Treatment of Mammary Carcinomas in HER-2 Transgenic Mice through Combination of Genetic Vaccine and an Agonist of Toll-Like Receptor 9

Author:

Aurisicchio Luigi1,Peruzzi Daniela1,Conforti Antonella1,Dharmapuri Sridhar1,Biondo Antonella1,Giampaoli Saverio1,Fridman Arthur2,Bagchi Ansu2,Winkelmann Christopher T.3,Gibson Raymond3,Kandimalla Ekambar R.4,Agrawal Sudhir4,Ciliberto Gennaro1,La Monica Nicola1

Affiliation:

1. 1Istituto di Ricerche di Biologia Molecolare, Oncology/Functional Department, Merck Research Labs, Rome, Italy;

2. 2Applied Computer Science and Mathematics, Merck Research Labs, Rahway, New Jersey;

3. 3Imaging Department, Merck Research Labs, West Point, Pennsylvania; and

4. 4Idera Pharmaceuticals, Cambridge, Massachusetts

Abstract

Abstract Purpose: Oligodeoxynucleotides containing unmethylated CpG dinucleotides induce innate and adaptive immunity through Toll-like receptor 9 (TLR9). In the present study, we have examined the ability of a novel agonist of TLR9, called immunomodulatory oligonucleotide (IMO), to enhance effects of a HER-2/neu plasmid DNA electroporation/adenovirus (DNA-EP/Ad) vaccine. Experimental Design: BALB/NeuT mice were treated with DNA-EP vaccine alone, IMO alone, or the combination of two agents starting at week 13, when all mice showed mammary neoplasia. Tumor growth and survival were documented. Antibody and CD8+ T-cell responses were determined. Peptide microarray analysis of sera was carried out to identify immunoreactive epitopes. Additionally, microCT and microPET imaging was carried out in an advanced-stage tumor model starting treatment at week 17 in BALB/NeuT mice. Results: The combination of DNA-EP and IMO resulted in significant tumor regression or delay to tumor progression. 2-Deoxy-2-[18F]fluoro-d-glucose microPET and microCT imaging of mice showed reduced tumor size in the DNA-EP/IMO combination treatment group. Mice treated with the combination produced greater antibody titers with IgG2a isotype switch and antibody-dependent cellular cytotoxicity activity than did mice treated with DNA-EP vaccine. An immunogenic B-cell linear epitope, r70, within the HER-2 dimerization domain was identified through microarray analysis. Heterologous DNA-EP/Ad vaccination combined with IMO increased mice survival. Conclusion: The combination of HER-2/neu genetic vaccine and novel agonist of TLR9 had potent antitumor activity associated with antibody isotype switch and antibody-dependent cellular cytotoxicity activities. These results support possible clinical trials of the combination of DNA-EP/Ad-based cancer vaccines and IMO.

Publisher

American Association for Cancer Research (AACR)

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