Your search keyword '"MANTOVANI B."' showing total 2 results

1. The role of complement in the stimulation of lysosomal enzyme release by polymorphonuclear leucocytes induced by immune complexes of IgG and of IgM.

Author

Lucisano, Y. M. and Mantovani, B.

Subjects

*COMPLEMENT (Immunology), *ENZYMES, *NEUTROPHILS, *IMMUNE complexes, *IMMUNOGLOBULIN G, *IMMUNOGLOBULIN M, *FLUIDS, *IMMUNOGLOBULINS

Abstract

The effect of complement components incorporated into precipitated immune complexes (IC) of IgG or of IgM on their capacity for stimulating lysosomal enzyme release from rabbit polymorphonuclear leucocytes was studied in vitro. We have found that: (i) complement causes an amplification in the stimulatory capacity of both classes of IC, the effect being dependent on the concentration of the IC, and higher for the IgM class; (ii) dose-effect experiments of competition by fluid-phase immunoglobulins have shown that IgG (in physiological or smaller concentrations) can inhibit greatly the stimulation by this class of immune complex; this inhibition can be prevented, however, by the presence of complement in the IC (a situation expected to occur in vivo); for IgM immune complexes there was no such competitive inhibition, so complement would not be necessary; (iii) the relevant complement factors must be located in the range Cl-C3. These results help us to understand the importance of complement (besides the welleknown generation of cheinotactic factors) in the mechanisms of tissue injury produced by neutrophils in immune complex diseases. [ABSTRACT FROM AUTHOR]

Published

1988

2. Precipitated immune complexes of IgM as well as of IgG can bind to rabbit polymorphonuclear leucocytes by only the immune complexes of IgG are readily phagocytosed.

Author

Furriel, R.P.M., Lucisano, Y.M., and Mantovani, B.

Subjects

IMMUNOGLOBULIN G, IMMUNOGLOBULIN M, IMMUNOGLOBULINS, LEUCOCYTES, IMMUNE complexes, CELL populations, CELL membranes, LABORATORY rabbits

Abstract

We have shown by in vitro experiments, using immunofluorescence techniques, that precipitated immune complexes of IgM antibodies and ovalbumin (ICIgM) are able to bind to rabbit blood polymorphonuclear leucocytes (PMN), as well as immune complexes of IgG antibodies (ICIgG). This binding capacity for both classes of immune complexes is exhibited by more than 80% of the PMN cell population and is independent of Ca2+ in the medium. For ICIgG the binding to PMN can be completely inhibited by preincubation of the cells with soluble IgG used at physiological concentrations (competition for the Fcγ receptors) while for ICIgM there is no such inhibition by fluid-phase IgM. After binding to the leucocytes there was a striking difference in the fate of ICIgM and ICIgG: whereas the ICIgG was readily phagocytosed (endocytosed), the ICIgM remained mostly on the cell surface, being only poorly endocytosed after I hr incubation at 37°. This was demonstrated by a quantitative fluorimetric method developed to assay phagocytosis of immune complexes, and was confirmed by a qualitative fluorescence quenching technique. These results may have implications for understanding the fate of these classes of immune complexes formed in circulation or deposited in tissues, and the participation of PMN in inflammatory reactions and tissue injury in immune complex diseases. [ABSTRACT FROM AUTHOR]

Published

1992