross-sectional study of 100 black patients with RA of >5 years were assessed for joint damage using a validated clinical method, the RA articular damage (RAAD) score. Potential predictors of joint damage that were documented included socio-demographics, smoking, body mass index (BMI), disease duration, delay in disease modifying antirheumatic drug (DMARD) initiation, global disease activity as measured by the disease activity score (DAS28), erythrocyte sedimentation rate (ESR), C reactive protein (CRP), and autoantibody status. The predictive value of variables was assessed by univariate and stepwise multivariate regression analyses. A p value <0.05 was considered significant. Results: The mean (SD) age was 56 (9.8) years, disease duration 17.5 (8.5) years, educational level 7.5 (3.5) years and DMARD lag was 9 (8.8) years. Female to male ratio was 10:1. The mean (SD) DAS28 was 4.9 (1.5) and total RAAD score was 28.3 (12.8). The mean (SD) BMI was 27.2 kg/m2 (6.2) and 93% of patients were rheumatoid factor (RF) positive. More than 90% of patients received between 2 to 3 DMARDs. Significant univariate predictors of a poor RAAD score were increasing age (p = 0.001), lower education level (p = 0.019), longer disease duration (p < 0.001), longer DMARD lag (p = 0.014), lower BMI (p = 0.025), high RF titre (p < 0.001) and high ESR (p = 0.008). The multivariate regression analysis showed that the only independent significant predictors of a higher mean RAAD score were older age at disease onset (p = 0.04), disease duration (p < 0.001) and RF titre (p < 0.001). There was also a negative association between BMI and the mean total RAAD score (p = 0.049). Conclusions: Patie

57. Effectiveness and safety of anti-tumour necrosis factor therapy with certolizumab pegol observed in real-life rheumatoid arthritis patients in Germany: results from the non-interventional FαsT study.

Author

Burmester G, Nüsslein H, von Hinüber U, Detert J, Richter C, Kumke T, Leunikava I, Lendl U, Fricke D, and Müller-Ladner U

Subjects
Double-Blind Method, Drug Therapy, Combination, Female, Germany, Humans, Male, Methotrexate, Middle Aged, Remission Induction, Treatment Outcome, Antirheumatic Agents therapeutic use, Arthritis, Rheumatoid drug therapy, Certolizumab Pegol therapeutic use, Tumor Necrosis Factor-alpha antagonists & inhibitors
Abstract

Objectives: To report the tolerability and effectiveness of certolizumab pegol (CZP) for the treatment of patients with active rheumatoid arthritis (RA) in a routine clinical practice setting., Methods: FαsT (NCT01069419) was a non-interventional, observational 104-week (wk) study performed at 163 sites in Germany. RA patients were treated according to the treating physician's discretion. Clinical remission (DAS28-CRP<2.6) at wk 104 was the primary endpoint of the study. Remission data based on ESR (DAS28-ESR<2.6) were also assessed. Secondary endpoints included the effect of CZP treatment on pain, physical function and disease activity. Safety data were collected at all study visits., Results: 1,117 patients were enrolled in the FαsT study (78% female, mean age: 55 years). Rapid responses were observed at wk 6 (18.7% and 12.9% patients in DAS28-CRP and DAS28-ESR remission, respectively) with improvements sustained over 2 years (20.0% and 13.9% patients achieved DAS28-CRP and DAS28-ESR remission, respectively at wk 104). Anti-TNF naïve patients exhibited greater improvements than anti-TNF experienced patients (mean DAS28-ESR change from baseline [CfB] -1.3, -1.5 and -1.7 for patients with ≥2, 1 and no anti-TNFs, respectively at wk104). Improvements were reported in all secondary endpoint measures. 1,111 patients were exposed to CZP for a total of 1,538 patient-years during the study. 2,000 treatment-emergent adverse events (TEAEs) were reported in 745 patients (67.1%); 9 (0.8%) experienced TEAEs with fatal outcome., Conclusions: CZP demonstrated efficacy and safety outcomes reflective of those observed in trial settings. Rapid reductions in disease activity and improvements in physical function were maintained up to wk 104.

Published
2019

58. Effects of treatment with etanercept versus methotrexate on sleep quality, fatigue and selected immune parameters in patients with active rheumatoid arthritis.

Author

Detert J, Dziurla R, Hoff P, Gaber T, Klaus P, Bastian H, Braun T, Schellmann S, Penzel T, Fietze I, Loeschmann PA, Jaehnig P, Straub RH, Burmester GR, and Buttgereit F

Subjects
Adolescent, Adult, Aged, Antirheumatic Agents adverse effects, Arthritis, Rheumatoid complications, Arthritis, Rheumatoid immunology, Arthritis, Rheumatoid physiopathology, Disability Evaluation, Drug Therapy, Combination, Etanercept adverse effects, Fatigue immunology, Fatigue physiopathology, Female, Humans, Male, Methotrexate adverse effects, Middle Aged, Patient Reported Outcome Measures, Pilot Projects, Polysomnography, Predictive Value of Tests, Prospective Studies, Remission Induction, Sleep Wake Disorders immunology, Sleep Wake Disorders physiopathology, Surveys and Questionnaires, Time Factors, Treatment Outcome, Young Adult, Antirheumatic Agents therapeutic use, Arthritis, Rheumatoid drug therapy, Etanercept therapeutic use, Fatigue prevention & control, Methotrexate therapeutic use, Sleep drug effects, Sleep Wake Disorders prevention & control
Abstract

Objectives: To compare sleep quality, disease activity and patient-reported outcomes such as fatigue and immune parameters in patients with rheumatoid arthritis treated with etanercept (ETA) or methotrexate (MTX)., Methods: Of 36 patients (28-joint Disease Activity Score, DAS28CRP≥3.2) in this 16-week (w), open, prospective study, 19 (11 women) received MTX 12.5-17 mg/w, and 17 (14 women) received ETA 25 mg x 2/w, alone or in combination with MTX. Clinical (DAS28CRP, visual analogue scale), laboratory (C-reactive protein [CRP]), sleep (polysomnography), functional (Multidimensional Fatigue Inventory; Health Assessment Questionnaire-Disability Index (HAQ-DI); 36-item Short-Form Health Survey (SF-36), immunological (humoral/cellular) and neuroendocrine (hormonal) parameters were recorded at baseline (BL), w8 and w16., Results: BL characteristics did not differ significantly between the ETA and MTX groups except disease duration: mean age (years): 48.6±8.8 vs. 49.4±16.6; mean disease duration (months): 19.6±46.3 vs. 81.2±79.2; and DAS28CRP: 4.4±0.9 vs. 4.4±1.7, respectively. DAS28CRP, SF-36, and HAQ-DI improved significantly in both groups from BL to w16 (p≤0.05). The DAS28CRP improvements at w16 (mean changes -1.8 in the ETA group, and -1.4 in MTX group), were not statistically significant from each other. The absolute values of sleep efficiency, total sleep time, and stage 2 sleep duration increased significantly in the ETA group, but no significant changes were reported in the MTX group., Conclusions: Both therapies improved disease activity, CRP, SF-36 and HAQ-DI, with faster, more pronounced changes in DAS28CRP in the ETA group, which alone had significantly improved sleep parameters.

Published
2016

59. Biologic monotherapy in the treatment of rheumatoid arthritis.

Author

Detert J and Klaus P

Abstract

Biologics, possibly in combination with a conventional disease-modifying antirheumatic drug (DMARD) - preferably methotrexate (MTX), are used in accordance with the recommendations of the international rheumatological societies. However, in clinical practice, this recommendation is often problematic, as many rheumatologists know from personal experience. The quality of life of the patient is affected mainly by drug-induced intolerances (eg, MTX). Thus, the acceptance of the patient to treatment is often so inadequate that a discontinuation of the drug is necessary. In daily practice, approximately 30% of patients with biological therapy receive no concomitant DMARD according to the register data.

Published
2015
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60. Circadian rhythms of cellular immunity in rheumatoid arthritis: a hypothesis-generating study.

Author

Spies CM, Hoff P, Mazuch J, Gaber T, Maier B, Strehl C, Hahne M, Jakstadt M, Huscher D, Burmester GR, Detert J, Kramer A, and Buttgereit F

Subjects
Adaptation, Physiological, Aged, Arthritis, Rheumatoid blood, Arthritis, Rheumatoid genetics, Arthritis, Rheumatoid physiopathology, Biomarkers blood, Case-Control Studies, Cytokines blood, Female, Humans, Immunity, Humoral, Inflammation Mediators blood, Lipopolysaccharide Receptors blood, Macrophages metabolism, Middle Aged, Monocytes metabolism, Period Circadian Proteins genetics, Pilot Projects, Postmenopause immunology, RNA, Messenger blood, Time Factors, Arthritis, Rheumatoid immunology, Circadian Rhythm genetics, Immunity, Cellular, Macrophages immunology, Monocytes immunology
Abstract

Objectives: The circadian rhythm of clinical symptoms in rheumatoid arthritis (RA) has been primarily attributed to circadian variations in humoral factors and hormones. In this study, we investigated circadian rhythms of cellular immunity in RA (CiRA study)., Methods: Peripheral blood of female postmenopausal patients with active RA (DAS 28 ≥ 4.2) (n=5) and female postmenopausal non-RA controls (n=5) was collected every 2 hours for 24 hours and analysed by flow cytometry, cytokine multiplex suspension array and quantitative RT-PCR of clock gene expression in isolated CD14+ monocytes. Endogenous circadian rhythms of macrophages were investigated by BMAL1-luciferase bioluminescence. Significance of circadian rhythms was tested by Cosinor analysis., Results: We found (i) circadian rhythms in the relative frequency of peripheral blood cell populations that were present in postmenopausal non-RA controls but absent in patients with active RA, (ii) circadian rhythms that were absent in non-RA controls but present in patients with RA and (iii) circadian rhythms that were present in both groups but with differences in peak phase or amplitude or amplitude/magnitude. The circadian rhythm in expression of the clock genes PER2 and PER3 in CD14+ monocytes was lost in patients with RA. The amplitude of BMAL1-luciferase bioluminescence tended to be lower in patients with RA than in non-RA controls., Conclusions: We conclude that (i) in RA some immune cell populations lose their normal circadian rhythms whereas others establish new 'inflammatory' circadian rhythms and (ii) these findings provide a good basis for further identifying pathophysiological aspects of RA chronobiology with potential therapeutic implications.

Published
2015

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