Effect of picibanil (OK432) on neutrophil-mediated antitumor activity: Implication of monocyte-derived neutrophil-activating factors
- 1 July 1992
- journal article
- Published by Springer Science and Business Media LLC in Cancer Immunology, Immunotherapy
- Vol. 35 (4), 277-282
- https://doi.org/10.1007/bf01789335
Abstract
Picibanil (OK432), an extract from streptococci, has been widely utilized to treat malignant ascites and pleural effusions. The antitumor mechanism is believed to include complement-mediated neutrophil activation. Employing a flow-cytometric analysis of actin polymerization as an indicator of cell activation as well as a tumor proliferation assay, we have found that monocytederived neutrophil-activating factors were involved in OK432-induced neutrophil activation as well as antitumor activity. OK432-stimulated (0.1 KE/ml; 0.01 mg/ml) monocyte supernatants (OKMS) induced neutrophil actin polymerization and chemotaxis. OKMS were responsible for neutrophil-mediated inhibition of human leukemic (CEM) cell proliferation and stimulated neutrophils to produce superoxide in the presence of CEM leukemic cells at an effector/target ratio higher than 20/1. In contrast, OK432 alone, OK432-stimulated lymphocyte supernatants, or OK432-stimulated neutrophil supernatants had no effect on neutrophil activation or suppression of tumor cell proliferation. OK432 in combination with mononuclear cells also had no effect on the inhibition of CEM cell proliferation. Pretreatment of OKMS at 56°C for 30 min did not affect its ability to activate neutrophils, implying that complement activation is not responsible for the neutrophil activation. Supernatants from OK432-stimulated mononuclear cells, as determined by enzyme-linked immunosorbent assays and radioimmunoassays, contained high levels of interleukin-8 (IL-8; 1567±145 pg/ml) and tumor necrosis factor (TNFα; 2105±152 pg/ml), low levels of leukotriene B4 (800±45 pg/ml) and IL-1β (180±22 pg/ml), but interferon γ was not detectable. IL-1β, IL-8, and TNFα transcripts, undetectable in untreated monocytes, increased significantly after 30–60 min exposure to OK432. These results suggest that neutrophil-activating factors from monocytes or resident macrophages may play an important role in the OK432-induced neutrophil activation and antitumor activity.Keywords
This publication has 35 references indexed in Scilit:
- Effect of Fibronectin on IgA-Mediated Uptake of Type III Group B Streptococci by PhagocytesThe Journal of Infectious Diseases, 1990
- Treatment of malignant ascites and pleurisy by a streptococcal preparation OK-432 with fresh frozen plasma—a mechanism of polymorphonuclear leukocyte (PMN) accumulationInternational Journal of Immunopharmacology, 1989
- Neutrophil migration induced by inflammatory stimuli is reduced by macrophage depletionInflammation Research, 1988
- Molecular cloning of a human monocyte-derived neutrophil chemotactic factor (MDNCF) and the induction of MDNCF mRNA by interleukin 1 and tumor necrosis factor.The Journal of Experimental Medicine, 1988
- Neutrophil-mediated tumor cell destruction in cancer ascites: II. A OK-432 attracts killer neutrophils through activation of complement C5Clinical Immunology and Immunopathology, 1987
- Molecular Cloning of the Complementary DNA for Human Tumor Necrosis FactorScience, 1985
- Chemotactic peptide-induced changes in neutrophil actin conformation.The Journal of cell biology, 1984
- Chemotactic peptide modulation of actin assembly and locomotion in neutrophils.The Journal of cell biology, 1984
- Cytochalasin D inhibits actin polymerization and induces depolymerization of actin filaments formed during platelet shape changeNature, 1981
- Number and evolutionary conservation of α- and β-tubulin and cytoplasmic β- and γ-actin genes using specific cloned cDNA probesCell, 1980