99 results on '"Raeven P"'
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2. Red blood cell transfusion-related dynamics of extracellular vesicles in intensive care patients: a prospective subanalysis
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Pierre Raeven, Katharina Karlhofer, Larissa S. Sztulman, Jonas Brugger, Konrad Hoetzenecker, Christoph Domenig, Gerda Leitner, Martin Posch, David M. Baron, and Andreas Spittler
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Medicine ,Science - Abstract
Abstract Extracellular vesicles (EVs) accumulate during packed red blood cell (PRBC) storage. To date, the involvement of EVs in transfusion-related immunomodulation (TRIM) has not been prospectively evaluated in intensive care unit (ICU) patients. This was a prospective subanalysis of a recent observational feasibility study in postoperative ICU patients after: (1) open aortic surgery (Aorta), (2) bilateral lung transplantation (LuTx), and (3) other types of surgery (Comparison). Patient plasma was collected three times each before and after leukoreduced PRBC transfusion at 30-min intervals. The total number of EVs and EVs derived from erythrocytes (EryEVs), total platelets (total PEVs), activated platelets, granulocytes (GEVs), monocytes, and myeloid cells in PRBC samples and patient plasma were analyzed by flow cytometry. Statistical analysis was performed by Spearman’s correlation test, linear mixed models and pairwise comparisons by Wilcoxon matched-pairs test. Twenty-three patients (Aorta n = 5, LuTx n = 9, Comparison n = 9) were included in the final analysis. All EV subgroups analyzed were detectable in all PRBCs samples (n = 23), but concentrations did not correlate with storage time. Moreover, all EVs analyzed were detectable in all plasma samples (n = 138), and EV counts were consistent before transfusion. Concentrations of total EVs, EryEVs, total PEVs, and GEVs increased after transfusion compared with baseline in the entire cohort but not in specific study groups. Furthermore, the change in plasma EV counts (total EVs and EryEVs) after transfusion correlated with PRBC storage time in the entire cohort. Extracellular vesicles were detectable in all PRBC and plasma samples. Individual EV subtypes increased after transfusion in the entire cohort, and in part correlated with storage duration. Future clinical studies to investigate the role of EVs in TRIM are warranted and should anticipate a larger sample size. Trial registration: Clinicaltrials.gov: NCT03782623.
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- 2024
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3. In vitro alternative for reactogenicity assessment of outer membrane vesicle based vaccines
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Molenaar-de Backer, Marijke W. A., Doodeman, Paulien, Rezai, Fereshte, Verhagen, Lisa M., van der Ark, Arno, Plagmeijer, Els M., Metz, Bernard, van Vlies, Naomi, Ophorst, Olga, and Raeven, René H. M.
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- 2023
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4. In vitro alternative for reactogenicity assessment of outer membrane vesicle based vaccines
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Marijke W. A. Molenaar-de Backer, Paulien Doodeman, Fereshte Rezai, Lisa M. Verhagen, Arno van der Ark, Els M. Plagmeijer, Bernard Metz, Naomi van Vlies, Olga Ophorst, and René H. M. Raeven
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Medicine ,Science - Abstract
Abstract Intrinsic or added immune activating molecules are key for most vaccines to provide desired immunity profiles but may increase systemic reactogenicity. Regulatory agencies require rabbit pyrogen testing (RPT) for demonstration of vaccine reactogenicity. Recently, the monocyte activation test (MAT) gained popularity as in vitro alternative, yet this assay was primarily designed to test pyrogen-free products. The aim was to adjust the MAT to enable testing of pyrogen containing vaccines in an early stage of development where no reference batch is yet available. The MAT and RPT were compared for assessing unknown safety profiles of pertussis outer membrane vesicle (OMV) vaccine candidates to those of Bexsero as surrogate reference vaccine. Pertussis OMVs with wild-type LPS predominantly activated TLR2 and TLR4 and were more reactogenic than Bexsero. However, this reactogenicity profile for pertussis OMVs could be equalized or drastically reduced compared to Bexsero or a whole-cell pertussis vaccine, respectively by dose changing, modifying the LPS, intranasal administration, or a combination of these. Importantly, except for LPS modified products, reactogenicity profiles obtained with the RPT and MAT were comparable. Overall, we demonstrated that this pertussis OMV vaccine candidate has an acceptable safety profile. Furthermore, the MAT proved its applicability to assess reactogenicity levels of pyrogen containing vaccines at multiple stages of vaccine development and could eventually replace rabbit pyrogen testing.
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- 2023
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5. Neoadjuvant immune checkpoint blockade triggers persistent and systemic Treg activation which blunts therapeutic efficacy against metastatic spread of breast tumors
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Olga S. Blomberg, Kevin Kos, Lorenzo Spagnuolo, Olga I. Isaeva, Hannah Garner, Max D. Wellenstein, Noor Bakker, Danique E.M. Duits, Kelly Kersten, Sjoerd Klarenbeek, Cheei-Sing Hau, Daphne Kaldenbach, Elisabeth A.M. Raeven, Kim Vrijland, Marleen Kok, and Karin E. de Visser
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Breast cancer metastasis ,myeloid cells ,neoadjuvant immune checkpoint blockade ,regulatory T cells ,resistance mechanisms ,Immunologic diseases. Allergy ,RC581-607 ,Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,RC254-282 - Abstract
ABSTRACTThe clinical successes of immune checkpoint blockade (ICB) in advanced cancer patients have recently spurred the clinical implementation of ICB in the neoadjuvant and perioperative setting. However, how neoadjuvant ICB therapy affects the systemic immune landscape and metastatic spread remains to be established. Tumors promote both local and systemic expansion of regulatory T cells (Tregs), which are key orchestrators of tumor-induced immunosuppression, contributing to immune evasion, tumor progression and metastasis. Tregs express inhibitory immune checkpoint molecules and thus may be unintended targets for ICB therapy counteracting its efficacy. Using ICB-refractory models of spontaneous primary and metastatic breast cancer that recapitulate the poor ICB response of breast cancer patients, we observed that combined anti-PD-1 and anti-CTLA-4 therapy inadvertently promotes proliferation and activation of Tregs in the tumor, tumor-draining lymph node and circulation. Also in breast cancer patients, Treg levels were elevated upon ICB. Depletion of Tregs during neoadjuvant ICB in tumor-bearing mice not only reshaped the intratumoral immune landscape into a state favorable for ICB response but also induced profound and persistent alterations in systemic immunity, characterized by elevated CD8+ T cells and NK cells and durable T cell activation that was maintained after treatment cessation. While depletion of Tregs in combination with neoadjuvant ICB did not inhibit primary tumor growth, it prolonged metastasis-related survival driven predominantly by CD8+ T cells. This study demonstrates that neoadjuvant ICB therapy of breast cancer can be empowered by simultaneous targeting of Tregs, extending metastasis-related survival, independent of a primary tumor response.
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- 2023
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6. Red blood cell transfusion-related eicosanoid profiles in intensive care patients—A prospective, observational feasibility study
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Pierre Raeven, Gerhard Hagn, Laura Niederstaetter, Jonas Brugger, Sophia Bayer-Blauensteiner, Christoph Domenig, Konrad Hoetzenecker, Martin Posch, Gerda Leitner, Christopher Gerner, and David M. Baron
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transfusion-related immunomodulation ,storage lesion ,transfusion ,eicosanoid ,arachidonic acid ,hydroxylated eicosatetraenoic acid ,Physiology ,QP1-981 - Abstract
Introduction: Eicosanoids are bioactive lipids present in packed red blood cells (PRBCs), and might play a role in transfusion-related immunomodulation (TRIM). We tested the feasibility of analyzing eicosanoid profiles in PRBC supernatant and in plasma samples of postoperative intensive care unit (ICU) patients transfused with one unit of PRBCs.Methods: We conducted a prospective, observational feasibility study enrolling postoperative ICU patients: 1) patients treated with acetylsalicylic acid following abdominal aortic surgery (Aorta); 2) patients on immunosuppressants after bilateral lung transplantation (LuTx); and 3) patients undergoing other types of major surgery (Comparison). Abundances of arachidonic acid (AA) and seven pre-defined eicosanoids were assessed by liquid chromatography and tandem mass spectrometry. PRBC supernatant was sampled directly from the unit immediately prior to transfusion. Spearman’s correlations between eicosanoid abundance in PRBCs and storage duration were assessed. Patient plasma was collected at 30-min intervals: Three times each before and after transfusion. To investigate temporal changes in eicosanoid abundances, we fitted linear mixed models.Results: Of 128 patients screened, 21 were included in the final analysis (Aorta n = 4, LuTx n = 8, Comparison n = 9). In total, 21 PRBC and 125 plasma samples were analyzed. Except for 20-hydroxyeicosatetraenoic acid (HETE), all analyzed eicosanoids were detectable in PRBCs, and their abundance positively correlated with storage duration of PRBCs. While 5-HETE, 12-HETE/8-HETE, 15-HETE, 20-HETE, and AA were detectable in virtually all plasma samples, 9-HETE and 11-HETE were detectable in only 57% and 23% of plasma samples, respectively.Conclusions: Recruitment of ICU patients into this transfusion study was challenging but feasible. Eicosanoid abundances increased in PRBC supernatants during storage. In plasma of ICU patients, eicosanoid abundances were ubiquitously detectable and showed limited fluctuations over time prior to transfusion. Taken together, larger clinical studies seem warranted and feasible to further investigate the role of PRBC-derived eicosanoids in TRIM.
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- 2023
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7. Barriers and enablers to physical activity behaviour in older adults during hospital stay: a qualitative study guided by the theoretical domains framework
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van Dijk - Huisman, Hanneke C., Raeven-Eijkenboom, Petra H., Magdelijns, Fabienne J. H., Sieben, Judith M., de Bie, Robert A., and Lenssen, Antoine F.
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- 2022
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8. Barriers and enablers to physical activity behaviour in older adults during hospital stay: a qualitative study guided by the theoretical domains framework
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Hanneke C. van Dijk - Huisman, Petra H. Raeven-Eijkenboom, Fabienne J. H. Magdelijns, Judith M. Sieben, Robert A. de Bie, and Antoine F. Lenssen
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Physical activity behaviour ,Hospital ,Older adults ,Barrier ,Enabler ,Theoretical domains framework ,Geriatrics ,RC952-954.6 - Abstract
Abstract Background Older adults admitted with an acute medical illness spent little time active during hospitalisation and this has been associated with negative health outcomes. Understanding which barriers and enablers influence the physical activity behaviour of hospitalised older adults is a first step towards identifying potentially modifiable factors and developing, evaluating and implementing targeted interventions aimed at increasing their physical activity behaviour. Using a theoretical framework has been found to be more successful in changing behaviour than using a non-theory driven approach. This study aimed to explore barriers and enablers to physical activity behaviour in older adults admitted to a hospital with an acute medical illness, as perceived by patients and healthcare professionals, and to categorise them using the Theoretical Domains Framework (TDF). Methods A qualitative study was conducted at a combined university and regional hospital in the Netherlands between January 2019 and February 2020. Older adults (≥70 years) admitted with an acute medical illness, and healthcare professionals (nurses, physicians, physiotherapists) were recruited using purposive sampling. Semi-structured interviews were audiotaped, transcribed and analysed using directed qualitative content analysis. Barriers and enablers to physical activity behaviour during hospitalisation were identified and coded using the TDF. Results Meaning saturation was determined after interviews with 12 patients and 16 healthcare professionals. A large number of barriers and enablers were identified and each categorised to 11 of the 14 domains of the TDF. The ‘Environmental Context and Resources’ domain in particular yielded many examples, and revealed that the hospital environment exerts an inactivating influence on patients. Conclusions The large number of identified barriers and enablers highlights the complexity of influencing older adults’ physical activity behaviour during hospitalisation. This overview of barriers and enablers to physical activity behaviour in older adults admitted to a hospital with an acute medical illness represents an initial step towards developing, evaluating and implementing theory-informed behaviour change interventions to improve hospitalised older adults’ physical activity levels. It can assist clinicians and researchers in selecting modifiable factors that can be targeted in future interventions.
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- 2022
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9. Tumor-associated macrophages promote intratumoral conversion of conventional CD4+ T cells into regulatory T cells via PD-1 signalling
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Kevin Kos, Camilla Salvagno, Max D. Wellenstein, Muhammad A. Aslam, Denize A. Meijer, Cheei-Sing Hau, Kim Vrijland, Daphne Kaldenbach, Elisabeth A.M. Raeven, Martina Schmittnaegel, Carola H. Ries, and Karin E. de Visser
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Breast cancer immunology ,regulatory T cells ,tumor-associated macrophages ,T cell plasticity ,Immunologic diseases. Allergy ,RC581-607 ,Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,RC254-282 - Abstract
While regulatory T cells (Tregs) and macrophages have been recognized as key orchestrators of cancer-associated immunosuppression, their cellular crosstalk within tumors has been poorly characterized. Here, using spontaneous models for breast cancer, we demonstrate that tumor-associated macrophages (TAMs) contribute to the intratumoral accumulation of Tregs by promoting the conversion of conventional CD4+ T cells (Tconvs) into Tregs. Mechanistically, two processes were identified that independently contribute to this process. While TAM-derived TGF-β directly promotes the conversion of CD4+ Tconvs into Tregs in vitro, we additionally show that TAMs enhance PD-1 expression on CD4+ T cells. This indirectly contributes to the intratumoral accumulation of Tregs, as loss of PD-1 on CD4+ Tconvs abrogates intratumoral conversion of adoptively transferred CD4+ Tconvs into Tregs. Combined, this study provides insights into the complex immune cell crosstalk between CD4+ T cells and TAMs in the tumor microenvironment of breast cancer, and further highlights that therapeutic exploitation of macrophages may be an attractive immune intervention to limit the accumulation of Tregs in breast tumors.
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- 2022
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10. Naturally circulating pertactin-deficient Bordetella pertussis strains induce distinct gene expression and inflammatory signatures in human dendritic cells
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Michiel M. Kroes, Alberto Miranda-Bedate, Elise S. Hovingh, Ronald Jacobi, Corrie Schot, Elder Pupo, René H. M. Raeven, Arno A. J. van der Ark, Jos P. M. van Putten, Jelle de Wit, Rob Mariman, and Elena Pinelli
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Pathogen adaptation ,pertactin ,dendritic cell ,transcriptomics ,RNAseq ,proteomics ,Infectious and parasitic diseases ,RC109-216 ,Microbiology ,QR1-502 - Abstract
Respiratory infections caused by Bordetella pertussis are reemerging despite high pertussis vaccination coverage. Since the introduction of the acellular pertussis vaccine in the late twentieth century, circulating B. pertussis strains increasingly lack expression of the vaccine component pertactin (Prn). In some countries, up to 90% of the circulating B. pertussis strains are deficient in Prn. To better understand the resurgence of pertussis, we investigated the response of human monocyte-derived dendritic cells (moDCs) to naturally circulating Prn-expressing (Prn-Pos) and Prn-deficient (Prn-Neg) B. pertussis strains from 2016 in the Netherlands. Transcriptome analysis of moDC showed enriched IFNα response-associated gene expression after exposure to Prn-Pos B. pertussis strains, whereas the Prn-Neg strains induced enriched expression of interleukin- and TNF-signaling genes, as well as other genes involved in immune activation. Multiplex immune assays confirmed enhanced proinflammatory cytokine secretion by Prn-Neg stimulated moDC. Comparison of the proteomes from the Prn-Pos and Prn-Neg strains revealed, next to the difference in Prn, differential expression of a number of other proteins including several proteins involved in metabolic processes. Our findings indicate that Prn-deficient B. pertussis strains induce a distinct and stronger immune activation of moDCs than the Prn-Pos strains. These findings highlight the role of pathogen adaptation in the resurgence of pertussis as well as the effects that vaccine pressure can have on a bacterial population.
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- 2021
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11. Thromboelastometry in patients with advanced chronic liver disease stratified by severity of portal hypertension
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Raeven, Pierre, Baron-Stefaniak, Joanna, Simbrunner, Benedikt, Stadlmann, Alexander, Schwabl, Philipp, Scheiner, Bernhard, Schaden, Eva, Eigenbauer, Ernst, Quehenberger, Peter, Mandorfer, Mattias, Baron, David Marek, and Reiberger, Thomas
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- 2020
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12. Temperature Influences the Composition and Cytotoxicity of Extracellular Vesicles in Staphylococcus aureus
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Paul Briaud, Andrew Frey, Emily C. Marino, Raeven A. Bastock, Riley E. Zielinski, Richard E. Wiemels, Rebecca A. Keogh, Erin R. Murphy, Lindsey N. Shaw, and Ronan K. Carroll
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Microbiology ,QR1-502 - Abstract
Extracellular vesicles (EVs) are lipid bilayer spheres that contain proteins, nucleic acids, and lipids secreted by bacteria. They are involved in Staphylococcus aureus
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- 2021
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13. Author’s reply to “Thromboelastometry in patients with advanced chronic liver disease: a complex interplay”
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Raeven, Pierre, Mandorfer, Mattias, Baron, David Marek, Reiberger, Thomas, and Simbrunner, Benedikt
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- 2021
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14. Genitourinary syndrome of lactation: a new perspective on postpartum and lactation-related genitourinary symptoms
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Perelmuter, Sara, Burns, Ramzy, Shearer, Katie, Grant, Raeven, Soogoor, Anantha, Jun, Soyoun, Meurer, Janine Alexis, Krapf, Jill, and Rubin, Rachel
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- 2024
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15. Health status among NEET adolescents and young adults in the United States, 2016–2018
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Raeven Faye Chandler and Alexis R. Santos Lozada
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Self-rated health ,Education/training ,Employment ,Adolescents ,NEET ,Young adults ,Public aspects of medicine ,RA1-1270 ,Social sciences (General) ,H1-99 - Abstract
Adolescents and young adults not employed or in education/training (NEET) could be at higher risk of adverse health outcomes. Approximately 4.6 million Americans aged between 16 and 24 fall in this group. However, differences in health between NEET and non-NEET population remain unaddressed. This study examines the association of NEET status and poor/fair self-reported health status (SRH), among adolescents and young adults in the United States. Data for this study come from the 2016–2018 National Survey on Drug Use and Health (NSDUH). Our analytical sample consisted of 53,690 respondents. We used logistic regression models to investigate the association between NEET and health status in the United States, while controlling for potential covariates. Approximately 14% of our analytical sample was classified as NEET. NEET report poor/fair health status at higher rates than their counterparts who remained in school and/or had a job (11.30% vs. 5.62%). The NEET population was older, had a higher proportion of non-Hispanic Blacks, engaged in more smoking but in less alcohol drinking than non-NEET. In our initial model, NEET were more likely report poor/fair SRH than their non-NEET counterparts (OR = 2.14; p
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- 2021
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16. hMRP8-ATTAC Mice: A New Model for Conditional and Reversible Neutrophil Ablation
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Danique E. M. Duits, Camilla Salvagno, Elisabeth A. M. Raeven, Kim Vrijland, Marjolein C. Stip, Cheei-Sing Hau, Daphne Kaldenbach, and Karin E. de Visser
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neutrophils ,neutrophil depletion ,novel transgenic mouse model ,in vivo neutrophil targeting ,cancer ,Cytology ,QH573-671 - Abstract
Neutrophils are not only crucial immune cells for the neutralization of pathogens during infections, but they are also key players in tissue repair and cancer. Several methods are available to investigate the in vivo role of neutrophils in these conditions, including the depletion of neutrophils with neutralizing antibodies against Ly6G, or the blockade of neutrophil recruitment with CXCR2 inhibitors. A limited number of transgenic mouse models were generated that rely on the disruption of genes important for neutrophil development or on the injection of diphtheria toxin to induce neutrophil ablation. However, these methods have various limitations, including a lack of neutrophil specificity, a lack of long-term efficacy, or a lack of the ability to conditionally deplete neutrophils. Therefore, we generated a transgenic mouse model for the inducible and reversible ablation of neutrophils using the ATTAC (Apoptosis Through Targeted Activation of Caspase 8) approach. With the ATTAC strategy, which relies on the expression of the caspase 8-FKBP fusion protein, apoptosis is induced upon administration of a chemical dimerizer (FK506 analogue) that facilitates the dimerization and activation of caspase 8. In order to achieve specific neutrophil depletion, we cloned the ATTAC construct under the human migration inhibitory factor-related protein 8 (hMRP8) promotor. The newly generated hMRP8-ATTAC mice expressed high levels of the transgene in neutrophils, and, as a consequence, dimerizer injection induced an efficient reduction of neutrophil levels in all the organs analyzed under homeostatic conditions. In situations with extensive pressure on the bone marrow to mobilize neutrophils, for instance in the context of cancer, effective neutrophil depletion in this model requires further optimization. In conclusion, we here describe the generation and characterization of a new transgenic model for conditional neutrophil ablation and highlight the need to improve the ATTAC strategy for the depletion of large numbers of rapidly generated short-lived cells, such as neutrophils.
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- 2022
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17. Lack of Cell Cycle Inhibitor p21 and Low CD4+ T Cell Suppression in Newborns After Exposure to IFN-β
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Jop Jans, Wendy W. Unger, Elisabeth A. M. Raeven, Elles R. Simonetti, Marc J. Eleveld, Ronald de Groot, Marien I. de Jonge, and Gerben Ferwerda
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interferon beta ,respiratory syncytial virus ,newborns ,immunity ,CD4 T cells ,proliferation ,Immunologic diseases. Allergy ,RC581-607 - Abstract
Type I IFNs, such as interferon alpha and interferon beta, are key regulators of the adaptive immune response during infectious diseases. Type I IFNs are induced upon infection, bind interferon α/β receptors on T-cells and activate intracellular pathways. The activating and inhibitory consequences of type I IFN-signaling are determined by cell type and cellular environment. The neonatal immune system is associated with increased vulnerability to infectious diseases which could partly be explained by an immature CD4+ T-cell compartment. Here, we show low IFN-β-mediated inhibition of CD4+ T-cell proliferation, phosphorylation of retinoblastoma protein and cytokine production in human newborns compared to adults. In addition, both naïve and total newborn CD4+ T-cells are unable to induce the cell-cycle inhibitor p21 upon exposure to IFN-β in contrast to adults. The distinct IFN-β-signaling in newborns provides novel insights into T cell functionality and regulation of T cell-dependent inflammation during early life immune responses.
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- 2021
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18. Staphylococcus aureus Responds to Physiologically Relevant Temperature Changes by Altering Its Global Transcript and Protein Profile
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Raeven A. Bastock, Emily C. Marino, Richard E. Wiemels, Donald L. Holzschu, Rebecca A. Keogh, Rachel L. Zapf, Erin R. Murphy, and Ronan K. Carroll
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Microbiology ,QR1-502 - Abstract
Enteric bacterial pathogens, like Escherichia coliStaphylococcus aureus
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- 2021
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19. Intranasal immunization with outer membrane vesicle pertussis vaccine confers broad protection through mucosal IgA and Th17 responses
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Raeven, René H. M., Rockx-Brouwer, Dedeke, Kanojia, Gaurav, van der Maas, Larissa, Bindels, Tim H. E., ten Have, Rimko, van Riet, Elly, Metz, Bernard, and Kersten, Gideon F. A.
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- 2020
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20. Racial/Ethnic Differences in Use of Health Care Services for Diabetes Management
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Chandler, Raeven Faye and Monnat, Shannon M.
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Research demonstrates consistent racial/ethnic disparities in access to and use of health care services for a variety of chronic conditions. Yet we know little about whether these disparities exist for use of health care services for diabetes management. Racial/ethnic minorities disproportionately suffer from diabetes, complications from diabetes, and diabetes-related mortality. Proper diabetes management can reduce the risk of complications and premature mortality. Using a large national data set (N = 37,705) of White, Black, Hispanic, Asian, and Native American U.S. adults aged 65 years and older who have been diagnosed with diabetes, we examine three specific types of health care provider (HCP) use for diabetes management: number of times seen by a health care professional for diabetes, number of times feet have been checked by a health care professional, and number of visits for a glycosylated hemoglobin check. We found that net of controls for a variety of demographic and socioeconomic characteristics, Blacks and Hispanics had significantly more visits to a HCP for their diabetes and significantly more glycosylated hemoglobin checks than Whites, and Blacks and Native Americans had significantly more HCP feet checks than Whites. Our results suggest that the reduced access to health care services traditionally found among racial/ethnic minorities does not hold for access to health care services for diabetes management, where racial/ethnic minority diabetics are actually more likely to use care than are White diabetics. Future research should examine whether higher use of health care services for diabetes among racial/ethnic minorities is due to greater disease severity among racial/ethnic minorities than among non-Hispanic Whites.
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- 2015
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21. Antibody Specificity Following a Recent Bordetella pertussis Infection in Adolescence Is Correlated With the Pertussis Vaccine Received in Childhood
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René H. M. Raeven, Larissa van der Maas, Jeroen L. A. Pennings, Kurt Fuursted, Charlotte Sværke Jørgensen, Elly van Riet, Bernard Metz, Gideon F. A. Kersten, and Tine Dalby
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Bordetella pertussis ,vaccination ,acellular pertussis vaccine ,whole-cell pertussis vaccine ,2-dimensional electrophoresis (2DE) ,antibody specificity ,Immunologic diseases. Allergy ,RC581-607 - Abstract
Bordetella (B.) pertussis resurgence affects not only the unvaccinated, but also the vaccinated population. Different vaccines are available, however, it is currently unknown whether the type of childhood vaccination has an influence on antibody responses following a B. pertussis infection later in life. Therefore, the study aim was to profile serum antibody responses in young adults with suspected B. pertussis infections, immunized during childhood with either whole-cell (wPV) or monocomponent acellular pertussis (aPV) vaccines. Serum anti-pertussis toxin (PTx) IgG antibody levels served as an indicator for a recent B. pertussis infection. Leftover sera from a diagnostic laboratory from 36 Danish individuals were included and divided into four groups based on immunization background (aPV vs. wPV) and serum anti-PTx IgG levels (– vs. +). Pertussis-specific IgG/IgA antibody levels and antigen specificity were determined by using multiplex immunoassays (MIA), one- and two-dimensional immunoblotting (1 & 2DEWB), and mass spectrometry. Besides enhanced anti-PTx levels, wPV(+) and aPV(+) groups showed increased IgG and IgA levels against pertactin, filamentous hemagglutinin, fimbriae 2/3, and pertussis outer membrane vesicles (OMV). In the wPV(–) and aPV(–) groups, only low levels of anti-OMV antibodies were detected. 1DEWB demonstrated that antibody patterns differed between groups but also between individuals with the same immunization background and anti-PTx levels. 2DWB analysis for serum IgG revealed 133 immunogenic antigens of which 40 were significantly different between groups allowing to differentiate wPV(+) and aPV(+) groups. Similarly, for serum IgA, 7 of 47 immunogenic protein spots were significantly different. This study demonstrated that B. pertussis infection-induced antibody responses were distinct on antigen level between individuals with either wPV or aPV immunization background. Importantly, only 2DEWB and not MIA could detect these differences indicating the potential of this method. Moreover, in individuals immunized with an aPV containing only PTx in childhood, the infection-induced antibody responses were not limited to PTx alone.
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- 2019
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22. An unconventional RNA-based thermosensor within the 5' UTR of Staphylococcus aureus cidA.
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Hebaallaha Hussein, Megan E Fris, Ahmed H Salem, Richard E Wiemels, Raeven A Bastock, Francesco Righetti, Caleb A Burke, Franz Narberhaus, Ronan K Carroll, Nahla S Hassan, Saleh A Mohamed, Afaf S Fahmy, and Erin R Murphy
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Medicine ,Science - Abstract
Staphylococcus aureus is a Gram-positive bacterial pathogen of global concern and a leading cause of bacterial infections worldwide. Asymptomatic carriage of S. aureus on the skin and in the anterior nares is common and recognized as a predisposing factor to invasive infection. Transition of S. aureus from the carriage state to that of invasive infection is often accompanied by a temperature upshift from approximately 33°C to 37°C. Such a temperature shift is known in other pathogens to influence gene expression, often resulting in increased production of factors that promote survival or virulence within the host. One mechanism by which bacteria modulate gene expression in response to temperature is by the regulatory activity of RNA-based thermosensors, cis-acting riboregulators that control translation efficiency. This study was designed to identify and characterize RNA-based thermosensors in S. aureus. Initially predicted by in silico analyses of the S. aureus USA300 genome, reporter-based gene expression analyses and site-specific mutagenesis were performed to demonstrate the presence of a functional thermosensor within the 5' UTR of cidA, a gene implicated in biofilm formation and survival of the pathogen. The nucleic sequence composing the identified thermosensor are sufficient to confer temperature-dependent post-transcriptional regulation, and activity is predictably altered by the introduction of site-specific mutations designed to stabilize or destabilize the structure within the identified thermosensor. The identified regulator is functional in both the native bacterial host S. aureus and in the distally related species Escherichia coli, suggesting that its regulatory activity is independent of host-specific factors. Interestingly, unlike the majority of bacterial RNA-based thermosensors characterized to date, the cidA thermosensor facilitates increased target gene expression at lower temperatures. In addition to the characterization of the first RNA-based thermosensor in the significant pathogen S. aureus, it highlights the diversity of function within this important class of ribo-regulators.
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- 2019
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23. The Role of Virulence Proteins in Protection Conferred by Bordetella pertussis Outer Membrane Vesicle Vaccines
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René H. M. Raeven, Naomi van Vlies, Merijn L. M. Salverda, Larissa van der Maas, Joost P. Uittenbogaard, Tim H. E. Bindels, Jolanda Rigters, Lisa M. Verhagen, Sabine Kruijer, Elly van Riet, Bernard Metz, and Arno A. J. van der Ark
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Bordetella pertussis ,virulence factors ,pertussis vaccine ,OMV ,outer membrane vesicles ,bvg ,Medicine - Abstract
The limited protective immunity induced by acellular pertussis vaccines demands development of novel vaccines that induce broader and longer-lived immunity. In this study, we investigated the protective capacity of outer membrane vesicle pertussis vaccines (omvPV) with different antigenic composition in mice to gain insight into which antigens contribute to protection. We showed that total depletion of virulence factors (bvg(-) mode) in omvPV led to diminished protection despite the presence of high antibody levels. Antibody profiling revealed overlap in humoral responses induced by vaccines in bvg(-) and bvg(+) mode, but the potentially protective responses in the bvg(+) vaccine were mainly directed against virulence-associated outer membrane proteins (virOMPs) such as BrkA and Vag8. However, deletion of either BrkA or Vag8 in our outer membrane vesicle vaccines did not affect the level of protection. In addition, the vaccine-induced immunity profile, which encompasses broad antibody and mixed T-helper 1, 2 and 17 responses, was not changed. We conclude that the presence of multiple virOMPs in omvPV is crucial for protection against Bordetella pertussis. This protective immunity does not depend on individual proteins, as their absence or low abundance can be compensated for by other virOMPs.
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- 2020
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24. Systemic inhibition and liver‐specific over‐expression of PAI‐1 failed to improve survival in all‐inclusive populations or homogenous cohorts of CLP mice
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Raeven, P., Drechsler, S., Weixelbaumer, K.M., Bastelica, D., Peiretti, F., Klotz, A., Jafarmadar, M., Redl, H., Bahrami, S., Alessi, M.C., Declerck, P.J., and Osuchowski, M.F.
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- 2014
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25. Meta-Analysis of Pulmonary Transcriptomes from Differently Primed Mice Identifies Molecular Signatures to Differentiate Immune Responses following Bordetella pertussis Challenge
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René H. M. Raeven, Jeroen L. A. Pennings, Elly van Riet, Gideon F. A. Kersten, and Bernard Metz
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Immunologic diseases. Allergy ,RC581-607 - Abstract
Respiratory infection with Bordetella pertussis leads to severe effects in the lungs. The resulting immunity and also immunization with pertussis vaccines protect against disease, but the induced type of immunity and longevity of the response are distinct. In this study the effects of priming, by either vaccination or infection, on a subsequent pathogen encounter were studied. To that end, three postchallenge transcriptome datasets of previously primed mice were combined and compared to the responses in unprimed control mice. In total, 205 genes showed different transcription activity. A coexpression network analysis assembled these genes into 27 clusters, combined into six groups with overlapping biological function. Local pulmonary immunity was only present in mice with infection-induced immunity. Complement-mediated responses were more prominent in mice immunized with an outer membrane vesicle pertussis vaccine than in mice that received a whole-cell pertussis vaccine. Additionally, 46 genes encoding for secreted proteins may serve as markers in blood for the degree of protection (Cxcl9, Gp2, and Pla2g2d), intensity of infection (Retnla, Saa3, Il6, and Il1b), or adaptive recall responses (Ighg, C1qb). The molecular signatures elucidated in this study contribute to better understanding of functional interactions in challenge-induced responses in relation to pertussis immunity.
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- 2017
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26. Why do they die? Comparison of selected aspects of organ injury and dysfunction in mice surviving and dying in acute abdominal sepsis
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Drechsler, Susanne, Weixelbaumer, Katrin M, Weidinger, Adelheid, Raeven, Pierre, Khadem, Anna, Redl, Heinz, van Griensven, Martijn, Bahrami, Soheyl, Remick, Daniel, Kozlov, Andrey, and Osuchowski, Marcin F
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- 2015
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27. Weight Status of Persons with Intellectual Disabilities
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Maaskant, Marian A., van Knijff-Raeven, Ankie G. M., van Schrojenstein Lantman-de Valk, Henny M. J., and Veenstra, Marja Y.
- Abstract
Background: The aim was to study the weight and weight status of the study group in 2002 and 2007, and to study the differences in weight and weight status between 2002 and 2007 and the risk groups for (becoming) overweight/obese. Materials and Methods: The Body Mass Index (BMI) of 336 clients of a Dutch service provider for persons with intellectual disabilities was calculated in 2002 and 2007. Results: The mean increase in BMI between 2002 and 2007 was 0.8 (2.2 kg). In 2002, 36% of the study group was overweight/obese; this was higher in 2007: 45%. The expected relationship between increase in BMI and the change in living circumstances could not be confirmed. Conclusions: Further research into health-control programmes, weight status, food-intake and physical exercise is recommended.
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- 2009
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28. Weighting the Weights: Agreement among Anthropometric Indicators Identifying the Weight Status of People with Intellectual Disabilities
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Verstraelen, C. J. F., Maaskant, M. A., and van Knijff-Raeven, A. G. M.
- Abstract
Background: The aims of this study were (1) to determine to what extent body mass index (BMI), waist circumference, fat free mass index (FFMI) and skinfold thickness are feasible measurement options in people with intellectual disabilities (ID) to measure their weight status, and (2) to assess the level of agreement among these methods. Methods: BMI, waist circumference, FFMI derived from the Bioelectrical Impedance Analyser and skinfold thickness were all determined in 76 people with intellectual disabilities. Results: BMI and waist circumference could be measured in all subjects. Skinfold thickness and FFMI failed in, respectively, five and 14 people. In general, intertest reliabilities were low. For underweight people, the agreement was acceptable. Conclusions: BMI and waist circumference were feasible measurement options. Agreements among the methods were low. Implications of these results are discussed.
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- 2009
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29. Immunological Signatures after Bordetella pertussis Infection Demonstrate Importance of Pulmonary Innate Immune Cells.
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René H M Raeven, Jolanda Brummelman, Larissa van der Maas, Wichard Tilstra, Jeroen L A Pennings, Wanda G H Han, Cécile A C M van Els, Elly van Riet, Gideon F A Kersten, and Bernard Metz
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Medicine ,Science - Abstract
Effective immunity against Bordetella pertussis is currently under discussion following the stacking evidence of pertussis resurgence in the vaccinated population. Natural immunity is more effective than vaccine-induced immunity indicating that knowledge on infection-induced responses may contribute to improve vaccination strategies. We applied a systems biology approach comprising microarray, flow cytometry and multiplex immunoassays to unravel the molecular and cellular signatures in unprotected mice and protected mice with infection-induced immunity, around a B. pertussis challenge. Pre-existing systemic memory Th1/Th17 cells, memory B-cells, and mucosal IgA specific for Ptx, Vag8, Fim2/3 were detected in the protected mice 56 days after an experimental infection. In addition, pre-existing high activity and reactivation of pulmonary innate cells such as alveolar macrophages, M-cells and goblet cells was detected. The pro-inflammatory responses in the lungs and serum, and neutrophil recruitment in the spleen upon an infectious challenge of unprotected mice were absent in protected mice. Instead, fast pulmonary immune responses in protected mice led to efficient bacterial clearance and harbored potential new gene markers that contribute to immunity against B. pertussis. These responses comprised of innate makers, such as Clca3, Retlna, Glycam1, Gp2, and Umod, next to adaptive markers, such as CCR6+ B-cells, CCR6+ Th17 cells and CXCR6+ T-cells as demonstrated by transcriptome analysis. In conclusion, besides effective Th1/Th17 and mucosal IgA responses, the primary infection-induced immunity benefits from activation of pulmonary resident innate immune cells, achieved by local pathogen-recognition. These molecular signatures of primary infection-induced immunity provided potential markers to improve vaccine-induced immunity against B. pertussis.
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- 2016
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30. Erratum: Molecular and cellular signatures underlying superior immunity against Bordetella pertussis upon pulmonary vaccination
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Raeven, R H M, Brummelman, J, Pennings, J L A, van der Maas, L, Helm, K, Tilstra, W, van der Ark, A, Sloots, A, van der Ley, P, van Eden, W, Jiskoot, W, van Riet, E, van Els, C A C M, Kersten, G F A, Han, W G H, and Metz, B
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- 2018
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31. Molecular signatures of the evolving immune response in mice following a Bordetella pertussis infection.
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René H M Raeven, Jolanda Brummelman, Jeroen L A Pennings, Olaf E M Nijst, Betsy Kuipers, Laura E R Blok, Kina Helm, Elly van Riet, Wim Jiskoot, Cecile A C M van Els, Wanda G H Han, Gideon F A Kersten, and Bernard Metz
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Medicine ,Science - Abstract
Worldwide resurgence of pertussis necessitates the need for improvement of pertussis vaccines and vaccination strategies. Since natural infections induce a longer-lasting immunity than vaccinations, detailed knowledge of the immune responses following natural infection can provide important clues for such improvement. The purpose was to elucidate the kinetics of the protective immune response evolving after experimental Bordetella pertussis (B. pertussis) infection in mice. Data were collected from (i) individual analyses, i.e. microarray, flow cytometry, multiplex immunoassays, and bacterial clearance; (ii) twelve time points during the infection; and (iii) different tissues involved in the immune responses, i.e. lungs, spleen and blood. Combined data revealed detailed insight in molecular and cellular sequence of events connecting different phases (innate, bridging and adaptive) of the immune response following the infection. We detected a prolonged acute phase response, broad pathogen recognition, and early gene signatures of subsequent T-cell recruitment in the lungs. Activation of particular transcription factors and specific cell markers provided insight into the time course of the transition from innate towards adaptive immune responses, which resulted in a broad spectrum of systemic antibody subclasses and splenic Th1/Th17 memory cells against B. pertussis. In addition, signatures preceding the local generation of Th1 and Th17 cells as well as IgA in the lungs, considered key elements in protection against B. pertussis, were established. In conclusion, molecular and cellular immunological processes in response to live B. pertussis infection were unraveled, which may provide guidance in selecting new vaccine candidates that should evoke local and prolonged protective immune responses.
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- 2014
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32. Overeenstemming tussen antropometrische methoden voor de bepaling van de gewichtsstatus
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Everink, I., Maaskant, M. A., van Knijff-Raeven, A. G. M., van Valk, H. M. J. Schrojenstein Lantman-de, and Buntinx, W. H. E.
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- 2010
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33. A non-lethal traumatic/hemorrhagic insult strongly modulates the compartment-specific PAI-1 response in the subsequent polymicrobial sepsis.
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Pierre Raeven, Alma Salibasic, Susanne Drechsler, Katrin Maria Weixelbaumer, Mohammad Jafarmadar, Martijn van Griensven, Soheyl Bahrami, and Marcin Filip Osuchowski
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Medicine ,Science - Abstract
IntroductionPlasminogen activator inhibitor 1 (PAI-1) is a key factor in trauma- and sepsis-induced coagulopathy. We examined how trauma-hemorrhage (TH) modulates PAI-1 responses in subsequent cecal ligation and puncture (CLP)-induced sepsis, and the association of PAI-1 with septic outcomes.MethodsMice underwent TH and CLP 48 h later in three separate experiments. In experiment 1, mice were sacrificed pre- and post-CLP to characterize the trajectory of PAI-1 in plasma (protein) and tissues (mRNA). Post-CLP dynamics in TH-CLP (this study) and CLP-Only mice (prior study) were then compared for modulatory effects of TH. In experiment 2, to relate PAI-1 changes to outcome, mice underwent TH-CLP and were sampled daily and followed for 14 days to compare non-survivors (DEAD) and survivors (SUR). In experiment 3, plasma and tissue PAI-1 expression were compared between mice predicted to die (P-DIE) and to live (P-LIVE).ResultsIn experiment 1, an early post-TH rise of circulating PAI-1 was contrasted by a delayed (post-TH) decrease of PAI-1 mRNA in organs. In the post-CLP phase, profiles of circulating PAI-1 were similar between TH-CLP and CLP-Only mice. Conversely, PAI-1 mRNA declined in the liver and heart of TH-CLP mice versus CLP-Only. In experiment 2, there were no DEAD/SUR differences in circulating PAI-1 prior to CLP. Post-CLP, circulating PAI-1 in DEAD was 2-4-fold higher than in SUR. PAI-1 increase heralded septic deaths up to 48 h prior but DEAD/SUR thrombomodulin (endothelial injury marker) levels were identical. In experiment 3, levels of circulating PAI-1 and its hepatic gene expression were higher in P-DIE versus P-LIVE mice and those increases closely correlated with liver dysfunction.ConclusionsTrauma modulated septic PAI-1 responses in a compartment-specific fashion. Only post-CLP increases in circulating PAI-1 predicted septic outcomes. In posttraumatic sepsis, pre-lethal release of PAI-1 was mostly of hepatic origin and was independent of endothelial injury.
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- 2013
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34. Knelpunten bij de uitvoering van palliatieve sedatie: Een praktische kaart met aandachtspunten voor de hulpverlener
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de Kinkelder, Adriaan, Broes, Mirjam, Raeven, Mick, Kimenai, Irmgard, and Schols, Jos
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- 2007
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35. Relationship between age/gender-induced survival changes and the magnitude of inflammatory activation and organ dysfunction in post-traumatic sepsis.
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Susanne Drechsler, Katrin Weixelbaumer, Pierre Raeven, Mohammad Jafarmadar, Anna Khadem, Martijn van Griensven, Soheyl Bahrami, and Marcin Filip Osuchowski
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Medicine ,Science - Abstract
Age/gender may likely influence the course of septic complications after trauma. We aimed to characterize the influence of age/gender on the response of circulating cytokines, cells and organ function in post-traumatic sepsis. We additionally tested whether post-traumatic responses alone can accurately predict outcomes in subsequent post-traumatic sepsis. A mouse 2-hit model of trauma/hemorrhage (TH, 1(st) hit) and cecal ligation and puncture (CLP, 2(nd) hit) was employed. 3, 15 and 20 month (m) old female (♀) and male (♂) CD-1 mice underwent sublethal TH followed by CLP 2 days later. Blood was sampled daily until day 6 post-TH and survival was followed for 16 days. To compare general response patterns among groups, we calculated two scores: the inflammatory response (including KC, MIP-1α, TNFα, MCP-1, IFNγ, IL-1β,-5,-6,-10) and the organ dysfunction score (Urea, ALT, AST and LDH). Moreover, mice were retrospectively divided into survivors (SUR) and dying (DIE) based on post-CLP outcome. In general, females survived better than males and their survival did not correspond to any specific estrus cycle phase. Pre-CLP phase: the post-TH inflammatory score was weakest in 3 m♂ but there were no changes among remaining groups (similar lack of differences in the organ dysfunction score). TH induced a 40% increase of IFNγ, MIP-1α and IL-5 in 15 m♂ SUR (vs. DIE) but predictive accuracy for post-CLP outcomes was moderate. Post-CLP phase: while stable in males, inflammatory response score in 15 m and 20 m females decreased with age at day 1 and 2 post-CLP. SUR vs. DIE differences in inflammatory and organ dysfunction score were evident but their magnitude was comparable across age/gender. Nearly identical activation of the humoral inflammatory and organ function compartments, both across groups and according to sepsis severity, suggests that they are not directly responsible for the age/gender-dependent disparity in TH-CLP survival in the studied young-to-mature population.
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- 2012
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36. Ruimte voor ondernemerschap en innovatie : Advies Taskforce Versnelling Innovatieproces Stalsystemen
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Thijssen, R., Ven, C. van de, Peet, G. van der, Bruinsma, T., Groot, J. de, Polinder, L., Kort, M., Amelsvoort, M. van, Stouthart, F., Kok, P., Hanskamp, H., Lent, J. van, Bergen, J. van, Boerman, J.K., Pieterse, X., Heerink, G., Monteny, G.J., Nijdam, E., Kager, H., Broeze, T., Hendrix, L., Coppens, R., Raeven, P., Eeden, N. van, Zuidema, C., Sütterlin, S., Plu, D., Thijssen, R., Ven, C. van de, Peet, G. van der, Bruinsma, T., Groot, J. de, Polinder, L., Kort, M., Amelsvoort, M. van, Stouthart, F., Kok, P., Hanskamp, H., Lent, J. van, Bergen, J. van, Boerman, J.K., Pieterse, X., Heerink, G., Monteny, G.J., Nijdam, E., Kager, H., Broeze, T., Hendrix, L., Coppens, R., Raeven, P., Eeden, N. van, Zuidema, C., Sütterlin, S., and Plu, D.
- Abstract
Om de veehouderij verder te verduurzamen, om verspilling van waardevolle nutriënten te voorkomen en efficiëntie te verhogen, en om de noodzakelijke bijdrage aan maatschappelijke opgaves te kunnen leveren, is het belangrijk dat er met grote snelheid nieuwe veehouderij-oplossingen en innovatieve stallen worden ontwikkeld en in de praktijk geïmplementeerd. Er is geen discussie over de stip aan de horizon: integraal duurzame, laag emitterende bedrijfs- en stalsystemen, met aandacht voor diergezondheid en dierenwelzijn, zullen de nieuwe standaard worden. Dit betekent dat het noodzakelijk is dat er versneld innovatie op gang komt om tot deze nieuwe veehouderij-oplossingen en stallen te komen.
- Published
- 2020
37. Fully integrated L-phenylalanine separation and concentration using reactive-extraction with liquid-liquid centrifuges in a fed-batch process with E. coli
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Rüffer, N., Heidersdorf, U., Kretzers, I., Sprenger, G. A., Raeven, L., and Takors, R.
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- 2004
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38. Multiplicity distributions and charged-neutral fluctuations
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Nayak, Tapan K, Aggarwal, MM, Agnihotri, A, Ahammed, Z, Angelis, ALS, Antonenko, V, Arefiev, V, Astakhov, V, Avdeitchikov, V, Awes, TC, Baba, PVKS, Badyal, SK, Baldine, A, Barabach, L, Barlag, C, Bathe, S, Batiounia, B, Bernier, T, Bhalla, KB, Bhatia, VS, Blume, C, Bock, R, Bohne, E-M, Bucher, D, Buijs, A, Buis, E-J, Büsching, H, Carlen, L, Chalyshev, V, Chattopadhyay, S, Chenawi, KE, Cherbatchev, R, Chujo, T, Claussen, A, Das, AC, Decowski, MP, Djordjadze, V, Donni, P, Doubovik, I, Dubey, AK, Dutta Majumdar, MR, Eliseev, S, Enosawa, K, Feldmann, H, Foka, P, Fokin, S, Frolov, V, Ganti, MS, Garpman, S, Gavrishchuk, O, Geurts, FJM, Ghosh, TK, Glasow, R, Gupta, SK, Guskov, B, Gustafsson, HA, Gutbrod, HH, Higuchi, R, Hrivanacova, I, Ippolitov, M, Kalechofsky, H, Kamermans, R, Kampert, K-H, Karadjev, K, Karpio, K, Kato, S, Kees, S, Kim, H, Kolb, BW, Kosarev, I, Koutcheryaev, I, Kugler, A, Kulinich, P, Kumar, V, Kurata, M, Kurita, K, Kuzmin, N, Langbein, I, Lebedev, A, Lee, YY, Löhner, H, Mahapatra, DP, Manko, V, Martin, M, Maximov, A, Mehdiyev, R, Mgebrichvili, G, Miake, Y, Mikhalev, D, Mishra, GC, Miyamoto, Y, Mohanty, B, Morrison, D, Mukhopadhyay, DS, Myalkovski, V, Naef, H, Nandi, BK, Nayak, SK, Nayak, TK, Neumaier, S, Nianine, A, Nikitine, V, Nikolaev, S, Nishimura, S, Nomokov, P, Nystrand, J, Obenshain, FE, Oskarsson, A, Otterlund, I, Pachr, M, Parfenov, A, Pavliouk, S, Peitzmann, T, Petracek, V, Plasil, F, Purschke, ML, Raeven, B, Rak, J, Raniwala, R, Raniwala, S, Ramamurthy, VS, Rao, NK, Retiere, F, Reygers, K, Roland, G, Rosselet, L, Roufanov, I, Rubio, JM, Sambyal, SS, Santo, R, Sato, S, Schlagheck, H, Schmidt, H-R, Shabratova, G, Sibiriak, I, Siemiarczuk, T, Sinha, BC, Slavine, N, Söderström, K, Solomey, N, Sood, G, Sørensen, SP, Stankus, P, Stefanek, G, Steinberg, P, Stenlund, E, Stüken, D, Sumbera, M, Svensson, T, Trivedi, MD, Tsvetkov, A, Twenhöfel, C, Tykarski, L, Urbahn, J, Eijndhoven, NV, Heeringen, WHV, Nieuwenhuizen, GJV, Vinogradov, A, Viyogi, YP, Vodopianov, A, Vörös, S, Vos, MA, Wyslouch, B, Yagi, K, Yokota, Y, and Young, GR
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- 2001
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39. Homogeneity versus diversity: inhibition of plasma PAI-1 in murine sepsis proved lethal in homogeneous cohorts but not in all-inclusive populations
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Raeven, P, Weixelbaumer, KM, Drechsler, S, Klotz, A, Jafarmadar, M, Khadem, A, Redl, H, Bahrami, S, Declerck, PJ, and Osuchowski, MF
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- 2012
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40. Neoadjuvant immune checkpoint blockade triggers persistent and systemic Tregactivation which blunts therapeutic efficacy against metastatic spread of breast tumors
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Blomberg, Olga S., Kos, Kevin, Spagnuolo, Lorenzo, Isaeva, Olga I., Garner, Hannah, Wellenstein, Max D., Bakker, Noor, Duits, Danique E.M., Kersten, Kelly, Klarenbeek, Sjoerd, Hau, Cheei-Sing, Kaldenbach, Daphne, Raeven, Elisabeth A.M., Vrijland, Kim, Kok, Marleen, and de Visser, Karin E.
- Abstract
ABSTRACTThe clinical successes of immune checkpoint blockade (ICB) in advanced cancer patients have recently spurred the clinical implementation of ICB in the neoadjuvant and perioperative setting. However, how neoadjuvant ICB therapy affects the systemic immune landscape and metastatic spread remains to be established. Tumors promote both local and systemic expansion of regulatory T cells (Tregs), which are key orchestrators of tumor-induced immunosuppression, contributing to immune evasion, tumor progression and metastasis. Tregsexpress inhibitory immune checkpoint molecules and thus may be unintended targets for ICB therapy counteracting its efficacy. Using ICB-refractory models of spontaneous primary and metastatic breast cancer that recapitulate the poor ICB response of breast cancer patients, we observed that combined anti-PD-1 and anti-CTLA-4 therapy inadvertently promotes proliferation and activation of Tregsin the tumor, tumor-draining lymph node and circulation. Also in breast cancer patients, Treglevels were elevated upon ICB. Depletion of Tregsduring neoadjuvant ICB in tumor-bearing mice not only reshaped the intratumoral immune landscape into a state favorable for ICB response but also induced profound and persistent alterations in systemic immunity, characterized by elevated CD8+ T cells and NK cells and durable T cell activation that was maintained after treatment cessation. While depletion of Tregsin combination with neoadjuvant ICB did not inhibit primary tumor growth, it prolonged metastasis-related survival driven predominantly by CD8+ T cells. This study demonstrates that neoadjuvant ICB therapy of breast cancer can be empowered by simultaneous targeting of Tregs,extending metastasis-related survival, independent of a primary tumor response.
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- 2023
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41. Multiply-Binding Polymeric Imidazole Ligands: Influence of Molecular Weight and Monomer Sequence on Colloidal Quantum Dot Stability
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Dunlap, John H., Loszko, Abigail F., Flake, Raeven A., Huang, Yucheng, Benicewicz, Brian C., and Greytak, Andrew B.
- Abstract
This study addresses the colloidal stability of polymer-coated core/shell CdSe/CdxZn1–xS quantum dots (QDs) in the presence of l-glutathione (GSH) under neutral conditions by means of photoluminescence (PL) and absorption spectroscopy. A reversible addition–fragmentation chain-transfer-mediated synthesis was employed to produce co-polymer ligands with different molecular weights in block and random sequences. Poly(ethylene glycol) sidechains were incorporated on a methacrylate backbone for solubility in phosphate-buffered saline. Imidazole-bearing histamine sidechains were installed postsynthetically to facilitate binding to the QD surface. Introduction of l-glutathione, an endogenous monothiol, to aqueous solutions of the polymer-coated QDs led to an increase in PL quantum yield, indicating an interaction between the QD and glutathione. The PL change was greatly diminished for block co-polymers versus random co-polymers of similar molecular weight and composition. Additionally, higher ligand populations were found upon initial purification of block co-polymer-coated QDs versus the random co-polymers. We demonstrate that glutathione does not significantly displace the polymer ligands from the QD surface, suggesting that PL changes are driven primarily through ligand association. The block co-polymers are more resistant to glutathione association, and indeed stronger binders, than the randomly ordered co-polymers, with higher-molecular-weight contributing to improved stability in both cases. To the best of our knowledge, this is the first study to directly compare the relative stability of block and random polymeric imidazole ligands and should aid in developing more stable ligand-exchanged QDs for bioimaging and biosensing, especially for in vivo and intracellular applications.
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- 2018
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42. Molecular and cellular signatures underlying superior immunity against Bordetella pertussis upon pulmonary vaccination
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Raeven, R HM, Brummelman, J, Pennings, J LA, van der Maas, L, Helm, K, Tilstra, W, van der Ark, A, Sloots, A, van der Ley, P, van Eden, W, Jiskoot, W, van Riet, E, van Els, C ACM, Kersten, G FA, Han, W GH, and Metz, B
- Abstract
Mucosal immunity is often required for protection against respiratory pathogens but the underlying cellular and molecular mechanisms of induction remain poorly understood. Here, systems vaccinology was used to identify immune signatures after pulmonary or subcutaneous immunization of mice with pertussis outer membrane vesicles. Pulmonary immunization led to improved protection, exclusively induced mucosal immunoglobulin A (IgA) and T helper type 17 (Th17) responses, and in addition evoked elevated systemic immunoglobulin G (IgG) antibody levels, IgG-producing plasma cells, memory B cells, and Th17 cells. These adaptive responses were preceded by unique local expression of genes of the innate immune response related to Th17 (e.g., Rorc) and IgA responses (e.g., Pigr) in addition to local and systemic secretion of Th1/Th17-promoting cytokines. This comprehensive systems approach identifies the effect of the administration route on the development of mucosal immunity, its importance in protection against Bordetella pertussis, and reveals potential molecular correlates of vaccine immunity to this reemerging pathogen.
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- 2018
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43. Molecular and cellular signatures underlying superior immunity against Bordetella pertussisupon pulmonary vaccination
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Raeven, R HM, Brummelman, J, Pennings, J LA, van der Maas, L, Helm, K, Tilstra, W, van der Ark, A, Sloots, A, van der Ley, P, van Eden, W, Jiskoot, W, van Riet, E, van Els, C ACM, Kersten, G FA, Han, W GH, and Metz, B
- Abstract
Mucosal immunity is often required for protection against respiratory pathogens but the underlying cellular and molecular mechanisms of induction remain poorly understood. Here, systems vaccinology was used to identify immune signatures after pulmonary or subcutaneous immunization of mice with pertussis outer membrane vesicles. Pulmonary immunization led to improved protection, exclusively induced mucosal immunoglobulin A (IgA) and T helper type 17 (Th17) responses, and in addition evoked elevated systemic immunoglobulin G (IgG) antibody levels, IgG-producing plasma cells, memory B cells, and Th17 cells. These adaptive responses were preceded by unique local expression of genes of the innate immune response related to Th17 (e.g., Rorc) and IgA responses (e.g., Pigr) in addition to local and systemic secretion of Th1/Th17-promoting cytokines. This comprehensive systems approach identifies the effect of the administration route on the development of mucosal immunity, its importance in protection against Bordetella pertussis, and reveals potential molecular correlates of vaccine immunity to this reemerging pathogen.
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- 2018
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44. Do Adverse Childhood Experiences Hurt Blacks Worse than Whites?: Race, Family Environments, and Health.
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Monnat, Shannon M., Chandler, Raeven Faye, and Sherman-Wilkins, Kyler J.
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This study is the first to examine racially heterogeneous associations between adverse childhood experiences (ACEs) that occurred in the family environment and adult physical health. Our study is also unique in that we simultaneously explored associations between adult health and the total count of different ACEs as well as between adult health and specific ACEs (physical, verbal, and sexual abuse, parental domestic violence and divorce, and living with someone who was depressed, abused alcohol, abused drugs, or was incarcerated). Using data from 45,892 U.S. non-Hispanic white and non-Hispanic black adults aged 18-64 from the 2009-2012 Behavioral Risk Factor Surveillance System, we found significant differences between whites and blacks in associations between adverse childhood family experiences and adult self-rated health and a prevalent chronic disease - diabetes. First, the negative graded association between the breadth of exposure to adverse childhood experiences (i.e., the cumulative number of different ACEs) and adult self-rated health is stronger for whites than for blacks. Second, while the probability of being diagnosed with diabetes increases with each cumulative ACE among whites, blacks who experienced a very high degree of ACEs during childhood (5 or more) actually have a much lower probability of a diabetes diagnosis than blacks who experienced no ACEs, even when accounting for access to and use of health care services. Third, specific ACEs demonstrate different associations with self-rated health and diabetes for blacks vs. whites. The positive association between parental divorce and diabetes is much stronger for whites than for blacks, and while parental incarceration is associated with worse self-rated health for whites, it is associated with better self-rated health for blacks. Overall, the results of this study highlight the differential salience of various adverse childhood conditions on adult health between whites and blacks, suggesting that adverse childhood experiences have a greater negative impact on health for whites than they do for blacks. Our paper concludes with a discussion of the implications of these findings for research on life course determinants of health. [ABSTRACT FROM AUTHOR]
- Published
- 2015
45. Racial/Ethnic Differences in Access to and Use of Physician Diabetes Care.
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Chandler, Raeven Faye and Monnat, Shannon M.
- Abstract
Racial/ethnic minorities disproportionately suffer from diabetes, complications from diabetes, and diabetes-related mortality. Proper diabetes physician care can reduce the risk of complications and premature mortality. Using a large national data set (N=20,171) of white, black, Hispanic, and Native American adults in the US who have been diagnosed with diabetes, we examine three specific types of physician care use for diabetes management: number of times seen by a healthcare professional for diabetes, number of times feet have been checked by a health care professional, and number of visits for a glycosylated hemoglobin check. We found that net of controls for a variety of demographic and socioeconomic characteristics, blacks, Hispanics, and Native Americans had significantly more visits to a health care provider for their diabetes than whites. Blacks and Native Americans had significantly more physician feet checks and significant more visits for glycosylated hemoglobin checks than whites. Our results suggest that the reduced access to health care services among racial minorities that is traditionally found in research on racial disparities in health care does not hold for access to diabetes physician care, where racial/ethnic minorities are actually more likely to use care than are whites. [ABSTRACT FROM AUTHOR]
- Published
- 2014
46. Non-infectious subcutaneous emphysema of the forearm in a 12-year-old schoolgirl
- Author
-
Raeven, P., primary, Haagen, A. A. M., additional, and de Hoog, D. E. N. M., additional
- Published
- 2009
- Full Text
- View/download PDF
47. Multiple organ dysfunction syndrome: the scapegoat? Assessment of organ dysfunction between surviving and dying mice in the acute phase of polymicrobial sepsis
- Author
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Osuchowski, M, primary, Weixelbaumer, K, additional, Raeven, P, additional, Remick, D, additional, Reise, K, additional, Kozlov, A, additional, van Griensven, M, additional, Redl, H, additional, and Bahrami, S, additional
- Published
- 2009
- Full Text
- View/download PDF
48. Immunoproteomic Profiling of Bordetella pertussis Outer Membrane Vesicle Vaccine Reveals Broad and Balanced Humoral Immunogenicity.
- Author
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Raeven, René H. M., van der Maas, Larissa, Tilstra, Wichard, Uittenbogaard, Joost P., Bindels, Tim H. E., Kuipers, Betsy, van der Ark, Arno, Pennings, Jeroen L. A., van Riet, Elly, Jiskoot, Wim, Kersten, Gideon F. A., and Metz, Bernard
- Published
- 2015
- Full Text
- View/download PDF
49. Tumor-associated macrophages promote intratumoral conversion of conventional CD4+T cells into regulatory T cells via PD-1 signalling
- Author
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Kos, Kevin, Salvagno, Camilla, Wellenstein, Max D., Aslam, Muhammad A., Meijer, Denize A., Hau, Cheei-Sing, Vrijland, Kim, Kaldenbach, Daphne, Raeven, Elisabeth A.M., Schmittnaegel, Martina, Ries, Carola H., and de Visser, Karin E.
- Abstract
ABSTRACTWhile regulatory T cells (Tregs) and macrophages have been recognized as key orchestrators of cancer-associated immunosuppression, their cellular crosstalk within tumors has been poorly characterized. Here, using spontaneous models for breast cancer, we demonstrate that tumor-associated macrophages (TAMs) contribute to the intratumoral accumulation of Tregsby promoting the conversion of conventional CD4+T cells (Tconvs) into Tregs. Mechanistically, two processes were identified that independently contribute to this process. While TAM-derived TGF-β directly promotes the conversion of CD4+Tconvsinto Tregsin vitro, we additionally show that TAMs enhance PD-1 expression on CD4+T cells. This indirectly contributes to the intratumoral accumulation of Tregs, as loss of PD-1 on CD4+Tconvsabrogates intratumoral conversion of adoptively transferred CD4+Tconvsinto Tregs. Combined, this study provides insights into the complex immune cell crosstalk between CD4+T cells and TAMs in the tumor microenvironment of breast cancer, and further highlights that therapeutic exploitation of macrophages may be an attractive immune intervention to limit the accumulation of Tregsin breast tumors.
- Published
- 2022
- Full Text
- View/download PDF
50. Induced hypothermia reduces the hepatic inflammatory response in a swine multiple trauma model.
- Author
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Fröhlich, Matthias, Hildebrand, Frank, Weuster, Matthias, Mommsen, Philipp, Mohr, Juliane, Witte, Ingo, Raeven, Pierre, Ruchholtz, Steffen, Flohé, Sascha, van Griensven, Martijn, Pape, Hans-Christoph, and Pfeifer, Roman
- Published
- 2014
- Full Text
- View/download PDF
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