Interleukin 1 can replace monocytes for the specific human B-cell response to a particulate antigen |
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Authors: | Aimé Vazquez Jean-François Balavoine Jean-François Delfraissy Hiro Wakasugi Pierre Galanaud |
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Affiliation: | 1. INSERM Unité 131, 32 rue des Carnets, 92140 Clamart, and Université Paris-Sud, Paris, France;2. Groupe d''Immunologie des Tumeurs, Institut Gustave Roussy, 94805 Villejuif, France |
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Abstract: | It is shown that the anti-trinitrophenyl (TNP) response of human B cells to trinitrophenyl polyacrylamide beads (TNP-PAA) is monocyte dependent. This response is abolished by extensive adherent cell depletion and restored by the addition of monocytes. The optimal response is obtained with 3% monocytes, higher numbers being suppressive. Supernatants from muramyl dipeptide (MDP)-activated monocytes can restore the response of monocyte-depleted preparations even when cells are cultured at suboptimal concentration. A partially purified preparation of interleukin (IL-1) has a comparable restorative ability. The following arguments suggest that monocytes do not function as antigen-presenting cells for this particulate antigen: (i) anti-genpulsed monocytes induce neither an anti-TNP response nor a specific T-cell proliferative response; (ii) allogeneic monocytes function as well as autologous monocytes to restore the response of nonadherent cells; (iii) HLA-DR-negative cells from the human leukemia cell line K562 can replace monocytes for this response. Monocyte supernatants do not replace T cells for the response of B-enriched lymphocytes, showing that T cells are directly involved in B-cell activation. |
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Keywords: | To whom correspondence should be addressed: INSERM Unité 131 32 rue des Carnets 92140 Clamart France. |
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