LIPOPOLYSACCHARIDE (LPS)-BINDING PROTEIN AND SOLUBLE CD14 FUNCTION AS ACCESSORY MOLECULES FOR LPS-INDUCED CHANGES IN ENDOTHELIAL BARRIER FUNCTION, IN-VITRO

被引:104
作者
GOLDBLUM, SE [1 ]
BRANN, TW [1 ]
DING, X [1 ]
PUGIN, J [1 ]
TOBIAS, PS [1 ]
机构
[1] Scripps Res Inst, DEPT IMMUNOL, LA JOLLA, CA 92073 USA
关键词
ENDOTOXIN; ADULT RESPIRATORY DISTRESS SYNDROME; VASCULAR PERMEABILITY;
D O I
10.1172/JCI117022
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
Bacterial LPS induces endothelial cell(EC) injury both in vivo and in vitro. We studied the effect of Escherichia coli 0111:B4 LPS on movement of C-14-BSA across bovine pulmonary artery EC monolayers. In the presence of serum, a 6-h LPS exposure augmented (P < 0.001) transendothelial C-14-BSA flux compared with the media control at concentrations greater than or equal to 0.5 ng/ml, and LPS(10 ng/ml) exposures of greater than or equal to 2-h increased (P < 0.005) the flux. In the absence of serum, LPS concentrations of up to 10 mu g/ml failed to increase C-14-BSA flux at 6 h. The addition of 10% serum increased EC sensitivity to the LPS stimulus by > 10,000-fold. LPS (10 ng/ml, 6 h) failed to increase C-14-BSA flux at serum concentrations < 0.5%, and maximum LPS-induced increments could be generated in the presence of greater than or equal to 2.5%. LPS-binding protein (LBP) and soluble CD14(sCD14) could each satisfy this serum requirement; either anti-LBP or anti-CD14 antibody each totally blocked (P < 0.00005) the LPS-induced changes in endothelial barrier function. LPS-LBP had a more rapid onset than did LPS-sCD14. The LPS effect in the presence of both LBP and sCD14 exceeded the effect in the presence of either protein alone. These data suggest that LBP and sCD14 each independently functions as an accessory molecule for LPS presentation to the non-CD14-bearing endothelial surface. However, in the presence of serum both molecules are required.
引用
收藏
页码:692 / 702
页数:11
相关论文
共 40 条
  • [1] ALBELDA SM, 1989, AM J PHYSIOL, V257, pL65
  • [2] ENDOTOXIN-MEDIATED ENDOTHELIAL-CELL INJURY AND ACTIVATION - ROLE OF SOLUBLE CD14
    ARDITI, M
    ZHOU, J
    DORIO, R
    RONG, GW
    GOYERT, SM
    KIM, KS
    [J]. INFECTION AND IMMUNITY, 1993, 61 (08) : 3149 - 3156
  • [3] ASHMUN RA, 1987, BLOOD, V69, P886
  • [4] BIOCHEMICAL-CHARACTERIZATION OF A SOLUBLE FORM OF THE 53-KDA MONOCYTE SURFACE-ANTIGEN
    BAZIL, V
    HOREJSI, V
    BAUDYS, M
    KRISTOFOVA, H
    STROMINGER, JL
    KOSTKA, W
    HILGERT, I
    [J]. EUROPEAN JOURNAL OF IMMUNOLOGY, 1986, 16 (12) : 1583 - 1589
  • [5] BEEKHUIZEN H, 1991, J IMMUNOL, V147, P3761
  • [6] BRIGHAM KL, 1986, AM REV RESPIR DIS, V133, P913
  • [7] INTERLEUKIN-1-ALPHA AND INTERLEUKIN-BETA AUGMENT PULMONARY-ARTERY TRANSENDOTHELIAL ALBUMIN FLUX INVITRO
    CAMPBELL, WN
    DING, XD
    GOLDBLUM, SE
    [J]. AMERICAN JOURNAL OF PHYSIOLOGY, 1992, 263 (01): : L128 - L136
  • [8] SOLUBLE CD14 PARTICIPATES IN THE RESPONSE OF CELLS TO LIPOPOLYSACCHARIDE
    FREY, EA
    MILLER, DS
    JAHR, TG
    SUNDAN, A
    BAZIL, V
    ESPEVIK, T
    FINLAY, BB
    WRIGHT, SD
    [J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1992, 176 (06) : 1665 - 1671
  • [9] PURIFICATION AND CHARACTERIZATION OF MURINE LIPOPOLYSACCHARIDE-BINDING PROTEIN
    GALLAY, P
    CARREL, S
    GLAUSER, MP
    BARRAS, C
    ULEVITCH, RJ
    TOBIAS, PS
    BAUMGARTNER, JD
    HEUMANN, D
    [J]. INFECTION AND IMMUNITY, 1993, 61 (02) : 378 - 383
  • [10] GARTNER SL, 1988, LAB INVEST, V59, P181