Induction of effective and antigen-specific antitumour immunity by a liposomal ErbB2/HER2 peptide-based vaccination construct

Roth, Audrey; Rohrbach, Florian; Weth, Robert; Frisch, Benoı̂t; Schuber, Francis; Wels, Winfried S.

doi:10.1038/sj.bjc.6602526

Cited by 38 publications

(17 citation statements)

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“…This could be explained by the absence of strong rejection antigens within the NY-ESO-1 sequence. Analysis of NY-ESO-1 using SYFPEITHI (46) and MAPPP (47) databases did not reveal peptide epitopes predicted to bind to MHC I of BALB/c mice with high affinity, whereas CTLA-4-ErbB2 222 and untargeted ErbB2 222 both contain the strong H-2K d -restricted TYLPTNASL epitope (20,32). In addition, NY-ESO-1 is an intracellular protein (29), which will limit the protective activity of potential vaccine-induced anti-NY-ESO-1 antibodies.…”

Section: Discussionmentioning

confidence: 99%

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DNA Vaccines Targeting Tumor Antigens to B7 Molecules on Antigen-Presenting Cells Induce Protective Antitumor Immunity and Delay Onset of HER-2/Neu-Driven Mammary Carcinoma

Sloots

Mastini

Rohrbach

et al. 2008

Clinical Cancer Research

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Purpose: Presentation of tumor antigens by professional antigen-presenting cells (APC) is critical for the induction of tumor-specificT-cell responses. To facilitate targeted delivery of tumor antigens to APC, we generated DNA vaccines that encode secreted fusion proteins consisting of the extracellular domain of CTLA-4 for binding to costimulatory B7 molecules on APC, fused to residues 1 to 222 of human ErbB2 (HER-2) or a corresponding 224 residues fragment of its rat homologue Neu. Experimental Design: Induction of humoral and cellular immune responses and antitumoral activity of the DNA vaccines were tested in murine tumor models with transfected renal carcinoma cells expressing the respective antigens and in transgenic BALB-neuT mice developing spontaneous Neu-driven mammary carcinomas. Results: Vaccination of BALB/c mice with CTLA-4-ErbB2 222 plasmid DNA markedly improved tumor-free survival on challenge with ErbB2-expressing Renca cells in comparison with untargeted ErbB2 222 , accompanied by induction of stronger ErbB2-specific antibody and CTL responses. Likewise, a CTLA-4 vaccine carrying the unrelated NY-ESO-1cancer-germline antigen was more effective than untargeted NY-ESO-1 in the protection of mice from challenge with NY-ESO-1-expressing tumor cells. Importantly, antitumoral activity of such a CTLA-4 fusion vaccine could be reproduced in immunotolerant BALB-neuT mice, where a corresponding CTLA-4-Neu 224 DNA vaccine markedly delayed the onset of spontaneous Neu-driven mammary carcinomas. Conclusions: Our results show that plasmid DNA vaccines for in vivo expression of tumor antigens targeted to APC induce potent immune responses and antitumoral activities, providing a rationale for further development of this approach for specific cancer immunotherapy.

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Section: Discussionmentioning

confidence: 99%

“…T-cell responses on vaccination with the CTLA-4-ErbB2 222 DNA vaccine were evaluated in ex vivo restimulation experiments followed by intracellular cytokine staining as described previously (20,32). Female BALB/c mice were vaccinated twice by intramuscular injection of plasmid DNA on days -21 and -7.…”

Section: Translational Relevancementioning

confidence: 99%

DNA Vaccines Targeting Tumor Antigens to B7 Molecules on Antigen-Presenting Cells Induce Protective Antitumor Immunity and Delay Onset of HER-2/Neu-Driven Mammary Carcinoma

Sloots

Mastini

Rohrbach

et al. 2008

Clinical Cancer Research

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“…The aim of this study was to develop a minimalist molecularly defined anti-tumor constructs based on the use of CTL epitope peptide in combination with a Th epitope to increase their efficiency [13]. Because of their weak immunogenicity when administered alone, delivery systems were needed to allow the physical association of such peptides with different TLR ligands used as adjuvants.…”

Section: Discussionmentioning

confidence: 99%

“…1). Thus, liposomal constructs in which the peptide is linked to an anchor without adjuvant properties and associated with a free adjuvant displayed the same antitumoral efficiency than liposomal constructs in which the peptide was linked to an anchor with adjuvant properties [13].…”

Section: Anti-tumor Activity Of Liposome Constructs Containing Epitopmentioning

confidence: 93%

“…MALP-2, Pam 2 Cys derivatives) and triacylated (Pam 3 Cys derivatives) lipopeptides, deriving from the N-terminal moiety of respective mycoplasmal and Escherichia coli lipoproteins, are powerful adjuvants which were used successfully to trigger cell activation and immune responses [9,10]. In a previous paper, we demonstrated that multivalent liposomes (Scheme 1A) containing CTL and Th epitope peptides, covalently anchored at liposome surface via Pam 3 CSS derivatives, a potent agonist of TLR2/TLR1 heterodimers [11,12] displayed potent anti-tumoral activities in both prophylactic and therapeutic vaccination settings [13]. Although highly promising, these constructs had some limitations.…”

Section: Introductionmentioning

confidence: 99%

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