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Effect of Exogenous Surfactant on the Development of Surfactant Synthesis in Premature Rabbit Lung

 

作者: MAURIZIO AMATO,   KEVIN PETIT,   HUMBERTO FIORE,   CYNTHIA DOYLE,   IVAN FRANTZ,   HEBER NIELSEN,  

 

期刊: Pediatric Research  (OVID Available online 2003)
卷期: Volume 53, issue 4  

页码: 671-678

 

ISSN:0031-3998

 

年代: 2003

 

出版商: OVID

 

数据来源: OVID

 

摘要:

Surfactant replacement is an effective therapy for neonatal respiratory distress syndrome. Full recovery from respiratory distress syndrome requires development of endogenous surfactant synthesis and metabolism. The influence of exogenous surfactant on the development of surfactant synthesis in premature lungs is not known. We hypothesized that different exogenous surfactants have different effects on the development of endogenous surfactant production in the premature lung. We treated organ cultures of d 25 fetal rabbit lung for 3 d with 100 mg/kg body weight of natural rabbit surfactant, Survanta, and Exosurf and measured their effects on the development of surfactant synthesis. Additional experiments tested how these surfactants and Curosurf affected surfactant protein (SP) SP-A, SP-B, and SP-C mRNA expression. Surfactant synthesis was measured as the incorporation of3H-choline and14C-glycerol into disaturated phosphatidylcholine recovered from lamellar bodies. Randomized-block ANOVA showed significant differences among treatments for incorporation of both labels (p< 0.01), with natural rabbit surfactant less than control, Survanta greater than control, and Exosurf unchanged. Additional experiments with natural rabbit surfactant alone showed no significant effects in doses up to 1000 mg/kg. Survanta stimulated disaturated phosphatidylcholine synthesis (173 ± 41% of control;p= 0.01), increased total lamellar body disaturated phosphatidylcholine by 22% (p< 0.05), and increased14C-disat-PC specific activity by 35% (p< 0.05). The response to Survanta was dose-dependent up to 1000 mg/kg. Survanta did not affect surfactant release. No surfactant altered the expression of mRNA for SP-A, SP-B, or SP-C. We conclude that surfactant replacement therapy can enhance the maturation of surfactant synthesis, but this potential benefit differs with different surfactant preparations.

 

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