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5. Combining genomewide association study and lung eQTL analysis provides evidence for novel genes associated with asthma

Author

Nieuwenhuis, M. A., Siedlinski, M., van den Berge, M., Granell, R., Li, X., Niens, M., van der Vlies, P., Altmüller, J., Nürnberg, P., Kerkhof, M., van Schayck, O. C., Riemersma, R. A., van der Molen, T., de Monchy, J. G., Bossé, Y., Sandford, A., Bruijnzeel-Koomen, C. A., Gerth van Wijk, R., ten Hacken, N. H., Timens, W., Boezen, H. M., Henderson, J., Kabesch, M., Vonk, J. M., Postma, D. S., Koppelman, G. H., Nieuwenhuis, M. A., Siedlinski, M., van den Berge, M., Granell, R., Li, X., Niens, M., van der Vlies, P., Altmüller, J., Nürnberg, P., Kerkhof, M., van Schayck, O. C., Riemersma, R. A., van der Molen, T., de Monchy, J. G., Bossé, Y., Sandford, A., Bruijnzeel-Koomen, C. A., Gerth van Wijk, R., ten Hacken, N. H., Timens, W., Boezen, H. M., Henderson, J., Kabesch, M., Vonk, J. M., Postma, D. S., and Koppelman, G. H.

Published
2016

6. Combining genomewide association study and lung eQTL analysis provides evidence for novel genes associated with asthma

Author

Nieuwenhuis, M.A., Siedlinski, M., van den Berge, M., Granell, R. (Raquel), Li, X., Niens, M., Vlies, P. (P.) van der, Altmüller, J. (Janine), Nürnberg, P. (Peter), Kerkhof, M. (Marjan), Schayck, O.C.P. (Onno), Riemersma, R.A. (Roland), Molen, T. (Thys) van der, Monchy, J.G. de, Bossé, Y., Sandford, A. (Andrew), Bruijnzeel-Koomen, C.A., Gerth van Wijk, R., ten Hacken, N.H., Timens, W. (Wim), Boezen, H.M. (Marike), Henderson, J., Kabesch, M. (Michael), Vonk, J.M. (Judith), Postma, D.S. (Dirkje), Koppelman, G.H. (Gerard), Nieuwenhuis, M.A., Siedlinski, M., van den Berge, M., Granell, R. (Raquel), Li, X., Niens, M., Vlies, P. (P.) van der, Altmüller, J. (Janine), Nürnberg, P. (Peter), Kerkhof, M. (Marjan), Schayck, O.C.P. (Onno), Riemersma, R.A. (Roland), Molen, T. (Thys) van der, Monchy, J.G. de, Bossé, Y., Sandford, A. (Andrew), Bruijnzeel-Koomen, C.A., Gerth van Wijk, R., ten Hacken, N.H., Timens, W. (Wim), Boezen, H.M. (Marike), Henderson, J., Kabesch, M. (Michael), Vonk, J.M. (Judith), Postma, D.S. (Dirkje), and Koppelman, G.H. (Gerard)

Abstract

Background: Genomewide association studies (GWASs) of asthma have identified single-nucleotide polymorphisms (SNPs) that modestly increase the risk for asthma. This could be due to phenotypic heterogeneity of asthma. Bronchial hyperresponsiveness (BHR) is a phenotypic hallmark of asthma. We aim to identify susceptibility genes for asthma combined with BHR and analyse the presence of cis-eQTLs among replicated SNPs. Secondly, we compare the genetic association of SNPs previously associated with (doctor's diagnosed) asthma to our GWAS of asthma with BHR. Methods: A GWAS was performed in 920 asthmatics with BHR and 980 controls. Top SNPs of our GWAS were analysed in four replication cohorts, and lung cis-eQTL analysis was performed on replicated SNPs. We investigated association of SNPs previously associated with asthma in our data. Results: A total of 368 SNPs were followed up for replication. Six SNPs in genes encoding ABI3BP, NAF1, MICA and the 17q21 locus replicated in one or more cohorts, with one locus (17q21) achieving genomewide significance after meta-analysis. Five of 6 replicated SNPs regulated 35 gene transcripts in whole lung. Eight of 20 asthma-associated SNPs from previous GWAS were significantly associated with asthma and BHR. Three SNPs, in IL-33 and GSDMB, showed larger effect sizes in our data compared to p

Published
2016
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7. Combining genomewide association study and lung eQTL analysis provides evidence for novel genes associated with asthma

Author

MS Dermatologie/Allergologie, Infection & Immunity, DIGD-Medisch 1, Nieuwenhuis, M. A., Siedlinski, M., van den Berge, M., Granell, R., Li, X., Niens, M., van der Vlies, P., Altmüller, J., Nürnberg, P., Kerkhof, M., van Schayck, O. C., Riemersma, R. A., van der Molen, T., de Monchy, J. G., Bossé, Y., Sandford, A., Bruijnzeel-Koomen, C. A., Gerth van Wijk, R., ten Hacken, N. H., Timens, W., Boezen, H. M., Henderson, J., Kabesch, M., Vonk, J. M., Postma, D. S., Koppelman, G. H., MS Dermatologie/Allergologie, Infection & Immunity, DIGD-Medisch 1, Nieuwenhuis, M. A., Siedlinski, M., van den Berge, M., Granell, R., Li, X., Niens, M., van der Vlies, P., Altmüller, J., Nürnberg, P., Kerkhof, M., van Schayck, O. C., Riemersma, R. A., van der Molen, T., de Monchy, J. G., Bossé, Y., Sandford, A., Bruijnzeel-Koomen, C. A., Gerth van Wijk, R., ten Hacken, N. H., Timens, W., Boezen, H. M., Henderson, J., Kabesch, M., Vonk, J. M., Postma, D. S., and Koppelman, G. H.

Published
2016

8. Combining genomewide association study and lung eQTL analysis provides evidence for novel genes associated with asthma

Author

Nieuwenhuis, M A, Siedlinski, M, van den Berge, M, Granell, R, Li, X, Niens, M, van der Vlies, P, Altmuller, J, Nurnberg, P, Kerkhof, M, van Schayck, OC, Riemersma, RA, van der Molen, T, de Monchy, J G, Bosse, Y, Sandford, A, Bruijnzeel-Koomen, CA, Gerth van Wijk, Roy, ten Hacken, N H, Timens, W, Boezen, HM, Henderson, J, Kabesch, M, Vonk, JM, Postma, DS, Koppelman, GH, Nieuwenhuis, M A, Siedlinski, M, van den Berge, M, Granell, R, Li, X, Niens, M, van der Vlies, P, Altmuller, J, Nurnberg, P, Kerkhof, M, van Schayck, OC, Riemersma, RA, van der Molen, T, de Monchy, J G, Bosse, Y, Sandford, A, Bruijnzeel-Koomen, CA, Gerth van Wijk, Roy, ten Hacken, N H, Timens, W, Boezen, HM, Henderson, J, Kabesch, M, Vonk, JM, Postma, DS, and Koppelman, GH

Published
2016

9. Combining genomewide association study and lung eQTL analysis provides evidence for novel genes associated with asthma

Author

Nieuwenhuis, M. A., primary, Siedlinski, M., additional, van den Berge, M., additional, Granell, R., additional, Li, X., additional, Niens, M., additional, van der Vlies, P., additional, Altmüller, J., additional, Nürnberg, P., additional, Kerkhof, M., additional, van Schayck, O. C., additional, Riemersma, R. A., additional, van der Molen, T., additional, de Monchy, J. G., additional, Bossé, Y., additional, Sandford, A., additional, Bruijnzeel-Koomen, C. A., additional, Gerth van Wijk, R., additional, ten Hacken, N. H., additional, Timens, W., additional, Boezen, H. M., additional, Henderson, J., additional, Kabesch, M., additional, Vonk, J. M., additional, Postma, D. S., additional, and Koppelman, G. H., additional

Published
2016
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10. Loss of intra-islet CD20 expression may complicate efficacy of B-cell-directed type 1 diabetes therapies.

Author

Serreze DV, Chapman HD, Niens M, Dunn R, Kehry MR, Driver JP, Haller M, Wasserfall C, Atkinson MA, Serreze, David V, Chapman, Harold D, Niens, Marijke, Dunn, Robert, Kehry, Marilyn R, Driver, John P, Haller, Michael, Wasserfall, Clive, and Atkinson, Mark A

Abstract

Objective: Consistent with studies in NOD mice, early clinical trials addressing whether depletion of B cells by the Rituximab CD20-specific antibody provides an effective means for type 1 diabetes reversal have produced promising results. However, to improve therapeutic efficacy, additional B-cell-depleting agents, as well as attempts seeking diabetes prevention, are being considered.Research Design and Methods: Autoantibodies, including those against insulin (IAAs), are used to identify at-risk subjects for inclusion in diabetes prevention trials. Therefore, we tested the ability of anti-CD20 to prevent diabetes in NOD mice when administered either before or after IAA onset.Results: The murine CD20-specific 18B12 antibody that like Rituximab, depletes the follicular (FO) but not marginal zone subset of B cells, efficiently inhibited diabetes development in NOD mice in a likely regulatory T-cell-dependent manner only when treatment was initiated before IAA detection. One implication of these results is that the FO subset of B cells preferentially contributes to early diabetes initiation events. However, most important, the inefficient ability of anti-CD20 treatment to exert late-stage diabetes prevention was found to be attributable to downregulation of CD20 expression upon B cell entry into pancreatic islets.Conclusions: These findings provide important guidance for designing strategies targeting B cells as a potential means of diabetes intervention. [ABSTRACT FROM AUTHOR]

Published
2011
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12. Genetic susceptibility to Hodgkin's lymphoma associated with the human leukocyte antigen region

Author

Diepstra, A., Niens, M., Te Meerman, G. J., Poppema, S., Anke van den Berg, Stem Cell Aging Leukemia and Lymphoma (SALL), and Translational Immunology Groningen (TRIGR)

Subjects
CD4(+) T-CELLS, EXPRESSION, Hodgkin disease, CLASS-II REGION, DISEASE, MAJOR HISTOCOMPATIBILITY COMPLEX, antigen presentation, hemic and lymphatic diseases, INCREASED FREQUENCY, Epstein-Barr virus, HLA antigens, EPSTEIN-BARR-VIRUS, REED-STERNBERG CELLS, HLA PHENOTYPES, CONCORDANCE, genetic predisposition, pathophysiology
Abstract

Based on the presence of an abundant inflammatory infiltrate, expression of a broad spectrum of cytokines and the professional antigen presenting phenotype of Hodgkin Reed-Sternberg cells it can be anticipated that immunological mechanisms play a major role in the pathogenesis of Hodgkin's lymphoma (HL). Genetic susceptibility to HL probably relates to functionality of the immune system and the large number of associations with the human leukocyte antigen (HLA) region in family and population-based studies supports this relation. In Epstein-Barr virus (EBV) positive HL cases, which usually demonstrate HLA class I expression, HRS cells should be able to present EBV derived antigenic peptides and trigger the immune system. This process depends on the affinity of the HLA binding groove for binding immunogenic peptides and thus on the HLA alleles. It can be anticipated that certain combinations of alleles predispose to or protect from the development of EBV positive HL. In EBV negative HL cases other antigenic peptides, related to malignant transformation, in combination with other HLA alleles may be involved. In addition, differential attraction and activation of inflammatory cells may influence HL subtype. In this article, possible roles of HLA in HL pathogenesis are explored and genetic associations of HLA with HL are reviewed and commented on.

14. Biological variation of cardiac markers in patients with aortic valve stenosis.

Author

Peeters FECM, Kietselaer BLJH, Hilderink J, van der Linden N, Niens M, Crijns HJGM, and Meex SJR

Abstract

Objective: Cardiac biomarkers hold promise for follow-up and management of aortic valve stenosis (AVS). When interpreting serial biomarker measurements of patients with AVS, it can be challenging to distinguish 'real changes' from 'random fluctuation'. Hence, robust estimation of the biological variation of these biomarkers is essential. In the present study we assessed biological variation of B-type natriuretic peptide (BNP), N-terminus pro-brain natriuretic peptide (NT-proBNP), high-sensitivity troponin-T and high-sensitivity troponin-I (hs-TnT and hs-TnI), and ST2 in subjects with stable AVS., Methods: Serial blood sampling was performed in 25 subjects with moderate AVS-confirmed by echocardiography-and all free from acute cardiovascular events in the past 6 months. Blood samples were taken on seven standardised occasions during 1 year. Analytical variation (CV A ), within-subject biological variation (CV I ), between-subject biological variation (CV G ), index of individuality (II) and reference change values were calculated for all cardiac biomarkers., Results: CV I was highest for BNP (62.0%, 95% CI 52.5 to 75.4) and lowest for hs-TnI (9.2%, 95% CI 2.8 to 13.8). CV G exceeded the CV I for all biomarkers except BNP, and ranged from 19.8% (95% CI 13.8 to 33.4) for ST2 to 57.2% (95% CI 40.4 to 97.3) for hs-TnT. NT-proBNP, hs-TnT and ST2 revealed CV A <5%, while BNP and hs-TnI showed a higher CV A (19.7 and 14.9, respectively). All biomarkers except BNP showed marked individuality, with II ranging from 0.21 to 0.67 (BNP 1.34)., Conclusion: This study provides the first biological variation estimates of cardiac biomarkers in patients with stable AVS. These estimates allow a more evidence-based interpretation of biomarker changes in the follow-up and management of patients with AVS., Trial Registration Number: NCT02510482., Competing Interests: Competing interests: None declared.

Published
2019
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15. Diurnal Rhythm of Cardiac Troponin: Consequences for the Diagnosis of Acute Myocardial Infarction.

Author

Klinkenberg LJ, Wildi K, van der Linden N, Kouw IW, Niens M, Twerenbold R, Rubini Gimenez M, Puelacher C, Daniel Neuhaus J, Hillinger P, Nestelberger T, Boeddinghaus J, Grimm K, Sabti Z, Bons JA, van Suijlen JD, Tan FE, Ten Kate J, Bekers O, van Loon LJ, van Dieijen-Visser MP, Mueller C, and Meex SJ

Subjects
Acute Disease, Aged, Female, Humans, Male, Troponin I blood, Circadian Rhythm physiology, Myocardial Infarction blood, Myocardial Infarction diagnosis, Troponin T blood
Abstract

Background: Interpretation of serial high-sensitivity cardiac troponin (hs-cTn) measurements for the diagnosis of acute myocardial infarction (AMI) assumes random fluctuation of hs-cTn around an individual's homeostatic set point. The aim of this study was to challenge this diagnostic concept., Methods: Study 1 examined the presence of a diurnal hs-cTn rhythm by hourly blood sampling, day and night, in 24 individuals without a recent history of AMI. Study 2 assessed morning vs evening diagnostic accuracy of hs-cTnT and hs-cTnI in a prospective multicenter diagnostic study of 2782 unselected patients, presenting to the emergency department with acute chest pain., Results: In study 1, hs-cTnT, but not hs-cTnI, exhibited a diurnal rhythm, characterized by gradually decreasing concentrations throughout daytime, rising concentrations during nighttime, to peak concentrations in the morning (mean 16.2 ng/L at 8:30 AM and 12.1 ng/L at 7:30 PM). In study 2, the hs-cTnT rhythm was confirmed by higher hs-cTnT concentrations in early-morning presenters compared to evening presenters with an adjudicated diagnosis of noncardiac disease. The diagnostic accuracy [area under the receiver-operation characteristics curve (AUC)] of hs-cTnT at presentation, 1 h, and for the combination of absolute changes with presenting concentration, were very high and comparable among patients presenting early morning as compared to evening (all AUC >0.93). hs-cTnI exhibited no diurnal rhythm with no differences in AUC among early-morning and evening presenters., Conclusions: Rhythmic diurnal variation of hs-cTnT is a general phenomenon that is not seen with hs-cTnI. While the diurnal hs-cTnT rhythm does not seem to affect the diagnostic accuracy of hs-cTnT for AMI, it should be considered when using hs-cTnT for screening purposes., Clinical Trial Registration: 1. Circadian Variation of Cardiac Troponin, NCT02091427, www.clinicaltrials.gov/ct2/show/NCT02091427. 2. Advantageous Predictors of Acute Coronary Syndrome Evaluation (APACE) Study, NCT00470587, www.clinicaltrials.gov/ct2/show/NCT00470587., (© 2016 American Association for Clinical Chemistry.)

Published
2016
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16. Direct comparison of clinical decision limits for cardiac troponin T and I.

Author

Kimenai DM, Henry RM, van der Kallen CJ, Dagnelie PC, Schram MT, Stehouwer CD, van Suijlen JD, Niens M, Bekers O, Sep SJ, Schaper NC, van Dieijen-Visser MP, and Meex SJ

Subjects
Adult, Age Distribution, Aged, Biomarkers blood, Clinical Decision-Making methods, Female, Humans, Male, Middle Aged, Prospective Studies, Reference Values, Sensitivity and Specificity, Sex Distribution, Myocardial Infarction diagnosis, Troponin I blood, Troponin T blood
Abstract

Objective: The 99th percentile upper reference limit of high-sensitivity cardiac troponin (hs-cTn) from a healthy reference population is used for diagnosing acute myocardial infarction (AMI). Accepted current thresholds of hs-cTnT (Roche) and hs-cTnI (Abbott) are 14 and 26 ng/L, respectively. Since thresholds for hs-cTnT and hs-cTnI were derived from different reference cohorts it is unclear whether they are biologically equivalent. We directly assessed sex-specific and age-specific 99th percentile upper reference limits of hs-cTnT and hs-cTnI in a single reference cohort, to investigate whether current divergent thresholds of hs-cTnT and hs-cTnI stem from intrinsic assay differences or reflect cohort variation., Methods: A healthy reference population was derived from a population-based cohort (the Maastricht Study: n=3451; age: 40-75 years). Individuals with diabetes mellitus, a history of cardiovascular disease, cardiac ischaemia on ECG, N-terminal pro-brain natriuretic peptide >125 ng/L or estimated glomerular filtration rate <60 mL/min/1.73 m(2) were excluded. Non-parametric analyses were performed to assess 99th percentile upper reference limits., Results: 1540 individuals were included in the healthy reference population (age 57±8 years, 52.4% women). Overall 99th percentile upper reference limits of hs-cTnT and hs-cTnI were 15 and 13 ng/L, respectively. Upper reference limits were higher in men than women (hs-cTnT: 16 vs 12 ng/L), (hs-cTnI: 20 vs 11 ng/L) and increased with age., Conclusions: Direct comparison reveals numerically similar thresholds for hs-cTnT and hs-cTnI assays. This finding is in line with recently reported underdiagnosis of AMI with the current decision limit of 26 ng/L for hs-cTnI, especially among women. Downwards adjustment of the hs-cTnI threshold, differentiated for sex, would equalise clinical decision limits for both assays, and may prevent further underdiagnosis of AMI., (Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://www.bmj.com/company/products-services/rights-and-licensing/)

Published
2016
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17. Bridging Mice to Men: Using HLA Transgenic Mice to Enhance the Future Prediction and Prevention of Autoimmune Type 1 Diabetes in Humans.

Author

Serreze DV, Niens M, Kulik J, and DiLorenzo TP

Subjects
Animals, Diabetes Mellitus, Type 1 immunology, Disease Models, Animal, Female, HLA Antigens immunology, Humans, Male, Mice, Mice, Inbred NOD, Mice, Transgenic, CD4-Positive T-Lymphocytes metabolism, Diabetes Mellitus, Type 1 prevention & control, HLA Antigens genetics, Insulin-Secreting Cells immunology
Abstract

Similar to the vast majority of cases in humans, the development of type 1 diabetes (T1D) in the NOD mouse model is due to T-cell mediated autoimmune destruction of insulin producing pancreatic β cells. Particular major histocompatibility complex (MHC) haplotypes (designated HLA in humans; and H2 in mice) provide the primary genetic risk factor for T1D development. It has long been appreciated that within the MHC, particular unusual class II genes contribute to the development of T1D in both humans and NOD mice by allowing for the development and functional activation of β cell autoreactive CD4 T cells. However, studies in NOD mice have revealed that through interactions with other background susceptibility genes, the quite common class I variants (K(d), D(b)) characterizing this strain's H2 (g7) MHC haplotype aberrantly acquire an ability to support the development of β cell autoreactive CD8 T cell responses also essential to T1D development. Similarly, recent studies indicate that in the proper genetic context some quite common HLA class I variants also aberrantly contribute to T1D development in humans. This review focuses on how "humanized" HLA transgenic NOD mice can be created and used to identify class I dependent β cell autoreactive CD8 T cell populations of clinical relevance to T1D development. There is also discussion on how HLA transgenic NOD mice can be used to develop protocols that may ultimately be useful for the prevention of T1D in humans by attenuating autoreactive CD8 T cell responses against pancreatic β cells.

Published
2016
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18. The effect of exercise training on the course of cardiac troponin T and I levels: three independent training studies.

Author

van der Linden N, Klinkenberg LJ, Leenders M, Tieland M, Verdijk LB, Niens M, van Suijlen JD, de Groot LC, Bekers O, van Loon LJ, van Dieijen-Visser MP, and Meex SJ

Subjects
Adult, Aged, Female, Humans, Male, Time Factors, Exercise, Troponin I blood, Troponin T blood
Abstract

With the introduction of high-sensitive assays, cardiac troponins became potential biomarkers for risk stratification and prognostic medicine. Observational studies have reported an inverse association between physical activity and basal cardiac troponin levels. However, causality has never been demonstrated. This study investigated whether basal cardiac troponin concentrations are receptive to lifestyle interventions such as exercise training. Basal high-sensitive cardiac troponin T (cTnT ) and I (cTnI) were monitored in two resistance-type exercise training programs (12-week (study 1) and 24-week (study 2)) in older adults (≥65 years). In addition, a retrospective analysis for high sensitive troponin I in a 24-week exercise controlled trial in (pre)frail older adults was performed (study 3). In total, 91 subjects were included in the final data analyses. There were no significant changes in cardiac troponin levels over time in study 1 and 2 (study 1: cTnT -0.13 (-0.33-+0.08) ng/L/12-weeks, cTnI -0.10 (-0.33-+0.12) ng/L/12-weeks; study 2: cTnT -1.99 (-4.79-+0.81) ng/L/24-weeks, cTnI -1.59 (-5.70-+2.51) ng/L/24-weeks). Neither was there a significant interaction between training and the course of cardiac troponin in study 3 (p = 0.27). In conclusion, this study provides no evidence that prolonged resistance-type exercise training can modulate basal cardiac troponin levels.

Published
2015
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19. Clinical Interpretation of Elevated Concentrations of Cardiac Troponin T, but Not Troponin I, in Nursing Home Residents.

Author

Cardinaels EP, Daamen MA, Bekers O, ten Kate J, Niens M, van Suijlen JD, van Dieijen-Visser MP, Brunner-La Rocca HP, Schols JM, and Mingels AM

Subjects
Aged, 80 and over, Biomarkers blood, Creatinine blood, Cystatin C blood, Female, Glomerular Filtration Rate, Heart Failure epidemiology, Humans, Kidney Diseases blood, Kidney Diseases epidemiology, Male, Netherlands epidemiology, Prognosis, Troponin I blood, Heart Failure blood, Nursing Homes, Troponin T blood
Abstract

Objective: Cardiac troponins T (cTnT) and I (cTnI) are the preferred biomarkers to detect myocardial damage. The present study explores the value of measuring cardiac troponins (cTn) in nursing home residents, by investigating its relation to heart failure and 1-year mortality using 1 cTnT and 2 cTnI assays that are widely used in clinical practice., Design: All participants underwent extensive clinical examinations and echocardiographic assessment for the diagnosis of heart failure. cTn was measured using high-sensitive (hs)- cTnT (Roche), hs-cTnI (Abbott), and sensitive cTnI (Beckman) assays. The glomerular filtration rate was estimated (eGFR) using serum creatinine and cystatin C concentrations. Data on all-cause mortality were collected at 1-year follow-up., Participants and Setting: Participants were 495 long-term nursing home residents, older than 65 years, of 5 Dutch nursing home organizations., Results: Median (IQR) concentrations were 20.6 (17.8-30.6), 6.8 (4.1-12.5), and 4.0 (2.0-8.0) ng/L for hs-cTnT, hs-cTnI, and cTnI, respectively. In total, 79% had elevated hs-cTnT concentrations, whereas only 9% and 5% of hs-cTnI and cTnI concentrations were elevated. Most important and independent determinants for higher hs-cTnT and hs-cTnI concentrations were heart failure and renal dysfunction. Whereas both heart failure (odds ratio [OR] 3.4) and eGFR lower than 60 mL/min/1.73 m(2) (OR 3.6) were equal contributors to higher hs-cTnT concentrations (all P < .001), hs-cTnI and cTnI were less associated with renal dysfunction (OR of, respectively, 1.9 and 2.1; P < .01) in comparison with heart failure (OR 4.3 and 4.7, respectively, P < .001). Furthermore, residents with higher hs-cTnT or hs-cTnI concentrations (fourth quartile) had respectively 4 versus 2 times more risk of 1-year mortality compared with lower concentrations., Conclusion: Regardless of their cardiac health, hs-cTnT but not hs-cTnI concentrations were elevated in almost all aged nursing home residents, questioning the use of the current diagnostic cutoff in elderly with high comorbidity. Nonetheless, measuring cardiac troponins, especially hs-cTnT, had a promising role in assessing future risk of mortality., (Copyright © 2015 AMDA – The Society for Post-Acute and Long-Term Care Medicine. Published by Elsevier Inc. All rights reserved.)

Published
2015
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20. Prevention of "Humanized" diabetogenic CD8 T-cell responses in HLA-transgenic NOD mice by a multipeptide coupled-cell approach.

Author

Niens M, Grier AE, Marron M, Kay TW, Greiner DL, and Serreze DV

Subjects
Animals, Cells, Cultured, Diabetes Mellitus, Type 1 metabolism, Diabetes Mellitus, Type 1 therapy, Enzyme-Linked Immunosorbent Assay, Female, Glucose-6-Phosphatase immunology, HLA-A2 Antigen genetics, Humans, Immunotherapy, Mice, Mice, Inbred NOD, Mice, Transgenic, Proteins immunology, Spleen cytology, CD8-Positive T-Lymphocytes immunology, HLA-A2 Antigen immunology
Abstract

Objective: Type 1 diabetes can be inhibited in standard NOD mice by autoantigen-specific immunotherapy targeting pathogenic CD8+ T-cells. NOD.β2m(null).HHD mice expressing human HLA-A2.1 but lacking murine major histocompatibility complex class I molecules develop diabetes characterized by CD8 T-cells recognizing certain autoantigenic peptides also targeted in human patients. These include peptides derived from the pancreatic β-cell proteins insulin (INS1/2 A(2-10) and INS1 B(5-14)) and islet-specific glucose-6-phosphatase catalytic subunit-related protein (IGRP(265-273) and IGRP(228-236)). Hence, NOD.β2m(null).HHD mice represent a model system for developing potentially clinically translatable interventions for suppressing diabetogenic HLA-A2.1-restricted T-cell responses., Research Design and Methods: Starting at 4-6 weeks of age, NOD.β2m(null).HHD female mice were injected intravenously with syngeneic splenocytes to which various admixtures of the four above-mentioned peptides were bound by the cross-linking agent ethylene carbodiimide (ECDI)., Results: Treatment with such cells bearing the complete cocktail of INS and IGRP epitopes (designated INS/IGRP-SPs) significantly inhibited diabetes development in NOD.β2m(null).HHD recipients compared with controls receiving splenocytes coupled with an irrelevant HLA-A2.1-restricted Flu16 peptide. Subsequent analyses found syngeneic splenocytes bearing the combination of the two ECDI-coupled IGRPs but not INS peptides (IGRP-SPs or INS-SPs) effectively inhibited diabetes development in NOD.β2m(null).HHD mice. This result was supported by enzyme-linked immunospot (ELISPOT) analyses indicating combined INS/IGRP-SPs diminished HLA-A2.1-restricted IGRP but not INS autoreactive CD8+ T-cell responses in NOD.β2m(null).HHD mice., Conclusions: These data support the potential of a cell therapy approach targeting HLA-A2.1-restricted IGRP autoreactive CD8 T-cells as a diabetes intervention approach in appropriate human patients.

Published
2011
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21. Bridging mice to men: using HLA transgenic mice to enhance the future prediction and prevention of autoimmune type 1 diabetes in humans.

Author

Serreze DV, Niens M, Kulik J, and Dilorenzo TP

Subjects
Amino Acid Sequence, Animals, Female, Genetic Predisposition to Disease, Glucose-6-Phosphatase genetics, Glucose-6-Phosphatase metabolism, Humans, Insulin genetics, Insulin metabolism, Mice, Mice, Inbred NOD, Proteins genetics, Proteins metabolism, Transgenes, Diabetes Mellitus, Type 1 genetics, Diabetes Mellitus, Type 1 immunology, Diabetes Mellitus, Type 1 prevention & control, HLA Antigens genetics, HLA Antigens immunology, Mice, Transgenic
Abstract

Similar to the vast majority of cases in humans, the development of type 1 diabetes (T1D) in the NOD mouse model is due to T-cell mediated autoimmune destruction of insulin-producing pancreatic beta cells. Particular major histocompatibility complex (MHC) haplotypes (designated HLA in humans and H2 in mice) provide the primary genetic risk factor for T1D development. It has long been appreciated that within the MHC, particular unusual class II genes contribute to the development of T1D in both humans and NOD mice by allowing for the development and functional activation of beta-cell autoreactive CD4 T cells. However, studies in NOD mice have revealed that through interactions with other background susceptibility genes, the quite common class I variants (K(d), D(b)) characterizing this strain's H2 ( g7 ) MHC haplotype aberrantly acquire an ability to support the development of beta cell autoreactive CD8 T-cell responses also essential to T1D development. Similarly, recent studies indicate that in the proper genetic context some quite common HLA class I variants also aberrantly contribute to T1D development in humans. This chapter will focus on how "humanized" HLA transgenic NOD mice can be created and used to identify class I-dependent beta cell autoreactive CD8 T-cell populations of clinical relevance to T1D development. There is also discussion on how HLA transgenic NOD mice can be used to develop protocols that may ultimately be useful for the prevention of T1D in humans by attenuating autoreactive CD8 T-cell responses against pancreatic beta cells.

Published
2010
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22. Serum chemokine levels in Hodgkin lymphoma patients: highly increased levels of CCL17 and CCL22.

Author

Niens M, Visser L, Nolte IM, van der Steege G, Diepstra A, Cordano P, Jarrett RF, Te Meerman GJ, Poppema S, and van den Berg A

Subjects
Chemokines blood, Genetic Predisposition to Disease, Genotype, Hodgkin Disease genetics, Hodgkin Disease pathology, Humans, Neoplasm Staging, Polymorphism, Single Nucleotide, Chemokine CCL17 blood, Chemokine CCL22 blood, Hodgkin Disease blood, Neoplasm Proteins blood
Abstract

Hodgkin lymphoma (HL) is characterized by a minority of neoplastic Hodgkin-Reed Sternberg (HRS) cells surrounded by a non-neoplastic reactive infiltrate. As immunological mechanisms appear to be crucial in classical HL pathogenesis, altered serum chemokine levels might be related to disease activity. Serum levels of nine chemokines were examined in 163 untreated HL patients and 334 controls. We investigated single nucleotide polymorphisms (SNPs) for association with serum CCL17 (thymus and activation-regulated chemokine, TARC) levels and HL susceptibility. Serum CCL17 and CCL22 (macrophage-derived chemokine, MDC) levels were significantly increased in 82% and 57% of the HL patients. Nodular sclerosis cases showed increased serum CCL17 and CCL22 levels (P < 0.001) and serum levels were correlated with Ann Arbor stage. Of nine patients with pre- and post-treatment serum samples, the majority showed decreased CCL17 and CCL22 levels after treatment. HRS cells expressed CCL17 and CCL22 in 77% and 75% of 74 cases. Three SNPs showed a trend of increased serum CCL17 levels with minor alleles in controls, but were not associated with HL susceptibility. CCL17 and CCL22 were the only chemokines with increased serum levels in the vast majority of HL patients, which provides further insight into the molecular mechanism(s) leading to infiltrations of reactive lymphocytes in HL.

Published
2008
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23. HLA-A*02 is associated with a reduced risk and HLA-A*01 with an increased risk of developing EBV+ Hodgkin lymphoma.

Author

Niens M, Jarrett RF, Hepkema B, Nolte IM, Diepstra A, Platteel M, Kouprie N, Delury CP, Gallagher A, Visser L, Poppema S, te Meerman GJ, and van den Berg A

Subjects
Adolescent, Adult, Aged, Aged, 80 and over, Epstein-Barr Virus Infections complications, Female, Genetic Predisposition to Disease, HLA-A1 Antigen, HLA-A2 Antigen, Haplotypes, Hodgkin Disease complications, Hodgkin Disease virology, Humans, Male, Middle Aged, Polymorphism, Single Nucleotide, Risk Factors, Epstein-Barr Virus Infections genetics, HLA-A Antigens genetics, Hodgkin Disease genetics
Abstract

Previous studies showed that the HLA class I region is associated with Epstein-Barr virus (EBV)-positive Hodgkin lymphoma (HL) and that HLA-A is the most likely candidate gene in this region. This suggests that antigenic presentation of EBV-derived peptides in the context of HLA-A is involved in the pathogenesis of EBV+ HL by precluding efficient immune responses. We genotyped exons 2 and 3, encoding the peptide-binding groove of HLA-A, for 32 single nucleotide polymorphisms in 70 patients with EBV+ HL, 31 patients with EBV- HL, and 59 control participants. HLA-A*01 was significantly overrepresented and HLA-A*02 was significantly underrepresented in patients with EBV+ HL versus controls and patients with EBV- HL. In addition, HLA-A*02 status was determined by immunohistochemistry or HLA-A*02-specific polymerase chain reaction (PCR) on 152 patients with EBV+ HL and 322 patients with EBV- HL. The percentage of HLA-A*02+ patients in the EBV+ HL group (35.5%) was significantly lower than in 6107 general control participants (53.0%) and the EBV- HL group (50.9%). Our results indicate that individuals carrying the HLA-A*02 allele have a reduced risk of developing EBV+ HL, while individuals carrying the HLA-A*01 allele have an increased risk. It is known that HLA-A*02 can present EBV-derived peptides and can evoke an effective immune response, which may explain the protective phenotype.

Published
2007
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24. The human leukocyte antigen class I region is associated with EBV-positive Hodgkin's lymphoma: HLA-A and HLA complex group 9 are putative candidate genes.

Author

Niens M, van den Berg A, Diepstra A, Nolte IM, van der Steege G, Gallagher A, Taylor GM, Jarrett RF, Poppema S, and te Meerman GJ

Subjects
Alleles, Case-Control Studies, Haplotypes, Homozygote, Humans, Lymphoma metabolism, Netherlands, Peptides chemistry, T-Lymphocytes, Cytotoxic immunology, Chromosome Mapping, Genes, MHC Class I, HLA-A Antigens genetics, Herpesvirus 4, Human metabolism, Hodgkin Disease genetics, Hodgkin Disease immunology, Hodgkin Disease virology, Polymorphism, Single Nucleotide
Abstract

Various studies have indicated that the human leukocyte antigen (HLA) region is associated with Hodgkin's lymphoma. We recently showed a specific association of the HLA class I region with EBV-positive Hodgkin's lymphoma cases. One haplotype of two consecutive microsatellite markers (D6S265 and D6S510) was overrepresented in the patient group, whereas another haplotype was underrepresented. Here, we did fine mapping of this region of approximately 400 kb as a next step to find the causative single-nucleotide polymorphism(s) (SNP). To select candidate SNPs for screening the total study population, several known SNPs were determined by sequencing two individuals homozygous for either of the above-mentioned associated haplotypes. Seven SNPs displayed different alleles in these two individuals and were therefore analyzed in the total study population, including 238 Hodgkin's lymphoma patients and 365 family-based controls. All seven SNPs showed significant association with the EBV-positive patient group. Two of these SNPs were analyzed in a Scottish Hodgkin's lymphoma population and revealed significant associations as well. The associated SNPs are located nearby two putative candidate genes: HLA-A and HLA complex group 9. HLA-A represents the most interesting target because of its consistent expression in EBV-positive Hodgkin's lymphoma cases and its ability to present EBV-derived peptides to cytotoxic T cells.

Published
2006
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25. A factorial experiment for optimizing the PCR conditions in routine genotyping.

Author

Niens M, Spijker GT, Diepstra A, and te Meerman GJ

Subjects
Analysis of Variance, Genetic Markers, Genotype, HLA Antigens analysis, HLA Antigens genetics, Hodgkin Disease genetics, Humans, Microsatellite Repeats, Histocompatibility Testing methods, Polymerase Chain Reaction methods, Sequence Analysis, DNA methods
Abstract

Although most PCRs would produce proper PCR products when first tried, a general optimization is required to yield the best results. This optimization is often achieved by changing one factor at a time. However, this may lead to suboptimal results, since interactions between conditions are difficult to detect with this approach. In the present study, we describe the factorial optimization of PCR conditions for microsatellite genotyping, by introducing small systematic variations in conditions during the genotyping process. The hypothesis was that small changes will not affect genotyping results, but will provide information about the optimality of current conditions. The conditions to vary were the concentrations of buffer, MgCl(2), dNTPs, primers, Taq polymerase and DNA, the annealing temperature (T(a)) and the number of cycles. We show that, by a 2(8) factorial experiment, it is possible to identify not only the factors responsible for obtaining good results, but also those responsible for bad results. However, the condition leading to the highest signals is not necessarily the best operational condition. The best operational condition is minimally sensitive to random pipetting fluctuations and yields reliable genotypes as well.

Published
2005
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26. The human leukocyte antigen region and colorectal cancer risk.

Author

de Jong MM, Niens M, Nolte IM, te Meerman GJ, van der Graaf WT, Mulder MJ, van der Steege G, Bruinenberg M, Schaapveld M, Sijmons RH, Hofstra RM, de Vries EG, and Kleibeuker JH

Subjects
Adult, Aged, Aged, 80 and over, Alleles, Case-Control Studies, Female, Genetic Markers, Genetic Predisposition to Disease, Genotype, Haplotypes, Humans, Linkage Disequilibrium, Male, Microsatellite Repeats, Middle Aged, Netherlands, Registries, Risk Factors, Colorectal Neoplasms genetics, HLA Antigens genetics
Abstract

Purpose: Recently, we found a certain haplotype in the human leukocyte antigen Class III subregion to be associated with breast cancer. Epidemiologic studies have shown that breast cancer and colorectal cancer have several risk factors in common. In view of these studies and because polymorphisms located in the human leukocyte antigen III region have been found to be associated with colorectal cancer, we wondered whether the same region also is involved in colorectal cancer susceptibility., Methods: The human leukocyte antigen region was genotyped with 14 microsatellite markers in germline DNA from 643 colorectal cancer patients and 841 family-based controls. Association analyses and the Haplotype Sharing Statistic were used to search for differences between patients and controls. Subgroup analyses were performed for gender, age at diagnosis, and localization of the tumor., Results: The Haplotype Sharing Statistic analysis revealed neither a difference in mean haplotype sharing between all patients and controls, nor in any of the subgroups. The single allele, genotype, and two-locus association analyses for all patients and for the different subgroups did not show an association with colorectal cancer for the 14 microsatellite markers. Also, no association was observed between the tumor necrosis factor-beta polymorphism and colorectal cancer., Conclusions: No association was observed between commonly occurring haplotypes and alleles in the human leukocyte antigen region and colorectal cancer risk.

Published
2005
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