Identification of binding sites for C-terminal pro-gastrin-releasing peptide (GRP)-derived peptides in renal cell carcinoma: a potential target for future therapy

Joseph Ischia; Oneel Patel; Kapil Sethi; Marianne S Nordlund; Damien Bolton; Arthur Shulkes; Graham S Baldwin

doi:10.1111/bju.12886

Identification of binding sites for C-terminal pro-gastrin-releasing peptide (GRP)-derived peptides in renal cell carcinoma: a potential target for future therapy

BJU Int. 2015 May;115(5):829-38. doi: 10.1111/bju.12886. Epub 2015 Jan 26.

Authors

Joseph Ischia¹, Oneel Patel, Kapil Sethi, Marianne S Nordlund, Damien Bolton, Arthur Shulkes, Graham S Baldwin

Affiliation

¹ Department of Surgery, Austin Health, University of Melbourne, Melbourne, Victoria, Australia.

PMID: 25130393
DOI: 10.1111/bju.12886

Abstract

Objective: To determine the expression and biology of the neuroendocrine growth factor gastrin-releasing peptide (GRP) and other proGRP-derived peptides in renal cancer.

Materials and methods: Receptor binding studies, enzyme-linked immunosorbent assay (ELISA) and radioimmunoassay, were used to quantitate the presence of proGRP-derived peptide receptors and their ligands in renal cancer cell lines and human renal cancers. Biological activity of proGRP peptides was confirmed with proliferation, migration, and extracellular-signal-regulated kinases 1 and 2 (ERK1/2) activation assays in vitro. In vivo, ACHN renal cancer xenografts were treated with proGRP-derived peptides to assess tumour size and necrosis. hypoxia-inducible factor 1α (HIF1α) and vascular endothelial growth factor (VEGF) expression were investigated with Western blotting and ELISA respectively, to determine the possible contribution of the proGRP peptides to tumour viability.

Results: In ACHN cells that expressed both proGRP- and GRP-receptors, the expression of proGRP binding sites was 80-fold greater than the GRP-receptor (GRPR). C-terminal proGRP-derived peptides stimulated the activation of ERK1/2, but with a different time course to GRP, consistent with the suggestion that these peptides may have unique cellular functions. Both GRP and proGRP47-68 stimulated proliferation and migration of ACHN cells in vitro, but only GRP reduced the extent of tumour necrosis in ACHN xenografts. GRP, but not proGRP47-68, was able to induce HIF1α and VEGF expression in ACHN cells. This may account in part for the reduction in necrosis after GRP treatment. C-terminal proGRP-derived peptides were present in all three renal cancer cell lines and a panel of human renal cancers, but mature amidated GRP was absent.

Conclusion: C-terminal proGRP peptides are more abundant in renal cancers and their cell lines than the more extensively studied amidated peptide, GRP. These results suggest that C-terminal proGRP-derived peptides may be a better target for novel renal cancer treatments.

Keywords: bombesin; gastrin-releasing peptide; kidney; renal cell carcinoma (RCC).

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Binding Sites
Carcinoma, Renal Cell / drug therapy
Carcinoma, Renal Cell / metabolism*
Cell Line, Tumor
Gastrin-Releasing Peptide / metabolism*
Humans
Kidney Neoplasms / drug therapy
Kidney Neoplasms / metabolism*
Peptides
Protein Precursors
Receptors, Bombesin / metabolism*

Substances

Peptides
Protein Precursors
Receptors, Bombesin
gastrin-releasing peptide precursor
Gastrin-Releasing Peptide