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1 Department of Large Animal Clinical Sciences and 2 Department of Pharmacology and Toxicology, Michigan State University, East Lansing, Michigan 48824
Neutrophilic inflammation in small airways (SA)
and bronchospasm mediated via muscarinic receptors are features of
chronic obstructive pulmonary disease in horses (COPD). Histamine,
serotonin, and leukotrienes (LTs) are reported to be involved in the
exacerbation of COPD, and currently, histamine has been shown to
increase tension response to electrical field simulation (EFS) in
equine SA. We tested the effects of these mediators and the effects of
activated neutrophils on the cholinergic responses in SA. Histamine,
serotonin, and LTD4 had a
synergistic effect on EFS responses and only an additive effect on the
tension response to exogenous ACh or methacholine. Atropine and TTX
entirely eliminated the EFS-induced tension response in the presence of
all three inflammatory mediators, indicating that augmentation of the
EFS response applies only to the endogenous cholinergic response.
Neutrophils isolated from control and COPD-affected horses were
activated by zymosan, producing 18.1 ± 2.3 and 25.0 ± 2.3 nmol
superoxide · 106
cells
1 · 30 min
1, respectively.
However, in contrast to the profound effect of mediators, incubation of
SA for over 1 h in a suspension of up to 30 × 106 zymosan-treated neutrophils/ml
did not significantly affect EFS responses of SA isolated from either
control or COPD-affected horses. We conclude that in equine SA
1) the endogenous cholinergic responses are subject to strong facilitation by inflammatory mediators; 2) activated neutrophils do not
affect cholinergic responses in SA; and
3) in acute bouts of equine COPD,
histamine, LTD4, and serotonin
(mediators primarily associated with type I allergic reaction) rather
than mediators derived from neutrophils most likely contribute to
increased cholinergic airway tone.
airway smooth muscle; chronic obstructive pulmonary disease; inflammatory mediators; neutrophil activation; zymosan
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