Phase I Clinical Trial of the Immunocytokine EMD 273063 in Melanoma Patients

King, David M.; Albertini, Mark R.; Schalch, Heidi; Hank, Jacquelyn A.; Gan, Jacek; Surfus, Jean E.; Mahvi, David; Schiller, Joan H.; Warner, Thomas F.; Kim, Kyung Mann; Eickhoff, Jens; Kendra, Kari; Reisfeld, Ralph A.; Gillies, Stephen D.; Sondel, Paul M.

doi:10.1200/jco.2004.11.035

Cited by 130 publications

(127 citation statements)

References 22 publications

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“…Anti-CD20mAb (Di-Leu-16) conjugated to IL-2 has demonstrated enhanced ADCC activity in comparison with the control anti-CD-20 (Rituximab) in SCID mice non-Hodgkin's lymphoma model (NHL) (Gillies et al, 2005). Phase I clinical trial of the immunocytokine EMD 273063, which is constructed of humanized anti-GD2 mAb linked to IL-2, in melanoma patients has been conducted with promising results (King et al, 2004). The immunocytokine induced immune activation, with reversible toxicity.…”

Section: Ab-cytokines/chemokines Conjugatesmentioning

confidence: 99%

Novel antibodies as anticancer agents

2007

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In recent years antibodies, whether generated by traditional hybridoma technology or by recombinant DNA strategies, have evolved from Paul Ehrlich's 'magic bullets' to a modern age 'guided missile'. In the recent years of immunologic research, we are witnessing development in the fields of antigen screening and protein engineering in order to create specific anticancer remedies. The developments in the field of recombinant DNA, protein engineering and cancer biology have let us gain insight into many cancer-related mechanisms. Moreover, novel techniques have facilitated tools allowing unique distinction between malignantly transformed cells, and regular ones. This understanding has paved the way for the rational design of a new age of pharmaceuticals: monoclonal antibodies and their fragments. Antibodies can select antigens on both a specific and a high-affinity account, and further implementation of these qualities is used to target cancer cells by specifically identifying exogenous antigens of cancer cell populations. The structure of the antibody provides plasticity resonating from its functional sites. This review will screen some of the many novel antibodies and antibody-based approaches that are being currently developed for clinical applications as the new generation of anticancer agents.

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Section: Ab-cytokines/chemokines Conjugatesmentioning

confidence: 99%

Novel antibodies as anticancer agents

2007

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“…ICs are synthetic proteins that combine both of these strategies via a tumor antigen-specific mAb fused to an immune-stimulating cytokine. Members of this novel class of immunotherapy have been shown to have significant antitumor and antimetastatic effects in several murine tumor models and are currently being investigated for clinical safety and anticancer potential in human patients with neuroblastoma (NB), melanoma, ovarian and prostate cancers [8,[21][22]32]. Our laboratories have been involved in the preclinical and clinical development of two ICs [39]: huKS-IL2, which consists of the humanized mAb huKS1/4 that recognizes epithelial cell adhesion molecule (EpCAM) and is linked to IL2; and hu14.18-IL2, which is an anti-disialoganglioside GD 2 mAb also linked to IL2.…”

Section: Introductionmentioning

confidence: 99%

Intratumoral immunocytokine treatment results in enhanced antitumor effects

Johnson

Lum

Rakhmilevich

et al. 2008

Cancer Immunol Immunother

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Immunocytokines (IC), consisting of tumor-specific monoclonal antibodies fused to the immunostimulatory cytokine interleukin 2 (IL2), exert significant antitumor effects in several murine tumor models. We investigated whether intratumoral (IT) administration of IC provided enhanced antitumor effects against subcutaneous tumors. Three unique ICs (huKS-IL2, hu14.18-IL2, and GcT84.66-IL2) were administered systemically or IT to evaluate their antitumor effects against tumors expressing the appropriate IC-targeted tumor antigens. The effect of IT injection of the primary tumor on a distant tumor was also evaluated. Here, we show that IT injection of IC resulted in enhanced antitumor effects against B16-KSA melanoma, NXS2 neuroblastoma, and human M21 melanoma xenografts when compared to intravenous (IV) IC injection. Resolution of both primary and distant subcutaneous tumors, and a tumor-specific memory response were demonstrated following IT treatment in immunocompetent mice bearing NXS2 tumors. The IT effect of huKS-IL2 IC was antigen-specific, enhanced compared to IL2 alone, and dose-dependent. Hu14.18-IL2 also showed greater IT effects than IL2 alone. The antitumor effect of IT IC did not always require T cells since IT IC induced antitumor effects against tumors in both SCID and nude mice. Localization studies using radiolabeled 111 In-GcT84.66-IL2 IC confirmed that IT injection resulted in a higher concentration of IC at the tumor site than IV administration. In conclusion, we suggest that IT IC is more effective than IV administration against palpable tumors. Further testing is required to determine how to potentially incorporate IT administration of IC into an antitumor regimen that optimizes local and systemic anticancer therapy.

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“…In the next step, ch14.18 was expressed as a fusion protein with IL-2, to target the cytokine directly to the tumor site [22]. This compound is already being tested in clinical trials [23].…”

Section: Introductionmentioning

confidence: 99%

Induction of IgG antibodies against the GD2 carbohydrate tumor antigen by vaccination with peptide mimotopes

et al. 2006

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The disialoganglioside GD2, a carbohydrate antigen, is expressed on all tumors of neuroectodermal origin, including melanoma, neuroblastoma, sarcoma and small cell lung cancer. Due to its specific expression on tumor surfaces, GD2 is an attractive target for immunotherapies. The mouse/human chimeric anti-GD2 mAb ch14.18 is already applied in melanoma and neuroblastoma trials as a passive immunotherapy. To establish an active immunotherapy alternative, we aimed to replace the poorly immunogenic ganglioside with immunogenic peptides. Previously, we used the ch14.18 antibody to select GD2 peptide mimics from a phage display library. In the present study, two mimics of the ch14.18 epitope were coupled to keyhole limpet hemocyanin and used for immunizing BALB/c mice. Induction of a specific humoral immune response towards the original antigen GD2, both purified and expressed on neuroblastoma and melanoma cells, could be demonstrated in ELISA, Western blot, and immunofluorohistochemistry. As the elicited antibodies were of the IgG isotype, the mimotope conjugates were capable of recruiting T cell help and inducing memory phenomena. In conclusion, we show that an epitope of the carbohydrate antigen GD2 can successfully be translated into immunogenic peptide mimotopes. Our immunization experiments indicate that GD2 mimotopes are suitable for active immunotherapy of GD2-expressing tumors.

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Phase I Clinical Trial of the Immunocytokine EMD 273063 in Melanoma Patients

Cited by 130 publications

References 22 publications

Novel antibodies as anticancer agents

Novel antibodies as anticancer agents

Intratumoral immunocytokine treatment results in enhanced antitumor effects

Induction of IgG antibodies against the GD2 carbohydrate tumor antigen by vaccination with peptide mimotopes

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