Search

Your search keyword '"Kramer BW"' showing total 348 results
Start Over Author "Kramer BW"
348 results on '"Kramer BW"'

1. Anti-inflammatory Effects of Naïve Stem Cells Dampen Systemic/Compartmental Overreactive Immune Responses

Author

de Munter Jpjm, de Hoo K, Kramer Bw, and Wolters ECh

Subjects
Immune system, medicine.drug_class, business.industry, Immunology, medicine, Stem cell, business, Anti-inflammatory
Abstract

A cytokine release syndrome (CRS), associated with elevated circulating levels of several cytokines including interleukin (IL)-6 and interferon (IFN)-γ, might be seen in some infectious insults, for instance in severe acute respiratory syndrome (SARS) induced by Coronavirus (Cov)-2, as well as following administration of natural and bispecific antibodies and, more recently, following adoptive T-cell therapies for cancer. Normally, inflammatory conditions activate the innate and adaptive immune systems, which results in the release of cytokines, responsible for the phagocytosis of apoptotic vesicles and resolution of inflammation. Pro-inflammatory cytokines such as IL-1β, tumor necrosis factor alpha (TNFα) and, especially in chronic inflammatory diseases, autoimmune diseases, cancer and cytokine storms, IL-6 play crucial roles in inflammation. In some instances, however, this release gets out of hand, and features of overzealous immune responses (macrophage activation syndromes) might occur, leading to cytokine release syndromes (CRS) with inflammatory signs such as fever, fatigue, nausea, and sometimes secondary organ dysfunction or multi-organ failure. Apart from specific vaccines and maybe the anti-viral remdesivir and/or dexamethasone for treatment of CRS, there are no convincing disease-modifying interventions. So far, though, non-antiviral and immune-targeted interventions, also affecting non-target cells, were found associated with many side effects. A more targeted or focused approach is thus needed. Pending the site of the CRS-inducing insult, CRSs may occur systemic or compartmental. Recently, preclinical research yielded a beneficial anti-inflammatory effect of fresh naive bone marrow-derived stem cells (bm-SCs) in the treatment of various compartmental CRSs in the immune-privileged central nervous system (CNS). Therefore, it is argued that bm-SCs might also play a disease-modifying role in the systemic CRS. Bm-SCs have the advantage of targeting only the cells of interest as they are very selective in their actions. In addition, they actively move to the sight of inflammation.

Published
2021

4. Towards Prepared mums (TOP-mums) for a healthy start, a lifestyle intervention for women with overweight and a child wish: Study protocol for a randomised controlled trial in the Netherlands

Author

Timmermans, YEG, de Kant, KDG, Reijnders, D, Kleijkers, LMP, Dompeling, E, Kramer, BW, Zimmermann, LJ, Steegers - Theunissen, Régine, Spaanderman, MEA, Vreugdenhil, ACE, Timmermans, YEG, de Kant, KDG, Reijnders, D, Kleijkers, LMP, Dompeling, E, Kramer, BW, Zimmermann, LJ, Steegers - Theunissen, Régine, Spaanderman, MEA, and Vreugdenhil, ACE

Published
2019

5. Perinatal insults and neurodevelopmental disorders may impact Huntington's disease age of diagnosis

Author

Barkhuizen, M, Rodrigues, Fb, Anderson, Dg, Winkens, B, REGISTRY Investigators of the European Huntington's Disease Network, Ristori, G, Romano, S, Ferraldeschi, M, Wild, Ej, Kramer, Bw, Gavilanes, Awd., RS: MHeNs - R3 - Neuroscience, Promovendi MHN, Kindergeneeskunde, FHML Methodologie & Statistiek, RS: CAPHRI - R6 - Promoting Health & Personalised Care, RS: GROW - R4 - Reproductive and Perinatal Medicine, and MUMC+: MA Medische Staf Kindergeneeskunde (9)

Subjects
Male, International Cooperation, Gestational Age, Article, Disease-Free Survival, Cohort Studies, Trinucleotide Repeats, Pregnancy, Neonatal, Developmental disorders, epidemiological, huntington's disease, modifier, neonatal, Humans, Registries, Age of Onset, Modifier, Proportional Hazards Models, Huntingtin Protein, OUTCOMES, Age Factors, Huntington's disease, ASSOCIATION, Middle Aged, TRENDS, PREVALENCE, Huntington Disease, Neurodevelopmental Disorders, Prenatal Exposure Delayed Effects, Epidemiological, Female
Abstract

Introduction The age of diagnosis of Huntington's disease (HD) varies among individuals with the same HTT CAG-repeat expansion size. We investigated whether early-life events, like perinatal insults or neurodevelopmental disorders, influence the diagnosis age. Methods We used data from 13,856 participants from REGISTRY and Enroll-HD, two large international multicenter observational studies. Disease-free survival analyses of mutation carriers with an HTT CAG repeat expansion size above and including 36 were computed through Kaplan-Meier estimates of median time until an HD diagnosis. Comparisons between groups were computed using a Cox proportional hazard survival model adjusted for CAG-repeat expansion length. We also assessed whether the group effect depended on gender and the affected parent. Results Insults in the perinatal period were associated with an earlier median age of diagnosis of 45.00 years (95%CI: 42.07–47.92) compared to 51.00 years (95%CI: 50.68–51.31) in the reference group, with a CAG-adjusted hazard ratio of 1.61 (95%CI: 1.26–2.06). Neurodevelopmental disorders were also associated with an earlier median age of diagnosis than the reference group of 47.00 years (95% CI: 43.38–50.62) with a CAG-adjusted hazard ratio of 1.42 (95%CI: 1.16–1.75). These associations did not change significantly with gender or affected parent. Conclusions These results, derived from large observational datasets, show that perinatal insults and neurodevelopmental disorders are associated with earlier ages of diagnosis of magnitudes similar to the effects of known genetic modifiers of HD. Given their clear temporal separation, these early events may be causative of earlier HD onset, but further research is needed to prove causation., Highlights • The CAG-repeat expansion does not fully explain the onset of Huntington's disease (HD). • In two large observational studies, birth complications were associated with the onset of HD. • Persons with disorders of brain development also had an earlier diagnosis of HD. • Early-life factors may be an environmental modifier of HD.

Published
2018

8. Die Surfactantproteine A und D: Wesentliche Faktoren des pulmonalen Abwehrsystems

Author

Speer Cp and Kramer Bw

Subjects
Vernix caseosa, Innate immune system, Immune system, Maternity and Midwifery, Pediatrics, Perinatology and Child Health, Obstetrics and Gynecology, Collectin, Chemotaxis, Pulmonary surfactant-associated protein B, Biology, Acquired immune system, Microbiology, Pulmonary Surfactant-Associated Protein A
Abstract

Surfactant proteins (SP) A and D play a key role in pulmonary host defense of preterm and term newborns. SP-A and SP-D have structural elements of both collagens and lectins, for which they are called "collectins". SP-A and SP-D coordinate the innate and adaptive immune response in the lung and convey protection against infection in amniotic fluid and vernix caseosa. They are pattern-recognizing molecules of the innate immune system that are involved in binding, agglutination of pathogens, chemotaxis of neutrophils, phagocytosis of pathogens, and production of reactive oxygen species. In addition, SP-A and SP-D interact with the adaptive immune system by reducing interleukin-2 production and T lymphocyte proliferation.

Published
2003

9. Applying extracellular vesicles based therapeutics in clinical trials - an ISEV position paper

Author

Lener, T, Gimona, M, Aigner, L, Boerger, V, Buzas, E, Camussi, G, Chaput, N, Chatterjee, D, Court, FA, del Portillo, HA, O'Driscoll, L, Fais, S, Falcon-Perez, JM, Felderhoff-Mueser, U, Fraile, L, Gho, YS, Goergens, A, Gupta, RC, Hendrix, A, Hermann, DM, Hill, AF, Hochberg, F, Horn, PA, de Kleijn, D, Kordelas, L, Kramer, BW, Kraemer-Albers, E-M, Laner-Plamberger, S, Laitinen, S, Leonardi, T, Lorenowicz, MJ, Lim, SK, Lotvall, J, Maguire, CA, Marcilla, A, Nazarenko, I, Ochiya, T, Patel, T, Pedersen, S, Pocsfalvi, G, Pluchino, S, Quesenberry, P, Reischl, IG, Rivera, FJ, Sanzenbacher, R, Schallmoser, K, Slaper-Cortenbach, I, Strunk, D, Tonn, T, Vader, P, van Balkom, BWM, Wauben, M, El Andaloussi, S, Thery, C, Rohde, E, Giebel, B, Lener, T, Gimona, M, Aigner, L, Boerger, V, Buzas, E, Camussi, G, Chaput, N, Chatterjee, D, Court, FA, del Portillo, HA, O'Driscoll, L, Fais, S, Falcon-Perez, JM, Felderhoff-Mueser, U, Fraile, L, Gho, YS, Goergens, A, Gupta, RC, Hendrix, A, Hermann, DM, Hill, AF, Hochberg, F, Horn, PA, de Kleijn, D, Kordelas, L, Kramer, BW, Kraemer-Albers, E-M, Laner-Plamberger, S, Laitinen, S, Leonardi, T, Lorenowicz, MJ, Lim, SK, Lotvall, J, Maguire, CA, Marcilla, A, Nazarenko, I, Ochiya, T, Patel, T, Pedersen, S, Pocsfalvi, G, Pluchino, S, Quesenberry, P, Reischl, IG, Rivera, FJ, Sanzenbacher, R, Schallmoser, K, Slaper-Cortenbach, I, Strunk, D, Tonn, T, Vader, P, van Balkom, BWM, Wauben, M, El Andaloussi, S, Thery, C, Rohde, E, and Giebel, B

Abstract

Extracellular vesicles (EVs), such as exosomes and microvesicles, are released by different cell types and participate in physiological and pathophysiological processes. EVs mediate intercellular communication as cell-derived extracellular signalling organelles that transmit specific information from their cell of origin to their target cells. As a result of these properties, EVs of defined cell types may serve as novel tools for various therapeutic approaches, including (a) anti-tumour therapy, (b) pathogen vaccination, (c) immune-modulatory and regenerative therapies and (d) drug delivery. The translation of EVs into clinical therapies requires the categorization of EV-based therapeutics in compliance with existing regulatory frameworks. As the classification defines subsequent requirements for manufacturing, quality control and clinical investigation, it is of major importance to define whether EVs are considered the active drug components or primarily serve as drug delivery vehicles. For an effective and particularly safe translation of EV-based therapies into clinical practice, a high level of cooperation between researchers, clinicians and competent authorities is essential. In this position statement, basic and clinical scientists, as members of the International Society for Extracellular Vesicles (ISEV) and of the European Cooperation in Science and Technology (COST) program of the European Union, namely European Network on Microvesicles and Exosomes in Health and Disease (ME-HaD), summarize recent developments and the current knowledge of EV-based therapies. Aspects of safety and regulatory requirements that must be considered for pharmaceutical manufacturing and clinical application are highlighted. Production and quality control processes are discussed. Strategies to promote the therapeutic application of EVs in future clinical studies are addressed.

Published
2015

11. O-061 Cell-based Therapy For Hypoxic-ischaemic Injury In The Preterm Brain

Author

Jellema, RK, primary, Wolfs, TGAM, additional, Lima Passos, V, additional, Zwanenburg, A, additional, Ophelders, DRMG, additional, Kuypers, E, additional, Hopman, AHN, additional, Dudink, J, additional, Steinbusch, HW, additional, Andriessen, P, additional, Germeraad, WTV, additional, Vanderlocht, J, additional, and Kramer, BW, additional

Published
2014
Full Text
View/download PDF

13. Effects of Intra-Amniotic Lipopolysaccharide and Maternal Betamethasone on Brain Inflammation in Fetal Sheep

Author

Kuypers, E, Jellema, RK, Ophelders, DRMG, Dudink, J, Nikiforou, M, Wolfs, TGAM, Nitsos, I, Pillow, JJ, Polglasem, GR, Kemp, MW, Saito, M, Newnham, JP, Jobe, AH, Kallapur, SG, Kramer, BW, Kuypers, E, Jellema, RK, Ophelders, DRMG, Dudink, J, Nikiforou, M, Wolfs, TGAM, Nitsos, I, Pillow, JJ, Polglasem, GR, Kemp, MW, Saito, M, Newnham, JP, Jobe, AH, Kallapur, SG, and Kramer, BW

Published
2013

14. Mesenchymal Stem Cells Induce T-Cell Tolerance and Protect the Preterm Brain after Global Hypoxia-Ischemia

Author

Jellema, RK, Wolfs, TGAM, Passos, VL, Ophelders, DRMG, Kuypers, E, Hopman, AHN, Dudink, J, Steinbusch, HW, Andriessen, P, Germeraad, WTV (Wilfred), Vanderlocht, J, Kramer, BW, Zwanenburg, A, Jellema, RK, Wolfs, TGAM, Passos, VL, Ophelders, DRMG, Kuypers, E, Hopman, AHN, Dudink, J, Steinbusch, HW, Andriessen, P, Germeraad, WTV (Wilfred), Vanderlocht, J, Kramer, BW, and Zwanenburg, A

Published
2013

15. A Clinical Prediction Rule for Histological Chorioamnionitis in Preterm Newborns

Author

Been, JV, Vanterpool, SF, de Rooij -, Jasmijn, Rours, Ingrid, Kornelisse, R.F., Dongen, MCJM, van Gool, CJAW, de Krijger, Ronald, Andriessen, P, Zimmermann, LJI, Kramer, BW, Been, JV, Vanterpool, SF, de Rooij -, Jasmijn, Rours, Ingrid, Kornelisse, R.F., Dongen, MCJM, van Gool, CJAW, de Krijger, Ronald, Andriessen, P, Zimmermann, LJI, and Kramer, BW

Abstract

Background: Histological chorioamnionitis (HC) is an intrauterine inflammatory process highly associated with preterm birth and adverse neonatal outcome. HC is often clinically silent and diagnosed postnatally by placental histology. Earlier identification could facilitate treatment individualisation to improve outcome in preterm newborns. Aim: Develop a clinical prediction rule at birth for HC and HC with fetal involvement (HCF) in preterm newborns. Methods: Clinical data and placental pathology were obtained from singleton preterm newborns (gestational age <= 32.0 weeks) born at Erasmus UMC Rotterdam from 2001 to 2003 (derivation cohort; n = 216) or Maxima MC Veldhoven from 2009 to 2010 (validation cohort; n = 206). HC and HCF prediction rules were developed with preference for high sensitivity using clinical variables available at birth. Results: HC and HCF were present in 39% and 24% in the derivation cohort and in 44% and 22% in the validation cohort, respectively. HC was predicted with 87% accuracy, yielding an area under ROC curve of 0.95 (95% CI = 0.92-0.98), a positive predictive value of 80% (95% CI = 74-84%), and a negative predictive value of 93% (95% CI = 88-96%). Corresponding figures for HCF were: accuracy 83%, area under ROC curve 0.92 (95% CI = 0.88-0.96), positive predictive value 59% (95% CI = 52-62%), and negati Conclusion: Using a clinical prediction rule composed of clinical variables available at birth, HC and HCF could be predicted with good test characteristics in preterm newborns. Further studies should evaluate the clinical value of these rules to guide early treatment individualisation.

Published
2012

38. Multiple intravenous doses of paracetamol result in a predictable pharmacokinetic profile in very preterm infants.

Author

Ganzewinkel, C, Derijks, L, Anand, KJS, Lingen, RA, Neef, C, Kramer, BW, and Andriessen, P

Subjects
DRUG dosage, ACETAMINOPHEN, PREMATURE infant diseases, PHARMACOKINETICS, HEPATOTOXICOLOGY
Abstract

Aim The therapeutic options available to treat neonatal pain are limited, and one alternative for nonopioid systemic treatment is paracetamol. However, pharmacokinetic data from prolonged administration of intravenous paracetamol in neonates are limited. The aim of this study was to present pharmacokinetics after multiple dose of intravenous paracetamol in very preterm infants of <32 weeks' gestation. Methods Fifteen very preterm infants received five, six-hourly doses of intravenous paracetamol (7.5 mg/kg). Blood samples were taken to measure paracetamol, glutathione and hepatic function, together with urine samples for paracetamol metabolites. Results A two-compartment pharmacokinetic model gave the best fit for all individual patients and resulted in a predictable pharmacokinetic profile. The estimated pharmacokinetic population parameters were volume of distribution 0.764 ± 0.225 L/kg, elimination rate constant (ke) 0.117 ± 0.091/h and intercompartment rate constants k12 0.607 ± 0.734/h and k21 1.105 ± 0.762/h. Conclusion Our study found that multiple doses of intravenous paracetamol resulted in a predictable pharmacokinetic profile in very preterm infants. Increases in postmenstrual age and weight were associated with increased clearance. No evidence of hepatotoxicity was found. [ABSTRACT FROM AUTHOR]

Published
2014
Full Text
View/download PDF

39. IL-1 mediates pulmonary and systemic inflammatory responses to chorioamnionitis induced by lipopolysaccharide.

Author

Kallapur SG, Nitsos I, Moss TJ, Polglase GR, Pillow JJ, Cheah FC, Kramer BW, Newnham JP, Ikegami M, Jobe AH, Kallapur, Suhas G, Nitsos, Ilias, Moss, Timothy J M, Polglase, Graeme R, Pillow, J Jane, Cheah, Fook-Choe, Kramer, Boris W, Newnham, John P, Ikegami, Machiko, and Jobe, Alan H

Abstract

Rationale: Chorioamnionitis frequently associates with preterm delivery and increased amniotic fluid IL-1, and causes fetal lung and systemic inflammation. However, chorioamnionitis is also associated with a paradoxical reduction in the incidence of surfactant deficiency-related respiratory distress syndrome in preterm infants.Objectives: To identify the role of IL-1 signaling in the mediation of pulmonary and systemic inflammation and lung maturation in a fetal sheep model of lipopolysaccharide (LPS) induced chorioamnionitis.Methods: After confirming the efficacy of recombinant human IL-1 receptor antagonist (rhIL-1ra), fetal sheep were exposed to intraamniotic (IA) injections of Escherichia coli LPS with or without prior IA injections of rhIL-1ra. Preterm lambs were delivered at 82% of term gestation.Measurements and Main Results: rhIL-1ra decreased IA LPS-induced lung inflammation assessed by decreased lung neutrophil and monocyte influx, inducible nitric oxide synthase expression, lung IL-6 and IL-1beta mRNA expression, and airway myeloperoxidase concentrations. rhIL-1ra inhibited IA LPS-induced fetal systemic inflammation assessed by decreased plasma IL-8, protein carbonyls, blood neutrophilia, and the expression of serum amyloid A3 mRNA in the liver. rhIL-1ra also partially blocked the lung maturational effects of IA LPS. Therefore blockade of IL-1 signaling in the amniotic compartment inhibited fetal lung and systemic inflammation and lung maturation in response to LPS-induced chorioamnionitis.Conclusions: IL-1 plays a central role in the pathogenesis of chorioamnionitis-induced fetal inflammatory responses. [ABSTRACT FROM AUTHOR]

Published
2009
Full Text
View/download PDF

42. Surfactant therapy - The conundrum of which infant should be given, when, which drug in what dose via which route of administration?

Author

Diggikar S, Galis R, Nagesh K, Pandita A, Ognean ML, Rüdiger M, Mazela J, and Kramer BW

Abstract

Surfactant therapy in preterm and term born infants has been a huge success story. In the meantime, we have very detailed answers to the five essential questions of each medical therapy: which infant should be treated, when, with which drug, in/at what dose, and via which route of administration. The answers to these questions depend on the gestational age of the infant. We have focused on preterm infants <28 weeks of gestation as they are the most vulnerable and may have the maximum benefit of appropriate treatment. Therefore, we performed a sub-group analysis for data available from the published trials in infants less than 28 weeks who received less/minimal invasive surfactant administration/therapy [LISA/MIST] versus intubation-surfactant-extubation (INSURE). The need for mechanical ventilation (MV) was significantly reduced by 28 % (RR:0.72, 95%CI:0.64-0.80, n = 548 infants) after LISA/MIST. The incidence of bronchopulmonary dysplasia (BPD) was significantly decreased by 30 % (RR:0.70, 95%CI:0.66-0.75, n = 6528 infants) after LISA/MIST. No difference in mortality was noted between the two groups. In the current review, we discuss the applicability of guidelines to individual patient groups like the infants <28 weeks and emphasize the individual assessment of published data by the treating physician., (Copyright © 2024. Published by Elsevier Ltd.)

Published
2024
Full Text
View/download PDF

43. ABCA3 c.838C>T (p.Arg280Cys, R280C) and c.697C>T (p.Gln233Ter, Q233X, Q233*) as Causative Variants for RDS: A Family Case Study and Literature Review.

Author

Ognean ML, Anciuc-Crauciuc M, Galiș R, Stepan AE, Stepan MD, Bănescu C, Grosu F, Kramer BW, and Cucerea M

Abstract

Background: Respiratory distress syndrome (RDS) is the primary cause of respiratory failure in preterm infants, but it also affects 5-7% of term infants. Dysfunctions in pulmonary surfactant metabolism, resulting from mutations of the lung surfactant genes, are rare diseases, ranging from fatal neonatal RDS to interstitial lung disease, associated with increased morbidity and mortality. This study aims to clarify the clinical significance of ABCA3 variants found in a specific family case, as existing data in the literature are inconsistent. Material and Methods: A family case report was conducted; targeted panel genetic testing identified a variant of the SFTPB gene and two variants of ABCA3 genes. Comprehensive research involving a systematic review of PubMed, Google Scholar databases, and genome browsers was used to clarify the pathogenicity of the two ABCA3 variants found in the index patient. Advanced prediction tools were employed to assess the pathogenicity of the two ABCA3 variants, ensuring the validity and reliability of our findings. Results: The index case exhibited fatal neonatal RDS. Genetic testing revealed the presence of the SFTPB p.Val267Ile variant, which was not previously reported but is a benign variant based on family genetic testing and history. Additionally, two ABCA3 gene variants were identified: c.697C>T, not yet reported, and c.838C>T. These variants were found to affect ABCA3 protein function and were likely associated with neonatal RDS. Prediction tools and data from nine other cases in the literature supported this conclusion. Conclusions: Based on in silico predictors, an analysis of the presented family, and cases described in the literature, it is reasonable to consider reclassifying the two ABCA3 variants identified in the index case as pathogenic/pathogenic. Reclassification will improve genetic counseling accuracy and facilitate correct diagnosis.

Published
2024
Full Text
View/download PDF

44. Milrinone in persistent pulmonary hypertension of newborn: a scoping review.

Author

Galis R, Mudura D, Trif P, Diggikar S, Prasath A, Ognean ML, Mazela J, Lacatusu A, Ramanathan R, Kramer BW, and Singh Y

Subjects
Humans, Infant, Newborn, Administration, Inhalation, Treatment Outcome, Extracorporeal Membrane Oxygenation, Milrinone therapeutic use, Milrinone administration & dosage, Persistent Fetal Circulation Syndrome drug therapy, Vasodilator Agents therapeutic use, Vasodilator Agents administration & dosage, Nitric Oxide administration & dosage, Nitric Oxide therapeutic use
Abstract

Persistent pulmonary hypertension of the newborn (PPHN) is a common neonatal condition in newborns admitted to the neonatal intensive care units (NICUs). PPHN has still a high mortality and morbidity. Inhaled nitric oxide (iNO) is the first line vasodilator therapy for PPHN in high income countries. In low-to-middle income countries (LMICs), availability of iNO remains scarce and expensive. The purpose of this scoping review was to evaluate the current existing literature for milrinone therapy in PPHN and to identify the knowledge gaps in milrinone use in infants with PPHN. The available evidence for milrinone remains limited both as monotherapy and as an adjuvant to iNO. The studies were heterogeneous, conducted in different settings, with different populations and more importantly the endpoints of these trials were short-term outcomes such as changes in oxygenation and blood pressure. Large prospective studies investigating long-term outcomes, mortality, and the need for Extracorporeal membrane oxygenation (ECMO) are warranted. Randomized controlled trials with milrinone as monotherapy are needed in LMICs where iNO availability remains limited. IMPACT: Milrinone has a potential role in the management of PPHN both as an adjuvant to iNO as well as a monotherapy. This scoping review identified the problems existing in the published literature on milrinone and the barriers to generalization of these results. Multi-centre randomized controlled trials on milrinone, especially involving centers from low- and middle-income countries are needed, where it can be evaluated as first-line pulmonary vasodilator therapy., (© 2024. The Author(s), under exclusive licence to the International Pediatric Research Foundation, Inc.)

Published
2024
Full Text
View/download PDF

45. Fecal microbiota and volatile metabolome pattern alterations precede late-onset meningitis in preterm neonates.

Author

Frerichs NM, Deianova N, El Manouni El Hassani S, Acharjee A, Quraishi MN, de Boode WP, Cossey V, Hulzebos CV, van Kaam AH, Kramer BW, d'Haens E, de Jonge WJ, Vijlbrief DC, van Weissenbruch MM, Daulton E, Wicaksono AN, Covington JA, Benninga MA, de Boer NKH, van Goudoever JB, Niemarkt HJ, and de Meij TGJ

Abstract

Objective: The fecal microbiota and metabolome are hypothesized to be altered before late-onset neonatal meningitis (LOM), in analogy to late-onset sepsis (LOS). The present study aimed to identify fecal microbiota composition and volatile metabolomics preceding LOM., Methods: Cases and gestational age-matched controls were selected from a prospective, longitudinal preterm cohort study (born <30 weeks' gestation) at nine neonatal intensive care units. The microbial composition (16S rRNA sequencing) and volatile metabolome (gas chromatography-ion mobility spectrometry (GC-IMS) and GC-time-of-flight-mass spectrometry (GC-TOF-MS)), were analyzed in fecal samples 1-10 days pre-LOM., Results: Of 1397 included infants, 21 were diagnosed with LOM (1.5%), and 19 with concomitant LOS (90%). Random Forest classification and MaAsLin2 analysis found similar microbiota features contribute to the discrimination of fecal pre-LOM samples versus controls. A Random Forest model based on six microbiota features accurately predicts LOM 1-3 days before diagnosis with an area under the curve (AUC) of 0.88 (n=147). Pattern recognition analysis by GC-IMS revealed an AUC of 0.70-0.76 (P<0.05) in the three days pre-LOM (n=92). No single discriminative metabolites were identified by GC-TOF-MS (n=66)., Conclusion: Infants with LOM could be accurately discriminated from controls based on preclinical microbiota composition, while alterations in the volatile metabolome were moderately associated with preclinical LOM., (© The Author(s) 2024. Published by Oxford University Press on behalf of Infectious Diseases Society of America.)

Published
2024
Full Text
View/download PDF

46. Association of Fortification with Human Milk versus Bovine Milk-Based Fortifiers on Short-Term Outcomes in Preterm Infants-A Meta-Analysis.

Author

Galis R, Trif P, Mudura D, Mazela J, Daly MC, Kramer BW, and Diggikar S

Subjects
Infant, Infant, Newborn, Humans, Infant, Premature, Milk, Human, Birth Weight, Gestational Age, Food, Fortified, Sepsis, Enterocolitis, Necrotizing
Abstract

This meta-analysis assessed short-term outcomes after using human milk-derived fortifiers (HMFs) compared with bovine milk fortifiers (BMFs) in preterm infants fed an exclusive human milk (HM) diet, either mother's own milk (MOM) or donor human milk (DHM). We searched PubMed, Embase, Google Scholar, CENTRAL and CINHAL between January 2015 and August 2023 for studies reporting outcomes in infants with ≤28 weeks gestation and/or birthweight ≤ 1500 g on an exclusive human milk diet fortified with HMF versus BMF. The primary outcomes were death and NEC (stage ≥ 2). Four studies with a total of 681 infants were included. Mortality was significantly lower in infants fed with an HM-HMFs diet (four studies, 681 infants; RR = 0.50, 95% CI = 0.26-0.94; p = 0.03; I 2 = 0%), NEC was similar between the two groups (four studies, 681 infants; RR = 0.48, 95% CI = 0.20-1.17; p = 0.11; I 2 = 39%). BPD was higher in the HM-BMFs group (four studies, 663 infants; RR = 0.83, 95% CI = 0.69-1.000; p = 0.05, I 2 = 0%), although not statistically significant. No differences were found for sepsis (RR = 0.97, 95% CI = 0.66-1.42; p = 0.96; I 2 = 26%) or combined ROP (four studies, 671 infants; RR = 0.64, 95% CI = 0.53-1.07; p = 0.28; I 2 = 69%). An HM-HMFs diet could possibly be associated with decreased mortality with no association with NEC, BPD, sepsis, or ROP. This meta-analysis was limited by the small number of studies included. However, the results should not be refuted for this reason as they provide an impetus for subsequent clinical trials to assess the observed associations.

Published
2024
Full Text
View/download PDF

47. Preterm birth and stillbirth during COVID-19 pandemic in Bihor County/Romania.

Author

Galis R, Trif P, Mudura D, Murvai R, Daina LG, Szasz F, Negrini R, Hatos A, Gyarmati BF, Daly MC, Mazela J, and Kramer BW

Abstract

Background: International studies have reported conflicting data about the effects of COVID-19 pandemic policy measures on maternal and neonatal health. A major impact was reported on stillbirth and prematurity. The published literature suggests that the economic setting influenced the effects of imposed mitigation measures with a more severe effect in low-income countries., Objectives: Our objective is to compare pregnancy outcomes at the only tertiary Maternity Hospital in Bihor County-Romania before and during the COVID-19 pandemic. This study aims to observe and document differences in perinatal outcomes across these periods, without inferring direct causation related to the pandemic or its associated restrictions., Materials and Methods: We used data from the registries of Public Health Services Bihor to conduct a retrospective cohort analysis of preterm births and stillbirths during the COVID-19 pandemic in Bihor County, Romania. Pregnancy outcomes were compared between the pandemic period (March 2020-February 2022) to the corresponding historical pre-COVID-19 period (March 2018-February 2020). Maternal socio-demographic variables and neonatal characteristics of these periods were also examined., Results: The COVID-19 pandemic period was associated with an increase in the stillbirth rate (RR: 1.53, 95% CI, 1.05-2.23). Preterm birth was significantly impacted during this period and showed changes when analyzing gestational age (RR: 0.88, 95% CI, 0.79-0.96) or birth weight (RR: 0.91, 95% CI, 0.82-1.00). The main cause of stillbirth was intrauterine asphyxia due to placental causes (67.6%) or cord pathology (12.6%), the most frequently encountered maternal pathology was cardiovascular (28.3%) or infectious (21.7%). Our study revealed no significant changes in terms of maternal and neonatal characteristics during the two-year pandemic period., Conclusions: Lockdown restrictions in Bihor County, Romania were associated with an increase in stillbirths, whilst preterm birth rate decreased. This raises concerns about whether pandemic policy measures may have led to a failure in identifying and offering proper care for pregnant women who were more likely to experience an antepartum loss. Further studies across the globe are needed in order to integrate comparable data that will help develop adequate protocols and policies for protecting maternal and child health during the next pandemic that will follow., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (© 2024 Galis, Trif, Mudura, Murvai, Daina, Szasz, Negrini, Hatos, Gyarmati, Daly, Mazela and Kramer.)

Published
2024
Full Text
View/download PDF

48. Identifying effect modifiers of systemic hydrocortisone treatment initiated 7-14 days after birth in ventilated very preterm infants on long-term outcome: secondary analysis of a randomised controlled trial.

Author

Halbmeijer NM, Sonnaert M, Swarte RM, Koopman-Esseboom C, van Stuijvenberg M, Mulder-de Tollenaer S, Tan RNGB, Mohns T, Bruneel E, Steiner K, Kramer BW, Debeer A, van Weissenbruch MM, Marechal Y, Blom H, Plaskie K, Offringa M, Merkus MP, Onland W, Leemhuis AG, and van Kaam AH

Subjects
Infant, Infant, Newborn, Humans, Hydrocortisone, Infant, Premature, Infant, Very Low Birth Weight, Glucocorticoids therapeutic use, Infant, Premature, Diseases drug therapy, Bronchopulmonary Dysplasia
Abstract

Objective: To explore clinical effect modifiers of systemic hydrocortisone in ventilated very preterm infants for survival and neurodevelopmental outcome at 2 years' corrected age (CA)., Design: Secondary analysis of a randomised placebo-controlled trial., Setting: Dutch and Belgian neonatal intensive care units., Patients: Infants born <30 weeks' gestational age (GA), ventilator-dependent in the second week of postnatal life., Intervention: Infants were randomly assigned to systemic hydrocortisone (cumulative dose 72.5 mg/kg; n=182) or placebo (n=190)., Main Outcome Measures: The composite of death or neurodevelopmental impairment (NDI) at 2 years' CA and its components. Candidate effect modifiers (GA, small for GA, respiratory index, sex, multiple births, risk of moderate/severe bronchopulmonary dysplasia or death) were analysed using regression models with interaction terms and subpopulation treatment effect pattern plots., Results: The composite outcome was available in 356 (96.0%) of 371 patients (one consent withdrawn). For this outcome, treatment effect heterogeneity was seen across GA subgroups (<27 weeks: hydrocortisone (n=141) vs placebo (n=156), 54.6% vs 66.2%; OR 0.61 (95% CI 0.38 to 0.98); ≥27 weeks: hydrocortisone (n=30) vs placebo (n=31), 66.7% vs 45.2%; OR 2.43 (95% CI 0.86 to 6.85); p=0.02 for interaction). This effect was also found for the component death (<27 weeks: 20.1% vs 32.1%; OR 0.53 (95% CI 0.32 to 0.90); ≥27 weeks: 28.1% vs 16.1%; OR 2.04 (95% CI 0.60 to 6.95); p=0.049 for interaction) but not for the component NDI. No differential treatment effects were observed across other subgroups., Conclusion: This secondary analysis suggests that in infants <27 weeks' GA, systemic hydrocortisone may improve the outcome death or NDI, mainly driven by its component death. There was insufficient evidence for other selected candidate effect modifiers., Competing Interests: Competing interests: AHvK reports grants from the Netherlands Organization for Health Research and Development (ZonMW) during the conduct of the study. No other disclosures were reported., (© Author(s) (or their employer(s)) 2024. No commercial re-use. See rights and permissions. Published by BMJ.)

Published
2024
Full Text
View/download PDF

49. Improved Efficacy of Delayed Treatment with Human Bone Marrow-Derived Stromal Cells Evaluated in Rats with Spinal Cord Injury.

Author

Aguado-Garrido M, García-Rama C, Romero-Ramírez L, Buzoianu-Anguiano V, Pérez-Rizo E, Kramer BW, and Mey J

Subjects
Rats, Humans, Male, Animals, Rats, Wistar, Bone Marrow pathology, Treatment Delay, Spinal Cord pathology, Recovery of Function, Stromal Cells pathology, Spinal Cord Injuries pathology, Mesenchymal Stem Cells physiology, Mesenchymal Stem Cell Transplantation methods
Abstract

The treatment of spinal cord injury (SCI) with uncultivated human bone marrow-derived stromal cells (bmSCs) prepared by negative selection has been proposed to be therapeutically superior to treatment with stem cells that were expanded in vitro. To explore their use in clinical trials, we studied the functional effects of delayed application at 7 days after SCI by testing different doses of bmSCs. Spinal cord contusion injury was induced in adult male Wistar rats at the thoracic level T9. Human bmSCs were prepared by negative selection without expansion in vitro (NeuroCells TM ). Treatment consisted of one 150 µL injection into the cisterna magna containing 0.5 or 2.5 million fresh bmSCs or 2.5 million bmSCs. The recovery of motor functions was evaluated during a surveillance period of six weeks (6 W), during which spinal cords were assessed histologically. Treatment resulted in a significant, dose-dependent therapeutic effect on the recovery of motor performance. The histological analysis revealed a lower degree of axonal degeneration and better survival of neurons and oligodendrocytes in bmSCs treated rats. Our results support delayed intrathecal application of bmSCs prepared by negative selection without expansion in vitro as a treatment of SCI.

Published
2024
Full Text
View/download PDF

50. Qualitative and Quantitative Electrocardiogram Parameters in a Large Cohort of Children with Duchenne Muscle Dystrophy in Comparison with Age-Matched Healthy Subjects: A Study from South India.

Author

Girija MS, Menon D, Polavarapu K, Preethish-Kumar V, Vengalil S, Nashi S, Keertipriya M, Bardhan M, Thomas PT, Kiran VR, Nishadham V, Sadasivan A, Huddar A, Unnikrishnan GK, Inbaraj G, Krishnamurthy A, Kramer BW, Sathyaprabha TN, and Nalini A

Abstract

Background: Electrocardiography (ECG) remains an excellent screening tool for cardiac assessment in Duchenne muscular dystrophy (DMD), but an accurate interpretation requires comparison with age-matched healthy controls., Objective: We examined various ECG parameters in children with DMD, in comparison with age-matched controls., Methods: Standard 12-lead ECG tracings of serial patients were screened for quality and selected. Controls were healthy, age-matched school-going children. Both quantitative and qualitative ECG parameters were analyzed., Results: After screening, ECGs from 252 patients with DMD (8.32 ± 3.12 years, 2-21 years) and ECGs from 151 age-matched healthy controls (9.72 ± 2.23, 4-19 years) were included. A significantly higher heart rate, shorter R-R interval, and taller R wave in V1 were seen across all age group of DMD in comparison to controls, with the difference increasing with age. While QT prolongation was seen in all age groups of DMD, QTc prolongation was seen only at 10 years or more. Incomplete right bundle branch block (RBBB) and pathological Q waves in inferolateral leads were exclusive in DMD, with the latter declining with age. Evidence for left ventricular (LV) pathology, such as tall R in V5/V6, increase in SV1 + RV6 height, and QRS complex duration, were seen only in the age group of 10 years or more., Conclusion: Stratification based on age and comparison with age-matched healthy subjects showed that several ECG parameters were influenced by age, and it also identified age-dependent evidence for LV pathology and QTc prolongation in DMD., Competing Interests: There are no conflicts of interest., (Copyright: © 2024 Annals of Indian Academy of Neurology.)

Published
2024
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results