Synergistic effects of bombesin and epidermal growth factor on cancers.

Liebow, Charles; Crean, David H.; Lee, Ming T.; Kamer, Angela R.; Mang, Thomas S.; Schally, Andrew V.

doi:10.1073/pnas.91.9.3804

Cited by 37 publications

(41 citation statements)

References 31 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…In our model, EGF neither alone nor in combination with bombesin altered the growth of A375-6 cells. These findings are in contrast to other observations with various tumour cell lines: RC-3095, another specific bombesin receptor antagonist, inhibited growth and phosphorylation of growth-related peptides; furthermore, these effects were more pronounced in combination with EGF [23].…”

Section: Discussioncontrasting

confidence: 99%

Identification of functional GRP‐preferring bombesin receptors on human melanoma cells

Pansky

Peng

Eberhard

et al. 1997

Eur J Clin Investigation

View full text Add to dashboard Cite

Abstract. Bombesin was originally isolated from amphibian skin, wherease its mammalian counterpart, gastrinreleasing peptide (GRP), was first identified in the nervous system of the gastrointestinal tract. Whether GRP is present in the human skin is not known. Bombesin-like peptides are also known to modulate growth. We therefore investigated whether human melanoma cell lines express functional GRP-preferring bombesin receptors and whether they alter growth or other specific cellular functions of these tumour cells. . Bombesin dose-dependently increased cytosolic calcium, but did not alter interleukin (IL) 1b-induced reduction of cell viability or IL-6 secretion, both A375-6-specific cell functions. Growth of A375-6 cells was not altered by bombesin or the specific GRP receptor antagonist BIM26226 as measured by [ 3 H]-thymidine incorporation or methylene blue assay, whereas insulin alone or in combination with other potential growth factors dose-dependently stimulated growth of these cells. The newly characterized GRP-preferring bombesin receptors on highly malignant human melanoma cells could initiate studies of growth effects on solid tumours or in vivo scanning using radiolabelled tracers.

show abstract

Section: Discussioncontrasting

confidence: 99%

Identification of functional GRP‐preferring bombesin receptors on human melanoma cells

Pansky

Peng

Eberhard

et al. 1997

Eur J Clin Investigation

View full text Add to dashboard Cite

show abstract

“…In several in vivo tumor models (including SCLC and estrogen-dependent and estrogen-independent MTX mouse mammary cancers), treatment with a synthetic bombesin/GRP antagonist, RC-3095, resulted in the downregulation of EGFR mRNA expression levels (Pinski et al, 1994;Halmos and Schally, 1997;Szepeshazi et al, 1997;Koppan et al, 1998). Moreover, Liebow et al showed that bombesin and EGF seemed to promote phosphorylation of similar substrates (Liebow et al, 1994). Bombesin, which binds with high affinities to multiple BLP receptors, including NMBR and bombesin receptor subtype 4 (Akeson et al, 1997), has been shown to transactivate EGFR in the PC-1 prostate cancer cell line (Prenzel et al, 1999).…”

Section: Discussionmentioning

confidence: 99%

Mitogenic effects of gastrin-releasing peptide in head and neck squamous cancer cells are mediated by activation of the epidermal growth factor receptor

et al. 2003

View full text Add to dashboard Cite

Head and neck squamous cell carcinomas (HNSCC) are characterized by upregulation of the epidermal growth factor receptor (EGFR), where EGFR serves as a potential therapeutic target. We previously reported that a gastrin-releasing peptide/gastrin-releasing peptide receptor (GRP/GRPR) autocrine growth pathway is activated early in HNSCC carcinogenesis. In the present study, we examined the mechanism of EGFR activation by GRP/GRPR in HNSCC proliferation. In HNSCC cells that express elevated levels of both GRPR and EGFR, we found that GRP induced rapid phosphorylation of EGFR as well as p44/42-MAPK activation. Using several EGFR-specific tyrosine kinase inhibitors and cells derived from EGFR knockout mice, we demonstrated that GRPinduced p44/42-MAPK activation was dependent upon EGFR activation. Further investigation demonstrated that cleavage of transforming growth factor-alpha (TGF-a) by matrix metalloproteinases mediated GRP-induced MAPK activation. In addition, HNSCC proliferation stimulated by GRP was eliminated upon specific inhibition of EGFR or MEK, and GRP failed to stimulate proliferation in EGFR-deficient cells. These results imply that the mitogenic effects of GRP in HNSCC are mediated by extracellular release of TGF-a and require the activation of an EGFR-dependent MEK/MAPK-dependent pathway.

show abstract

“…The mechanisms responsible for these effects need to be clarified fully. Liebow et al (55) showed that BN-like peptides can up-regulate EGFRs in various cancers, and BN antagonists block this action. Consequently, BN͞GRP antagonists seem to inhibit MDA-MB-435 human estrogen-independent breast carcinoma by blocking the effects of BN-like peptides and inducing a down-regulation of the HER system.…”

Section: Discussionmentioning

confidence: 99%

Bombesin antagonists inhibit growth of MDA-MB-435 estrogen-independent breast cancers and decrease the expression of the ErbB-2/HER-2 oncoprotein and c- jun and c- fos oncogenes

Bajo

Schally

Krupa

et al. 2002

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

Synergistic effects of bombesin and epidermal growth factor on cancers.

Cited by 37 publications

References 31 publications

Identification of functional GRP‐preferring bombesin receptors on human melanoma cells

Identification of functional GRP‐preferring bombesin receptors on human melanoma cells

Mitogenic effects of gastrin-releasing peptide in head and neck squamous cancer cells are mediated by activation of the epidermal growth factor receptor

Bombesin antagonists inhibit growth of MDA-MB-435 estrogen-independent breast cancers and decrease the expression of the ErbB-2/HER-2 oncoprotein and c- jun and c- fos oncogenes

Contact Info

Product

Resources

About