Role of interleukin-8 (IL-8) and an inhibitory effect of erythromycin on IL-8 release in the airways of patients with chronic airway diseases.

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Infection and Immunity, October 1994, p. 4145-4152, Vol. 62, No. 10
0019-9567/1994/$04.00+0 DOI:

research-article

Role of interleukin-8 (IL-8) and an inhibitory effect of erythromycin on IL-8 release in the airways of patients with chronic airway diseases.

K Oishi, F Sonoda, S Kobayashi, A Iwagaki, T Nagatake, K Matsushima, and K Matsumoto

Department of Internal Medicine, Nagasaki University, Japan.

ABSTRACT

To evaluate of the role of interleukin-8 (IL-8), a chemotacticcytokine, in the continuous neutrophil accumulation in the airwaysof patients with chronic airway disease (CAD) and persistentPseudomonas aeruginosa infection, we investigated the cell population,IL-8 levels, IL-1 beta levels, tumor necrosis factor (TNF) activities,and neutrophil elastase (NE) activities of bronchoalveolar lavage(BAL) fluids in 17 CAD patients (with P. aeruginosa infections[CAD+PA], n = 9; without any bacterial infections [CAD-PA],n = 8) and 8 normal volunteers. We found significant elevationsof neutrophil numbers, IL-8/albumin ratios, and NE/albumin ratiosin BAL fluids from CAD patients, in the following rank order:CAD+PA > CAD-PA > normal volunteers. IL-1 beta/albuminratios were elevated only in CAD+PA, while no TNF bioactivitywas detected in BAL fluids. The neutrophil numbers correlatedsignificantly with the IL-8/albumin ratios and NE/albumin ratiosin the BAL fluids of CAD patients. When anti-human IL-8 immunoglobulinG was used for neutralizing neutrophil chemotactic factor (NCF)activities in BAL fluids, the mean reduction rate of NCF activitiesin CAD+PA patients was significantly higher than that in CAD-PApatients. We also evaluated the effects of low-dose, long-termerythromycin therapy in BAL fluids from three CAD+PA and twoCAD-PA patients. Treatment with erythromycin caused significantreductions of neutrophil numbers, IL-8/albumin ratios, and NE/albuminratios in BAL fluids from these patients. To elucidate the mechanismof erythromycin therapy, we also examined whether erythromycinsuppressed IL-8 production by human alveolar macrophages andneutrophils in vitro. We demonstrated a moderate inhibitoryeffect of erythromycin on IL-8 production in Pseudomonas-stimulatedneutrophils but not in alveolar macrophages. Our data supportthe view that persistent P. aeruginosa infection enhances IL-8production and IL-8-derived NCF activity, causing neutrophilaccumulation in the airways and the progressive lung injuriesobserved in patients with CAD. The clinical efficacy of erythromycintherapy for CAD patients might be partly mediated through areduced IL-8 production, diminishing neutrophil accumulationand NE release in the airways.

Infection and Immunity, October 1994, p. 4145-4152, Vol. 62, No. 10
0019-9567/1994/$04.00+0 DOI:

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