HER2-Specific T-Cell Immune Responses in Patients Vaccinated with Truncated HER2 Protein Complexed with Nanogels of Cholesteryl Pullulan

Purpose: We developed a complex of tumor antigen protein with a novel nanoparticle antigen delivery system of cholesteryl pullulan (CHP). To target HER2 antigen, we prepared truncated HER2 protein 1-146 (146HER2) complexed with CHP, the CHP-HER2 vaccine. We designed a clinical study to assess the sa...

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Veröffentlicht in:Clinical cancer research 2006-12, Vol.12 (24), p.7397-7405
Hauptverfasser: KITANO, Shigehisa, KAGEYAMA, Shinichi, NISHIKAWA, Masakatsu, SUNAMOTO, Junzo, AKIYOSHI, Kazunari, KANEMATSU, Takashi, SCOTT, Andrew M, MURPHY, Roger, HOFFMAN, Eric W, OLD, Lloyd J, SHIKU, Hiroshi, NAGATA, Yasuhiro, MIYAHARA, Yoshihiro, HIASA, Atsunori, NAOTA, Hiroaki, OKUMURA, Satoshi, IMAI, Hiroshi, SHIRAISHI, Taizo, MASUYA, Masahiro
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Sprache:eng
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Zusammenfassung:Purpose: We developed a complex of tumor antigen protein with a novel nanoparticle antigen delivery system of cholesteryl pullulan (CHP). To target HER2 antigen, we prepared truncated HER2 protein 1-146 (146HER2) complexed with CHP, the CHP-HER2 vaccine. We designed a clinical study to assess the safety of the vaccine and HER2-specific T-cell immune responses measured by the newly developed enzyme-linked immunospot assay with mRNA-transduced phytohemagglutinin-stimulated CD4 + T cells in HLA-A2402-positive patients with therapy-refractory HER2-expressing cancers. Experimental Design: Nine patients with various types of solid tumors were enrolled. Each patient was s.c. vaccinated biweekly with 300 μg of CHP-HER2 vaccine for three times followed by booster doses. HER2-specific T-cell responses were evaluated by enzyme-linked immunospot assay by targeting autologous phytohemagglutinin-stimulated CD4 + T cells transduced with 146HER2-encoding mRNA to cover both identified peptides and unknown epitopes for MHC class I and class II that might exist in the sequence of the vaccine protein. Results: CHP-HER2 vaccine was well tolerated; the only adverse effect was grade 1 transient skin reaction at the sites of vaccination. HER2-specific CD8 + and/or CD4 + T-cell immune responses were detected in five patients who received four to eight vaccinations, among whom both T-cell responses were detected in these patients. In four patients with CD8 + T-cell responses, two patients reacted to previously identified HER2 63-71 peptide and the other two reacted only to 146HER2 mRNA-transduced cells. Conclusions: CHP-HER2 vaccine was safe and induced HER2-specific CD8 + and/or CD4 + T-cell immune responses.
ISSN:1078-0432
1557-3265
DOI:10.1158/1078-0432.CCR-06-1546