Addition of systemic IL2 increases effectiveness of hu14.18-IL2 immunocytokine therapy against NXS2 murine neuroblastoma

Introduction: The hu14.18-IL2 immunocytokine (IC) links rhIL2 to humanized anti-GD2 monoclonal antibody hu14.18 and inhibits NXS2 tumor growth in A/J mice. This study combined systemic IL2 with hu14.18-IL2 therapy to increase antitumor effects. Methods: A/J mice with subcutaneous NXS2 tumors receive...

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Published inJournal of the American College of Surgeons Vol. 199; no. 3; pp. 54 - 55
Main Authors Yang, Jeannie C., Neal, Zane, Rakhmilevich, Alexander, Buhtoiarov, Ilia, Lum, Hillary, Imboden, Michael, Hank, Jacquelyn, Lode, Holger, Reisfeld, Ralph, Gillies, Stephen, Sondel, Paul
Format Journal Article
LanguageEnglish
Published Elsevier Inc 01.09.2004
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Summary:Introduction: The hu14.18-IL2 immunocytokine (IC) links rhIL2 to humanized anti-GD2 monoclonal antibody hu14.18 and inhibits NXS2 tumor growth in A/J mice. This study combined systemic IL2 with hu14.18-IL2 therapy to increase antitumor effects. Methods: A/J mice with subcutaneous NXS2 tumors received rhIL2 (50,000 IU/d by continuous infusion pump) × 7 d, IC (5 micrograms/d × 5), IC (22 micrograms/d × 5), or combined rhIL2 and IC (5 micrograms/d). Mice were also depleted of NK or T cells during combined therapy. Proliferation assays of human and murine cells with high-affinity IL2Rs (T cells) or intermediate-affinity IL2Rs (NK cells) were performed. Results: The combination of systemic IL2 and IC therapy resulted in durable resolution of NXS2 tumors. This antitumor effect was greater than that achieved by either rhIL2 or IC alone (p = 0.026 and 0.007). The efficacy of the combined treatment was dependent on NK and T cells. Although IL2 in the form of an immunocytokine and rhIL2 induce similar proliferation of human NK and T cells, the immunocytokine is less potent than rhIL2 at stimulating murine NK and T cells (3 to 20-fold less, respectively). Conclusions: The combination of systemic IL2 and hu14.18-IL2 is more effective than either therapy alone in A/J mice bearing subcutaneous NXS2 tumors and involves both NK and T cells. This may be the result of NK cell activation and expansion prior to IC treatment and reflect the stronger IL2-mediated action of rhIL2 than IC on murine IL2R-bearing cells.
ISSN:1072-7515
1879-1190
DOI:10.1016/j.jamcollsurg.2004.05.112