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CD200 in growing rat lungs: developmental expression and control by dexamethasone
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  • 作者:Mang-Hung Tsai (1)
    Chin-Chen Chu (2) (3)
    Tsui-Shan Wei (4)
    Mei-Miao Chiu (5)
    Chiu-Yun Chang (6)
    I-Hua Wei (1)
    Hsiung-Fei Chien (7)
    Hui-Min Chen (6) (8)
    Ching-Hsiang Wu (6)
    Ya-Fen Jiang-Shieh (4)

    1. Department of Anatomy
    ; China Medical University ; Taichung ; 404 ; Taiwan
    2. Department of Anesthesiology
    ; Chi Mei Medical Center ; Tainan ; 710 ; Taiwan
    3. Department of Recreation and Health-Care Management
    ; Chia Nan University of Pharmacy and Science ; Tainan ; 717 ; Taiwan
    4. Department of Anatomy
    ; College of Medicine ; National Cheng Kung University ; No. 1 University Road ; Tainan ; 701 ; Taiwan
    5. Institute of Anatomy and Cell Biology
    ; School of Medicine ; National Yang-Ming University ; Taipei ; 112 ; Taiwan
    6. Department of Anatomy
    ; College of Medicine ; Taipei Medical University ; Taipei ; 110 ; Taiwan
    7. Department of Surgery
    ; College of Medicine ; National Taiwan University ; No. 250 Wu-Hsing Street ; Taipei ; 110 ; Taiwan
    8. Electron Microscopy Center
    ; College of Medicine ; Taipei Medical University ; Taipei ; 110 ; Taiwan
  • 关键词:CD200 ; Alveolar endothelium ; Development ; Pulmonary ; Dexamethasone ; Rat (Wistar)
  • 刊名:Cell and Tissue Research
  • 出版年:2015
  • 出版时间:March 2015
  • 年:2015
  • 卷:359
  • 期:3
  • 页码:729-742
  • 全文大小:3,315 KB
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  • 刊物类别:Biomedical and Life Sciences
  • 刊物主题:Biomedicine
    Human Genetics
    Proteomics
    Molecular Medicine
  • 出版者:Springer Berlin / Heidelberg
  • ISSN:1432-0878
文摘
CD200 belongs to cell adhesion molecules of the immunoglobulin superfamily. It lacks intracellular signaling motifs and exerts immunosuppressive effect in various tissues. We have reported previously that CD200 is predominantly associated with the capillary network in the alveolar septum of adult rats. The alveolar endothelial cells express CD200, which is confined to their luminal cell membrane facing the blood-air barrier. Our present results show that lung CD200 protein increases gradually with advancing age, being maximally expressed in the early postnatal (P) period. CD200 protein expression, however, declines at P5 but increases again after P7, reaching the adult level at P21. In developing lungs in fetal and neonatal stages, double-immunofluorescence staining has confirmed intense CD200 immunoreactivity delineating the vascular profiles in the double layers of the alveolar capillaries; this staining becomes diffuse and patchy with time. Unlike in adult lungs, immunoelectron microscopy has revealed that CD200 expression in fetal and early postnatal lungs is localized over the entire luminal cell membrane and in the cytoplasm of the endothelia. CD200 expression is progressively redistributed to a specific luminal domain of alveolar endothelia during pulmonary microvascular maturation. In neonatal rats treated with dexamethasone, the amount of lung CD200 significantly increases and is also elevated with time. Upregulation of endothelial CD200 has further been confirmed in isolated pulmonary microvascular endothelial cells treated with dexamethasone. Thus, lung CD200 is developmentally regulated, possibly under hormonal influence.

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