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1 October 2002 Inhibition of tumor growth in mice with severe combined immunodeficiency is mediated by heat shock protein 70 (Hsp70)-peptide–activated, CD94 positive natural killer cells
Christian Moser, Christin Schmidbauer, Ulrich Gürtler, Catharina Gross, Mathias Gehrmann, Gerald Thonigs, Karin Pfister, Gabriele Multhoff
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Abstract

Previously, we reported that the major stress-inducible heat shock protein 70 (Hsp70) acts as a recognition structure for natural killer (NK) cells, if localized on the cell surface of tumor cells. Incubation of purified NK cells with low-dose interleukin (IL)-2 (100 IU/mL) plus recombinant Hsp70-protein or the immunogenic 14-mer Hsp70-peptide TKDNNLLGRFELSG450–463, termed TKD (2 μg/mL), enhances the cytolytic activity against Hsp70 membrane-positive (CX ) but not against Hsp70-negative (CX−) tumor cells. Here, we show that the cytolytic activity against Hsp70-positive tumor cells is inducible by incubation of unseparated peripheral blood mononuclear cells (PBMNC) with low-dose IL-2 plus TKD. Cell sorting experiments revealed that within the PBMNC population CD94 /CD3− NK cells, and not CD94−/CD3 T cells, mediate the cytotoxic activity against Hsp70-positive tumor cells. The antitumoral effect of PBMNC stimulated either with IL-2 plus TKD or with IL-2 alone was assessed in tumor-bearing severe combined immunodeficiency/beige mice. A single intravenous (iv) injection of 40 × 106 IL-2 plus TKD-stimulated PBMNC (containing 5.2 × 106 NK cells) on day 4 results in a 60% reduction in tumor size, from 3.89 g to 1.56 g. In contrast, the adoptive transfer of the identical amount PBMNC stimulated with low-dose IL-2 only (containing 4.4 × 106 NK cells) reduces the tumor size only less than 10% (3.64 g). A phenotypic characterization of the excised tumors revealed that predominantly Hsp70-positive tumor cells were eliminated by TKD-activated PBMNC. Kinetic studies demonstrate that the in vivo cytolytic capacity of TKD-stimulated PBMNC is dependent on the effector to target cell ratio. An iv injection of effector cells on day 1 or 2 after tumor cell inoculation results in significantly smaller tumors (0.77 g or 0.89 g) on day 21 as compared with mice that were immunoreconstituted on day 4 or 8 (1.39 g or 2.23 g). The tumor size of nonimmunoreconstituted control animals was 3.55 g.

Christian Moser, Christin Schmidbauer, Ulrich Gürtler, Catharina Gross, Mathias Gehrmann, Gerald Thonigs, Karin Pfister, and Gabriele Multhoff "Inhibition of tumor growth in mice with severe combined immunodeficiency is mediated by heat shock protein 70 (Hsp70)-peptide–activated, CD94 positive natural killer cells," Cell Stress & Chaperones 7(4), 365-373, (1 October 2002). https://doi.org/10.1379/1466-1268(2002)007<0365:IOTGIM>2.0.CO;2
Received: 19 March 2002; Accepted: 1 May 2002; Published: 1 October 2002
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