Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: UNIPROT:P04626 (
erbB-2
)
5,251
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Five overlapping fragments of rat
HER-2/neu
have been expressed in recombinant Listeria monocytogenes. Each fragment of
HER-2/neu
is secreted as a fusion protein with a truncated, nonhemolytic form of listeriolysin O (LLO). Lm-LLO-EC1, Lm-LLO-
EC2
, and Lm-LLO-EC3 overlap the extracellular domain of
HER-2/neu
, whereas Lm-LLO-IC1 and Lm-LLO-IC2 span the intracellular domain. All five strains controlled the growth of established NT-2 tumors, a rat
HER-2/neu
-expressing tumor line derived from a spontaneously arising mammary tumor in a FVB/N
HER-2/neu
-transgenic mouse. The antitumor effect of each of these vaccine constructs was abrogated by the in vivo depletion of CD8(+) T cells, although only one known epitope has been defined previously and is present in Lm-LLO-
EC2
. Anti-
HER-2/neu
CTL responses were generated by each of the rLm vaccine constructs. With the use of a panel of 3T3 cell lines expressing overlapping fragments of
HER-2/neu
, regions of
HER-2/neu
with potential CD8(+) T cell epitopes have been defined. DNA vaccines expressing either a fragment or full-length
HER-2/neu
were constructed in LLO-fused and non-LLO-fused forms. CTL analysis of the DNA vaccines revealed a broadening in the regions of
HER-2/neu
recognizable as targets when the target Ag is fused to LLO. These studies show the efficacy of L. monocytogenes-based
HER-2/neu
vaccines in a murine model of breast cancer and also that the immunogenicity of self-Ags can be increased by fusion to LLO and delivery by L. monocytogenes revealing subdominant epitopes.
...
PMID: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. 1614 11
The
HER-2/neu
oncogene has >25 HLA epitopes, yet only one FVB/N mouse CD8(+) T-cell epitope has been mapped to date. This epitope has been termed the immunodominant epitope for the FVB/N mouse, but we propose that the vaccination strategy determines the dominance of epitopes. Using a series of overlapping peptides, we have mapped another CD8(+) T-cell epitope that emerges in the FVB/N mouse following vaccination with Listeria monocytogenes-based vaccines that express fragments of
HER-2/neu
. Following the identification of this novel H-2K(q)-restricted epitope, we sought to compare the T-cell response to this epitope with the previously identified PDSLRDLSVF epitope. This newly identified epitope and the previously identified epitope lie within fragments contained in different vaccines, the PDSLRDLSVF epitope in Lm-LLO-
EC2
and the newly identified PYNYLSTEV epitope in Lm-LLO-EC1; thus, it has been possible to compare the responses of these epitopes independent of any competing response between the epitopes. CTL analysis of individual peptide-pulsed target cells and intracellular cytokine stain for IFN-gamma produced by splenocytes from Lm-LLO-EC1 compared with Lm-LLO-
EC2
vaccinated FVB/N mice shows that there is no difference between the responses generated to either of these epitopes. We also show that the avidity of the CD8(+) T cells for either of these epitopes is similar based on the concentration of peptide necessary to mediate similar levels of lysis of target cells. In addition,
HER-2/neu
DNA vaccination followed by CTL analysis further showed that both of these peptides can emerge as epitopes.
...
PMID:Vaccination strategy determines the emergence and dominance of CD8+ T-cell epitopes in a FVB/N rat HER-2/neu mouse model of breast cancer. 1688 78
Immunoediting of tumor-associated antigens occurs in response to immune pressure. We show that the mutation of residues within epitopes of
HER-2/neu
leads to the outgrowth of autochthonous tumors after immunizing
HER-2/neu
transgenic mice with Listeria monocytogenes therapeutic vaccines expressing fragments of
HER-2/neu
. Three of these vaccines target the extracellular domain (LmLLO-EC1, LmLLO-
EC2
, and LmLLO-EC3), and two of these vaccines target the intracellular domain (Lm-LLO-IC1 and Lm-LLO-IC2). Mutations occurred in the regions of the
HER-2/neu
molecule targeted by the Listeria strain expressing that region, which suggests that the rate of generation of escape mutants was a significant factor in the efficacy of each vaccine. A longer delay in the onset of tumors after immunotherapy occurred with the vaccine that targeted the kinase domain. We verified that the mutations in this domain occurred within novel CD8(+) T-cell epitopes, and that the mutation of these residues abrogated CTL responses to these epitopes. The long delay in the onset of tumors after immunotherapy targeting the kinase domain may be because this region of
HER-2/neu
cannot undergo extensive mutations without impairing its ability to signal cell growth.
...
PMID:Immunoediting sculpts tumor epitopes during immunotherapy. 1733 14
