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2. Gender biased neuroprotective effect of Transferrin Receptor 2 deletion in multiple models of Parkinson’s disease

Author

Milanese, C. (Chiara), Gabriels, S. (Sylvia), Barnhoorn, S. (Sander), Cerri, S. (Silvia), Ulusoy, A. (Ayse), Gornati, S.V. (Simona), Wallace, D.F. (Daniel F.), Blandini, F. (Fabio), Di Monte, D.A. (Donato A.), Subramaniam, V.N. (V. Nathan), Mastroberardino, P.G. (Pier), Milanese, C. (Chiara), Gabriels, S. (Sylvia), Barnhoorn, S. (Sander), Cerri, S. (Silvia), Ulusoy, A. (Ayse), Gornati, S.V. (Simona), Wallace, D.F. (Daniel F.), Blandini, F. (Fabio), Di Monte, D.A. (Donato A.), Subramaniam, V.N. (V. Nathan), and Mastroberardino, P.G. (Pier)

Abstract

Alterations in the metabolism of iron and its accumulation in the substantia nigra pars compacta accompany the pathogenesis of Parkinson’s disease (PD). Changes in iron homeostasis also occur during aging, which constitutes a PD major risk factor. As such, mitigation of iron overload via chelation strategies has been considered a plausible disease modifying approach. Iron chelation, however, is imperfect because of general undesired side effects and lack of specificity; more effective approaches would rely on targeting distinctive pathways responsible for iron overload in brain regions relevant to PD and, in particular, the substantia nigra. We have previously demonstrated that the Transferrin/Transferrin Receptor 2 (TfR2) iron import mechanism functions in nigral dopaminergic neurons, is perturbed in PD models and patients, and therefore constitutes a potential therapeutic target to halt iron accumulation. To validate this hypothesis, we generated mice with targeted deletion of TfR2 in dopaminergic neurons. In these animals, we modeled PD with multiple approaches, based either on neurotoxin exposure or alpha-synuclein proteotoxic mechanisms. We found that TfR2 deletion can provide neuroprotection against dopaminergic degeneration, and against PD- and aging-related iron overload. The effects, however, were significantly more pronounced in females rather than in males. Our data indicate that the TfR2 iron import pathway represents an amenable strategy to hamper PD progression. Data also suggest, however, that therapeutic strategies targeting TfR2 should consider a potential sexual dimorphism in neuroprotective response.

Published
2020
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3. Abstract 382: Reduced Mitochondrial Function and Metabolic Dysregulation in Aneurysmal Fibulin-4 Mice

Author

Pluijm, Ingrid, Heijningen, P. M., Ijpma, A., Vliet, N., Sluiter, W., Davis, E. C., Ringuette, L. J., Dekkers, D. H. W., Ghazi, S., Que, I., Kaijzel, E. L., Te Riet, L., Gabriels, S. I. C., Mastroberardino, P. G., Linden, R., Vermeij, M., Demmers, J. A., Devashish Das, Yanagisawa, H., Kanaar, R., and Essers, J.

Subjects
Physiology, Cardiology and Cardiovascular Medicine
Abstract

Thoracic aortic aneurysms are a life-threatening condition often diagnosed too late. The underlying mechanism is largely unknown. An accurate and early predictive biomarker for aneurysm formation has not yet been identified, although some molecular processes, such as disturbed TGF-β signalling, have been implicated. To discover novel robust biomarkers, we aimed to better understand the molecular mechanisms involved in aneurysm initiation and progression. In Fibulin-4 R/R mice, the extracellular matrix protein Fibulin-4 is 4-fold reduced, resulting in progressive ascending aneurysm formation and early death around 3 months of age. We performed LC-MS/MS proteomics and transcriptomics analyses on the aortas of Fibulin-4 R/R and Fibulin-4 +/+ mice. Protein and gene data sets were separately analysed for genotype specific differences with Ingenuity Pathway analysis tools. Intriguingly, we observed alterations in mitochondrial composition in aortas from Fibulin-4 R/R mice. Consistently, functional studies in Fibulin-4 R/R vascular smooth muscle cells (VSMCs) revealed lower oxygen consumption rates, but increased acidification rates compared to Fibulin-4 +/+ . The mitochondria in VSMCs of Fibulin-4 R/R mice were reduced in size and had increased complex I-IV levels. Furthermore, aortas of aneurysmal Fibulin-4 R/R mice displayed increased levels of ROS. Consistent with these findings, gene expression analyses revealed the dysregulation of metabolic pathways. In accordance, ketone levels in the blood of Fibulin-4 R/R mice were reduced and liver fatty acids were decreased, while liver glycogen was increased. As predicted by these findings, activity of PGC1α, a key regulator between mitochondrial function and organismal metabolism, was downregulated in Fibulin-4 R/R VSMCs. In conclusion, our data indicate altered mitochondrial function and metabolic dysregulation, leading to increased ROS levels and altered energy production, as a novel mechanism, which may contribute to thoracic aortic aneurysm formation. This discovery will not only provide new biomarkers that can be validated in human aortas, but they will also provide the rational for new interventions such as alterations in diet to prevent aneurysm formation.

Published
2015
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4. Lectures

Author

Chen, D. S., primary, Feltquate, D. M., additional, Smothers, F., additional, Hoos, A., additional, Langermann, S., additional, Marshall, S., additional, May, R., additional, Fleming, M., additional, Hodi, F. S., additional, Senderowicz, A., additional, Wiman, K. G., additional, de Dosso, S., additional, Fiedler, W., additional, Gianni, L., additional, Cresta, S., additional, Schulze-Bergkamen, H. B., additional, Gurrieri, L., additional, Salzberg, M., additional, Dietrich, B., additional, Danielczyk, A., additional, Baumeister, H., additional, Goletz, S., additional, Sessa, C., additional, Strumberg, D., additional, Schultheis, B., additional, Santel, A., additional, Gebhardt, F., additional, Meyer-Sabellek, W., additional, Keil, O., additional, Giese, K., additional, Kaufmann, J., additional, Maio, M., additional, Choy, G., additional, Covre, A., additional, Parisi, G., additional, Nicolay, H., additional, Fratta, E., additional, Fonsatti, E., additional, Sigalotti, L., additional, Coral, S., additional, Taverna, P., additional, Azab, M., additional, Deutsch, E., additional, Lepechoux, C., additional, Pignon, J. P., additional, Tao, Y. T., additional, Rivera, S., additional, Bourgier, B. C., additional, Angokai, M., additional, Bahleda, R., additional, Slimane, K., additional, Angevin, E., additional, Besse, B. B., additional, Soria, J. C., additional, Dragnev, K., additional, Beumer, J. H., additional, Anyang, B., additional, Ma, T., additional, Galimberti, F., additional, Erkmen, C. P., additional, Nugent, W., additional, Rigas, J., additional, Abraham, K., additional, Johnstone, D., additional, Memoli, V., additional, Dmitrovsky, E., additional, Voest, E. E., additional, Siu, L., additional, Janku, F., additional, Tsimberidou, A., additional, Kurzrock, R., additional, Tabernero, J., additional, Rodon, J., additional, Berger, R., additional, Onn, A., additional, Batist, G., additional, Bresson, C., additional, Lazar, V., additional, Molenaar, J. J., additional, Koster, J., additional, Ebus, M., additional, Zwijnenburg, D. A., additional, van Sluis, P., additional, Lamers, F., additional, Schild, L., additional, van der Ploeg, I., additional, Caron, H. N., additional, Versteeg, R., additional, Pouyssegur, J., additional, Marchiq, I., additional, Chiche, J., additional, Roux, D., additional, Le Floch, R., additional, Critchlow, S. E., additional, Wooster, R. F., additional, Agresta, S., additional, Yen, K. E., additional, Janne, P. A., additional, Plummer, E. R., additional, Trinchieri, G., additional, Ellis, L., additional, Chan, S. L., additional, Yeo, W., additional, Chan, A. T., additional, Mouliere, F., additional, El Messaoudi, S., additional, Gongora, C., additional, Lamy, P. J., additional, del Rio, M., additional, Lopez-Crapez, E., additional, Gillet, B., additional, Mathonnet, M., additional, Pezet, D., additional, Ychou, M., additional, Thierry, A. R., additional, Ribrag, V., additional, Vainchenker, W., additional, Constantinescu, S., additional, Keilhack, H., additional, Umelo, I. A., additional, Noeparast, A., additional, Chen, G., additional, Renard, M., additional, Geers, C., additional, Vansteenkiste, J., additional, Teugels, E., additional, de Greve, J., additional, Rixe, O., additional, Qi, X., additional, Chu, Z., additional, Celerier, J., additional, Leconte, L., additional, Minet, N., additional, Pakradouni, J., additional, Kaur, B., additional, Cuttitta, F., additional, Wagner, A. J., additional, Zhang, Y. X., additional, Sicinska, E., additional, Czaplinski, J. T., additional, Remillard, S. P., additional, Demetri, G. D., additional, Weng, S., additional, Debussche, L., additional, Agoni, L., additional, Reddy, E. P., additional, Guha, C., additional, Silence, K., additional, Thibault, A., additional, de Haard, H., additional, Dreier, T., additional, Ulrichts, P., additional, Moshir, M., additional, Gabriels, S., additional, Luo, J., additional, Carter, C., additional, Rajan, A., additional, Khozin, S., additional, Thomas, A., additional, Lopez-Chavez, A., additional, Brzezniak, C., additional, Doyle, L., additional, Keen, C., additional, Manu, M., additional, Raffeld, M., additional, Giaccone, G., additional, Lutzker, S., additional, Melief, J. M., additional, Eckhardt, S. G., additional, Trusolino, L., additional, Migliardi, G., additional, Zanella, E. R., additional, Cottino, F., additional, Galimi, F., additional, Sassi, F., additional, Marsoni, S., additional, Comoglio, P. M., additional, Bertotti, A., additional, Hidalgo, M., additional, Weroha, S. J., additional, Haluska, P., additional, Becker, M. A., additional, Harrington, S. C., additional, Goodman, K. M., additional, Gonzalez, S. E., additional, al Hilli, M., additional, Butler, K. A., additional, Kalli, K. R., additional, Oberg, A. L., additional, Huijbers, I. J., additional, Bin Ali, R., additional, Pritchard, C., additional, Cozijnsen, M., additional, Proost, N., additional, Song, J. Y., additional, Krimpenfort, P., additional, Michalak, E., additional, Jonkers, J., additional, Berns, A., additional, Banerji, U., additional, Stewart, A., additional, Thavasu, P., additional, Banerjee, S., additional, and Kaye, S. B., additional

Published
2013
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12. The interface between SARS-CoV-2 and non-communicable diseases (NCDs) in a high HIV/TB burden district level hospital setting, Cape Town, South Africa.

Author

Mnguni AT, Schietekat D, Ebrahim N, Sonday N, Boliter N, Schrueder N, Gabriels S, Cois A, Tamuzi JL, Tembo Y, Davies MA, English R, and Nyasulu PS

Subjects
Adult, Humans, SARS-CoV-2, South Africa epidemiology, Hospitals, District, Obesity, COVID-19 epidemiology, Noncommunicable Diseases epidemiology, Hypertension epidemiology, Diabetes Mellitus epidemiology, HIV Infections epidemiology, Stroke, Renal Insufficiency, Chronic
Abstract

Background: COVID-19 experiences on noncommunicable diseases (NCDs) from district-level hospital settings during waves I and II are scarcely documented. The aim of this study is to investigate the NCDs associated with COVID-19 severity and mortality in a district-level hospital with a high HIV/TB burden., Methods: This was a retrospective observational study that compared COVID-19 waves I and II at Khayelitsha District Hospital in Cape Town, South Africa. COVID-19 adult patients with a confirmed SARS-CoV-2 polymerase chain reaction (PCR) or positive antigen test were included. In order to compare the inter wave period, clinical and laboratory parameters on hospital admission of noncommunicable diseases, the Student t-test or Mann-Whitney U for continuous data and the X2 test or Fishers' Exact test for categorical data were used. The role of the NCD subpopulation on COVID-19 mortality was determined using latent class analysis (LCA)., Findings: Among 560 patients admitted with COVID-19, patients admitted during wave II were significantly older than those admitted during wave I. The most prevalent comorbidity patterns were hypertension (87%), diabetes mellitus (65%), HIV/AIDS (30%), obesity (19%), Chronic Kidney Disease (CKD) (13%), Congestive Cardiac Failure (CCF) (8.8%), Chronic Obstructive Pulmonary Disease (COPD) (3%), cerebrovascular accidents (CVA)/stroke (3%), with similar prevalence in both waves except HIV status [(23% vs 34% waves II and I, respectively), p = 0.022], obesity [(52% vs 2.5%, waves II and I, respectively), p <0.001], previous stroke [(1% vs 4.1%, waves II and I, respectively), p = 0.046]. In terms of clinical and laboratory findings, our study found that wave I patients had higher haemoglobin and HIV viral loads. Wave II, on the other hand, had statistically significant higher chest radiography abnormalities, fraction of inspired oxygen (FiO2), and uraemia. The adjusted odds ratio for death vs discharge between waves I and II was similar (0.94, 95%CI: 0.84-1.05). Wave I had a longer average survival time (8.0 vs 6.1 days) and a shorter average length of stay among patients discharged alive (9.2 vs 10.7 days). LCA revealed that the cardiovascular phenotype had the highest mortality, followed by diabetes and CKD phenotypes. Only Diabetes and hypertension phenotypes had the lowest mortality., Conclusion: Even though clinical and laboratory characteristics differed significantly between the two waves, mortality remained constant. According to LCA, the cardiovascular, diabetes, and CKD phenotypes had the highest death probability., Competing Interests: The authors received no specific funding for this work., (Copyright: © 2023 Mnguni et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.)

Published
2023
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13. The clinical and epidemiological characteristics of a series of patients living with HIV admitted for COVID-19 in a district hospital.

Author

Mnguni AT, Schietekat D, Ebrahim N, Sonday N, Boliter N, Schrueder N, Gabriels S, Sigwadhi LN, Zemlin AE, Chapanduka ZC, Ngah V, Yalew A, Jalavu T, Abdullah I, Tamuzi JL, Tembo Y, Davies MA, English R, and Nyasulu PS

Subjects
Humans, Male, Middle Aged, Glycated Hemoglobin, HIV, Hospitals, District, Leukocytosis, SARS-CoV-2, South Africa epidemiology, Female, Adult, COVID-19 epidemiology, COVID-19 mortality, HIV Infections complications, HIV Infections drug therapy, HIV Infections epidemiology
Abstract

Background: The coronavirus disease 2019 (COVID-19) pandemic continues to evolve. Globally, COVID-19 continues to strain even the most resilient healthcare systems, with Omicron being the latest variant. We made a thorough search for literature describing the effects of the COVID-19 in a high human immunodeficiency virus (HIV)/tuberculosis (TB) burden district-level hospital setting. We found scanty literature., Methods: A retrospective observational study was conducted at Khayelitsha District Hospital in Cape Town, South Africa (SA) over the period March 2020-December 2021. We included confirmed COVID-19 cases with HIV infection aged from 18 years and above. Analysis was performed to identify predictors of mortality or hospital discharge among people living with HIV (PLWH). Predictors investigated include CD4 count, antiretroviral therapy (ART), TB, non-communicable diseases, haematological, and biochemical parameters., Findings: This cohort of PLWH with SARS-CoV-2 infection had a median (IQR) age of 46 (37-54) years, male sex distribution of 29.1%, and a median (IQR) CD4 count of 267 (141-457) cells/mm3. Of 255 patients, 195 (76%) patients were discharged, 60 (24%) patients died. One hundred and sixty-nine patients (88%) were on ART with 73(28%) patients having acquired immunodeficiency syndrome (AIDS). After multivariable analysis, smoking (risk ratio [RR]: 2.86 (1.75-4.69)), neutrophilia [RR]: 1.024 (1.01-1.03), and glycated haemoglobin A1 (HbA1c) [RR]: 1.01 (1.007-1.01) were associated with mortality., Conclusion: The district hospital had a high COVID-19 mortality rate among PLWH. Easy-to-access biomarkers such as CRP, neutrophilia, and HbA1c may play a significant role in informing clinical management to prevent high mortality due to COVID-19 in PLWH at the district-level hospitals., (© 2023. The Author(s).)

Published
2023
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14. The Affordances of Visual Modes in Pedagogy on the Physics of Motion in Physiotherapy Education.

Author

Gabriels S, Muna N, and le Roux K

Subjects
Female, Humans, Motion, Physical Therapy Modalities, Problem Solving, Learning, Physics
Abstract

The concept of angular motion is foundational knowledge in physiotherapy, applied for example in measuring joint range of motion. Yet research points to university students' poor understanding of the concept. Visuals are commonly promoted as valuable for creating opportunities for meaningful learning of the physics of motion. In this chapter we report on a lecturer's use of the affordances of visual modes-images, gestures and objects-in pedagogy on angular motion in the first year of a professional physiotherapy degree programme at a South African university. Using a multimodal social semiotic perspective that positions multimodal language as contextualised, motivated and central to meaning-making, we analysed recorded lectures and an interview with the lecturer. We show that, in organising her pedagogy, the lecturer used affordances of the image mode to create static images representing the spatial arrangement of multiple concepts and their relations simultaneously. This mode was the central site used to promote conceptually meaningful problem-solving, but was strengthened by her use of the affordances of gesture and an object to communicate motion. The lecturer strategically integrated the modes of verbal speech and written text into the visual complex, supporting the development of conceptual meaning and the acquisition of the language modes employed for problem-solving procedures. Her choices were motivated by a deep, contextual understanding of the role of physics in physiotherapy and of the diverse knowledge, language experiences and resources of first-year students. Our findings regarding the affordances of visual modes can inform collaborative education development within the health sciences., (© 2022. The Author(s), under exclusive license to Springer Nature Switzerland AG.)

Published
2022
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15. Lung cancer screening: intention to participate and acceptability among Belgian smokers.

Author

Kellen E, Gabriels S, Van Hal G, and Goossens MC

Subjects
Adult, Belgium epidemiology, Cross-Sectional Studies, Humans, Intention, Mass Screening methods, Smokers, Early Detection of Cancer methods, Lung Neoplasms diagnosis, Lung Neoplasms epidemiology, Lung Neoplasms prevention & control
Abstract

Objective: Next to the obvious benefits of tobacco-use cessation, lung cancer screening using low-dose computed tomography (LDCT) scans has been proposed as a means to lower lung cancer burden. Achieving an impact of any cancer screening program on cancer-specific mortality largely depends on the uptake. The aim of this study was to estimate the acceptability and intention to participate in a lung cancer screening program among Belgian current or former smokers., Methods: A cross-sectional online survey was carried out among adults from the Belgian population. Sampling took place within an existing online panel., Results: In total, 83.6% of all respondents (n = 2727), including current or former smokers and never smokers, believed that offering lung cancer screening to current or former smokers is a good idea. 84.3% of all current or former smokers (n = 1534) answered that they would likely or very likely participate in a screening program for lung cancer. The majority of current smokers that were willing to be screened said they would also want to receive tobacco-use cessation counseling in parallel with screening (71.8%; n = 486), whereas 9% (n = 61) would decline., Conclusions: These findings suggest that a Belgian lung cancer screening program would be acceptable and could be well-attended by current or former smokers. Further research should focus on how smokers can be best reached to propose screening, and how tobacco-use cessation counseling can be successfully integrated in a lung cancer screening program., (Copyright © 2020 Wolters Kluwer Health, Inc. All rights reserved.)

Published
2021
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16. Gender biased neuroprotective effect of Transferrin Receptor 2 deletion in multiple models of Parkinson's disease.

Author

Milanese C, Gabriels S, Barnhoorn S, Cerri S, Ulusoy A, Gornati SV, Wallace DF, Blandini F, Di Monte DA, Subramaniam VN, and Mastroberardino PG

Subjects
Animals, Disease Models, Animal, Female, Gender Identity, Humans, Mice, Neuroprotective Agents pharmacology, Neuroprotective Agents therapeutic use, Parkinson Disease genetics, Receptors, Transferrin metabolism
Abstract

Alterations in the metabolism of iron and its accumulation in the substantia nigra pars compacta accompany the pathogenesis of Parkinson's disease (PD). Changes in iron homeostasis also occur during aging, which constitutes a PD major risk factor. As such, mitigation of iron overload via chelation strategies has been considered a plausible disease modifying approach. Iron chelation, however, is imperfect because of general undesired side effects and lack of specificity; more effective approaches would rely on targeting distinctive pathways responsible for iron overload in brain regions relevant to PD and, in particular, the substantia nigra. We have previously demonstrated that the Transferrin/Transferrin Receptor 2 (TfR2) iron import mechanism functions in nigral dopaminergic neurons, is perturbed in PD models and patients, and therefore constitutes a potential therapeutic target to halt iron accumulation. To validate this hypothesis, we generated mice with targeted deletion of TfR2 in dopaminergic neurons. In these animals, we modeled PD with multiple approaches, based either on neurotoxin exposure or alpha-synuclein proteotoxic mechanisms. We found that TfR2 deletion can provide neuroprotection against dopaminergic degeneration, and against PD- and aging-related iron overload. The effects, however, were significantly more pronounced in females rather than in males. Our data indicate that the TfR2 iron import pathway represents an amenable strategy to hamper PD progression. Data also suggest, however, that therapeutic strategies targeting TfR2 should consider a potential sexual dimorphism in neuroprotective response.

Published
2021
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17. ARGX-117, a therapeutic complement inhibiting antibody targeting C2.

Author

Van de Walle I, Silence K, Budding K, Van de Ven L, Dijkxhoorn K, de Zeeuw E, Yildiz C, Gabriels S, Percier JM, Wildemann J, Meeldijk J, Simons PJ, Boon L, Cox L, Holgate R, Urbanus R, Otten HG, Leusen JHW, Blanchetot C, de Haard H, Hack CE, and Boross P

Subjects
Animals, Antibodies, Monoclonal blood, Antibodies, Monoclonal pharmacokinetics, Calcium, Complement Activation drug effects, Complement C2 analysis, Complement C2 metabolism, Complement Inactivating Agents blood, Complement Inactivating Agents pharmacokinetics, Epitope Mapping, Female, Humans, Hydrogen-Ion Concentration, Macaca fascicularis, Male, Antibodies, Monoclonal pharmacology, Complement C2 antagonists & inhibitors, Complement Inactivating Agents pharmacology
Abstract

Background: Activation of the classical and lectin pathway of complement may contribute to tissue damage and organ dysfunction of antibody-mediated diseases and ischemia-reperfusion conditions. Complement factors are being considered as targets for therapeutic intervention., Objective: We sought to characterize ARGX-117, a humanized inhibitory monoclonal antibody against complement C2., Methods: The mode-of-action and binding characteristics of ARGX-117 were investigated in detail. Furthermore, its efficacy was analyzed in in vitro complement cytotoxicity assays. Finally, a pharmacokinetic/pharmacodynamic study was conducted in cynomolgus monkeys., Results: Through binding to the Sushi-2 domain of C2, ARGX-117 prevents the formation of the C3 proconvertase and inhibits classical and lectin pathway activation upstream of C3 activation. As ARGX-117 does not inhibit the alternative pathway, it is expected not to affect the antimicrobial activity of this complement pathway. ARGX-117 prevents complement-mediated cytotoxicity in in vitro models for autoimmune hemolytic anemia and antibody-mediated rejection of organ transplants. ARGX-117 exhibits pH- and calcium-dependent target binding and is Fc-engineered to increase affinity at acidic pH to the neonatal Fc receptor, and to reduce effector functions. In cynomolgus monkeys, ARGX-117 dose-dependently reduces free C2 levels and classical pathway activity. A 2-dose regimen of 80 and 20 mg/kg separated by a week, resulted in profound reduction of classical pathway activity lasting for at least 7 weeks., Conclusions: ARGX-117 is a promising new complement inhibitor that is uniquely positioned to target both the classical and lectin pathways while leaving the alternative pathway intact., (Copyright © 2020 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2021
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18. Variable ability of rapid tests to detect Mycobacterium tuberculosis rpoB mutations conferring phenotypically occult rifampicin resistance.

Author

Torrea G, Ng KCS, Van Deun A, André E, Kaisergruber J, Ssengooba W, Desmaretz C, Gabriels S, Driesen M, Diels M, Asnong S, Fissette K, Gumusboga M, Rigouts L, Affolabi D, Joloba M, and De Jong BC

Subjects
Antitubercular Agents, Bacterial Proteins drug effects, DNA-Directed RNA Polymerases drug effects, Genes, Bacterial, Genotype, Microbial Sensitivity Tests, Mycobacterium tuberculosis drug effects, Bacterial Proteins genetics, DNA-Directed RNA Polymerases genetics, Drug Resistance, Bacterial genetics, Mutation, Mycobacterium tuberculosis genetics, Rifampin pharmacology
Abstract

We compared the ability of commercial and non-commercial, phenotypic and genotypic rapid drug susceptibility tests (DSTs) to detect rifampicin resistance (RR)-conferring 'disputed' mutations frequently missed by Mycobacterium Growth Indicator Tube (MGIT), namely L430P, D435Y, L452P, and I491F. Strains with mutation S450L served as positive control while wild-types were used as negative control. Of the 38 mutant strains, 5.7% were classified as RR by MGIT, 16.2% by Trek Sensititre MYCOTB MIC plate, 19.4% by resazurin microtiter plate assay (REMA), 50.0% by nitrate reductase assay (NRA), and 62.2% by microscopic observation direct susceptibility testing (MODS). Reducing MGIT rifampicin concentration to 0.5 µg/ml, and/or increasing incubation time, enhanced detection of disputed mutations from 5.7% to at least 65.7%, particularly for mutation I491F (from 0.0 to 75.0%). Compared with MGIT at standard pre-set time with 0.25 µg/ml ECOFF as breakpoint, we found a statistically significant increase in the ability of MGIT to resolve disputed mutants and WT strains at extended incubation period of 15 and 21 days, with 0.5 µg/ml and 1 µg/ml ECOFF respectively. MODS detected 75.0% of the I491F strains and NRA 62.5%, while it was predictably missed by all molecular assays. Xpert MTB/RIF, Xpert Ultra, and GenoscholarTB-NTM + MDRTB detected all mutations within the 81 bp RR determining region. Only GenoType MTBDRplus version 2 missed mutation L430P in 2 of 11 strains. Phenotypic and genotypic DSTs varied greatly in detecting occult rifampicin resistance. None of these methods detected all disputed mutations without misclassifying wild-type strains.

Published
2019
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19. Activation of the DNA damage response in vivo in synucleinopathy models of Parkinson's disease.

Author

Milanese C, Cerri S, Ulusoy A, Gornati SV, Plat A, Gabriels S, Blandini F, Di Monte DA, Hoeijmakers JH, and Mastroberardino PG

Subjects
Animals, Ataxia Telangiectasia Mutated Proteins metabolism, Cell Line, Tumor, DNA Damage, Disease Models, Animal, Dopaminergic Neurons metabolism, Histones genetics, Histones metabolism, Humans, Mice, Mice, Inbred C57BL, Mitochondria metabolism, Parkinson Disease metabolism, Reactive Oxygen Species metabolism, Substantia Nigra metabolism, Tumor Suppressor p53-Binding Protein 1 genetics, Tumor Suppressor p53-Binding Protein 1 metabolism, alpha-Synuclein genetics, DNA Repair, Parkinson Disease pathology, Substantia Nigra pathology, alpha-Synuclein metabolism
Abstract

The involvement of DNA damage and repair in aging processes is well established. Aging is an unequivocal risk factor for chronic neurodegenerative diseases, underscoring the relevance of investigations into the role that DNA alterations may have in the pathogenesis of these diseases. Consistently, even moderate impairment of DNA repair systems facilitates the onset of pathological features typical of PD that include derangement of the dopaminergic system, mitochondrial dysfunction, and alpha-synuclein stress. The latter establishes a connection between reduced DNA repair capacity and a cardinal feature of PD, alpha-synuclein pathology. It remains to be determined, however, whether alpha-synuclein stress activates in vivo the canonical signaling cascade associated with DNA damage, which is centered on the kinase ATM and substrates such as γH2Ax and 53BP1. Addressing these issues would shed light on age-related mechanisms impinging upon PD pathogenesis and neurodegeneration in particular. We analyzed two different synucleinopathy PD mouse models based either on intranigral delivery of AAV-expressing human alpha-synuclein, or intrastriatal injection of human alpha-synuclein pre-formed fibrils. In both cases, we detected a significant increase in γH2AX and 53BP1 foci, and in phospho-ATM immunoreactivity in dopaminergic neurons, which collectively indicate DNA damage and activation of the DNA damage response. Mechanistic experiments in cell cultures indicate that activation of the DNA damage response is caused, at least in part, by pro-oxidant species because it is prevented by exogenous or endogenous antioxidants, which also rescue mitochondrial anomalies caused by proteotoxic alpha-synuclein. These in vivo and in vitro findings reveal that the cellular stress mediated by alpha-synuclein-a pathological hallmark in PD-elicits DNA damage and activates the DNA damage response. The toxic cascade leading to DNA damage involves oxidant stress and mitochondrial dysfunction The data underscore the importance of DNA quality control for preservation of neuronal integrity and protection against neurodegenerative processes.

Published
2018
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20. Mitochondrial Complex I Reversible S-Nitrosation Improves Bioenergetics and Is Protective in Parkinson's Disease.

Author

Milanese C, Tapias V, Gabriels S, Cerri S, Levandis G, Blandini F, Tresini M, Shiva S, Greenamyre JT, Gladwin MT, and Mastroberardino PG

Subjects
Animals, Antioxidants metabolism, Behavior, Animal, Cell Respiration drug effects, Cell Survival, Cytoprotection, Disease Models, Animal, Fibroblasts, Humans, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2 genetics, Male, Mitochondria drug effects, Motor Activity, Mutation, Neurons metabolism, Nitrites administration & dosage, Nitrites metabolism, Oxidation-Reduction, Oxidative Stress, Parkinson Disease genetics, Parkinson Disease pathology, Protective Agents administration & dosage, Rats, Tyrosine 3-Monooxygenase metabolism, Electron Transport Complex I metabolism, Energy Metabolism drug effects, Mitochondria metabolism, Parkinson Disease metabolism
Abstract

Aims: This study was designed to explore the neuroprotective potential of inorganic nitrite as a new therapeutic avenue in Parkinson's disease (PD)., Results: Administration of inorganic nitrite ameliorates neuropathology in phylogenetically distinct animal models of PD. Beneficial effects are not confined to prophylactic treatment and also occur if nitrite is administered when the pathogenic cascade is already active. Mechanistically, the effect is mediated by both complex I S-nitrosation, which under nitrite administration is favored over formation of other forms of oxidation, and down-stream activation of the antioxidant Nrf2 pathway. Nitrite also rescues respiratory reserve capacity and increases proton leakage in LRRK2 PD patients' dermal fibroblasts., Innovation: The study proposes an unprecedented approach based on the administration of the nitrosonium donor nitrite to contrast complex I and redox anomalies in PD. Dysfunctional mitochondrial complex I propagates oxidative stress in PD, and treatments mitigating this defect may, therefore, limit disease progression. Therapeutic complex I targeting has been successfully achieved in ischemia/reperfusion by using nitrosonium donors such as nitrite to reversibly modify its subunits and protect from oxidative damage after reperfusion. This evidence led to the innovative hypothesis that nitrite could exert protective effects also in pathological conditions where complex I dysfunction occurs in normoxia, such as in PD., Conclusions: Overall, these results demonstrate that administration of inorganic nitrite improves mitochondrial function in PD, and it, therefore, represents an amenable intervention to hamper disease progression. Antioxid. Redox Signal. 28, 44-61.

Published
2018
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21. Inefficient DNA Repair Is an Aging-Related Modifier of Parkinson's Disease.

Author

Sepe S, Milanese C, Gabriels S, Derks KW, Payan-Gomez C, van IJcken WF, Rijksen YM, Nigg AL, Moreno S, Cerri S, Blandini F, Hoeijmakers JH, and Mastroberardino PG

Subjects
Animals, Corpus Striatum pathology, Corpus Striatum ultrastructure, DNA-Binding Proteins metabolism, Dopaminergic Neurons pathology, Dopaminergic Neurons ultrastructure, Endonucleases metabolism, Fibroblasts metabolism, Fibroblasts pathology, Humans, Mice, Aging pathology, DNA Repair, Parkinson Disease pathology
Abstract

The underlying relation between Parkinson's disease (PD) etiopathology and its major risk factor, aging, is largely unknown. In light of the causative link between genome stability and aging, we investigate a possible nexus between DNA damage accumulation, aging, and PD by assessing aging-related DNA repair pathways in laboratory animal models and humans. We demonstrate that dermal fibroblasts from PD patients display flawed nucleotide excision repair (NER) capacity and that Ercc1 mutant mice with mildly compromised NER exhibit typical PD-like pathological alterations, including decreased striatal dopaminergic innervation, increased phospho-synuclein levels, and defects in mitochondrial respiration. Ercc1 mouse mutants are also more sensitive to the prototypical PD toxin MPTP, and their transcriptomic landscape shares important similarities with that of PD patients. Our results demonstrate that specific defects in DNA repair impact the dopaminergic system and are associated with human PD pathology and might therefore constitute an age-related risk factor for PD., (Copyright © 2016 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published
2016
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22. Accurate and sensitive diagnosis of geminiviruses through enrichment, high-throughput sequencing and automated sequence identification.

Author

Hagen C, Frizzi A, Gabriels S, Huang M, Salati R, Gabor B, and Huang S

Subjects
Geminiviridae classification, Geminiviridae genetics, High-Throughput Screening Assays, Molecular Sequence Data, Geminiviridae isolation & purification, Solanum lycopersicum virology, Plant Diseases virology, Sequence Analysis, DNA methods
Abstract

Existing diagnostic techniques used to identify plant-infecting DNA viruses and their associated molecules are often limited in their specificity and can be challenged by samples containing multiple viruses. We adapted a simple method of amplifying circular viral DNA and, in combination with high-throughput sequencing and bioinformatic analysis, used it as a virus diagnostic method. We validated this diagnostic method with a plant sample infected with a tomato yellow leaf curl geminivirus infectious clone and also compared PCR- and high-throughput-sequencing diagnostics on a geminivirus-infected field sample, showing that both methods gave similar results. Finally, we analyzed infected field samples of pepper from Mexico and tomato from India using this approach, demonstrating that it is both sensitive and capable of simultaneously identifying multiple discrete DNA viruses and subviral DNA elements in densely infected samples.

Published
2012
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