Activity of pulmonary intravascular macrophages in cats and dogs with and without adult Dirofilaria immitis

Pulmonary intravascular macrophages (PIMs), large (20–80 μm diameter) monocytes are present in sheep, pigs, and horses, but not in dogs, rats, rabbits, or primates. The present study evaluated the phagocytic activity of various organs in cats and dogs and determined the influence of Dirofilaria immi...

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Bibliographic Details
Published in:Veterinary parasitology 2008-12, Vol.158 (3), p.171-176
Main Authors: Dillon, A.R., Warner, A.E., Brawner, W., Hudson, J., Tillson, M.
Format: Article
Language:English
Subjects:
adult animals
animal tissues
Animals
Canine heartworm
Cat Diseases - immunology
Cat Diseases - parasitology
Cats
cell death
colloids
Dirofilaria immitis
Dirofilaria immitis - immunology
Dirofilaria immitis - parasitology
dirofilariasis
Dirofilariasis - immunology
Dirofilariasis - parasitology
Dog Diseases - immunology
Dog Diseases - parasitology
Dogs
Feline heartworm
heartworms
inflammation
intravenous injection
jugular vein
liver
Lung - parasitology
Lung - pathology
lungs
macrophages
Macrophages, Alveolar - cytology
Macrophages, Alveolar - immunology
Macrophages, Alveolar - ultrastructure
Microscopy, Electron, Transmission - veterinary
Microvilli - pathology
Microvilli - ultrastructure
monocytes
mortality
necropsy
Organ Specificity
pets
phagocytosis
Primates
pulmonary artery
Pulmonary Artery - parasitology
Pulmonary Artery - ultrastructure
Pulmonary intravascular macrophage
pulmonary intravascular macrophages
pulmonary parenchyma
Random Allocation
signs and symptoms (animals and humans)
temporal variation
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Summary:Pulmonary intravascular macrophages (PIMs), large (20–80 μm diameter) monocytes are present in sheep, pigs, and horses, but not in dogs, rats, rabbits, or primates. The present study evaluated the phagocytic activity of various organs in cats and dogs and determined the influence of Dirofilaria immitis infections on PIM activity. Live or dead adult heartworm (HW) was transplanted via jugular venotomy into cats and dogs. Cats (four per group) were allocated to five groups: surgical controls—no HW, dead HW for 1 week, live HW for 1 week, dead HW for 3 weeks, or live HW for 3 weeks. Radioactive technetium (Tc-99m, 1.2 mCi in 0.3 ml) sulfa-colloid was injected intravenously. All cats with HW were clinically asymptomatic and developed radiographic pulmonary parenchymal changes. No gross changes were visible at necropsy for cats with HW; inflammatory changes were less severe in cats with live HW. In cats with dead HW for 3 weeks, worms were present but folded, flattened, and located in distal pulmonary arteries. Uninfected control dogs and those with dead HW did not demonstrate any PIM activity. In control cats, lungs were the primary phagocytic organ after systemic IV colloid injection (72.5% of the total recovered radioactive dose). The lung and liver together represented over 95% of the recovered Tc-99m colloid in all cats. In each group of cats with HW, phagocytic activity of the lung was significantly less ( p < 0.001) than the PIM activity of controls. Cats with dead HW at 1 week (50.1%) had a significant ( p < 0.019) decrease in PIM activity compared with cats with dead HW at 3 weeks (59.5%). The PIM activity in cats with live HW was significantly decreased ( p < 0.001) from that in groups with dead HW, but there was no significant difference between the two groups infected with live worms. There were no significant differences in recovery between any groups in pairwise analysis of the spleen, heart, skeletal muscle, kidney, bone marrow, or blood. Significant increases ( p < 0.001) in liver activity for each group inversely reflected the decreased lung activity; consistent with increased hepatic uptake of Tc colloid “escaping” a relatively suppressed lung macrophage system. Transmission electron microscopy confirmed PIM glycocalyx changes and vacuolization, moderate Type 1 cell damage and Type II cell hypertrophy in cats with dead HW. There was no evidence of PIM death. The significant decrease in PIM activity in groups with dead HW and a greater decrease
ISSN:0304-4017
1873-2550
DOI:10.1016/j.vetpar.2008.09.004