DUAL EFFECTS OF FORMYLPEPTIDES ON THE ADHESION OF ENDOTOXIN-PRIMED HUMAN NEUTROPHILS

被引:11
作者
BELLAVITE, P [1 ]
CHIRUMBOLO, S [1 ]
LIPPI, G [1 ]
ANDRIOLI, G [1 ]
BONAZZI, L [1 ]
FERRO, I [1 ]
机构
[1] OSPED POLICLIN,SERV IMMUNOTRASFUS,VERONA,ITALY
关键词
PRIMING; NEUTROPHIL MODULATION; ADHESION; ENDOTOXIN; CHEMOTAXIS; CYCLIC AMP;
D O I
10.1002/cbf.290110403
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Neutrophils, treated with sequential additions of bacterial products such as endotoxin (E. Coli lipopolysaccharide, LPS) and the chemotactic peptide N-formyl-methionyl-leucyl-phenylalanine (fMLP), undergo to metabolic activation and express membrane-anchoring proteins that promote adhesion to serum-coated culture wells. By investigating the dose-response relationships of these phenomena, we have found that: (a) resting neutrophils do not produce a significant amount of superoxide (O-2(-)) and show only minimal adhesion to serum-coated plastic surfaces; (b) fully activatory doses (> 5 x 10(-8)M) of fMLP induce the release of O-2(-) and a significant increase of the cell adhesion; (c) pretreatment of the cells for 1 h with LPS augments cell adhesion to serum-coated culture wells in the absence of further stimulation and primes the neutrophils to enhanced fMLP-dependent O-2(-) release; (d) addition of low, substimulatory doses of fMLP (from 10(-10)M to 5 x 10(-9)M) inhibits and reverses the adhesion of LPS-treated cells, (e) high fMLP doses (> 10(-7)M) are additive to LPS in promoting adhesion. Phorbol-myristate acetate(> 10(-9)M) increased adhesion in both normal and LPS-treated neutrophils, but low doses of this stimulant did not inhibit adhesion. Low doses (10(-9)M) of fMLP increased intracellular cyclic AMP in both normal and LPS-treated neutrophils, suggesting that stimulus-induced rises in cAMP may be the negative signal responsible for down-modulation of adhesion. Low (5 x 10(-9)M) and high (5 x 10(-7)M) fMLP doses induced the same increase of expression of CD11/CD18 integrins, indicating that the inhibition of adhesion caused by low doses is not due to quantitative down-regulation of integrins. These findings may provide an in vitro model of the complex biological events involved in the regulation of neutrophil adhesion.
引用
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页码:231 / 239
页数:9
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