Potentiation of the in vitro cytotoxic response to syngeneic lymphoma cells by soluble products of tuberculin-sensitive lymphoid cells stimulated with PPD |
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Authors: | Olusola Alaba Irwin D Bernstein Peter W Wright Karl Erik Hellström |
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Institution: | 1. Divisions of Tumor Immunology and Pediatric Oncology, Fred Hutchinson Cancer Research Center Seattle, Washington 98104 U.S.A.;2. Departments of Pediatrics, Medicine, Microbiology and Pathology, University of Washington, Seattle, Washington 98104 U.S.A. |
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Abstract: | Spleen cells from rats immunized with the syngeneic (C58NT)D Gross virus induced lymphoma have previously been shown to differentiate into cytotoxic effector cells following restimulation with tumor cells in vitro. Previous work has also demonstrated that the addition of PPD-primed syngeneic spleen cells and PPD to cultures of (C58NT)D-primed spleen cells will potentiate the in vitro cytotoxic response to tumor antigens. In the studies presented here, the potentiating effect was found to be mediated by a soluble factor(s) released by nonadherent cells from BCG-primed rats. The release of this immunopotentiating factor(IPF) required the presence of PPD and varied with the concentration of PPD added. IPF was produced by BCG-primed spleen, lymph node, and thymus cells. Maximal production of IPF in PPD-stimulated cultures was obtained after 6–12 hr of incubation. Supernatants obtained after 30 hr of incubation lacked apparent IPF activity when tested initially, but activity was recovered after mild heat treatment. Recovery of IPF activity after heat exposure is best explained by the presence of a heat-labile inhibitor. IPF itself is stable to heat treatment to 56 °C for 40 min. IPF was also shown to be capable of enhancing immune responses to histocompatibility antigens in vitro. |
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Keywords: | Send reprint requests to Warren Strober M D National Institutes of Health Bldg 10 Room 4N116 Bethesda Md 20205 |
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