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4. Assessment of Key Characteristics, Methodology, and Effect Size Measures Used in Meta-Analysis of Human-Health-Related Animal Studies

Author

Hooijmans, Carlijn R., Donders, Rogier, Magnuson, Kristen, Wever, Kimberley E., Ergün, Mehmet, Rooney, Andrew A., Walker, Vickie, and Langendam, Miranda W.

Abstract

Since the early 1990s the number of systematic reviews (SR) of animal studies has steadily increased. There is, however, little guidance on when and how to conduct a meta-analysis of human-health-related animal studies. To gain insight about the methods that are currently used we created an overview of the key characteristics of published meta-analyses of animal studies, with a focus on the choice of effect size measures. An additional goal was to learn about the rationale behind the meta-analysis methods used by the review authors. We show that important details of the meta-analyses are not fully described, only a fraction of all human-health-related meta-analyses provided rationales for their decision to use specific effect size measures. In addition, our data may suggest that authors make post-hoc decisions to switch to another effect size measure during the course of their meta-analysis, and possibly search for significant effects. Based on analyses in this paper we recommend that review teams: 1) publish a review protocol before starting the conduct of a SR, prespecifying all methodological details (providing special attention to the planned meta-analysis including the effect size measure and the rational behind choosing a specific effect size, prespecifying subgroups and restricting the number of subgroup analyses), 2) always use the Preferred Reporting Items for Systematic Review and Meta-Analyses (PRISMA) checklist to report your SR of animal studies, and 3) use the random effects model (REM) in human-health-related meta-analysis of animal studies, unless the assumptions for using the fixed effect model (FEM) are all met.

Published
2022
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13. Strategy for developing data standards in support of automation of Systematic Reviews.

Author

Hooijmans, Carlijn R, Wever, Kimberley E, Macleod, Malcolm R, Whaley, Paul, and Bannach‐Brown, Alexandra

Subjects
*AUTOMATION, *STAKEHOLDERS, *INTERNETWORKING
Abstract

The current report is the result of the recent EFSA‐EBTC initiative to advance the use of automation tools in systematic reviews. The working group members identified the need for data exchange standards to facilitate transferring data between SR automation tools without loss or changes in data as a first priority. Closely related objectives identified were the concurrent development of data guidance and data content standards, and a strategy for governance of the resulting data standards, including their maintenance and regular updates. These conversations led up to the organization of workshops to initiate the development of data standards, as described in the current report. The EFSA‐EBTC collaboration organized a four half‐day workshop for an extensive group of stakeholders actively involved in the development or use of SR automation tools. The main objectives were 1) to generate a common understanding of the needs and hurdles for data standards in SR automation, 2) to collate viewpoints from all relevant stakeholders on how such standards may be developed, and 3) to kick‐off the development process. Three preparatory workshops preceding the final workshop were organized to clarify the scope and objectives of the main workshop. This external scientific report contains the summary of the preparatory and main workshops, as well as the proposed strategy for the process of how these data standards could be developed. The recommended next steps for development focus on further refining the aims, analysis of the landscape, interoperability with existing standards, setting up the infrastructure (e.g., establishing a governance structure and working groups containing all essential stakeholders), and the process of actual data standard development, launching and monitoring adoption of the standards. [ABSTRACT FROM AUTHOR]

Published
2024
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14. Reduced uterine perfusion pressure as a model for preeclampsia and fetal growth restriction in murine: a systematic review and meta-analysis.

Author

Kammen, Caren M. van, Taal, Seija E. L., Wever, Kimberley E., Granger, Joey P., Lely, A. Titia, and Terstappen, Fieke

Subjects
FETAL growth retardation, PREECLAMPSIA, PHENOTYPIC plasticity, PERFUSION, BLOOD pressure
Abstract

The reduced uterine perfusion pressure (RUPP) model is frequently used to study preeclampsia and fetal growth restriction. An improved understanding of influential factors might improve reproducibility and reduce animal use considering the variability in RUPP phenotype. We performed a systematic review and meta-analysis by searching Medline and Embase (until 28 March, 2023) for RUPP studies in murine. Primary outcomes included maternal blood pressure (BP) or proteinuria, fetal weight or crown-rump length, fetal reabsorptions, or antiangiogenic factors. We aimed to identify influential factors by meta-regression analysis. We included 155 studies. Our meta-analysis showed that the RUPP procedure results in significantly higher BP (MD = 24.1 mmHg; [22.6; 25.7]; n = 148), proteinuria (SMD = 2.3; [0.9; 3.8]; n = 28), fetal reabsorptions (MD = 50.4%; [45.5; 55.2]; n = 42), circulating soluble FMS-like tyrosine kinase-1 (sFlt-1) (SMD = 2.6; [1.7; 3.4]; n = 34), and lower fetal weight (MD = −0.4 g; [−0.47; −0.34]; n = 113. The heterogeneity (variability between studies) in primary outcomes appeared ≥90%. Our meta-regression identified influential factors in the method and time point of BP measurement, randomization in fetal weight, and type of control group in sFlt-1. The RUPP is a robust model considering the evident differences in maternal and fetal outcomes. The high heterogeneity reflects the observed variability in phenotype. Because of underreporting, we observed reporting bias and a high risk of bias. We recommend standardizing study design by optimal time point and method chosen for readout measures to limit the variability. This contributes to improved reproducibility and thereby eventually improves the translational value of the RUPP model. [ABSTRACT FROM AUTHOR]

Published
2024
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15. Understanding changes in echocardiographic parameters at different ages following fetal growth restriction: a systematic review and meta-analysis.

Author

van de Meent, Mette, Nijholt, Kirsten T., Joemmanbaks, Shary C. A., Kooiman, Judith, Schipper, Henk S., Wever, Kimberley E., Lely, A. Titia, and Terstappen, Fieke

Subjects
FETAL growth retardation, GESTATIONAL age, GLOBAL longitudinal strain, ECHOCARDIOGRAPHY, VENTRICULAR septum
Abstract

Fetal growth restriction (FGR) increases cardiovascular risk by cardiac remodeling and programming. This systematic review and meta-analysis across species examines the use of echocardiography in FGR offspring at different ages. PubMed and Embase.com were searched for animal and human studies reporting on echocardiographic parameters in placental insufficiency-induced FGR offspring. We included six animal and 49 human studies. Although unable to perform a meta-analysis of animal studies because of insufficient number of studies per individual outcome, all studies showed left ventricular dysfunction. Our meta-analyses of human studies revealed a reduced left ventricular mass, interventricular septum thickness, mitral annular peak velocity, and mitral lateral early diastolic velocity at neonatal age. No echocardiographic differences during childhood were observed, although the small age range and number of studies limited these analyses. Only two studies at adult age were performed. Meta-regression on other influential factors was not possible due to underreporting. The few studies on myocardial strain analysis showed small changes in global longitudinal strain in FGR offspring. The quality of the human studies was considered low and the risk of bias in animal studies was mostly unclear. Echocardiography may offer a noninvasive tool to detect early signs of cardiovascular predisposition following FGR. Clinical implementation yet faces multiple challenges including identification of the most optimal timing and the exact relation to long-term cardiovascular function in which echocardiography alone might be limited to reflect a child's vascular status. Future research should focus on myocardial strain analysis and the combination of other (non)imaging techniques for an improved risk estimation. [ABSTRACT FROM AUTHOR]

Published
2024
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21. Designing, conducting, and reporting reproducible animal experiments.

Author

Wilson, Emma, Ramage, Fiona J., Wever, Kimberley E., Sena, Emily S., Macleod, Malcolm R., and Currie, Gillian L.

Subjects
ANIMAL experimentation, REPRODUCIBLE research, SCIENTIFIC community, PREPRINTS, EXPERIMENTAL design
Abstract

In biomedicine and many other fields, there are growing concerns around the reproducibility of research findings, with many researchers bein g unable to replicate their own or others' results. This raises important questions as to the validity and usefulness of much published research. In this review, we aim to engage researchers in the issue of research reproducibility and equip them with the necessary tools to increase the reproducibility of their research. We first high light the causes and potential impact of non-reproducible research and emphasise the benefits of working reproducibly for the researcher and broader research community. We address specific targets for improvement and steps that individual researchers can take to increase the reproducibility of their work. We next provide recommendations for improving the design and conduct of experiments, focusing on in vivo animal experiments. We describe common sources of poor internal validity of experiments and offer practical guidance for limiting these potential sources of bias at different experi mental stages, as well as discussing other important considerations during experimental design. We provide a list of key resources available to researchers to improve experimental design, conduct, and reporting. We then discuss the importance of open research practices such as study preregistration and the use of preprints and describe recommendations around data management and sharing. Our review emphasises the importance of reproducible work and aims to empower every individual researcher to contribute to the reproducibility of research in their field. [ABSTRACT FROM AUTHOR]

Published
2023
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22. Systematic reviews of animal studies -- Report of an international symposium.

Author

Fausak, Erik, Funaro, Melissa C., Kepsel, Andrea C., Eldermire, Erin R. B., Foster, Margaret, Norton, Hannah F., Mears, Kim, Crews, Molly E., Brennan, Marnie, Currie, Gillian L., LaFollette, Megan R., O'Connor, Annette, Smith, Adrian J., Wever, Kimberley E., and Fricke, Suzanne

Subjects
INFORMATION professionals, CONFERENCES & conventions, RESEARCH personnel, GROUP work in research
Abstract

Objective: The Symposium on Animal Systematic Reviews held 24 May 2022, sought to bring organisations working on animal literature searching and systematic reviews together into the same virtual space for introductions and discussion. Background: Groups working on animal research synthesis are often siloed into preclinical, veterinary, and One Health settings. This symposium sought to define commonalities and differences in methodologies, resources, and philosophies and to discuss future needs. Methods: The 3-hour virtual symposium for veterinarians, researchers, and information specialists began with introductions by panelists from organisations involved in searching the literature for animal studies and conducting systematic reviews. This was followed by a panel discussion and question and answer period. Results: Panelists identified a need to ensure planning and accurate description of primary animal studies as a precursor to quality systematic reviews. They acknowledged and discussed differences in evidence synthesis expectations and tools based on the type of review, the types of studies available on the topic, and the focus on preclinical, veterinary, or One Health topics. Conclusion: The need to increase the speed and quality of evidence reviews, and to automate updates, requires investing in the development of both skilled teams and platforms. The symposium provided a chance to identify existing resources, define challenges, and note gaps unique to systematic reviews of animal studies. Application: This symposium acts as a baseline for ongoing discussions centred on improving the culture and pipeline for evidence syntheses of animal studies that inform decision-making. [ABSTRACT FROM AUTHOR]

Published
2023
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27. Allopurinol to reduce cardiovascular morbidity and mortality: A systematic review and meta-analysis.

Author

van der Pol, Karel H., Wever, Kimberley E., Verbakel, Mariette, Visseren, Frank L. J., Cornel, Jan H., and Rongen, Gerard A.

Subjects
*ALLOPURINOL, *DRUG-eluting stents, *CARDIOVASCULAR diseases risk factors, *MYOCARDIAL infarction, *RANDOMIZED controlled trials
Abstract

Aims: To compare the effectiveness of allopurinol with no treatment or placebo for the prevention of cardiovascular events in hyperuricemic patients. Methods and results: Pubmed, Web of Science and Cochrane library were searched from inception until July 2020. Randomized controlled trials (RCT) and observational studies in hyperuricemic patients without significant renal disease and treated with allopurinol, versus placebo or no treatment were included. Outcome measures were cardiovascular mortality, myocardial infarction, stroke, or a combined endpoint (CM/MI/S). For RCT's a random effects meta-analysis was performed. For observational studies a narrative synthesis was performed. Of the original 1995 references we ultimately included 26 RCT's and 21 observational studies. We found a significantly reduced risk of combined endpoint (Risk Ratio 0.65 [95% CI] [0.46 to 0.91]; p = 0.012) and myocardial infarction (RR 0.47 [0.27 to 0.80]; p = 0.01) in the allopurinol group compared to controls. We found no significant effect of allopurinol on stroke or cardiovascular mortality. Of the 15 observational studies with sufficient quality, allopurinol was associated with reduced cardiovascular mortality in 1 out of 3 studies that reported this outcome, myocardial infarction in 6 out of 8, stroke in 4 out of 7, and combined end-point in 2 out of 2. Cardiovascular benefit was only observed when allopurinol therapy was prolonged for more than 6 months and when an appropriate allopurinol dose was administered (300 mg or more/day) or sufficient reduction of serum urate concentration was achieved (<0.36 mmol/l). Conclusions: Data from RCT's and observational studies indicate that allopurinol treatment reduces cardiovascular risk in patients with hyperuricemia. However, the quality of evidence from RCTs is low to moderate. To establish whether allopurinol lowers the risk of cardiovascular events a well-designed and adequately powered randomized, placebo-controlled trial is needed in high-risk patients with hyperuricemia. Systematic review registration: PROSPERO registration CRD42018089744 [ABSTRACT FROM AUTHOR]

Published
2021
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28. Towards a reporting guideline for developmental and reproductive toxicology testing in C. elegans and other nematodes.

Author

van der Voet, Monique, Teunis, Marc, Louter-van de Haar, Johanna, Stigter, Nienke, Bhalla, Diksha, Rooseboom, Martijn, Wever, Kimberley E, Krul, Cyrille, Pieters, Raymond, Wildwater, Marjolein, and van Noort, Vera

Subjects
REPRODUCTIVE toxicology, DEVELOPMENTAL toxicology, TOXICITY testing, CAENORHABDITIS elegans, NEMATODES, RISK assessment, CONTAINER gardening
Abstract

Implementation of reliable methodologies allowing Reduction, Refinement, and Replacement (3Rs) of animal testing is a process that takes several decades and is still not complete. Reliable methods are essential for regulatory hazard assessment of chemicals where differences in test protocol can influence the test outcomes and thus affect the confidence in the predictive value of the organisms used as an alternative for mammals. Although test guidelines are common for mammalian studies, they are scarce for non-vertebrate organisms that would allow for the 3Rs of animal testing. Here, we present a set of 30 reporting criteria as the basis for such a guideline for Developmental and Reproductive Toxicology (DART) testing in the nematode Caenorhabditis elegans. Small organisms like C. elegans are upcoming in new approach methodologies for hazard assessment; thus, reliable and robust test protocols are urgently needed. A literature assessment of the fulfilment of the reporting criteria demonstrates that although studies describe methodological details, essential information such as compound purity and lot/batch number or type of container is often not reported. The formulated set of reporting criteria for C. elegans testing can be used by (i) researchers to describe essential experimental details (ii) data scientists that aggregate information to assess data quality and include data in aggregated databases (iii) regulators to assess study data for inclusion in regulatory hazard assessment of chemicals. [ABSTRACT FROM AUTHOR]

Published
2021
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29. A 3-year evaluation of preclinicaltrials.eu reveals room for improvement in preregistration of animal studies.

Author

van der Naald, Mira, Chamuleau, Steven A. J., Menon, Julia M. L., de Leeuw, Wim, de Haan, Judith J., Duncker, Dirk J., and Wever, Kimberley E.

Subjects
SCIENTIFIC community, LABORATORY animals, RESEARCH protocols
Abstract

In 2018, the first registry dedicated to preregistration of animal study protocols was launched. Despite international support, the overall number of (pre)registered protocols is still low, illustrating the need for pushing the preregistration agenda among researchers and policymakers. This Community Page article presents a 3-year evaluation of the first platform dedicated to preregistration of animal studies, www.preclinicaltrials.eu, and comparable platforms, encouraging the scientific community to embrace preregistration in a move towards more effective animal research. [ABSTRACT FROM AUTHOR]

Published
2021
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30. Epidemiology and reporting characteristics of preclinical systematic reviews.

Author

Hunniford, Victoria T., Montroy, Joshua, Fergusson, Dean A., Avey, Marc T., Wever, Kimberley E., McCann, Sarah K., Foster, Madison, Fox, Grace, Lafreniere, Mackenzie, Ghaly, Mira, Mannell, Sydney, Godwinska, Karolina, Gentles, Avonae, Selim, Shehab, MacNeil, Jenna, Sikora, Lindsey, Sena, Emily S., Page, Matthew J., Macleod, Malcolm, and Moher, David

Subjects
ANIMAL experimentation, ANIMAL species, EPIDEMIOLOGY, TEST validity
Abstract

In an effort to better utilize published evidence obtained from animal experiments, systematic reviews of preclinical studies are increasingly more common—along with the methods and tools to appraise them (e.g., SYstematic Review Center for Laboratory animal Experimentation [SYRCLE's] risk of bias tool). We performed a cross-sectional study of a sample of recent preclinical systematic reviews (2015–2018) and examined a range of epidemiological characteristics and used a 46-item checklist to assess reporting details. We identified 442 reviews published across 43 countries in 23 different disease domains that used 26 animal species. Reporting of key details to ensure transparency and reproducibility was inconsistent across reviews and within article sections. Items were most completely reported in the title, introduction, and results sections of the reviews, while least reported in the methods and discussion sections. Less than half of reviews reported that a risk of bias assessment for internal and external validity was undertaken, and none reported methods for evaluating construct validity. Our results demonstrate that a considerable number of preclinical systematic reviews investigating diverse topics have been conducted; however, their quality of reporting is inconsistent. Our study provides the justification and evidence to inform the development of guidelines for conducting and reporting preclinical systematic reviews. A cross sectional study of a sample of recent preclinical systematic reviews reveals deficiencies in reporting and provides the justification and evidence to inform the development of specific guidelines for conducting and reporting preclinical systematic reviews. [ABSTRACT FROM AUTHOR]

Published
2021
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31. Facilitating healthcare decisions by assessing the certainty in the evidence from preclinical animal studies.

Author

Hooijmans, Carlijn R., de Vries, Rob B. M., Ritskes-Hoitinga, Merel, Rovers, Maroeska M., Leeflang, Mariska M., IntHout, Joanna, Wever, Kimberley E., Hooft, Lotty, de Beer, Hans, Kuijpers, Ton, Macleod, Malcolm R., Sena, Emily S., ter Riet, Gerben, Morgan, Rebecca L., Thayer, Kristina A., Rooney, Andrew A., Guyatt, Gordon H., Schünemann, Holger J., Langendam, Miranda W., and null, null

Subjects
ENVIRONMENTAL health, DRUG development, CLINICAL trials, MEDICAL research, LABORATORY animals
Abstract

Laboratory animal studies are used in a wide range of human health related research areas, such as basic biomedical research, drug research, experimental surgery and environmental health. The results of these studies can be used to inform decisions regarding clinical research in humans, for example the decision to proceed to clinical trials. If the research question relates to potential harms with no expectation of benefit (e.g., toxicology), studies in experimental animals may provide the only relevant or controlled data and directly inform clinical management decisions. Systematic reviews and meta-analyses are important tools to provide robust and informative evidence summaries of these animal studies. Rating how certain we are about the evidence could provide important information about the translational probability of findings in experimental animal studies to clinical practice and probably improve it. Evidence summaries and certainty in the evidence ratings could also be used (1) to support selection of interventions with best therapeutic potential to be tested in clinical trials, (2) to justify a regulatory decision limiting human exposure (to drug or toxin), or to (3) support decisions on the utility of further animal experiments. The Grading of Recommendations, Assessment, Development, and Evaluation (GRADE) approach is the most widely used framework to rate the certainty in the evidence and strength of health care recommendations. Here we present how the GRADE approach could be used to rate the certainty in the evidence of preclinical animal studies in the context of therapeutic interventions. We also discuss the methodological challenges that we identified, and for which further work is needed. Examples are defining the importance of consistency within and across animal species and using GRADE’s indirectness domain as a tool to predict translation from animal models to humans. [ABSTRACT FROM AUTHOR]

Published
2018
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32. A systematic review of discomfort due to toe or ear clipping in laboratory rodents.

Author

Wever, Kimberley E., Geessink, Florentine J., Brouwer, Michelle A. E., Tillema, Alice, and Ritskes-Hoitinga, Merel

Subjects
*TOES, *EAR physiology, *ANIMAL welfare, *BLOOD pressure, *LABORATORY rodents, *SYSTEMATIC reviews, *PHYSIOLOGY
Abstract

Toe clipping and ear clipping (also ear notching or ear punching) are frequently used methods for individual identification of laboratory rodents. These procedures potentially cause severe discomfort, which can reduce animal welfare and distort experimental results. However, no systematic summary of the evidence on this topic currently exists. We conducted a systematic review of the evidence for discomfort due to toe or ear clipping in rodents. The review methodology was pre-specified in a registered review protocol. The population, intervention, control, outcome (PICO) question was: In rodents, what is the effect of toe clipping or ear clipping, compared with no clipping or sham clipping, on welfare-related outcomes? Through a systematic search in PubMed, Embase, Web of Science and grey literature, we identified seven studies on the effect of ear clipping on animal welfare, and five such studies on toe clipping. Studies were included in the review if they contained original data from an in vivo experiment in rodents, assessing the effect of toe clipping or ear clipping on a welfare-related outcome. Case studies and studies applying unsuitable co-interventions were excluded. Study quality was appraised using an extended version of SYstematic Review Centre for Laboratory animal Experimentation (SYRCLE)’s risk of bias tool for animal studies. Study characteristics and outcome measures were highly heterogeneous, and there was an unclear or high risk of bias in all studies. We therefore present a narrative synthesis of the evidence identified. None of the studies reported a sample size calculation. Out of over 60 different outcomes, we found evidence of discomfort due to ear clipping in the form of increased respiratory volume, vocalization and blood pressure. For toe clipping, increased vocalization and decreased motor activity in pups were found, as well as long-term effects in the form of reduced grip strength and swimming ability in adults. In conclusion, there is too little evidence to reliably assess discomfort due to toe or ear clipping, and the quality of the available evidence is uncertain. Adequately powered, high-quality studies reporting reliable, relevant outcome measures are needed to accurately assess the impact of these identification techniques. Until more reliable evidence is available, any effect of toe clipping or ear clipping on animal welfare and study results cannot be confirmed or excluded. [ABSTRACT FROM AUTHOR]

Published
2017
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33. Risk of bias reporting in the recent animal focal cerebral ischaemia literature.

Author

Bahor, Zsanett, Jing Liao, Macleod, Malcolm R., Bannach-Brown, Alexandra, McCann, Sarah K., Wever, Kimberley E., Thomas, James, Ottavi, Thomas, Howells, David W., Rice, Andrew, Ananiadou, Sophia, and Sena, Emily

Subjects
CEREBRAL ischemia, RESEARCH bias, ANIMAL experimentation, LACUNAR stroke, LITERATURE reviews
Abstract

Background: Findings from in vivo research may be less reliable where studies do not report measures to reduce risks of bias. The experimental stroke community has been at the forefront of implementing changes to improve reporting, but it is not known whether these efforts are associated with continuous improvements. Our aims here were firstly to validate an automated tool to assess risks of bias in published works, and secondly to assess the reporting of measures taken to reduce the risk of bias within recent literature for two experimental models of stroke. Methods: We developed and used text analytic approaches to automatically ascertain reporting of measures to reduce risk of bias from full-text articles describing animal experiments inducing middle cerebral artery occlusion (MCAO) or modelling lacunar stroke. Results: Compared with previous assessments, there were improvements in the reporting of measures taken to reduce risks of bias in the MCAO literature but not in the lacunar stroke literature. Accuracy of automated annotation of risk of bias in the MCAO literature was 86% (randomization), 94% (blinding) and 100% (sample size calculation); and in the lacunar stroke literature accuracy was 67% (randomization), 91% (blinding) and 96% (sample size calculation). Discussion: There remains substantial opportunity for improvement in the reporting of animal research modelling stroke, particularly in the lacunar stroke literature. Further, automated tools perform sufficiently well to identify whether studies report blinded assessment of outcome, but improvements are required in the tools to ascertain whether randomization and a sample size calculation were reported. [ABSTRACT FROM AUTHOR]

Published
2017
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35. A systematic review and meta-analysis of the protective effects of metformin in experimental myocardial infarction.

Author

Hesen, Nienke A., Riksen, Niels P., Aalders, Bart, Ritskes-Hoitinga, Merel, El Messaoudi, Saloua, and Wever, Kimberley E.

Subjects
MYOCARDIAL infarction treatment, METFORMIN, CARDIOVASCULAR diseases, ALTERNATIVE medicine, SYSTEMATIC reviews, META-analysis
Abstract

Metformin improves cardiovascular prognosis in patients with diabetes mellitus, compared to alternative glucose-lowering drugs, despite similar glycemic control. Direct cardiovascular protective properties have therefore been proposed, and studied in preclinical models of myocardial infarction. We now aim to critically assess the quality and outcome of these studies. We present a systematic review, quality assessment and meta-analysis of the effect of metformin in animal studies of experimental myocardial infarction. Through a comprehensive search in Pubmed and EMBASE, we identified 27 studies, 11 reporting on ex vivo experiments and 18 reporting on in vivo experiments. The primary endpoint infarct size as percentage of area at risk was significantly reduced by metformin in vivo (MD -18.11[-24.09,-12.14]) and ex vivo (MD -18.70[-25.39, -12.02]). Metformin improved the secondary endpoints left ventricular ejection fraction (LVEF) and left ventricular end systolic diameter. A borderline significant effect on mortality was observed, and there was no overall effect on cardiac hypertrophy. Subgroup analyses could be performed for comorbidity and timing of treatment (infarct size and mortality) and species and duration of ischemia (LVEF), but none of these variables accounted for significant amounts of heterogeneity. Reporting of possible sources of bias was extremely poor, including randomization (reported in 63%), blinding (33%), and sample size calculation (0%). As a result, risk of bias (assessed using SYRCLE’s risk of bias tool) was unclear in the vast majority of studies. We conclude that metformin limits infarct-size and improves cardiac function in animal models of myocardial infarction, but our confidence in the evidence is lowered by the unclear risk of bias and residual unexplained heterogeneity. We recommend an adequately powered, high quality confirmatory animal study to precede a randomized controlled trial of acute administration of metformin in patients undergoing reperfusion for acute myocardial infarction. [ABSTRACT FROM AUTHOR]

Published
2017
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36. Effects of Remote Ischemic Preconditioning on Heme Oxygenase-1 Expression and Cutaneous Wound Repair.

Author

Cremers, Niels A. J., Wever, Kimberley E., Wong, Ronald J., van Rheden, René E. M., Vermeij, Eline A., van Dam, Gooitzen M., Carels, Carine E., Lundvig, Ditte M. S., and Wagener, Frank A. D. T. G.

Subjects
*WOUND healing, *HEME oxygenase, *ISCHEMIC preconditioning, *TISSUE wounds, *SKIN injuries
Abstract

Skin wounds may lead to scar formation and impaired functionality. Remote ischemic preconditioning (RIPC) can induce the anti-inflammatory enzyme heme oxygenase-1 (HO-1) and protect against tissue injury. We aim to improve cutaneous wound repair by RIPC treatment via induction of HO-1. RIPC was applied to HO-1-luc transgenic mice and HO-1 promoter activity and mRNA expression in skin and several other organs were determined in real-time. In parallel, RIPC was applied directly or 24h prior to excisional wounding in mice to investigate the early and late protective effects of RIPC on cutaneous wound repair, respectively. HO-1 promoter activity was significantly induced on the dorsal side and locally in the kidneys following RIPC treatment. Next, we investigated the origin of this RIPC-induced HO-1 promoter activity and demonstrated increased mRNA in the ligated muscle, heart and kidneys, but not in the skin. RIPC did not change HO-1 mRNA and protein levels in the wound 7 days after cutaneous injury. Both early and late RIPC did not accelerate wound closure nor affect collagen deposition. RIPC induces HO-1 expression in several organs, but not the skin, and did not improve excisional wound repair, suggesting that the skin is insensitive to RIPC-mediated protection. [ABSTRACT FROM AUTHOR]

Published
2017
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37. Repeated remote ischemic preconditioning and isoflurane anesthesia in an experimental model of renal ischemia-reperfusion injury.

Author

Menting, Theo P., Ergun, Mehmet, Bruintjes, Moira H. D., Wever, Kimberley E., Lomme, Roger M. L. M., van Goor, Harry, and Warlé, Michiel C.

Subjects
ANIMAL experimentation, HISTOLOGICAL techniques, ISCHEMIA, ISOFLURANE, KIDNEY function tests, KIDNEYS, RATS, REPERFUSION injury, RESEARCH funding, T-test (Statistics), STATISTICAL power analysis, NEPHRECTOMY, DESCRIPTIVE statistics, ISCHEMIC preconditioning
Abstract

Background: In animal studies, remote ischemic preconditioning (RIPC) and anesthetic preconditioning are successful in reducing renal ischemia reperfusion injury (IRI), however the protective effect of RIPC may be improved by repeating the RIPC stimulus. Methods: Sprague-Dawley rats underwent unilateral nephrectomy followed by 30 min of renal pedicle clamping. Animals were allocated into six groups: sham, control (IRI), RepISO (daily isoflurane anesthesia), RIPC (single dose isoflurane anesthesia and single dose RIPC), RepISO + RIPC (7-day isoflurane anesthesia and single dose RIPC) and RepISO + RepRIPC (7-day isoflurane anesthesia with 7-day RIPC). RIPC was applied by 3x5 min of cuff inflation on both thighs. Serum creatinine and urea levels were measured and histology was obtained at day two. Results: RepISO diminished renal IRI, as reflected by a significant reduction in serum creatinine levels as compared to the control group, 170 ± 74 resp. 107 ± 29 µmol/L. The other preconditioning protocols showed similar reduction in serum creatinine levels as compared to the control group. No significant differences were observed between the different preconditioning protocols. For urea levels, only RepISO + RIPC resulted in significantly lower levels as compared to the control group, 14 ± 4 resp. 22 ± 7 mmol/L (p = 0.010). In the preconditioning groups only RepISO showed less histological damage as compared to controls 1.73 ± 1.19 resp. 2.91 ± 1.22 (p = 0.032). Conclusions: In this study no additional protective effect of repeated ischemic preconditioning was observed as compared to single dose RIPC. Repeated administration of isoflurane provided stronger protection against renal IRI as compared to single dose isoflurane. [ABSTRACT FROM AUTHOR]

Published
2017
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38. Renal Perfusion and Function during Pneumoperitoneum: A Systematic Review and Meta-Analysis of Animal Studies.

Author

Wever, Kimberley E., Bruintjes, Moira H. D., Warlé, Michiel C., and Hooijmans, Carlijn R.

Subjects
*INTRA-abdominal pressure, *PNEUMOPERITONEUM, *LAPAROSCOPIC surgery, *KIDNEY failure, *ANIMAL models in research
Abstract

Both preclinical and clinical studies indicate that raised intra-abdominal pressure (IAP) associated with pneumoperitoneum during laparoscopic surgical procedures can cause renal damage, the severity of which may be influenced by variables such as pressure level and duration. Several of these variables have been investigated in animal studies, but synthesis of all preclinical data has not been performed. This systematic review summarizes all available pre-clinical evidence on this topic, including an assessment of its quality and risk of bias. We performed meta-analysis to assess which aspects of the pneumoperitoneum determine the severity of its adverse effects. A systematic search in two databases identified 55 studies on the effect of pneumoperitoneum on renal function which met our inclusion criteria. There was high heterogeneity between the studies regarding study design, species, sex, pressure and duration of pneumoperitoneum, and type of gas used. Measures to reduce bias were poorly reported, leading to an unclear risk of bias in the majority of studies. Details on randomisation, blinding and a sample size calculation were not reported in ≥80% of the studies. Meta-analysis showed an overall increase in serum creatinine during pneumoperitoneum, and a decrease in urine output and renal blood flow. Subgroup analysis indicated that for serum creatinine, this effect differed between species. Subgroup analysis of pressure level indicated that urine output decreased as IAP level increased. No differences between types of gas were observed. Data were insufficient to reliably assess whether sex or IAP duration modulate the effect of pneumoperitoneum. Four studies assessing long-term effects indicated that serum creatinine normalized ≥24 hours after desufflation of pneumoperitoneum at 15mmHg. We conclude that harmful effects on renal function and perfusion during pneumoperitoneum appear to be robust, but evidence on long-term effects is very limited. The reliability and clinical relevance of these findings for healthy patients and patients at high risk of renal impairment remain uncertain. We emphasize the need for rigorous reporting of preclinical research methodology, which is of vital importance for clinical translation of preclinical data. [ABSTRACT FROM AUTHOR]

Published
2016
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39. Preclinical Evidence for the Efficacy of Ischemic Postconditioning against Renal Ischemia-Reperfusion Injury, a Systematic Review and Meta-Analysis.

Author

Jonker, Simone J., Menting, Theo P., Warlé, Michiel C., Ritskes-Hoitinga, Merel, and Wever, Kimberley E.

Subjects
KIDNEY disease diagnosis, ISCHEMIA diagnosis, REPERFUSION injury, MEDICAL quality control, SYSTEMATIC reviews, META-analysis
Abstract

Background: Renal ischemia-reperfusion injury (IRI) is a major cause of kidney damage after e.g. renal surgery and transplantation. Ischemic postconditioning (IPoC) is a promising treatment strategy for renal IRI, but early clinical trials have not yet replicated the promising results found in animal studies. Method: We present a systematic review, quality assessment and meta-analysis of the preclinical evidence for renal IPoC, and identify factors which modify its efficacy. Results: We identified 39 publications studying >250 control animals undergoing renal IRI only and >290 animals undergoing renal IRI and IPoC. Healthy, male rats undergoing warm ischemia were used in the vast majority of studies. Four studies applied remote IPoC, all others used local IPoC. Meta-analysis showed that both local and remote IPoC ameliorated renal damage after IRI for the outcome measures serum creatinine, blood urea nitrogen and renal histology. Subgroup analysis indicated that IPoC efficacy increased with the duration of index ischemia. Measures to reduce bias were insufficiently reported. Conclusion: High efficacy of IPoC is observed in animal models, but factors pertaining to the internal and external validity of these studies may hamper the translation of IPoC to the clinical setting. The external validity of future animal studies should be increased by including females, comorbid animals, and transplantation models, in order to better inform clinical trial design. The severity of renal damage should be taken into account in the design and analysis of future clinical trials. [ABSTRACT FROM AUTHOR]

Published
2016
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40. Determinants of the Efficacy of Cardiac Ischemic Preconditioning: A Systematic Review and Meta-Analysis of Animal Studies.

Author

Wever, Kimberley E., Hooijmans, Carlijn R., Riksen, Niels P., Sterenborg, Thomas B., Sena, Emily S., Ritskes-Hoitinga, Merel, and Warlé, Michiel C.

Subjects
*CORONARY heart disease treatment, *DRUG efficacy, *SYSTEMATIC reviews, *META-analysis, *MYOCARDIAL infarction
Abstract

Background: Ischemic preconditioning (IPC) of the heart is a protective strategy in which a brief ischemic stimulus immediately before a lethal ischemic episode potently limits infarct size. Although very promising in animal models of myocardial infarction, IPC has not yet been successfully translated to benefit for patients. Objective: To appraise all preclinical evidence on IPC for myocardial infarction and identify factors hampering translation. Methods and results: Using systematic review and meta-analysis, we identified 503 animal studies reporting infarct size data from 785 comparisons between IPC-treated and control animals. Overall, IPC reduced myocardial infarction by 24.6% [95%CI 23.5, 25.6]. Subgroup analysis showed that IPC efficacy was reduced in comorbid animals and non-rodents. Efficacy was highest in studies using 2–3 IPC cycles applied <45 minutes before myocardial infarction. Local and remote IPC were equally effective. Reporting of study quality indicators was low: randomization, blinding and a sample size calculation were reported in 49%, 11% and 2% of publications, respectively. Conclusions: Translation of IPC to the clinical setting may be hampered by the observed differences between the animals used in preclinical IPC studies and the patient population, regarding comorbidity, sex and age. Furthermore, the IPC protocols currently used in clinical trials could be optimized in terms of timing and the number of ischemic cycles applied. In order to inform future clinical trials successfully, future preclinical studies on IPC should aim to maximize both internal and external validity, since poor methodological quality may limit the value of the preclinical evidence. [ABSTRACT FROM AUTHOR]

Published
2015
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42. Remote ischemic preconditioning to reduce contrast-induced nephropathy: study protocol for a randomized controlled trial.

Author

Sterenborg, Thomas B., Menting, Theo P., de Waal, Yvonne, Donders, Rogier, Wever, Kimberley E., Lemson, M. Susan, van der Vliet, Daan J. A., Wetzels, Jack F., SchultzeKool, Leo J., and Warlé, Michiel C.

Subjects
OSMOLAR concentration, KIDNEY diseases, ISCHEMIA, CLINICAL trials, ANGIOPLASTY
Abstract

Background Despite the increasing use of pre- and posthydration protocols and low-osmolar instead of high-osmolar iodine-containing contrast media, the incidence of contrast-induced nephropathy (CIN) is still significant. There is evidence that contrast media cause ischemiareperfusion injury of the medulla. Remote ischemic preconditioning (RIPC) is a noninvasive, safe, and low-cost method to reduce ischemia-reperfusion injury. Methods The RIPCIN study is a multicenter, single-blinded, randomized controlled trial in which 76 patients at risk of CIN will receive standard hydration combined with RIPC or hydration with sham preconditioning. RIPC will be applied by four cycles of 5 min ischemia and 5 min reperfusion of the forearm by inflating a blood pressure cuff at 50 mmHg above the actual systolic pressure. The primary outcome measure will be the change in serum creatinine from baseline to 48 to 72 h after contrast administration. Discussion A recent pilot study reported that RIPC reduced the incidence of CIN after coronary angioplasty. The unusual high incidence of CIN in this study is of concern and limits its generalizability. Therefore, we propose a randomized controlled trial to study whether RIPC reduces contrast-induced kidney injury in patients at risk for CIN according to the Dutch guidelines. [ABSTRACT FROM AUTHOR]

Published
2014
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43. How systemic inflammation modulates adenosine metabolism and adenosine receptor expression in humans in vivo.

Author

Ramakers, Bart P., Wever, Kimberley E., Kox, Matthijs, Den Broek, Petra H. Van, Mbuyi, Faustin, Rongen, Gerard, Masereeuw, Rosalinde, Van Der Hoeven, Johannes G., Smits, Paul, Riksen, Niels P., and Pickkers, Peter

Subjects
*ADENOSINES, *METABOLISM, *ENDOTOXEMIA, *MESSENGER RNA, *ADENOSINE deaminase, *ADENOSINE kinase
Abstract

The article explores the changes in adenosine metabolism and signaling both in vivo during experimental human endotoxemia and in vitro. Results reveal that expression of 5'ectonucleotidase messenger RNA was upregulated, while adenosine deaminase messenger RNA was downregulated. Both adenosine deaminase and adenosine kinase activity was significantly reduced. It is concluded that adenosine metabolism and signaling undergo adaptive changes during human experimental endotoxemia.

Published
2012
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44. Ischemic Preconditioning in the Animal Kidney, a Systematic Review and Meta-Analysis.

Author

Wever, Kimberley E., Menting, Theo P., Rovers, Maroeska, Van Der Vliet, J. Adam, Rongen, Gerard A., Masereeuw, Rosalinde, Ritskes-Hoitinga, Merel, Hooijmans, Carlijn R., and Warlé, Michiel

Subjects
*ISCHEMIA, *META-analysis, *REPERFUSION injury, *CREATININE, *BLOOD urea nitrogen, *KIDNEYS
Abstract

Ischemic preconditioning (IPC) is a potent renoprotective strategy which has not yet been translated successfully into clinical practice, in spite of promising results in animal studies. We performed a unique systematic review and meta-analysis of animal studies to identify factors modifying IPC efficacy in renal ischemia/reperfusion injury (IRI), in order to enhance the design of future (clinical) studies. An electronic literature search for animal studies on IPC in renal IRI yielded fifty-eight studies which met our inclusion criteria. We extracted data for serum creatinine, blood urea nitrogen and histological renal damage, as well as study quality indicators. Meta-analysis showed that IPC reduces serum creatinine (SMD 1.54 [95%CI 1.16, 1.93]), blood urea nitrogen (SMD 1.42 [95% CI 0.97, 1.87]) and histological renal damage (SMD 1.12 [95% CI 0.89, 1.35]) after IRI as compared to controls. Factors influencing IPC efficacy were the window of protection (<24 h = early vs. ≥24 h = late) and animal species (rat vs. mouse). No difference in efficacy between local and remote IPC was observed. In conclusion, our findings show that IPC effectively reduces renal damage after IRI, with higher efficacy in the late window of protection. However, there is a large gap in study data concerning the optimal window of protection, and IPC efficacy may differ per animal species. Moreover, current clinical trials on RIPC may not be optimally designed, and our findings identify a need for further standardization of animal experiments. [ABSTRACT FROM AUTHOR]

Published
2012
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46. Diannexin Protects against Renal Ischemia Reperfusion Injury and Targets Phosphatidylserines in Ischemic Tissue.

Author

Wever, Kimberley E., Wagener, Frank A. D. T. G., Frielink, Cathelijne, Boerman, Otto C., Scheffer, Gert J., Allison, Anthony, Masereeuw, Rosalinde, and Rongen, Gerard A.

Subjects
*ANNEXINS, *RENAL artery, *ISCHEMIA, *REPERFUSION injury, *PHOSPHATIDYLSERINES, *KIDNEY tubules, *PATHOLOGICAL physiology
Abstract

Renal ischemia/reperfusion injury (IRI) frequently complicates shock, renal transplantation and cardiac and aortic surgery, and has prognostic significance. The translocation of phosphatidylserines to cell surfaces is an important pro-inflammatory signal for cell-stress after IRI. We hypothesized that shielding of exposed phosphatidylserines by the annexin A5 (ANXA5) homodimer Diannexin protects against renal IRI. Protective effects of Diannexin on the kidney were studied in a mouse model of mild renal IRI. Diannexin treatment before renal IRI decreased proximal tubule damage and leukocyte influx, decreased transcription and expression of renal injury markers Neutrophil Gelatinase Associated Lipocalin and Kidney Injury Molecule-1 and improved renal function. A mouse model of ischemic hind limb exercise was used to assess Diannexin biodistribution and targeting. When comparing its biodistribution and elimination to ANXA5, Diannexin was found to have a distinct distribution pattern and longer blood half-life. Diannexin targeted specifically to the ischemic muscle and its affinity exceeded that of ANXA5. Targeting of both proteins was inhibited by pre-treatment with unlabeled ANXA5, suggesting that Diannexin targets specifically to ischemic tissues via phosphatidylserine-binding. This study emphasizes the importance of phosphatidylserine translocation in the pathophysiology of IRI. We show for the first time that Diannexin protects against renal IRI, making it a promising therapeutic tool to prevent IRI in a clinical setting. Our results indicate that Diannexin is a potential new imaging agent for the study of phosphatidylserine-exposing organs in vivo. [ABSTRACT FROM AUTHOR]

Published
2011
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47. Prenatal Amino Acid Supplementation to Improve Fetal Growth: A Systematic Review and Meta-Analysis.

Author

Terstappen, Fieke, Tol, Angela J. C., Gremmels, Hendrik, Wever, Kimberley E., Paauw, Nina D., Joles, Jaap A., M. van der Beek, Eline, and Lely, A. Titia

Abstract

Aberrant fetal growth remains a leading cause of perinatal morbidity and mortality and is associated with a risk of developing non-communicable diseases later in life. We performed a systematic review and meta-analysis combining human and animal studies to assess whether prenatal amino acid (AA) supplementation could be a promising approach to promote healthy fetal growth. PubMed, Embase, and Cochrane libraries were searched to identify studies orally supplementing the following AA groups during gestation: (1) arginine family, (2) branched chain (BCAA), and (3) methyl donors. The primary outcome was fetal/birth weight. Twenty-two human and 89 animal studies were included in the systematic review. The arginine family and, especially, arginine itself were studied the most. Our meta-analysis showed beneficial effects of arginine and (N-Carbamyl) glutamate (NCG) but not aspartic acid and citrulline on fetal/birth weight. However, no effects were reported when an isonitrogenous control diet was included. BCAA and methyl donor supplementation did not affect fetal/birth weight. Arginine family supplementation, in particular arginine and NCG, improves fetal growth in complicated pregnancies. BCAA and methyl donor supplementation do not seem to be as promising in targeting fetal growth. Well-controlled research in complicated pregnancies is needed before ruling out AA supplements or preferring arginine above other AAs. [ABSTRACT FROM AUTHOR]

Published
2020
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48. A Systematic Review on Transplantation Studies of the Retinal Pigment Epithelium in Animal Models.

Author

Koster, Céline, Wever, Kimberley E., Wagstaff, Philip E., van den Hurk, Koen T., Hooijmans, Carlijn R., and Bergen, Arthur A.

Subjects
*META-analysis, *SCANNING laser ophthalmoscopy, *PHOTORECEPTORS, *RHODOPSIN, *ANIMAL models in research, *ANIMAL pigments, *ANIMAL behavior
Abstract

The retinal pigment epithelium (RPE) and the adjacent light-sensitive photoreceptors form a single functional unit lining the back of the eye. Both cell layers are essential for normal vision. RPE degeneration is usually followed by photoreceptor degeneration and vice versa. There are currently almost no effective therapies available for RPE disorders such as Stargardt disease, specific types of retinitis pigmentosa, and age-related macular degeneration. RPE replacement for these disorders, especially in later stages of the disease, may be one of the most promising future therapies. There is, however, no consensus regarding the optimal RPE source, delivery strategy, or the optimal experimental host in which to test RPE replacement therapy. Multiple RPE sources, delivery methods, and recipient animal models have been investigated, with variable results. So far, a systematic evaluation of the (variables influencing) efficacy of experimental RPE replacement parameters is lacking. Here we investigate the effect of RPE transplantation on vision and vision-based behavior in animal models of retinal degenerated diseases. In addition, we aim to explore the effect of RPE source used for transplantation, the method of intervention, and the animal model which is used. Methods: In this study, we systematically identified all publications concerning transplantation of RPE in experimental animal models targeting the improvement of vision (e.g., outcome measurements related to the morphology or function of the eye). A variety of characteristics, such as species, gender, and age of the animals but also cell type, number of cells, and other intervention characteristics were extracted from all studies. A risk of bias analysis was performed as well. Subsequently, all references describing one of the following outcomes were analyzed in depth in this systematic review: a-, b-, and c-wave amplitudes, vision-based, thickness analyses based on optical coherence tomography (OCT) data, and transplant survival based on scanning laser ophthalmoscopy (SLO) data. Meta-analyses were performed on the a- and b-wave amplitudes from electroretinography (ERG) data as well as data from vision-based behavioral assays. Results: original research articles met the inclusion criteria after two screening rounds. Overall, most studies were categorized as unclear regarding the risk of bias, because many experimental details were poorly reported. Twenty-three studies reporting one or more of the outcome measures of interest were eligible for either descriptive (thickness analyses based on OCT data; n = 2) or meta-analyses. RPE transplantation significantly increased ERG a-wave (Hedges' g 1.181 (0.471–1.892), n = 6) and b-wave (Hedges' g 1.734 (1.295–2.172), n = 42) amplitudes and improved vision-based behavior (Hedges' g 1.018 (0.826–1.209), n = 96). Subgroup analyses revealed a significantly increased effect of the use of young and adolescent animals compared to adult animals. Moreover, transplanting more cells (in the range of 105 versus in the range of 104) resulted in a significantly increased effect on vision-based behavior as well. The origin of cells mattered as well. A significantly increased effect was found on vision-based behavior when using ARPE-19 and OpRegen® RPE. Conclusions: This systematic review shows that RPE transplantation in animal models for retinal degeneration significantly increases a- and b- wave amplitudes and improves vision-related behavior. These effects appear to be more pronounced in young animals, when the number of transplanted cells is larger and when ARPE-19 and OpRegen® RPE cells are used. We further emphasize that there is an urgent need for improving the reporting and methodological quality of animal experiments, to make such studies more comparable. [ABSTRACT FROM AUTHOR]

Published
2020
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49. The usefulness of systematic reviews of animal studies: shooting the messenger.

Author

Hooijmans, Carlijn R., Wever, Kimberley E., Ritskes ‐ Hoitinga, Merel, and Scheffer, Gert ‐ Jan

Subjects
*SYSTEMATIC reviews, *NEUROTOXICOLOGY, ANIMAL research
Abstract

A letter to the editor is presented in response to the article "What lessons for clinical practice can be learned from systematic reviews of animal studies? The case of anesthetic neurotoxicity," by A. W. Loepke and I. Vutskits in the 2016 issue is presented.

Published
2016
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