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半胱氨酸蛋白酶3和白细胞介素8在高氧暴露下早产大鼠肺组织中的动态表达及其意义 被引量:3

Temporal expression and significance of caspase-3 and interlenkin-8 in the lungs of preterm rats exposed to hyperoxia
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摘要 目的 探讨半胱氨酸蛋白酶-3(Caspase-3)及白细胞介素-8(IL-8)在早产大鼠高氧肺损伤中的动态表达及其意义。方法孕21d的SD早产大鼠生后第2天,随机分为空气组和高氧组(均n=40)。高氧组大鼠予以85%高氧持续暴露,空气组大鼠置于空气中。于暴露1、4、7、14和21d每组各处死8只大鼠,收集肺组织标本,苏木精咿红染色观察肺组织病理形态学变化,双抗夹心ELISA法检测IL-8含量,免疫组化和Western blot检测Caspase-3表达。结果高氧暴露后肺泡腔内可见有坏死脱落细胞、炎症细胞渗出增多、间质水肿,肺组织结构紊乱,肺泡形成明显滞后,肺泡结构简单化和囊泡化;与空气对照组比较,高氧暴露4、7和14d肺组织Caspase-3和IL-8含量均明显增高(P〈0.01)。结论在高氧所致早产大鼠肺损伤中细胞凋亡和坏死共存,两者共同参与了早产大鼠高氧肺损伤的病理过程。 Objective To explore the temporal expression and significance of Caspase-3 and interleukin-8( IL-8 )in hyperoxia-indueed lung injury in preterm rats. Methods Two-day-old Sprague-Dawley preterm rats were randomly divided into Air group and Hyperoxia group (each rats in each group). Rats in the Hyperoxia group were exposed to 85% O2 , while rats in the Air group were exposed to air. The rats in each group were sacrificed at 1,4, 7, 14 and 21 days after exposure ( 8 rats at each time point), and lung tissues were collected. Pathomorphology of lungs was observed by hematoxylin-eosine staining. The contents of IL-8 in the homogenate of lungs were detected using ELISA. The expression of Caspase-3 was detected by immunohistochemistry and Western blot. Results ( 1 ) Lung histopathology: after hyperoxia exposure 1 day, no significant effects on alveoli were found; but on days 4 and 7, alveolitis appeared: there were nacrotie abacission cells in alveolar space, increased inflammatory cells infiltration, lung interstitial edema; on days 14 and 21, lung structure derangement, decreased number of alveoli, simplified and vesicular lung structure, all of which showed the retardation of alveolar formation. (2) the contents of IL-8 in the homogenate of lungs had no significant change on day 1 but increased significantly on days 4, 7 and 14 compared with air control group (P 〈 0. 01 for all). (3) Immunohistochemistry detected the expression of Caspase-3 in the lung: the intensity of Caspase-3 expression increased significantly on days 4, 7 and 14 compared with air control group ( P 〈 0. 01 ). (4) Western blotting detected the expression of easpase-3 in the lung: the pattern of dynamic expression of Caspase-3 was similar to the restdts of immunohistochemistry. Conclusions Both apoptesis and necrosis contribute to ceil death during hyperoxia. Apoptesis and necrosis may both play an important role in hyperoxia-indueed lung injury in preterm rats.
作者 刘伟 常立文 李文斌
机构地区 华中科技大学同济医学院附属同济医院儿科
出处 《中华儿科杂志》 CAS CSCD 北大核心 2008年第3期229-233,共5页 Chinese Journal of Pediatrics
基金 国家自然科学基金资助项目(30471824) 国家“十五”科技攻关项目(2004BA720A11)
关键词 半胱氨酸天冬氨酸蛋白酶 白细胞介素8 高氧症 肺疾病 婴儿 早产 Caspases Interleukin-8 Hyperoxia Lung diseases Infant, premature
分类号 R686 [医药卫生—骨科学]
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参考文献10

  • 1Atlante A, Bobba A, Calissano P, et aL The apoptosis/necrosis transition in cerebellar granule cells depends on the mutual relationship of the antioxidant and the proteolytic systems which regulate ROS production and cytochrome c release en route to death. J Neurochem, 2003, 84:960-971.
  • 2Zhivotovsky B, Burgess DH, Orrenins S. Proteases in apoptosis. Experientia, 1996, 52:968-978.
  • 3钱莉玲,常立文,张谦慎,容志惠.85%高浓度氧长期暴露诱发早产大鼠肺损伤(英文)[J].中国当代儿科杂志,2003,5(2):95-99. 被引量:21
  • 4Takahashi M, Masuyama J, Ikeda U,et aL Effects of endogenous endothelial interleukin-8 on neutrophil migration across an endothelial monolayer. Cardiovasc Res, 1995,29:670-675.
  • 5Desmarquest P, Chadelat K, Corroyer S, et aL Effect of hyperoxia on human maerophage cytokine response. Respir Med, 1998,92 : 951-960.
  • 6夏世文,常立文,张晓慧,刘汉楚.新生儿氧疗时血浆中氧化及抗氧化水平的动态观察[J].中国实用儿科杂志,2002,17(4):204-206. 被引量:10
  • 7Cohen GM. Caspase:the executioners of apoptosis. Caspases: the executioners of apoptosis. Biochem J, 1997, 326:1-16.
  • 8张向峰,Hussein D.Foda.高氧所致急性肺损伤小鼠肺组织细胞凋亡和坏死的研究[J].中华结核和呼吸杂志,2004,27(7):465-468. 被引量:11
  • 9Kazzaz JA, Xu J, Palaia TA, et aL Cellular oxygen toxicity, oxidant injury without apoptosis. J Biol Chem,1996,271:15182-15186.
  • 10Sekido N, Mukaida N, Harada A, et aL Prevention of lung reperfusion injury in rabbits by a monoclonal antibody against interleukin-8. Nature, 1993,365:654-657.

二级参考文献29

  • 1[1]Vento G,Mele MC,Mordente A,et al.High total antioxidant activity and uric acid in tracheobronchial aspirate fluid of preterm infants during oxidative stress:an adaptive response to hyperoxia?Acta Pediatr,2000,89:336
  • 2[2]Neefjes VME,Evelo CTA,Baars L,et al.Erythrocyte glutathione stransferase as marker of oxidative stress at birth.Arch Dis Child Fetal Neonatal Ed,1999,81:130
  • 3[3]James H,Roum,Borok,et al.Glutathione aerosol suppresses lung epithelial surface inflammatory cell-derived oxidants in cystic fibrosis.J Appl Physiol,1999,87(1):438
  • 4[4]Bettina C,Shock,Ian S,et al.Antioxidants and protein carbonyls in bronchoalveolar lavage fluid of children:normal data.Pediatric research,2001,49(2):155
  • 5[5]Jain A,Mehta T.Glutathione metabolism in newborns:evidence for glutahione deficiency in plasma brochoalveolar lavage fluid and lymphocytes in preterm.Pediatr Pulmonol,1995,20(3):160
  • 6[6]Moison RMW,Haasnoot AA,Van D,et al.Red blood cell glutathione and plasma sufhydryls in chronic lung disease of the newborn.Acta Pediatr,1997,86:1363
  • 7[7]Christine C,Winterbourn,Chan T,et al.Protein carbonyls and lipid peroxidation products as oxidation markers in preterm infant plasma:associations with chronic lung disease and retinopathy and effects of selenium supplement.Pediatrics Research,2000,48(1):84
  • 8[8]Huertas JR,Pulomine N,Ochoa JJ,et al.Lipid peroxidation and antioxidants in erythrocyte membranes of full-term and preterm newborns.Biofactors,1998,8(1~2):133
  • 9[9]Saugstad OD.Bronchopulmonary dysplasia and oxidative stress:are we closer to an understanding of the pathogenesis of BPD?Acta Paditric,1997,86(12):1277
  • 10[7]Jobe AJ. The new BPD: an arrest of lung development [J]. Pediatr Res, 1999, 46(6): 641-643.

共引文献38

同被引文献39

  • 1刘雪雁,薛辛东.高氧致慢性肺疾病新生大鼠肺组织尿激酶型纤溶酶原激活因子和纤溶酶原激活物抑制因子1表达的动态改变及意义[J].中华儿科杂志,2008,46(6):458-463. 被引量:2
  • 2喻文亮,陆铸今,王莹,施丽萍,匡凤梧,张剑晖,谢敏慧,钱素云,樊寻梅,孙波.小儿急性呼吸窘迫综合征前瞻性多中心临床流行病学研究[J].中华急诊医学杂志,2005,14(6):448-453. 被引量:57
  • 3谭利平,许峰,匡凤梧,方芳,卢仲毅,王兴勇.高氧性肺损伤中MAPK信号途径的表达及其作用机制[J].第四军医大学学报,2007,28(12):1061-1064. 被引量:14
  • 4Morse D, Otterbein LE, Watkins S, et al. Deficiency in the c -Jun NH2 - terminal kinase signaling pathway confers susceptibility to hyperoxic lung injury in mice [ J ]. Am J Physiol Lung Cell Mol Physiol, 2003,285( 1 ) :250 -257.
  • 5Li LF, Liao SK, Ko YS, et al. Hyperoxia increases ventilator - induced lung injury via mitogen - activated protein kinases : A prospective, controlled animal experiment[J]. Crit Care,2007,11 ( 1 ) :R25.
  • 6Xu D, Perez RE, Rezaiekhaligh MH,et al, Knockdown of ERp57 increases BiP/GRP78 induction and protects against hyperoxia and tunicamycin - induced apoptosis[ J]. Am J Physiol Lung Cell Mol Physiol,2009, 297(1) :44 -51.
  • 7Kolliputi N, Waxman AB. IL - 6 cytoprotection in hyperoxic acute lung injury occurs via suppressor of cytokine signaling - 1 - induced apoptosis signal - regulating kinase - 1 degradation [ J ]. Am J Respir Cell Mol Biol,2009,40( 3 ) :314 - 324.
  • 8Young LR,Pasula R, Gulleman PM,et al. Susceptibility of Hermansky- Pudlak mice to bleomycin - induced type Ⅱ cell apoptosis and fibrosis [ J 1. Am J Respir Cell Mol Biol,2007,37 (1) :67 -74.
  • 9Das KC, Ravi D, Holland W. Increased apoptosis and expression of p21 and p53 in premature infant baboon model of bronchopulmonary dysplasia [ J ]. Antioxid Redox Signal,2004,6 ( 1 ) : 109 - 116.
  • 10de Paepe ME, Mao Q, Chao Y,et al. Hyperoxia -induced apoptosis and Fas/FasL expression in lung epithelial cells [ J ]. Am J Physiol Lung Cell Mol Physiol,2005,289 (4) :647 - 659.

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中华儿科杂志
2008年 第3期

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