TY - JOUR
T1 - Cytokine production by rabbit alveolar macrophages
T2 - Differences between activated and suppressor cell phenotypes
AU - Kobayashi, Hiroyuki
AU - Kobayashi, Makiko
AU - Heming, Thomas A.
AU - Bidani, Akhil
AU - Pollard, Richard B.
AU - Suzuki, Fujio
PY - 1999/9/1
Y1 - 1999/9/1
N2 - The differences between cytokine-producing profiles of activated macrophages (A-Mφ) and suppressor macrophages (S-Mφ) were examined. A-Mφ, which exhibited cytotoxicity against RK-13 cells, were generated from resident rabbit alveolar Mφ by treatment with lymphokine solution (culture fluids of rabbit spleen cells stimulated with concanavalin A [Con A]). S-Mφ, which were able to inhibit cellular proliferations of rabbit spleen cells stimulated with Con A, were generated from resident alveolar Mφ by treatment with 1-methyladenosine (an immunosuppressive molecule in tumourous ascites fluids). When A-Mφ were stimulated with lipopolysaccharide (LPS) in vitro, the cells produced significantly more interleukin (IL)-1 (~1.4 times), IL-6 (~2.1 times), IL-12 (~60 times), and tumour necrosis factor-α (TNF-α) (~37 times) than did resting macrophages (R-Mφ) stimulated with LPS as control cells. After the stimulation with LPS, both A-Mφ and R-Mφ did not produce transforming growth factor-β (TGF-β). In contrast, when S-Mφ were stimulated with LPS in vitro, the cells produced significantly more TGF-β (~1.6 times) and significantly less IL-6 (~1.8 times) than did control cells. Also, S-Mφ did not produce IL-1, IL-12, and TNF-α into their culture fluids after the stimulation with LPS. These results show the differences between cytokine-producing profiles of A-Mφ and S-Mφ and characteristics of their cytokine-producing profiles are analogous to T cell subsets. Differences displayed in the cytokine profiles may contribute to the effector (A-Mφ) or the suppressor (S-Mφ) functions of alveolar Mφ.
AB - The differences between cytokine-producing profiles of activated macrophages (A-Mφ) and suppressor macrophages (S-Mφ) were examined. A-Mφ, which exhibited cytotoxicity against RK-13 cells, were generated from resident rabbit alveolar Mφ by treatment with lymphokine solution (culture fluids of rabbit spleen cells stimulated with concanavalin A [Con A]). S-Mφ, which were able to inhibit cellular proliferations of rabbit spleen cells stimulated with Con A, were generated from resident alveolar Mφ by treatment with 1-methyladenosine (an immunosuppressive molecule in tumourous ascites fluids). When A-Mφ were stimulated with lipopolysaccharide (LPS) in vitro, the cells produced significantly more interleukin (IL)-1 (~1.4 times), IL-6 (~2.1 times), IL-12 (~60 times), and tumour necrosis factor-α (TNF-α) (~37 times) than did resting macrophages (R-Mφ) stimulated with LPS as control cells. After the stimulation with LPS, both A-Mφ and R-Mφ did not produce transforming growth factor-β (TGF-β). In contrast, when S-Mφ were stimulated with LPS in vitro, the cells produced significantly more TGF-β (~1.6 times) and significantly less IL-6 (~1.8 times) than did control cells. Also, S-Mφ did not produce IL-1, IL-12, and TNF-α into their culture fluids after the stimulation with LPS. These results show the differences between cytokine-producing profiles of A-Mφ and S-Mφ and characteristics of their cytokine-producing profiles are analogous to T cell subsets. Differences displayed in the cytokine profiles may contribute to the effector (A-Mφ) or the suppressor (S-Mφ) functions of alveolar Mφ.
KW - Alveolar macrophages
KW - Classification
KW - Cytokine-producing profiles
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U2 - 10.1016/S0165-2478(99)00114-5
DO - 10.1016/S0165-2478(99)00114-5
M3 - Article
C2 - 10528798
AN - SCOPUS:0032887037
SN - 0165-2478
VL - 69
SP - 339
EP - 346
JO - Immunology Letters
JF - Immunology Letters
IS - 3
ER -