Fusion to Listeriolysin O and Delivery by <i>Listeria monocytogenes</i> Enhances the Immunogenicity of HER-2/neu and Reveals Subdominant Epitopes in the FVB/N Mouse

Singh, Ram; Dominiecki, Mary E.; Jaffee, Elizabeth M.; Paterson, Yvonne

doi:10.4049/jimmunol.175.6.3663

Cited by 103 publications

(134 citation statements)

References 43 publications

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“…Likewise, using the TRAMP mouse model of prostate cancer, Grossmann et al (16) reported the ability to recruit T CD8 against the SV40 Tag-V epitope, but did not assess the effect on tumor progression. Singh et al (54) recently described the discovery of subdominant T CD8 epitopes within the HER-2/neu Ag that could induce an antitumor response in mice that express HER-2/neu, but the ability of immunization to control spontaneous mammary tumors in these mice remains to be determined. Thus, to our knowledge, the effect of T CD8 specific for an immunorecessive tumor epitope on spontaneous tumor progression has not previously been explored.…”

Section: Discussionmentioning

confidence: 99%

Accumulation of CD8+ T Cells in Advanced-Stage Tumors and Delay of Disease Progression following Secondary Immunization against an Immunorecessive Epitope

Ryan

Schell

2006

The Journal of Immunology

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Self-reactive T cells that survive the process of positive and negative selection during thymocyte development represent potential effector cells against tumors that express these same self-Ags. We have previously shown that CD8+ T lymphocytes (TCD8) specific for an immunorecessive epitope, designated epitope V, from the SV40 large T Ag (Tag) escape thymic deletion in line SV11 Tag-transgenic mice. In contrast, these mice are tolerant to the three most dominant Tag epitopes. The majority of the residual epitope V-specific TCD8 have a low avidity for the target epitope, but a prime/boost regimen can expand higher avidity clones in vivo. Whether higher avidity TCD8 targeting this epitope are affected by Tag-expressing tumors in the periphery or can be recruited for control of tumor progression remains unknown. In the current study, we determined the fate of naive TCR-transgenic TCD8 specific for Tag epitope V (TCR-V cells) following transfer into SV11 mice bearing advanced-stage choroid plexus tumors. The results indicate that TCR-V cells are rapidly triggered by the endogenous Tag and acquire effector function, but fail to accumulate within the tumors. Primary immunization enhanced TCR-V cell frequency in the periphery and promoted entry into the brain, but a subsequent booster immunization caused a dramatic accumulation of TCR-V T cells within the tumors and inhibited tumor progression. These results indicate that epitope V provides a target for CD8+ T cells against spontaneous tumors in vivo, and suggests that epitopes with similar properties can be harnessed for tumor immunotherapy.

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Section: Discussionmentioning

confidence: 99%

Accumulation of CD8+ T Cells in Advanced-Stage Tumors and Delay of Disease Progression following Secondary Immunization against an Immunorecessive Epitope

Ryan

Schell

2006

The Journal of Immunology

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“…The NT-2 tumor cell line, which expresses high levels of rat HER2/neu protein, was derived from a spontaneous mammary tumor in these mice 7 and grown as described previously. 4 DHFR-G8 (3T3/neu) cells were obtained from the American Type Culture Collection and were grown according to the American Type Culture Collection recommendations. The EMT6-Luc cell line was a generous gift from Dr John Ohlfest (University of Minnesota, MN) and was grown in C-RPMI medium.…”

Section: Mice and Cell Linesmentioning

confidence: 99%

“…3 In the first approaches to target the HER2/neu antigen using Listeria monocytogenes (Lm), Listeria-based vaccines expressing small fragments of the extra and intracellular domains of the rat and human HER2/neu protein were constructed. 4,5 We also generated a Listeria vaccine (Lm-LLO-ChHer2) using a chimeric protein by fusing two of the extracellular and one intracellular fragments of the human HER2/neu, including most of the known major histocompatibility complex (MHC) class I epitopes of the protein. 5 All of these vaccines were shown to be immunogenic and efficacious in regressing preestablished tumors in FVB/N mice and delay the onset of spontaneous mammary tumors in HER2/neu-expressing transgenic animals.…”

Section: Introductionmentioning

confidence: 99%

Development of a live and highly attenuated Listeria monocytogenes-based vaccine for the treatment of Her2/neu-overexpressing cancers in human

et al. 2010

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A chimeric human Her2/neu gene (ChHer2) harboring most of the known major histocompatibility complex class I epitopes of the HER2/neu oncogene was expressed as a fusion protein to a non-hemolytic fragment of listeriolysin O (LLO), by the highly attenuated Listeria vector LmddA, which lacks antibiotic selection markers and the ability to spread from cell-to-cell. This construct (ADXS31-164) was tested for immunogenicity and anti-tumor effects in mice. Despite being highly attenuated, ADXS31-164 proved to be efficacious in breaking immune tolerance toward the HER2/neu self-antigen. ADXS31-164 elicited strong T-cell immune responses in experimental animals. In tumors, ADXS31-164 caused a reduction in regulatory T cells (Treg) accompanied by an increase in the CD8 þ /Treg ratio. Comparison of this vaccine with the conventional antibiotic resistant Listeria vector (Lm-LLO-ChHer2) shows that ADXS31-164 is more efficacious in delaying tumor growth in Her2/neu transgenic animals. Because of its well-defined attenuation mechanism and independence from antibiotic selection markers, ADXS31-164 is potentially more suitable for human use. These results support the future clinical development of this vaccine for the treatment of HER2/neuoverexpressing malignancies, such as breast, colorectal and pancreatic cancers.

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“…Mouse GM-CSF plasmid (CMV1-GM-CSF) was kindly provided by Dr Stephen Johnston (the Center for Innovations in Medicine, the Biodesign Institute at Arizona State University) (Chambers and Johnston, 2003). The listerial pGG-34 plasmid, expressing the positive regulatory factor A (prfA), was developed in the laboratory of Yvonne Paterson, University of Pennsylvania, PA, USA (Singh et al, 2005). The prfA-negative strain XFL-7 of LM (Gunn et al, 2001) has been used in this study.…”

Section: Plasmids and Listeria Monocytogenesmentioning

confidence: 99%

“…Direct killing of tumour cells occurs through the function of CD8 T cells, but the killing may be enhanced through the activation of CD4 T cells (Hsieh et al, 1993). It has been shown that vaccine antigens delivered through LM are effective against primary tumours in animal models (Pan et al, 1999;Gunn et al, 2001;Singh et al, 2005). As discussed earlier, metastases, and not the primary tumour, contributes most to breast cancer morbidity and mortality.…”

mentioning

confidence: 99%

Mage-b vaccine delivered by recombinant Listeria monocytogenes is highly effective against breast cancer metastases

et al. 2008

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New therapies are needed that target breast cancer metastases. In previous studies, we have shown that vaccination with pcDNA3.1-Mage-b DNA vaccine is effective against breast cancer metastases. In the study presented here, we have further enhanced the efficacy of Mage-b vaccination through the improved delivery of the vaccine using recombinant Listeria monocytogenes (LM). Three overlapping fragments of Mage-b as well as the complete protein-encoding region of Mage-b have been expressed as a fusion protein with a truncated non-cytolytic form of listeriolysin O (LLO) in recombinant LM. These different Mage-b vaccine strains were preventively tested for their efficacy against breast cancer metastases in a syngeneic mouse tumour model 4T1. The LM-LLO-Mageb/2nd, expressing position 311 -660 of the cDNA of Mage-b, was the most effective vaccine strain against metastases in the 4T1 mouse breast tumour model. Vaccination with LM-LLO-Mage-b/2nd dramatically reduced the number of metastases by 96% compared with the saline group and by 88% compared with the vector control group (LM-LLO), and this correlated with strong Mage-b-specific CD8 T-cell responses in the spleen, after restimulation with Mage-b. However, no effect of LM-LLO-Mage-b/2nd was observed on 4T1 primary tumours, which may be the result of a complete absence of Mage-b-specific immune responses in the draining lymph nodes. Vaccination with LM-LLO-Mage-b/2nd could be an excellent follow-up after removal of the primary tumour, to eliminate metastases and residual tumour cells.

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Fusion to Listeriolysin O and Delivery by Listeria monocytogenes Enhances the Immunogenicity of HER-2/neu and Reveals Subdominant Epitopes in the FVB/N Mouse

Cited by 103 publications

References 43 publications

Accumulation of CD8+ T Cells in Advanced-Stage Tumors and Delay of Disease Progression following Secondary Immunization against an Immunorecessive Epitope

Accumulation of CD8+ T Cells in Advanced-Stage Tumors and Delay of Disease Progression following Secondary Immunization against an Immunorecessive Epitope

Development of a live and highly attenuated Listeria monocytogenes-based vaccine for the treatment of Her2/neu-overexpressing cancers in human

Mage-b vaccine delivered by recombinant Listeria monocytogenes is highly effective against breast cancer metastases

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