David Tanaka scite author profile

Inflammation may contribute to lung injury and impaired alveolar development in bronchopulmonary dysplasia. We treated hyperoxia-exposed newborn rats with antibodies to the neutrophil chemokine cytokine-induced neutrophil chemoattractant-1 (CINC-1) during 95% O2 exposure to reduce adverse effects of hyperoxia-induced inflammation on lung development. Rats were exposed at birth to air, 95% O2, or 95% O2 + anti-CINC-1 (injected on days 3 and 4). Bromodeoxyuridine (BrdU) was injected 6 h before death. Anti-CINC-1 treatment improved weight gain but not survival at day 8. Anti-CINC-1 reduced bronchoalveolar lavage neutrophils at day 8 to levels equal to air controls. Total detectable lung CINC-1 was reduced to air control levels. Lung compliance was improved by anti-CINC-1, achieving air control levels in the 10-microg anti-CINC-1 group. Anti-CINC-1 preserved proliferating cell nuclear antigen expression in airway epithelium despite 95% O2 exposure. BrdU incorporation was depressed by hyperoxia but preserved by anti-CINC-1 to levels similar to air control. Alveolar volume and surface density were decreased by hyperoxia but preserved by anti-CINC-1 to levels equal to air control. Blockade of neutrophil influx in newborns may avert early lung injury and avoid alveolar developmental arrest that contributes to bronchopulmonary dysplasia.

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Antenatal magnesium sulfate and spontaneous intestinal perforation in infants less than 25 weeks gestation

Rattray

Kraus

Drinker

et al. 2014

J Perinatol

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Feeding practices and other risk factors for developing transfusion-associated necrotizing enterocolitis

DeRienzo

Smith

Tanaka

et al. 2014

Early Human Development

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Aims Determine the incidence of and risk factors for necrotizing enterocolitis (NEC) and transfusion-associated NEC (TANEC) in very-low-birth-weight (VLBW) infants pre/post implementation of a peri-transfusion feeding protocol. Study Design A retrospective cohort study was conducted including all inborn VLBW infants admitted to the Duke intensive care nursery from 2002–10. We defined NEC using Bell’s modified criteria IIA and higher and TANEC as NEC occurring within 48 hours of a packed red blood cell (pRBC) transfusion. We compared demographic and laboratory data for TANEC vs. other NEC infants and the incidence of TANEC pre/post implementation of our peri-transfusion feeding protocol. We also assessed the relationship between pre-transfusion hematocrit and pRBC unit age with TANEC. Results A total of 148/1380 (10.7%) infants developed NEC. Incidence of NEC decreased after initiating our peri-transfusion feeding protocol: 126/939 (12%) to 22/293 (7%), P=0.01. The proportion of TANEC did not change: 51/126 (41%) vs. 9/22 (41%), P>0.99. TANEC infants were smaller, more likely to develop surgical NEC, and had lower mean pre-transfusion hematocrits prior to their TANEC transfusions compared with all other transfusions before their NEC episode: 28% vs. 33%, P<0.001. Risk of TANEC was inversely related to pre-transfusion hematocrit: odds ratio 0.87 (0.79–0.95). Conclusions Pre-transfusion hematocrit is inversely related to risk of TANEC, which suggests that temporally maintaining a higher baseline hemoglobin in infants most at risk of NEC may be protective. The lack of difference in TANEC pre-/post-implementation of our peri-transfusion feeding protocol, despite an overall temporal decrease in NEC, suggests other unmeasured interventions may account for the observed decreased incidence of NEC.

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Online clinical tool to estimate risk of bronchopulmonary dysplasia in extremely preterm infants

Greenberg

McDonald

Laughon

et al. 2022

Arch Dis Child Fetal Neonatal Ed

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ObjectiveDevelop an online estimator that accurately predicts bronchopulmonary dysplasia (BPD) severity or death using readily-available demographic and clinical data.DesignRetrospective analysis of data entered into a prospective registry.SettingInfants cared for at centres of the United States Neonatal Research Network between 2011 and 2017.PatientsInfants 501–1250 g birth weight and 23 0/7–28 6/7 weeks’ gestation.InterventionsNone.Main outcome measuresSeparate multinomial regression models for postnatal days 1, 3, 7, 14 and 28 were developed to estimate the individual probabilities of death or BPD severity (no BPD, grade 1 BPD, grade 2 BPD, grade 3 BPD) defined according to the mode of respiratory support administered at 36 weeks’ postmenstrual age.ResultsAmong 9181 included infants, birth weight was most predictive of death or BPD severity on postnatal day 1, while mode of respiratory support was the most predictive factor on days 3, 7, 14 and 28. The predictive accuracy of the models increased at each time period from postnatal day 1 (C-statistic: 0.674) to postnatal day 28 (C-statistic 0.741). We used these results to develop a web-based model that provides predicted estimates for BPD by postnatal day.ConclusionThe probability of BPD or death in extremely preterm infants can be estimated with reasonable accuracy using a limited amount of readily available clinical information. This tool may aid clinical prognostication, future research, and center-specific quality improvement surrounding BPD prevention.Trial registration numberNCT00063063

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David Tanaka

Anti-neutrophil chemokine preserves alveolar development in hyperoxia-exposed newborn rats

Antenatal magnesium sulfate and spontaneous intestinal perforation in infants less than 25 weeks gestation

Feeding practices and other risk factors for developing transfusion-associated necrotizing enterocolitis

Online clinical tool to estimate risk of bronchopulmonary dysplasia in extremely preterm infants

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