Literature DB >> 14654536

Immunization of cancer patients with HER-2/neu-derived peptides demonstrating high-affinity binding to multiple class II alleles.

Lupe G Salazar1, John Fikes, Scott Southwood, Glenn Ishioka, Keith L Knutson, Theodore A Gooley, Kathy Schiffman, Mary L Disis.   

Abstract

PURPOSE: The purpose of this study was to immunize patients with HER-2/neu-overexpressing cancer with a multipeptide vaccine comprised of four class II HER-2/neu peptides that had been identified as the most immunogenic in a previous clinical trial. Furthermore, we questioned whether MHC binding affinity could predict the in vivo immunogenicity of the HER-2/neu helper peptides. EXPERIMENTAL
DESIGN: Four putative class II HER-2/neu peptides, which were found to generate detectable specific T-cell responses (stimulation index > 2) in a majority of patients in a previous study, were used to formulate a single vaccine. The multipeptide vaccine was administered intradermally with granulocyte macrophage colony-stimulating factor as an adjuvant. Ten patients with HER-2/neu overexpressing breast or lung cancer were enrolled. HER-2/neu peptide-and protein-specific T cell and antibody immune responses were measured. Competitive inhibition assays were used to analyze the class II HER-2/neu peptides for their binding affinity to 14 common HLA-DR alleles.
RESULTS: Twenty-five percent of patients developed HER-2/neu peptide-specific T-cell immunity, and 50% developed HER-2/neu peptide-specific antibody immunity. No patient developed HER-2/neu protein-specific T cell or antibody immunity. The majority of peptides exhibited high binding affinity, in vitro, to >/==" BORDER="0">3 of the 14 DR alleles analyzed.
CONCLUSION: The group of peptides used in this study demonstrated high binding affinity to multiple DR alleles suggesting that in vitro binding affinity may be able to predict the in vivo immunogenicity of class II peptides. However, only a minority of patients immunized with the multipeptide vaccine developed HER-2/neu peptide-specific T cell or antibody immunity, and none developed HER-2/neu protein-specific immunity.

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Year:  2003        PMID: 14654536

Source DB:  PubMed          Journal:  Clin Cancer Res        ISSN: 1078-0432            Impact factor:   12.531


  25 in total

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Review 2.  Use of tumour-responsive T cells as cancer treatment.

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Review 4.  Therapeutic cancer vaccines and translating vaccinomics science to the global health clinic: emerging applications toward proof of concept.

Authors:  Megan M O'Meara; Mary L Disis
Journal:  OMICS       Date:  2011-07-06

Review 5.  Selection of epitopes from self-antigens for eliciting Th2 or Th1 activity in the treatment of autoimmune disease or cancer.

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6.  Vaccine-Induced Memory CD8+ T Cells Provide Clinical Benefit in HER2 Expressing Breast Cancer: A Mouse to Human Translational Study.

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Journal:  Clin Cancer Res       Date:  2019-01-11       Impact factor: 12.531

7.  Polyclonal immune responses to antigens associated with cancer signaling pathways and new strategies to enhance cancer vaccines.

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Review 8.  Tumor vaccines for breast cancer.

Authors:  Karen S Anderson
Journal:  Cancer Invest       Date:  2009-05       Impact factor: 2.176

9.  Biologic and immunologic effects of preoperative trastuzumab for ductal carcinoma in situ of the breast.

Authors:  Henry M Kuerer; Aman U Buzdar; Elizabeth A Mittendorf; Francisco J Esteva; Anthony Lucci; Luis M Vence; Laszlo Radvanyi; Funda Meric-Bernstam; Kelly K Hunt; William Fraser Symmans
Journal:  Cancer       Date:  2010-08-24       Impact factor: 6.860

10.  Synergism from combined immunologic and pharmacologic inhibition of HER2 in vivo.

Authors:  Michael A Morse; Junping Wei; Zachary Hartman; Wenle Xia; Xiu-Rong Ren; Gangjun Lei; William T Barry; Takuya Osada; Amy C Hobeika; Sharon Peplinski; Haixiang Jiang; Gayathri R Devi; Wei Chen; Neil Spector; Andrea Amalfitano; H Kim Lyerly; Timothy M Clay
Journal:  Int J Cancer       Date:  2010-06-15       Impact factor: 7.396

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