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Interleukin 8 (IL-8) and growth-related oncogene alpha (Gro-alpha) delay neutrophil apoptosis, which is thought to be important for the resolution of inflammation. We hypothesized that (IL-8) and Gro-alpha interfere with extracellular death receptor signaling or intracellular caspase activation to suppress neutrophil apoptosis. In addition, we sought to determine if prolonged neutrophil half-life was associated with preservation of function. Polymorphonuclear leukocytes (PMN) were cultured with IL-8 or Gro-alpha (0-100 ng/mL) in normoxia or hypoxia, and the extent of apoptosis was assessed by histology and TdT-mediated dUTP nick end labeling (TUNEL). Subsequently, to determine the role of apoptotic-associated receptors, PMN were cultured with IL-8 and neutralizing monoclonal antibody to Fas (CD95), TNFR55, and TNFR75. To establish the effect of IL-8 or Gro-alpha on pro-apoptotic caspase activity, the cleavage of specific colorimetric substrates was assessed. Functional changes in PMN included the capacity to produce superoxide anion and phagocytosis of Escherichia coli. At the 100 ng/mL dose, the addition of IL-8 and Gro-alpha maximally suppressed PMN apoptosis from 54% (untreated) to 5% and 6%, respectively. The addition of neutralizing antibodies to Fas, TNFR55, or R75 caused no change in IL-8 suppression of apoptosis. Caspase 3 activity was markedly suppressed at 24 h by the inclusion of either IL-8 and Gro-alpha. IL-8 and Gro-alpha-stimulated PMN released more superoxide anion and had an increased phagocytic index vs. control PMN. IL-8 and Gro-alpha suppress neutrophil apoptosis to a similar level that is not influenced by oxygen tension at high doses. The effect of IL-8 and Gro-alpha does not depend on activation of the Fas, TNFR55, or R75 receptor pathways but involves suppression of caspase 3 activity. IL-8 or Gro-alpha extends the functional half-life of neutrophils and may explain their role in disease states such as acute respiratory distress syndrome.

Titel:	CXC chemokine suppression of polymorphonuclear leukocytes apoptosis and preservation of function is oxidative stress independent.
Autor/in / Beteiligte Person:	Dunican, AL ; Leuenroth, SJ ; Ayala, A ; Simms, HH
Link:	Full Text Finder (Volltext)
Zeitschrift:	Shock (Augusta, Ga.), Jg. 13 (2000-03-01), Heft 3, S. 244-50
Veröffentlichung:	2002- : Philadelphia : Lippincott Williams & Wilkins ; <i>Original Publication</i>: Augusta, GA : BioMedical Press, [1994-, 2000
Medientyp:	academicJournal
ISSN:	1073-2322 (print)
DOI:	10.1097/00024382-200003000-00012
Schlagwort:	Antibodies pharmacology Apoptosis drug effects Caspase 3 Caspase 8 Caspase 9 Caspases drug effects Caspases metabolism Cells, Cultured Chemokine CXCL1 Chemotactic Factors pharmacology Growth Substances pharmacology Humans Interleukin-8 metabolism Interleukin-8 pharmacology Neutrophils drug effects Receptors, Tumor Necrosis Factor immunology Tumor Necrosis Factor-alpha pharmacology Apoptosis physiology Chemokines, CXC metabolism Chemotactic Factors metabolism Growth Substances metabolism Intercellular Signaling Peptides and Proteins Neutrophils physiology Oxidative Stress
Sonstiges:	Nachgewiesen in: MEDLINE Sprachen: English Publication Type: Journal Article; Research Support, U.S. Gov't, P.H.S. Language: English [Shock] 2000 Mar; Vol. 13 (3), pp. 244-50. MeSH Terms: Intercellular Signaling Peptides and Proteins* ; Oxidative Stress* ; Apoptosis / physiology ; Chemokines, CXC / metabolism ; Chemotactic Factors / metabolism ; Growth Substances / metabolism ; Neutrophils / *physiology ; Antibodies / pharmacology ; Apoptosis / drug effects ; Caspase 3 ; Caspase 8 ; Caspase 9 ; Caspases / drug effects ; Caspases / metabolism ; Cells, Cultured ; Chemokine CXCL1 ; Chemotactic Factors / pharmacology ; Growth Substances / pharmacology ; Humans ; Interleukin-8 / metabolism ; Interleukin-8 / pharmacology ; Neutrophils / drug effects ; Receptors, Tumor Necrosis Factor / immunology ; Tumor Necrosis Factor-alpha / pharmacology Grant Information: GM53114 United States GM NIGMS NIH HHS Substance Nomenclature: 0 (Antibodies) ; 0 (CXCL1 protein, human) ; 0 (Chemokine CXCL1) ; 0 (Chemokines, CXC) ; 0 (Chemotactic Factors) ; 0 (Growth Substances) ; 0 (Intercellular Signaling Peptides and Proteins) ; 0 (Interleukin-8) ; 0 (Receptors, Tumor Necrosis Factor) ; 0 (Tumor Necrosis Factor-alpha) ; EC 3.4.22.- (CASP3 protein, human) ; EC 3.4.22.- (CASP8 protein, human) ; EC 3.4.22.- (CASP9 protein, human) ; EC 3.4.22.- (Caspase 3) ; EC 3.4.22.- (Caspase 8) ; EC 3.4.22.- (Caspase 9) ; EC 3.4.22.- (Caspases) Entry Date(s): Date Created: 20000316 Date Completed: 20000413 Latest Revision: 20190915 Update Code: 20240513

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CXC chemokine suppression of polymorphonuclear leukocytes apoptosis and preservation of function is oxidative stress independent.