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01.10.2003 | Original Article

A preclinical study comparing approaches for augmenting the immunogenicity of a heptavalent KLH-conjugate vaccine against epithelial cancers

verfasst von: Govind Ragupathi, Fusataka Koide, Natarajan Sathyan, Ella Kagan, Maria Spassova, William Bornmann, Polly Gregor, Celso A. Reis, Henrik Clausen, Samuel J. Danishefsky, Philip O. Livingston

Erschienen in: Cancer Immunology, Immunotherapy | Ausgabe 10/2003

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Abstract

Previously using a series of monovalent vaccines, we demonstrated that the optimal method for inducing an antibody response against cancer cell-surface antigens is covalent conjugation of the antigens to keyhole limpet hemocyanin (KLH) and the use of a saponin adjuvant. We have prepared a heptavalent-KLH conjugate vaccine containing the seven epithelial cancer antigens GM2, Globo H, Lewis^y, TF(c), Tn(c), STn(c), and glycosylated MUC1. In preparation for testing this vaccine in the clinic, we tested the impact on antibody induction of administering the individual conjugates plus adjuvant compared with a mixture of the seven conjugates plus adjuvant, and of several variables thought to augment immunogenicity. These include approaches for decreasing suppressor cell activity or increasing helper T-lymphocyte activity (low dose cyclophosphamide or anti-CTLA-4 MAb), different saponin adjuvants at various doses (QS-21 and GPI-0100), and different methods of formulation (lyophilization and use of polysorbate 80). We find that: (1) Immunization with the heptavalent-KLH conjugate plus GPI-0100 vaccine induces antibodies against the seven antigens of comparable titer to those induced by the individual-KLH conjugate vaccines, high titers of antibodies against Tn (median ELISA titer IgM/IgG 320/10,240), STn (640/5,120), TF (320/10,240), MUC1 (80/20,480), and globo H (640/40); while lower titers of antibodies against Lewis^y (160/0) and only occasional antibodies against GM2 are induced. (2) These antibodies reacted with the purified synthetic antigens by ELISA, and with naturally expressed antigens on the cancer cell surface by FACS. (3) None of the approaches for further altering the suppressor cell/helper T-cell balance nor changes to the standard formulation by lyophilization or use of polysorbate 80 had any impact on antibody titers. (4) An optimal dose of saponin adjuvant, QS-21 (50 μg) or GPI-0100 (1000 μg), is required for optimal antibody titers. This heptavalent vaccine is sufficiently optimized for testing in the clinic.

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Titel: A preclinical study comparing approaches for augmenting the immunogenicity of a heptavalent KLH-conjugate vaccine against epithelial cancers
verfasst von: Govind Ragupathi
Fusataka Koide
Natarajan Sathyan
Ella Kagan
Maria Spassova
William Bornmann
Polly Gregor
Celso A. Reis
Henrik Clausen
Samuel J. Danishefsky
Philip O. Livingston
Publikationsdatum: 01.10.2003
Verlag: Springer-Verlag
Erschienen in: Cancer Immunology, Immunotherapy / Ausgabe 10/2003
Print ISSN: 0340-7004
Elektronische ISSN: 1432-0851
DOI: https://doi.org/10.1007/s00262-003-0399-2

Springer Medizin

A preclinical study comparing approaches for augmenting the immunogenicity of a heptavalent KLH-conjugate vaccine against epithelial cancers

Abstract

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Springer Medizin

Abstract

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