Autocrine interaction between IL-5 and IL-1β mediates altered responsiveness of atopic asthmatic sensitized airway smooth muscle
Hakon Hakonarson, … , Sing Chuang, Michael M. Grunstein
Hakon Hakonarson, … , Sing Chuang, Michael M. Grunstein
Published September 1, 1999
Citation Information: J Clin Invest. 1999;104(5):657-667. https://doi.org/10.1172/JCI7137.
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Article

Autocrine interaction between IL-5 and IL-1β mediates altered responsiveness of atopic asthmatic sensitized airway smooth muscle

Abstract

T-helper type 2 (Th2) cytokines have been implicated in the pathogenesis of the pulmonary inflammatory response and altered bronchial responsiveness in allergic asthma. To elucidate the mechanism of Th2-dependent mediation of altered airway responsiveness in the atopic asthmatic state, the expression and actions of specific cytokines were examined in isolated rabbit and human airway smooth muscle (ASM) tissues and cultured cells passively sensitized with sera from atopic asthmatic patients or nonatopic/nonasthmatic (control) subjects. Relative to control tissues, the atopic asthmatic sensitized ASM exhibited significantly enhanced maximal isometric contractility to acetylcholine and attenuated relaxation responses to isoproterenol. These proasthmatic changes in agonist responsiveness were ablated by pretreating the atopic sensitized tissues with either an IL-5 receptor blocking antibody (IL-5ra) or the human recombinant IL-1 receptor antagonist (IL-1ra), whereas an IL-4 neutralizing antibody had no effect. Moreover, relative to controls, atopic asthmatic sensitized ASM cells demonstrated an initial, early (after 3 hours of incubation) increased mRNA expression and protein release of IL-5. This was followed (after 6 hours of incubation) by an enhanced mRNA expression and release of IL-1β protein, an effect that was inhibited in sensitized cells pretreated with IL-5ra. Extended studies demonstrated that naive ASM exposed to exogenously administered IL-5 exhibited an induced upregulated mRNA expression and protein release of IL-1β associated with proasthmatic-like changes in ASM constrictor and relaxant responsiveness, and that these effects were ablated in tissues pretreated with IL-1ra. Taken together, these observations provide new evidence that (a) the Th2 cytokine IL-5 and the pleiotropic proinflammatory cytokine IL-1β are endogenously released by atopic asthmatic sensitized ASM and mechanistically interact to mediate the proasthmatic perturbations in ASM responsiveness; and (b) the nature of this interaction is given by an initial endogenous release of IL-5, which then acts to induce the autologous release of IL-1β by the sensitized ASM itself, resulting in its autocrine manifestation of the proasthmatic phenotype.

Authors

Hakon Hakonarson, Neil Maskeri, Carrie Carter, Sing Chuang, Michael M. Grunstein

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Figure 1

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Comparison of contractile dose-response relationships to ACh in paired h...
Comparison of contractile dose-response relationships to ACh in paired human control serum–treated (open circles) and human atopic asthmatic serum–treated rabbit ASM segments in the absence (closed circles) and presence (open squares) of maximum effective concentrations of IL-5ra (a) and IL-1ra (b). Relative to controls, the heightened constrictor responses to ACh in the atopic asthmatic serum–sensitized tissues were prevented by cotreatment of tissues with either IL-5ra or IL-1ra. Data represent mean ± SE values from 6 paired experiments.