RÉSUMÉ
BACKGROUND: The severe acute respiratory syndrome corona virus 2 (SARS-CoV-2) pandemic causes a high burden of acute and long-term morbidity and mortality worldwide despite global efforts in containment, prophylaxis, and therapy. With unprecedented speed, the global scientific community has generated pivotal insights into the pathogen and the host response evoked by the infection. However, deeper characterization of the pathophysiology and pathology remains a high priority to reduce morbidity and mortality of coronavirus disease 2019 (COVID-19). METHODS: NAPKON-HAP is a multi-centered prospective observational study with a long-term follow-up phase of up to 36 months post-SARS-CoV-2 infection. It constitutes a central platform for harmonized data and biospecimen for interdisciplinary characterization of acute SARS-CoV-2 infection and long-term outcomes of diverging disease severities of hospitalized patients. RESULTS: Primary outcome measures include clinical scores and quality of life assessment captured during hospitalization and at outpatient follow-up visits to assess acute and chronic morbidity. Secondary measures include results of biomolecular and immunological investigations and assessment of organ-specific involvement during and post-COVID-19 infection. NAPKON-HAP constitutes a national platform to provide accessibility and usability of the comprehensive data and biospecimen collection to global research. CONCLUSION: NAPKON-HAP establishes a platform with standardized high-resolution data and biospecimen collection of hospitalized COVID-19 patients of different disease severities in Germany. With this study, we will add significant scientific insights and provide high-quality data to aid researchers to investigate COVID-19 pathophysiology, pathology, and chronic morbidity.
Sujet(s)
COVID-19 , Humains , COVID-19/épidémiologie , SARS-CoV-2 , Pandémies/prévention et contrôle , Qualité de vie , Allemagne/épidémiologie , Études observationnelles comme sujetRÉSUMÉ
Rationale: Mechanical ventilation (MV) is life-saving but may evoke ventilator-induced lung injury (VILI). Objectives: To explore how the circadian clock modulates severity of murine VILI via the core clock component BMAL1 (basic helix-loop-helix ARNT like 1) in myeloid cells. Methods: Myeloid cell BMAL1-deficient (LysM (lysozyme 2 promoter/enhancer driving cre recombinase expression)Bmal1-/-) or wild-type control (LysMBmal1+/+) mice were subjected to 4 hours MV (34 ml/kg body weight) to induce lung injury. Ventilation was initiated at dawn or dusk or in complete darkness (circadian time [CT] 0 or CT12) to determine diurnal and circadian effects. Lung injury was quantified by lung function, pulmonary permeability, blood gas analysis, neutrophil recruitment, inflammatory markers, and histology. Neutrophil activation and oxidative burst were analyzed ex vivo. Measurements and Main Results: In diurnal experiments, mice ventilated at dawn exhibited higher permeability and neutrophil recruitment compared with dusk. Experiments at CT showed deterioration of pulmonary function, worsening of oxygenation, and increased mortality at CT0 compared with CT12. Wild-type neutrophils isolated at dawn showed higher activation and reactive oxygen species production compared with dusk, whereas these day-night differences were dampened in LysMBmal1-/- neutrophils. In LysMBmal1-/- mice, circadian variations in VILI severity were dampened and VILI-induced mortality at CT0 was reduced compared with LysMBmal1+/+ mice. Conclusions: Inflammatory response and lung barrier dysfunction upon MV exhibit diurnal variations, regulated by the circadian clock. LysMBmal1-/- mice are less susceptible to ventilation-induced pathology and lack circadian variation of severity compared with LysMBmal1+/+ mice. Our data suggest that the internal clock in myeloid cells is an important modulator of VILI.
Sujet(s)
Horloges circadiennes , Lésion pulmonaire induite par la ventilation mécanique , Souris , Animaux , Horloges circadiennes/génétique , Facteurs de transcription ARNTL/génétique , Facteurs de transcription ARNTL/métabolisme , Poumon , Lésion pulmonaire induite par la ventilation mécanique/génétique , Lésion pulmonaire induite par la ventilation mécanique/métabolisme , Rythme circadien/génétique , Souris de lignée C57BLRÉSUMÉ
Introduction: Inflammation is a major pathological feature of pulmonary arterial hypertension (PAH), particularly in the context of inflammatory conditions such as systemic sclerosis (SSc). The endothelin system and anti-endothelin A receptor (ETA) autoantibodies have been implicated in the pathogenesis of PAH, and endothelin receptor antagonists are routinely used treatments for PAH. However, immunological functions of the endothelin B receptor (ETB) remain obscure. Methods: Serum levels of anti-ETB receptor autoantibodies were quantified in healthy donors and SSc patients with or without PAH. Age-dependent effects of overexpression of prepro-endothelin-1 or ETB deficiency on pulmonary inflammation and the cardiovascular system were studied in mice. Rescued ETB-deficient mice (ETB-/-) were used to prevent congenital Hirschsprung disease. The effects of pulmonary T-helper type 2 (Th2) inflammation on PAH-associated pathologies were analyzed in ETB-/- mice. Pulmonary vascular hemodynamics were investigated in isolated perfused mouse lungs. Hearts were assessed for right ventricular hypertrophy. Pulmonary inflammation and collagen deposition were assessed via lung microscopy and bronchoalveolar lavage fluid analyses. Results: Anti-ETB autoantibody levels were elevated in patients with PAH secondary to SSc. Both overexpression of prepro-endothelin-1 and rescued ETB deficiency led to pulmonary hypertension, pulmonary vascular hyperresponsiveness, and right ventricular hypertrophy with accompanying lymphocytic alveolitis. Marked perivascular lymphocytic infiltrates were exclusively found in ETB-/- mice. Following induction of pulmonary Th2 inflammation, PAH-associated pathologies and perivascular collagen deposition were aggravated in ETB-/- mice. Conclusion: This study provides evidence for an anti-inflammatory role of ETB. ETB seems to have protective effects on Th2-evoked pathologies of the cardiovascular system. Anti-ETB autoantibodies may modulate ETB-mediated immune homeostasis.
Sujet(s)
Hypertension artérielle pulmonaire , Récepteur de l'endothéline de type B , Animaux , Autoanticorps/immunologie , Endothéline-1/immunologie , Hypertension artérielle pulmonaire primitive familiale/immunologie , Humains , Hypertrophie ventriculaire droite/immunologie , Inflammation/immunologie , Souris , Hypertension artérielle pulmonaire/immunologie , Récepteur de l'endothéline de type B/immunologie , Sclérodermie systémique/immunologieRÉSUMÉ
Idiopathic pulmonary fibrosis (IPF) is a deadly condition characterized by progressive respiratory dysfunction. Exacerbations due to airway infections are believed to promote disease progression, and presence of Streptococcus in the lung microbiome has been associated with the progression of IPF and mortality. The aim of this study was to analyze the effect of lung fibrosis on susceptibility to pneumococcal pneumonia and bacteremia. The effects of subclinical (low dose) infection with Streptococcus pneumoniae were studied in a well characterized fos-related antigen-2 (Fra-2) transgenic (TG) mouse model of spontaneous, progressive pulmonary fibrosis. Forty-eight hours after transnasal infection with S. pneumoniae, bacterial load was assessed in lung tissue, bronchoalveolar lavage (BAL), blood, and spleen. Leukocyte subsets and cytokine levels were analyzed in BAL and blood. Lung compliance and arterial blood gases were assessed. In contrast to wildtype mice, low dose lung infection with S. pneumoniae in Fra-2 TG mice resulted in substantial pneumonia including weight loss, increased lung bacterial load, and bacteremia. BAL alveolar macrophages were reduced in Fra-2 TG mice compared to the corresponding WT mice. Proinflammatory cytokines and chemokines (IL-1ß, IL-6, TNF-α, and CXCL1) were elevated upon infection in BAL supernatant and plasma of Fra-2 TG mice. Lung compliance was decreased in Fra-2 TG mice following low dose infection with S. pneumoniae. Pulmonary fibrosis increases susceptibility to pneumococcal pneumonia and bacteremia possibly via impaired alveolar bacterial clearance.
Sujet(s)
Antigène-2 apparenté à fos , Macrophages alvéolaires , Pneumonie à pneumocoques , Fibrose pulmonaire , Streptococcus pneumoniae/métabolisme , Animaux , Cytokines/génétique , Cytokines/métabolisme , Modèles animaux de maladie humaine , Prédisposition aux maladies , Antigène-2 apparenté à fos/génétique , Antigène-2 apparenté à fos/métabolisme , Macrophages alvéolaires/métabolisme , Macrophages alvéolaires/microbiologie , Macrophages alvéolaires/anatomopathologie , Souris , Souris transgéniques , Pneumonie à pneumocoques/génétique , Pneumonie à pneumocoques/métabolisme , Pneumonie à pneumocoques/microbiologie , Pneumonie à pneumocoques/anatomopathologie , Fibrose pulmonaire/génétique , Fibrose pulmonaire/métabolisme , Fibrose pulmonaire/microbiologie , Fibrose pulmonaire/anatomopathologieRÉSUMÉ
Respiratory infections caused by multidrug-resistant Acinetobacter baumannii are difficult to treat and associated with high mortality among critically ill hospitalized patients. Bacteriophages (phages) eliminate pathogens with high host specificity and efficacy. However, the lack of appropriate preclinical experimental models hampers the progress of clinical development of phages as therapeutic agents. Therefore, we tested the efficacy of a purified lytic phage, vB_AbaM_Acibel004, against multidrug-resistant A. baumannii clinical isolate RUH 2037 infection in immunocompetent mice and a human lung tissue model. Sham- and A. baumannii-infected mice received a single-dose of phage or buffer via intratracheal aerosolization. Group-specific differences in bacterial burden, immune and clinical responses were compared. Phage-treated mice not only recovered faster from infection-associated hypothermia but also had lower pulmonary bacterial burden, lower lung permeability, and cytokine release. Histopathological examination revealed less inflammation with unaffected inflammatory cellular recruitment. No phage-specific adverse events were noted. Additionally, the bactericidal effect of the purified phage on A. baumannii was confirmed after single-dose treatment in an ex vivo human lung infection model. Taken together, our data suggest that the investigated phage has significant potential to treat multidrug-resistant A. baumannii infections and further support the development of appropriate methods for preclinical evaluation of antibacterial efficacy of phages.
Sujet(s)
Infections à Acinetobacter/thérapie , Acinetobacter baumannii , Myoviridae/physiologie , Phagothérapie , Pneumopathie bactérienne/thérapie , Infections à Acinetobacter/immunologie , Infections à Acinetobacter/microbiologie , Infections à Acinetobacter/anatomopathologie , Acinetobacter baumannii/effets des médicaments et des substances chimiques , Acinetobacter baumannii/virologie , Animaux , Antibactériens/pharmacologie , Cytokines/métabolisme , Multirésistance bactérienne aux médicaments , Femelle , Humains , Poumon/immunologie , Poumon/microbiologie , Poumon/anatomopathologie , Souris , Souris de lignée C57BL , Phagothérapie/effets indésirables , Pneumopathie bactérienne/immunologie , Pneumopathie bactérienne/microbiologie , Pneumopathie bactérienne/anatomopathologieRÉSUMÉ
BACKGROUND: Community-acquired pneumonia and associated sepsis cause high mortality despite antibiotic treatment. Uncontrolled inflammatory host responses contribute to the unfavorable outcome by driving lung and extrapulmonary organ failure. The complement fragment C5a holds significant proinflammatory functions and is associated with tissue damage in various inflammatory conditions. The authors hypothesized that C5a concentrations are increased in pneumonia and C5a neutralization promotes barrier stabilization in the lung and is protective in pneumococcal pulmonary sepsis. METHODS: The authors investigated regulation of C5a in pneumonia in a prospective patient cohort and in experimental pneumonia. Two complementary models of murine pneumococcal pneumonia were applied. Female mice were treated with NOX-D19, a C5a-neutralizing L-RNA-aptamer. Lung, liver, and kidney injury and the inflammatory response were assessed by measuring pulmonary permeability (primary outcome), pulmonary and blood leukocytes, cytokine concentrations in lung and blood, and bacterial load in lung, spleen, and blood, and performing histologic analyses of tissue damage, apoptosis, and fibrin deposition (n = 5 to 13). RESULTS: In hospitalized patients with pneumonia (n = 395), higher serum C5a concentrations were observed compared to healthy subjects (n = 24; 6.3 nmol/l [3.9 to 10.0] vs. 4.5 nmol/l [3.8 to 6.6], median [25 to 75% interquartile range]; difference: 1.4 [95% CI, 0.1 to 2.9]; P = 0.029). Neutralization of C5a in mice resulted in lower pulmonary permeability in pneumococcal pneumonia (1.38 ± 0.89 vs. 3.29 ± 2.34, mean ± SD; difference: 1.90 [95% CI, 0.15 to 3.66]; P = 0.035; n = 10 or 11) or combined severe pneumonia and mechanical ventilation (2.56 ± 1.17 vs. 7.31 ± 5.22; difference: 4.76 [95% CI, 1.22 to 8.30]; P = 0.011; n = 9 or 10). Further, C5a neutralization led to lower blood granulocyte colony-stimulating factor concentrations and protected against sepsis-associated liver injury. CONCLUSIONS: Systemic C5a is elevated in pneumonia patients. Neutralizing C5a protected against lung and liver injury in pneumococcal pneumonia in mice. Early neutralization of C5a might be a promising adjunctive treatment strategy to improve outcome in community-acquired pneumonia.
Sujet(s)
Aptamères nucléotidiques/administration et posologie , Complément C5a/antagonistes et inhibiteurs , Pneumonie à pneumocoques/sang , Pneumonie à pneumocoques/prévention et contrôle , Sepsie/sang , Sepsie/prévention et contrôle , Animaux , Anticorps neutralisants/administration et posologie , Marqueurs biologiques/sang , Études de cohortes , Complément C5a/métabolisme , Femelle , Facteurs immunologiques/antagonistes et inhibiteurs , Facteurs immunologiques/sang , Souris , Souris de lignée C57BL , Études prospectivesRÉSUMÉ
PURPOSE OF REVIEW: In this brief review, we discuss the current epidemiological data and latest results from basic research on the cardiovascular sequelae after lower respiratory tract infection. RECENT FINDINGS: Novel epidemiological evidence substantiates the association between pneumonia and subsequent cardiovascular events (CVEs) in the short- and long-term after viral or bacterial acute infection. Biomarkers such as cardiac troponin or coronary artery calcium may represent useful predictive tools for the detection of cardiac involvement during and after pneumonia. Particularly, Streptococcus pneumoniae directly cause cardiac damage by invasion into the myocardium and formation of microscopic lesions finally leading to the development of cardiac scarring in rodents and nonhuman primates. In addition, a causal relationship between pulmonary inflammation and atherosclerotic plaque formation in systemic arteries has emerged that appears to involve a mechanistic role for neutrophil granulocytes. However, many key pathomechanisms by which pneumonia may trigger or promote subsequent CVEs still remain unclear. SUMMARY: Pneumonia may deleteriously impact cardiovascular function. Direct cardiomyocyte destruction by pathogens as well as host inflammatory response associated effects including atherosclerotic plaque development and/or rupture have been observed. Details of underlying mechanisms need to be further investigated to deliver future perspectives for the prevention of CVEs subsequent to pneumonia.
Sujet(s)
Maladies cardiovasculaires/épidémiologie , Maladies cardiovasculaires/microbiologie , Pneumopathie infectieuse/complications , Animaux , Marqueurs biologiques/sang , Maladies cardiovasculaires/sang , Humains , Inflammation/microbiologie , Pneumopathie infectieuse/microbiologie , Pneumonie à pneumocoques/complications , Troponine/sangRÉSUMÉ
The emergence of multidrug-resistant bacteria constitutes a great challenge for modern medicine, recognized by leading medical experts and politicians worldwide. Rediscovery and implementation of bacteriophage therapy by Western medicine might be one solution to the problem of increasing antibiotic failure. In some Eastern European countries phage therapy is used for treating infectious diseases. However, while the European Medicines Agency (EMA) advised that the development of bacteriophage-based therapies should be expedited due to its significant potential, EMA emphasized that phages cannot be recommended for approval before efficacy and safety have been proven by appropriately designed preclinical and clinical trials. More evidence-based data is required, particularly in the areas of pharmacokinetics, repeat applications, immunological reactions to the application of phages as well as the interactions and effects on bacterial biofilms and organ-specific environments. In this brief review we summarize advantages and disadvantages of phage therapy and discuss challenges to the establishment of phage therapy as approved treatment for multidrug-resistant bacteria.
Sujet(s)
Infections bactériennes/thérapie , Bactériophages/physiologie , Multirésistance bactérienne aux médicaments , Phagothérapie/méthodes , Administration par inhalation , Animaux , Bactéries/effets des médicaments et des substances chimiques , Bactéries/virologie , Essais cliniques comme sujet , Europe , Humains , SourisRÉSUMÉ
BACKGROUND: Community-acquired pneumonia (CAP) remains a major cause of death worldwide. Mechanisms underlying the detrimental outcome despite adequate antibiotic therapy and comorbidity management are still not fully understood. METHODS: To model timely versus delayed antibiotic therapy in patients, mice with pneumococcal pneumonia received ampicillin twice a day starting early (24 h) or late (48 h) after infection. Clinical readouts and local and systemic inflammatory mediators after early and late antibiotic intervention were examined. RESULTS: Early antibiotic intervention rescued mice, limited clinical symptoms and restored fitness, whereas delayed therapy resulted in high mortality rates. Recruitment of innate immune cells remained unaffected by antibiotic therapy. However, both early and late antibiotic intervention dampened local levels of inflammatory mediators in the alveolar spaces. Early treatment protected from barrier breakdown, and reduced levels of vascular endothelial growth factor (VEGF) and perivascular and alveolar edema formation. In contrast, at 48 h post infection, increased pulmonary leakage was apparent and not reversed by late antibiotic treatment. Concurrently, levels of VEGF remained high and no beneficial effect on edema formation was evident despite therapy. Moreover, early but not late treatment protected mice from a vast systemic inflammatory response. CONCLUSIONS: Our data show that only early antibiotic therapy, administered prior to breakdown of the alveolar-capillary barrier and systemic inflammation, led to restored fitness and rescued mice from fatal streptococcal pneumonia. The findings highlight the importance of identifying CAP patients prior to lung barrier failure and systemic inflammation and of handling CAP as a medical emergency.
Sujet(s)
Antibactériens/administration et posologie , Pneumonie à pneumocoques/traitement médicamenteux , Pneumonie à pneumocoques/mortalité , Facteurs temps , Ampicilline/administration et posologie , Ampicilline/usage thérapeutique , Analyse de variance , Animaux , Antibactériens/usage thérapeutique , Liquide de lavage bronchoalvéolaire/cytologie , Chimiokine CCL2/analyse , Chimiokine CCL2/sang , Chimiokine CCL3/analyse , Chimiokine CCL3/sang , Modèles animaux de maladie humaine , Test ELISA/méthodes , Femelle , Souris , Souris de lignée C57BL , Statistique non paramétrique , Streptococcus pneumoniae/effets des médicaments et des substances chimiques , Streptococcus pneumoniae/pathogénicité , Analyse de survieRÉSUMÉ
BACKGROUND: Antibiotic exposure alters the microbiota, which can impact the inflammatory immune responses. Critically ill patients frequently receive antibiotic treatment and are often subjected to mechanical ventilation, which may induce local and systemic inflammatory responses and development of ventilator-induced lung injury (VILI). The aim of this study was to investigate whether disruption of the microbiota by antibiotic therapy prior to mechanical ventilation affects pulmonary inflammatory responses and thereby the development of VILI. METHODS: Mice underwent 6-8 weeks of enteral antibiotic combination treatment until absence of cultivable bacteria in fecal samples was confirmed. Control mice were housed equally throughout this period. VILI was induced 3 days after completing the antibiotic treatment protocol, by high tidal volume (HTV) ventilation (34 ml/kg; positive end-expiratory pressure = 2 cmH2O) for 4 h. Differences in lung function, oxygenation index, pulmonary vascular leakage, macroscopic assessment of lung injury, and leukocyte and lymphocyte differentiation were assessed. Control groups of mice ventilated with low tidal volume and non-ventilated mice were analyzed accordingly. RESULTS: Antibiotic-induced microbiota depletion prior to HTV ventilation led to aggravation of VILI, as shown by increased pulmonary permeability, increased oxygenation index, decreased pulmonary compliance, enhanced macroscopic lung injury, and increased cytokine/chemokine levels in lung homogenates. CONCLUSIONS: Depletion of the microbiota by broad-spectrum antibiotics prior to HTV ventilation renders mice more susceptible to developing VILI, which could be clinically relevant for critically ill patients frequently receiving broad-spectrum antibiotics.
Sujet(s)
Antibactériens/effets indésirables , Microbiote/effets des médicaments et des substances chimiques , Lésion pulmonaire induite par la ventilation mécanique/physiopathologie , Animaux , Antibactériens/usage thérapeutique , Gazométrie sanguine/méthodes , Modèles animaux de maladie humaine , Poumon/physiopathologie , Souris , Souris de lignée C57BL , Ventilation artificielle/effets indésirables , Ventilation artificielle/méthodes , Lésion pulmonaire induite par la ventilation mécanique/complications , Lésion pulmonaire induite par la ventilation mécanique/traitement médicamenteuxRÉSUMÉ
BACKGROUND: Community-acquired pneumonia (CAP) is a significant cause of morbidity and mortality worldwide. Despite effective antimicrobial therapy, CAP can induce pulmonary endothelial hyperpermeability resulting in life-threatening lung failure due to an exaggerated host-pathogen interaction. Treatment of acute lung injury is mainly supportive because key elements of inflammation-induced barrier disruption remain undetermined. Angiopoietin-1 (Ang-1)-mediated Tie2 activation reduces, and the Ang-1 antagonist Ang-2 increases, inflammation and endothelial permeability in sepsis. Vasculotide (VT) is a polyethylene glycol-clustered Tie2-binding peptide that mimics the actions of Ang-1. The aim of our study was to experimentally test whether VT is capable of diminishing pneumonia-induced lung injury. METHODS: VT binding and phosphorylation of Tie2 were analyzed using tryptophan fluorescence spectroscopy and phospho-Tie-2 enzyme-linked immunosorbent assay. Human and murine lung endothelial cells were investigated by immunofluorescence staining and electric cell-substrate impedance sensing. Pulmonary hyperpermeability was quantified in VT-pretreated, isolated, perfused, and ventilated mouse lungs stimulated with the pneumococcal exotoxin pneumolysin (PLY). Furthermore, Streptococcus pneumoniae-infected mice were therapeutically treated with VT. RESULTS: VT showed dose-dependent binding and phosphorylation of Tie2. Pretreatment with VT protected lung endothelial cell monolayers from PLY-induced disruption. In isolated mouse lungs, VT decreased PLY-induced pulmonary permeability. Likewise, therapeutic treatment with VT of S. pneumoniae-infected mice significantly reduced pneumonia-induced hyperpermeability. However, effects by VT on the pulmonary or systemic inflammatory response were not observed. CONCLUSIONS: VT promoted pulmonary endothelial stability and reduced lung permeability in different models of pneumococcal pneumonia. Thus, VT may provide a novel therapeutic perspective for reduction of permeability in pneumococcal pneumonia-induced lung injury.
Sujet(s)
Perméabilité capillaire/effets des médicaments et des substances chimiques , Poumon/effets des médicaments et des substances chimiques , Fragments peptidiques/pharmacocinétique , Animaux , Infections communautaires/traitement médicamenteux , Modèles animaux de maladie humaine , Cellules endothéliales/métabolisme , Femelle , Souris , Souris de lignée C57BL , Fragments peptidiques/usage thérapeutique , Pneumonie à pneumocoques/traitement médicamenteux , Spectrométrie de fluorescence/méthodes , Statistique non paramétrique , Streptococcus pneumoniae/métabolisme , Streptococcus pneumoniae/pathogénicitéRÉSUMÉ
Dysregulation of the innate immune system drives lung injury and its systemic sequelae due to breakdown of vascular barrier function, harmful hyperinflammation and microcirculatory failure, which contribute to the unfavourable outcome of patients with severe pneumonia. A variety of promising therapeutic targets have been identified and numerous innovative therapeutic approaches demonstrated to improve lung injury in experimental preclinical studies. However, at present specific preventive or curative strategies for the treatment of lung failure in pneumonia in addition to antibiotics are still missing. The aim of this mini-review is to give a short overview of some, but not all, adjuvant therapeutic strategies for pneumonia and its most important complications, sepsis and acute respiratory distress syndrome, and briefly discuss future perspectives.
Sujet(s)
Antibactériens/usage thérapeutique , Facteurs immunologiques/usage thérapeutique , Poumon/effets des médicaments et des substances chimiques , Pneumopathie bactérienne/thérapie , Transplantation de cellules souches , Interactions hôte-pathogène , Humains , Immunité innée/effets des médicaments et des substances chimiques , Poumon/immunologie , Poumon/microbiologie , Poumon/anatomopathologie , Pneumopathie bactérienne/complications , Pneumopathie bactérienne/diagnostic , Pneumopathie bactérienne/immunologie , Pneumopathie bactérienne/microbiologie , Résultat thérapeutiqueRÉSUMÉ
Structured hydrogels showing form stability and elastic properties individually tailorable on different length scales are accessible in a one-step process. They support cell adhesion and differentiation and display growing pore size during degradation. In vivo experiments demonstrate their efficacy in biomaterial-induced bone regeneration, not requiring addition of cells or growth factors.
Sujet(s)
Implant résorbable , Matériaux biocompatibles/synthèse chimique , Régénération osseuse , Hydrogels/synthèse chimique , Animaux , Matériaux biocompatibles/composition chimique , Matériaux biocompatibles/usage thérapeutique , Régénération osseuse/physiologie , Cal osseux/physiopathologie , Adhérence cellulaire/physiologie , Différenciation cellulaire/physiologie , Lignée cellulaire , Survie cellulaire , Cellules cultivées , Élasticité , Femelle , Fémur/traumatismes , Fibroblastes/physiologie , Gélatine/composition chimique , Humains , Hydrogels/composition chimique , Hydrogels/usage thérapeutique , Test de matériaux , Cellules souches mésenchymateuses/physiologie , Stimulation physique/instrumentation , Stimulation physique/méthodes , Porosité , Rat Sprague-DawleyRÉSUMÉ
Multiple synostoses syndrome 2 (SYNS2) is a rare genetic disease characterized by multiple fusions of the joints of the extremities, like phalangeal joints, carpal and tarsal joints or the knee and elbows. SYNS2 is caused by point mutations in the Growth and Differentiation Factor 5 (GDF5), which plays an essential role during skeletal development and regeneration. We selected one of the SYNS2-causing GDF5 mutations, p.N445T, which is known to destabilize the interaction with the Bone Morphogenetic Protein (BMP) antagonist NOGGIN (NOG), in order to generate the superagonistic GDF5 variant GDF5(N445T). In this study, we tested its capacity to support regeneration in a rat critical-sized defect model in vivo. MicroCT and histological analyses indicate that GDF5(N445T)-treated defects show faster and more efficient healing compared to GDF5 wild type (GDF5(wt))-treated defects. Microarray-based gene expression and quantitative PCR analyses from callus tissue point to a specific acceleration of the early phases of bone healing, comprising the inflammation and chondrogenesis phase. These results support the concept that disease-deduced growth factor variants are promising lead structures for novel therapeutics with improved clinical activities.
Sujet(s)
Facteur-5 de croissance et de différenciation/physiologie , Synostose/physiopathologie , Cicatrisation de plaie , Animaux , Femelle , Facteur-5 de croissance et de différenciation/génétique , Humains , Mutation ponctuelle , Rats , Rat Sprague-Dawley , Synostose/génétique , Transcription génétiqueRÉSUMÉ
During hematoma formation following injury, an inflammatory reaction ensues as an initial step in the healing process. As granulation tissue matures, revascularization is a prerequisite for successful healing. The hypothesis of this study was that scarless tissue reconstitution in the regenerative bone healing process is dependent on a balanced immune reaction that initiates revasculatory steps. To test this hypothesis, cellular composition and expression profiles of a bone hematoma (regenerative, scarless) was compared with a muscle soft tissue hematoma (healing with a scar) in a sheep model. Upregulation of regulatory T helper cells and anti-inflammatory cytokine expression (IL-10) coincided with an upregulation of angiogenic factors (HIF1α and HIF1α regulated genes) in the regenerative bone hematoma but not in the soft tissue hematoma. These results indicate that the timely termination of inflammation and early onset of revascularization are interdependent and essential for a regenerative healing process. Prolonged pro-inflammatory signaling occurring in a delayed bone-healing model supports the finding that timely termination of inflammation furthers the regenerative process. Differing cellular compositions are due to different cell sources invading the hematoma, determining the ensuing cytokine expression profile and thus paving the path for regenerative healing in bone or the formation of scar tissue in muscle injury.
Sujet(s)
Os et tissu osseux/anatomopathologie , Néovascularisation physiologique/immunologie , Cicatrisation de plaie/immunologie , Agents angiogéniques/métabolisme , Animaux , Vaisseaux sanguins/croissance et développement , Moelle osseuse/anatomopathologie , Cytokines/métabolisme , Femelle , Hématome/immunologie , Hématome/anatomopathologie , Sous-unité alpha du facteur-1 induit par l'hypoxie/génétique , Sous-unité alpha du facteur-1 induit par l'hypoxie/métabolisme , Inflammation/immunologie , Inflammation/anatomopathologie , Sous-unité alpha du récepteur à l'interleukine-2/métabolisme , Activation des lymphocytes/immunologie , Numération des lymphocytes , Ostéotomie , Antigènes CD31/métabolisme , Ovis , Transduction du signal/génétique , Lymphocytes T auxiliaires/immunologie , Lymphocytes T régulateurs/immunologie , Facteurs temps , Régulation positiveRÉSUMÉ
The cytosolic nucleotide oligomerization domain (NOD)-like receptors NOD1 and NOD2 are important contributors to the intracellular recognition of pathogens including Chlamydophila pneumoniae, but little is known about their influence on allergen-induced airway inflammation. In BALB/c mice, we observed that infection with C. pneumoniae before systemic sensitization with ovalbumin (OVA) and local OVA airway exposure diminished airway hyperresponsiveness (AHR). Thus, the impact of the NOD1 agonist FK156 and the NOD2 agonist muramyl dipeptide given 6 hours before each sensitization or airway challenge was evaluated regarding AHR, OVA-specific plasma immunoglobulins, bronchoalveolar lavage fluid differentials, and cytokines. Spleen dendritic cells of FK156-treated mice were isolated and cocultured with OVA-specific T cells isolated from DO11.10 mice, and T-cell proliferation was quantified after OVA restimulation. T-cell proliferation was investigated in vivo in lungs and lymph nodes of FK156-treated and OVA-exposed DO11.10 mice. FK156, but not muramyl dipeptide, reduced AHR and pulmonary eosinophilic infiltration if given before OVA sensitization or challenge, whereas T-helper (Th)2 cytokines were not diminished. Dendritic cells from FK156-treated mice evoked less OVA-specific T-cell proliferation as compared with solvent-treated controls. Similarly, antigen-specific T-cell activation in lung tissue was diminished after FK156 treatment. We conclude that NOD1 activation reduced AHR in allergen-induced lung inflammation, which was accompanied by a reduction of allergen-specific T-cell proliferation.
Sujet(s)
Allergènes/immunologie , Hyperréactivité bronchique/immunologie , Protéine adaptatrice de signalisation NOD1/immunologie , Lymphocytes auxiliaires Th2/immunologie , Animaux , Prolifération cellulaire , Chlamydophila pneumoniae/immunologie , Cytokines/immunologie , Cellules dendritiques/immunologie , Femelle , Immunoglobulines/immunologie , Inflammation/immunologie , Ligature , Poumon/immunologie , Noeuds lymphatiques/immunologie , Activation des lymphocytes/immunologie , Souris , Souris de lignée BALB C , Protéine adaptatrice de signalisation NOD2/immunologie , Ovalbumine/immunologie , Appareil respiratoire/immunologieRÉSUMÉ
INTRODUCTION: Local application of bone morphogenetic proteins (BMPs) at the fracture site is known to stimulate bone regeneration. However, recent studies illustrate that the BMP-initiated mineralization may be enhanced by additional mechanical stimulation. Therefore, bone healing was monitored in vivo in order to investigate the effect of mechanical loading on the initiation and maturation of mineralization after cytokine treatment. We hypothesized that the mechanical stimulation would further enhance the efficacy of BMP2 treatment. METHOD: Female Sprague-Dawley rats underwent a 5-mm defect, stabilized with an external fixator. Type I collagen scaffolds containing 50 µg of BMP2 diluted in a solvent or solvent only were placed into the defects. The BMP2-treated specimens and control specimens were then each divided into two groups: one that underwent mechanical loading and a nonloaded group. In vivo loading began immediately after surgery and continued once per week for the entire 6-week experimental period. For all groups, the newly formed callus tissue was quantitatively evaluated first by in vivo microcomputed tomography at 2, 4, and 6 weeks and further by histologic or histomorphometric analysis at 6 weeks postoperation. RESULTS: Mechanical stimulation with BMP2 treatment significantly enhanced mineralized tissue volume and mineral content at 2 weeks. Histological analysis demonstrated a significantly greater area of fibrous connective tissue including bone marrow in the stimulated group, suggesting reconstitution of the endosteal canal and more advanced bone remodeling present in the mechanical loaded group. Both groups receiving BMP2 underwent massive bone formation, achieving bony bridging after only 2 weeks, while both control groups, receiving solvent only, revealed a persisting nonunion, filled with fibrous connective tissue, prolapsed muscle tissue, and a sealed medullary canal at week 6. CONCLUSION: Mechanical loading further enhanced the efficacy of BMP2 application evidenced by increased mineralized tissue volume and mineralization at the stage of bony callus bridging. These data suggest that already a minimal amount of mechanical stimulation through load bearing or exercise may be a promising adjunct stimulus to enhance the efficacy of cytokine treatment in segmental defects. Further studies are required to elucidate the mechanistic interplay between mechanical and biological stimuli.
Sujet(s)
Protéine morphogénétique osseuse de type 2/administration et posologie , Fractures du fémur/traitement médicamenteux , Fractures du fémur/physiopathologie , Consolidation de fracture/effets des médicaments et des substances chimiques , Cals vicieux/traitement médicamenteux , Cals vicieux/physiopathologie , Mécanotransduction cellulaire , Animaux , Calcification physiologique/effets des médicaments et des substances chimiques , Synergie des médicaments , Femelle , Consolidation de fracture/physiologie , Stimulation physique/méthodes , Rats , Rat Sprague-Dawley , Résultat thérapeutiqueRÉSUMÉ
This study addresses the hypothesis that callus formation, patterning, and mineralisation are impaired during the early phase of critical sized bone defect healing, and may relate to inter-fragmentary tissue strains within the bone defect area. Twenty four 12 week old Sprague Dawley rats were used for this study. They were divided into two groups defined by the femur bone defect size: (i) 1 mm resulting in normal healing (NH), and (ii) a large sized 5 mm defect resulting in critical healing (CH). Callus formation, patterning, and mineralisation kinetics in both groups were examined in the periosteal and osteotomy gap regions using a novel longitudinal study setup. Finite element analyses on µCT generated tomograms were used to determine inter-fragmentary tissue strain patterns and compared to callus formation and patterning over the course of time. Using a novel longitudinal study technique with µCT, in vivo tracking and computer simulation approaches, this study demonstrates that: (i) periosteal bone formation and patterning are significantly influenced by bone defect size as early as 2 weeks; (ii) osteotomy gap callus formation and patterning are influenced by bone defect size, and adapt towards a non-union in critical cases by deviating into a medullary formation route as early as 2 weeks after osteotomy; (iii) the new bone formation in the osteotomy gap enclosing the medullary cavity in the CH group is highly mineralised; (iv) inter-fragmentary strain patterns predicted during the very early soft callus tissue phase (less than 2 weeks) are concurrent with callus formation and patterning at later stages. In conclusion, bone defect size influences early onset of critical healing patterns.
Sujet(s)
Cal osseux/physiologie , Fémur/physiologie , Cicatrisation de plaie , Animaux , Femelle , Fémur/imagerie diagnostique , Fémur/chirurgie , Ostéotomie , Périoste/physiologie , Rats , Rat Sprague-Dawley , Contrainte mécanique , Microtomographie aux rayons XRÉSUMÉ
Bone healing commences with an inflammatory reaction which initiates the regenerative healing process leading in the end to reconstitution of bone. An unbalanced immune reaction during this early bone healing phase is hypothesized to disturb the healing cascade in a way that delays bone healing and jeopardizes the successful healing outcome. The immune cell composition and expression pattern of angiogenic factors were investigated in a sheep bone osteotomy model and compared to a mechanically-induced impaired/delayed bone healing group. In the impaired/delayed healing group, significantly higher T cell percentages were present in the bone hematoma and the bone marrow adjacent to the osteotomy gap when compared to the normal healing group. This was mirrored in the higher cytotoxic T cell percentage detected under delayed bone healing conditions indicating longer pro-inflammatory processes. The highly activated periosteum adjourning the osteotomy gap showed lower expression of hematopoietic stem cell markers and angiogenic factors such as heme oxygenase and vascular endothelial growth factor. This indicates a deferred revascularization of the injured area due to ongoing pro-inflammatory processes in the delayed healing group. Results from this study suggest that there are unfavorable immune cells and factors participating in the initial healing phase. In conclusion, identifying beneficial aspects may lead to promising therapeutical approaches that might benefit further by eliminating the unfavorable factors.
Sujet(s)
Os et tissu osseux/anatomopathologie , Os et tissu osseux/physiopathologie , Inflammation/anatomopathologie , Régénération/physiologie , Cicatrisation de plaie , Agents angiogéniques/métabolisme , Animaux , Marqueurs biologiques/métabolisme , Moelle osseuse/anatomopathologie , Régénération osseuse , Os et tissu osseux/immunologie , Os et tissu osseux/chirurgie , Cytotoxicité immunologique , Femelle , Hématome/anatomopathologie , Cellules souches hématopoïétiques/anatomopathologie , Numération des lymphocytes , Lymphocytes/anatomopathologie , Ostéotomie , Périoste/anatomopathologie , Périoste/physiopathologie , Périoste/chirurgie , Ovis , Lymphocytes T/anatomopathologieRÉSUMÉ
OBJECTIVES: The hypothesis of the study was that the incidence of pin loosening and pin infection would increase, whereas the general stability of the pin-bone interface would decrease with ongoing implantation time. The aim of this study was to analyze the biologic reactions of the bone tissue adjacent to the pin to determine the relationship among the osseous anchorage of pins, the incidence of infections, and the histologic appearance. METHODS: Three groups of sheep received a tibial osteotomy stabilized by external fixators. The pin-bone interface was analyzed biomechanically, radiologically, microbiologically, and histologically after 3, 6, and 9 weeks. RESULTS/CONCLUSIONS: Contrary to common opinion, pin anchorage was not altered biomechanically throughout the 9 weeks of the study. This effect might be attributed to an increasing remodeling found in the callus and cortex around the pins and was likely assisted by a strict pin care routine and a low infection rate.