Apoptosis and proliferation in lungs of ventilated and oxygen-treated preterm infants

May, Michael J.; Strobel, Pablo; Preisshofen, T; Seidenspinner, Silvia; Marx, Alexander; Speer, C P

doi:10.1183/09031936.03.00038403

Cited by 60 publications

(48 citation statements)

References 36 publications

(60 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Apparently, the development of BPD can be primed by exposure to prenatal pulmonary inflammation, which can be aggravated by postnatal events (8,52,53). Structural changes by apoptosis of parenchymal cells were induced in the course of injury and inflammation in the airways and lungs (54). Apparently, alveolar inflammation affects endothelial function and angiogenesis (8).…”

Section: Discussionmentioning

confidence: 99%

Decreased Expression of Angiogenic Factors in Placentas with Chorioamnionitis after Preterm Birth

et al. 2005

View full text Add to dashboard Cite

Chorioamnionitis and funisitis are associated with neonatal morbidity and mortality. We hypothesized that chorioamnionitis may stress fetal endothelium, activate proinflammatory gene transcription. and affect angiogenic homeostasis in fetal capillaries. Placentas from preterm infants were stained for heat-shock protein 70, nuclear factor-B, hypoxia-inducible factor-1␣, and vascular endothelial growth factor (VEGF). VEGF receptors (VEGF-R) 1 and 2 as well as the receptor tyrosine kinase with immunoglobulin and epidermal growth factor homology domains (TIE-2), which is involved in vascular remodeling, were quantified. Immunohistochemistry was analyzed by counting positive capillaries in placental terminal villi. Staining intensity was quantified by a three-step semiquantitative scale. The samples were divided into three matched groups according to histology: chorioamnionitis with funisitis ("funisitis"), chorioamnionitis without funisitis ("chorioamnionitis"), and control group with no inflammation. In tissues from the funisitis or chorioamnionitis group, heat-shock protein 70 expression was increased over the control group. More nuclear factor-B-positive nuclei of endothelial cells in capillaries were counted in the funisitis and chorioamnionitis groups. Expression of VEGF and VEGF-R1 and -R2 were reduced in cases of funisitis or chorioamnionitis in comparison with controls. Hypoxia-inducible factor-1␣ expression tended to be slightly lower in the funisitis and chorioamnionitis groups but did not reach statistical significance. We speculate that cellular stress and changes in angiogenic homeostasis induced by proinflammatory activation of fetal endothelium in chorioamnionitis may not be limited to the placenta but may also involve other fetal organs. (Pediatr Res 58: 607-612, 2005) Abbreviations BPD, bronchopulmonary dysplasia CI, confidence interval HIF-1␣ hypoxia-inducible factor-1␣ HRP, horseradish peroxidase HSP70, heat-shock protein 70 IL, interleukin NF-B, nuclear factor-B TIE-2, tyrosine kinase with immunoglobulin and epidermal growth factor homology domains-2 VEGF, vascular endothelial growth factor VEGF-R, vascular endothelial growth factor receptor Chorioamnionitis is very common in preterm birth (1). Microbial infection of the amnion and chorion are detected in 60% of all preterm deliveries (2). Funisitis is diagnosed as an infiltration of neutrophils in the umbilical cord vessels (3) and can be considered as a progression of chorioamnionitis with systemic inflammatory response syndrome of the fetus (4). Although fetal inflammation reduces the incidence of respiratory distress syndrome (5,6) and increases the survival of preterm infants (7), the fetal inflammatory response has been associated with increased neonatal morbidity. The mechanisms by which fetal inflammation increases the incidence of bronchopulmonary dysplasia (BPD) (8), retinopathy of prematurity (9), intracranial hemorrhage (10), cerebral palsy, and adverse neurodevelopmental outcome (11-13) are not fully understood. Recently, a new poten...

show abstract

Section: Discussionmentioning

confidence: 99%

Decreased Expression of Angiogenic Factors in Placentas with Chorioamnionitis after Preterm Birth

et al. 2005

View full text Add to dashboard Cite

show abstract

“…In this rheostat, ceramide stimulates apoptosis and cell cycle arrest, and sphingosine-1-phosphate stimulates cell survival and proliferation. Increased apoptosis has been found in epithelial cells of BPD patients [8] and in animal models of BPD [9], and total lung ceramide levels are upregulated in hyperoxia-exposed neonatal rats [10]. To date, no detailed analysis of the sphingolipid metabolome in the hyperoxia-induced BPD model [11] has been reported.…”

Section: Introductionmentioning

confidence: 99%

Amelioration of hyperoxia-induced lung injury using a sphingolipid-based intervention

et al. 2012

View full text Add to dashboard Cite

The aim of this study was to characterise lung function and bronchoalveolar lavage sphingolipid profile in newborn mice during hyperoxia exposure and recovery in room air, and to examine the effect of D-sphingosine supplementation during recovery.Newborn mice were exposed to 80% oxygen for 4 weeks and allowed to recover in room air for another 4 weeks. Lung function measurements and morphometrical analysis of lung tissue were performed and bronchoalveolar lavage fluid was collected during hyperoxia and recovery with and without D-sphingosine supplementation.Hyperoxia exposure altered lung function, which partially recovered in room air. Lungs had fewer and enlarged alveoli which persisted during recovery. Multiple sphingolipids were significantly increased after hyperoxia. Ceramides were increased after 2 weeks of recovery, but normalised to control values after 4 weeks. The addition of D-sphingosine during the first 5 days of recovery accelerated the normalisation of ceramide levels at 2 weeks and partially reversed the hyperoxia-induced increase in alveolar size and arrest in alveolarisation at 4 weeks.Exposure of newborn mice to hyperoxia caused restrictive and obstructive lung function changes that partially recovered in room air, while alveolar morphology remained abnormal. Hyperoxia increased ceramide levels, with normalisation after recovery. D-sphingosine addition during recovery reduced ceramide levels and ameliorated hyperoxia-induced alveolar arrest. @ERSpublications D-sphingosine during recovery reduced ceramide levels and ameliorated hyperoxia-induced alveolar arrest in mice

show abstract

“…The main pathological hallmark of BPD is an arrest of alveolar development, characterized by large and simplified distal airspaces (4,5). In addition, several recent reports have shown that the lungs of ventilated preterm infants with early BPD show markedly increased levels of alveolar epithelial cell death (6)(7)(8).…”

mentioning

confidence: 99%

Fate and Effects of Adult Bone Marrow Cells in Lungs of Normoxic and Hyperoxic Newborn Mice

Fritzell

Mao²,

Gundavarapu³

et al. 2009

Am J Respir Cell Mol Biol

View full text Add to dashboard Cite

Cell-based therapy in adult lung injury models is associated with highly variable donor cell engraftment and epithelial reconstitution. The role of marrow-derived cell therapy in neonatal lung injury is largely unknown. In this study, we determined the fate and effects of adult bone marrow cells in a model of neonatal lung injury. Wild-type mice placed in a normoxic or hyperoxic (95% O 2 ) environment received bone marrow cells from animals expressing green fluorescent protein (GFP) at Postnatal Day (P)5. Controls received vehicle buffer. Lungs were analyzed between Post-Transplantation (TPX) Day 2 and Week 8. The volume of GFP-immunoreactive donor cells, monitored by stereologic volumetry, remained constant between Post-TPX Weeks 1 and 8 and was similar in normoxic and hyperoxiaexposed recipients. Virtually all marrow-derived cells showed colocalization of GFP and the pan-macrophage marker, F4/80, by double immunofluorescence studies. Epithelial transdifferentiation was not seen. Marrow cell administration had adverse effects on somatic growth and alveolarization in normoxic mice, while no effects were discerned in hyperoxia-exposed recipients. Reexposure of marrowtreated animals to hyperoxia at P66 resulted in significant expansion of the donor-derived macrophage population. In conclusion, intranasal administration of unfractionated bone marrow cells to newborn mice does not achieve epithelial reconstitution, but establishes persistent alveolar macrophage chimerism. The predominantly adverse effects of marrow treatment in newborn lungs are likely due to macrophage-associated paracrine effects. While this model and route of cell therapy may not achieve epithelial reconstitution, the role of selected stem cell populations and/or alternate routes of administration for cell-based therapy in injured newborn lungs deserve further investigation.Keywords: stem cells; cell therapy; lung injury; newborns; BPD Premature infants with structurally immature lungs born between 23 and 28 weeks of gestation are at risk for development of bronchopulmonary dysplasia (BPD) or chronic lung disease of the newborn, a condition associated with high perinatal morbidity and mortality (1). An estimated 30% of infants with a birth weight between 500 and 1,500 g will develop BPD. Many of these infants require long-term ventilation and/or supplemental oxygen (2, 3). The main pathological hallmark of BPD is an arrest of alveolar development, characterized by large and simplified distal airspaces (4, 5). In addition, several recent reports have shown that the lungs of ventilated preterm infants with early BPD show markedly increased levels of alveolar epithelial cell death (6-8).We recently demonstrated that increased alveolar epithelial apoptosis in newborn mice is sufficient to disrupt alveolar remodeling (9), supporting our central hypothesis that loss of alveolar epithelial cells may play a critical role in the arrested alveolar development seen in BPD. The potential for stem cell-based therapy aimed at restoring or protecting the alveol...

show abstract

Apoptosis and proliferation in lungs of ventilated and oxygen-treated preterm infants

Cited by 60 publications

References 36 publications

Decreased Expression of Angiogenic Factors in Placentas with Chorioamnionitis after Preterm Birth

Decreased Expression of Angiogenic Factors in Placentas with Chorioamnionitis after Preterm Birth

Amelioration of hyperoxia-induced lung injury using a sphingolipid-based intervention

Fate and Effects of Adult Bone Marrow Cells in Lungs of Normoxic and Hyperoxic Newborn Mice

Contact Info

Product

Resources

About