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Strain‐dependency of leukotriene C 4 generation from isolated lungs of immunized mice
Author(s) -
ZuanyAmorim Claudia,
Vargaftig B. Boris,
Maclouf Jacques,
Pretolani Marina
Publication year - 1994
Publication title -
british journal of pharmacology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.432
H-Index - 211
eISSN - 1476-5381
pISSN - 0007-1188
DOI - 10.1111/j.1476-5381.1994.tb13215.x
Subject(s) - strain (injury) , chemistry , biology , microbiology and biotechnology , immunology , medicine
1 The antigen‐induced leukotriene C 4 (LTC 4 )‐like‐material release from isolated perfused lungs of actively sensitized Swiss, Balb/C and CBA/J mice was compared. The intra‐tracheal (i.t.) instillation of 1 and 100 μg ovalbumin to lungs from Swiss mice was followed by a dose‐dependent generation of LTC 4 ‐like material into the effluent, as detected by radio‐immunoassay and h.p.l.c., followed by an enzyme‐immunoassay. In contrast, lungs from sensitized Balb/C and CBA/J mice failed to exhibit LTC 4 ‐like‐material release in amounts above the basal values. No histamine secretion was observed when lungs of the three strains of mice were challenged with ovalbumin. 2 The i.t. instillation of 1 or 10 μg platelet‐activating factor (PAF) or of 100 μg arachidonic acid to lungs from non‐sensitized mice, induced the release of comparable amounts of LTC 4 ‐like‐material in the effluent, irrespective to the strain. However, N‐formyl‐ l ‐methionyl‐ l ‐leucyl‐ l ‐phenylalanine (fMLP, 0.1, 10 μg), was more effective in inducing the release of LTC 4 ‐like‐material from lung from Swiss and CBA, than from Balb/C, mice. 3 The intraplantar injection of 0.01 μg ovalbumin to sensitized Swiss mice induced an intense oedema formation, as measured plethysmographically, while Balb/C mice required a dose of antigen at least 10 fold higher for a similar response. CBA/J mice did not respond to antigen challenge in terms of oedema formation. The intraplantar injection of PAF or fMLP to non‐immunized mice induced an oedema of similar intensity in all the strains considered. Accordingly, the different responses to ovalbumin of the three strains of mice is not accounted for by different paw responsiveness to inflammatory mediators. 4 Swiss and CBA/J mice exhibited higher titers of circulating IgG antibodies, as measured by passive cutaneous anaphylaxis (PCA), than Balb/C mice. Conversely, lower IgE titers were measured in the serum of sensitized Swiss and CBA/J mice, as compared to Balb/C. 5 Our results demonstrate a strain‐dependency of antigen‐induced LTC 4 release from lungs from sensitized mice. This difference is related to the ability of sensitized animals to develop immediate hypersensitivity responses, such as paw oedema formation, but not to the antibody subclass involved in the immunization. Strain‐dependent factors may influence the intensity of the response to antigen stimulation. It is thus essential to characterize the different components of the immune response when mouse models for studying hypersensitivity reactions are developed.

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