2009
DOI: 10.1128/cvi.00046-09
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Specific Antibodies Elicited by a Novel DNA Vaccine Targeting Gastrin-Releasing Peptide Inhibit Murine Melanoma Growth In Vivo

Abstract: The elevated expression and receptor binding of gastrin-releasing peptide (GRP) in various types of cancer, especially in malignant melanoma of the skin, suggest that GRP might be a putative target for immunotherapy in neoplastic diseases. We have therefore constructed a novel DNA vaccine coding for six tandem repeats of a fragment of GRP from amino acids 18 to 27 (GRP6) flanked by helper T-cell epitopes for increased immunogenicity, including HSP65, a tetanus toxoid fragment from amino acids 830 to 844 (T), p… Show more

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Cited by 19 publications
(10 citation statements)
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“…Silencing of GRPR/GRP by siRNA-delivery has been shown to decrease the signaling cascades leading to proliferation and the growth of neuroblastomas[39], ovarian-cancers[35] and lung-cancers[46]. Another novel approach reported to be effective[47] in silencing the autocrine-growth effect of Bn-related peptides is to immunize animals containing melanomas which possess GRPR and produce GRP, with a DNA-vaccine contain GRP-fragments coupled to tetanus-toxoid and helper-T cell epitopes. Administration intramuscularly of this vaccine decreased B16-F10 melanoma lung invasion and tumor associated angiogenesis[47].…”
Section: General: Use Of Bnr-antagonists For Anti-growth Effects Omentioning
confidence: 99%
“…Silencing of GRPR/GRP by siRNA-delivery has been shown to decrease the signaling cascades leading to proliferation and the growth of neuroblastomas[39], ovarian-cancers[35] and lung-cancers[46]. Another novel approach reported to be effective[47] in silencing the autocrine-growth effect of Bn-related peptides is to immunize animals containing melanomas which possess GRPR and produce GRP, with a DNA-vaccine contain GRP-fragments coupled to tetanus-toxoid and helper-T cell epitopes. Administration intramuscularly of this vaccine decreased B16-F10 melanoma lung invasion and tumor associated angiogenesis[47].…”
Section: General: Use Of Bnr-antagonists For Anti-growth Effects Omentioning
confidence: 99%
“…Recent data indicate that angiogenesis is not only essential for rapidly growing macroscopic tumors, but also contributes to the micro-scopic premalignant phase of neoplastic progression, further cementing its status as an integral hallmark of cancer[40]. A novel DNA vaccine targeting GRP significantly reduced tumor-associated angiogenesis and vascularization of intradermal tumors of C57BL/6 mouse-derived B16 melanoma cells (B16- F10)[41]. GRP has been reported to stimulate GPR receptor-induced pro-angiogenic gene expression as well as the expression of various angiogenic markers, including platelet-endothelial cell adhesion molecule (PECAM-1) and vascular endothelial growth factor (VEGF)[35],[41].…”
Section: Discussionmentioning
confidence: 99%
“…A novel DNA vaccine targeting GRP significantly reduced tumor-associated angiogenesis and vascularization of intradermal tumors of C57BL/6 mouse-derived B16 melanoma cells (B16- F10)[41]. GRP has been reported to stimulate GPR receptor-induced pro-angiogenic gene expression as well as the expression of various angiogenic markers, including platelet-endothelial cell adhesion molecule (PECAM-1) and vascular endothelial growth factor (VEGF)[35],[41]. High titers of GRP-specific Abs could neutralize elevated levels of the GRP self-peptide made by tumor cells and block the GRP/GRPR autocrine loop of GRP-dependent tumors.…”
Section: Discussionmentioning
confidence: 99%
“…Particular success was reported for xenogeneic strategies, viral delivery systems, and the use of IL-2 as an adjuvant [ 101 ]. In mouse models, efficacy of DNA vaccines encoding for all known melanoma-associated antigens was reported including gp100 (melanocyte protein 17/Pmel-17), GRP (gastrin-releasing peptide) [ 102 ], MAGE-1 (melanoma-associated antigen) [ 103 ], MART-1, MUC-18/MCAM [ 104 ], TRP-1 (tyrosinase-related protein-1/gp75), TRP-2, or tyrosinase. Also inhibitor of apoptosis proteins (IAPs) like ML-IAP (melanoma inhibitor of apoptosis protein) [ 105 ] and survivin [ 106 ] were used.…”
Section: Melanomamentioning
confidence: 99%