Somatostatin and dopamine receptor interaction in prostate and lung cancer cell lines

Arvigo, Marica; Gatto, Federico; Ruscica, Massimiliano; Ameri, Pietro; Dozio, Elena; Albertelli, Manuela; Culler, Michael D.; Motta, Marcella; Minuto, Francesco; Magni, Paolo; Ferone, Diego

doi:10.1677/joe-10-0342

Cited by 27 publications

(16 citation statements)

References 34 publications

(49 reference statements)

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“…These results were confirmed in non-endocrine tumor cells, natively expressing SST receptors and D2R. It was shown that these receptors can interact in the absence of agonists [55] and the treatment with the chimeric compound targeting both receptor types (BIM-23A760) significantly increased the sst5/D2R and sst2/D2R dimers. …”

Section: Somatostatin Receptor Signal Transduction Homo- and Hetementioning

confidence: 60%

Peptide Receptor Targeting in Cancer: The Somatostatin Paradigm

Barbieri

Bajetto

Pattarozzi

et al. 2013

International Journal of Peptides

107

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Peptide receptors involved in pathophysiological processes represent promising therapeutic targets. Neuropeptide somatostatin (SST) is produced by specialized cells in a large number of human organs and tissues. SST primarily acts as inhibitor of endocrine and exocrine secretion via the activation of five G-protein-coupled receptors, named sst1–5, while in central nervous system, SST acts as a neurotransmitter/neuromodulator, regulating locomotory and cognitive functions. Critical points of SST/SST receptor biology, such as signaling pathways of individual receptor subtypes, homo- and heterodimerization, trafficking, and cross-talk with growth factor receptors, have been extensively studied, although functions associated with several pathological conditions, including cancer, are still not completely unraveled. Importantly, SST exerts antiproliferative and antiangiogenic effects on cancer cells in vitro, and on experimental tumors in vivo. Moreover, SST agonists are clinically effective as antitumor agents for pituitary adenomas and gastro-pancreatic neuroendocrine tumors. However, SST receptors being expressed by tumor cells of various tumor histotypes, their pharmacological use is potentially extendible to other cancer types, although to date no significant results have been obtained. In this paper the most recent findings on the expression and functional roles of SST and SST receptors in tumor cells are discussed.

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Section: Somatostatin Receptor Signal Transduction Homo- and Hetementioning

confidence: 60%

Peptide Receptor Targeting in Cancer: The Somatostatin Paradigm

Barbieri

Bajetto

Pattarozzi

et al. 2013

International Journal of Peptides

107

View full text Add to dashboard Cite

show abstract

“…However, these results were obtained in non-pituitary cell lines (CHO or HEK293) stably expressing exogenous receptors, and there is so far no evidence for receptor dimerization in pituitary cells. Recently, somatostatin and D 2 receptors interaction has been demonstrated in prostate cancer cell line, LNCaP, and in non-small cell lung cancer line, Calu-6 (Arvigo et al, 2010). Postreceptor mechanisms involved in the enhanced potency following receptor dimer activation have not yet been characterized.…”

Section: Gh Secretion and Gh Mrna Expressionmentioning

confidence: 99%

Somatostatin analogs and chimeric somatostatin–dopamine molecules differentially regulate human growth hormone and prolactin gene expression and secretion in vitro

Gruszka¹,

Culler²,

Melmed³

2012

Molecular and Cellular Endocrinology

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“…Over the past several years, evidence that dopamine receptors are expressed in cancer cells outside the nervous system has been increasing. DRD2 expression has been found in abnormally proliferating Jurkat cells, prostate cancer lines (LnCAP), and lung cancer stem cells (Arvigo et al, 2010;Basu et al, 2010;Yeh et al, 2012).…”

Section: Discussionmentioning

confidence: 99%

Repurposing the Antipsychotic Trifluoperazine as an Antimetastasis Agent

Pulkoski‐Gross

Zheng

et al. 2014

Mol Pharmacol

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Because cancer cell invasion is a critical determinant of metastasis, targeting invasion is a viable approach to prevent metastasis. Utilizing a novel three-dimensional high-throughput invasion assay, we screened a National Cancer Institute compound library and discovered compounds demonstrating inhibitory effects on cancer cell invasion. One hit, trifluoperazine, suppresses invasion of human cancer cell lines while displaying a limited cytotoxicity profile. This inhibition is due to the interference with cancer cell migratory ability but not proteolytic ac-

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Somatostatin and dopamine receptor interaction in prostate and lung cancer cell lines

Cited by 27 publications

References 34 publications

Peptide Receptor Targeting in Cancer: The Somatostatin Paradigm

Peptide Receptor Targeting in Cancer: The Somatostatin Paradigm

Somatostatin analogs and chimeric somatostatin–dopamine molecules differentially regulate human growth hormone and prolactin gene expression and secretion in vitro

Repurposing the Antipsychotic Trifluoperazine as an Antimetastasis Agent

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