Central and peripheral actions of somatostatin on the growth hormone–IGF-I axis

Murray, Robert; Kim, Ki-Won; Ren, Shaolei; Chelly, Marjorie; Umehara, Yutaka; Melmed, Shlomo

doi:10.1172/jci19933

Cited by 139 publications

(88 citation statements)

References 60 publications

(27 reference statements)

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“…In light of the activation of transcription factors such as C/EBPs and Stat3 in all the trout SSTR-expressing cells and the observed linakge between ERK and PI3K/Akt and these transcription factors in mammalian systems (Chung 1997, Schrem et al 2004, Cui et al 2008, it is possible that alterations in the activity state of C/EBPb and Stat3 and the modulation of GHR and IGF1 transcription may underlie SS inhibition of GHR and IGF1 expression in trout liver cells. SS-induced activation of Stat5 also was linked to reduced hepatic GH binding in rat hepatocytes (Murray et al 2004). It was shown recently that increased ERK and Akt activation was attended by increased p53 activation (Tanel & Averill-Bates 2007), suggesting that SSTR1A/ SSTR2-triggered ERK and/or PI3K/Akt activation of p53 may underlie, at least in part, SS-induced inhibition of IGFR expression in native gill filaments of trout.…”

Section: Discussionmentioning

confidence: 91%

Rainbow trout somatostatin receptor subtypes SSTR1A, SSTR1B, and SSTR2 differentially activate the extracellular signal-regulated kinase and phosphatidylinositol 3-kinase signaling pathways in transfected cells

Hagemeister

Kittilson²,

Bergan³

et al. 2010

Journal of Molecular Endocrinology

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Previously, we reported that extracellular signal-regulated kinase (ERK) and protein kinase B (Akt), a downstream target of phosphatidylinositol 3-kinase (PI3K), mediated somatostatin (SS) inhibition of GH receptor, IGF1, and IGF1 receptor expression. In this study, we used Chinese hamster ovary-K1 cells that stably transfected individually with trout SS receptors (SSTR1A, SSTR1B, and SSTR2) to elucidate receptor-effector pathway linkages. SS induced ERK and Akt activation in a time-and concentration-related manner in all SSTR-expressing cells; however, the PI3K/Akt pathway was activated to a greater extent through SSTR1A than through either SSTR1B or SSTR2, whereas the ERK pathway was activated to a greater extent though SSTR2 than through either SSTR1A or SSTR1B. Although the ERK pathway inhibitor U0126 had no effect on Akt activation, the PI3K inhibitor LY294002 reduced ERK activation to near control levels in all SSTR-expressing cell lines, suggesting some cross talk between the pathways, possibly at the level of c-Raf, the phosphorylation of which also was induced by SS via each SSTR. Pertussis toxin (PTX) completely abolished SS-induced activation of ERK and Akt in SSTR1A-, SSTR1B-, and SSTR2-expressing cells, suggesting that these receptors link to the ERK and PI3K/Akt pathways via PTX-sensitive G-proteins. SS-induced activation of Elk1, Stat3, and C/EBPb also was mediated by each of the trout SSTRs. These findings establish important receptor-effector pathway linkages for fish SSTRs and provide insight into the molecular mechanisms by which SSs may elicit diverse physiological effects in target cells.

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Section: Discussionmentioning

confidence: 91%

Rainbow trout somatostatin receptor subtypes SSTR1A, SSTR1B, and SSTR2 differentially activate the extracellular signal-regulated kinase and phosphatidylinositol 3-kinase signaling pathways in transfected cells

Hagemeister

Kittilson²,

Bergan³

et al. 2010

Journal of Molecular Endocrinology

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“…Moreover, the suppressive effect of somatostatin on insulin secretion (13) may result in reduced hepatic IGF1 production, and hence lower serum IGF1 levels, in as much as insulin stimulates hepatic GHR synthesis and activity (30). Moreover, data from rodent studies show that somatostatin directly suppresses hepatic IGF1 production and possibly also the receptor-mediated clearance of GH (12), and a study in healthy human subjects indicates that somatostatin exerts GH-antagonistic effects directly in skeletal muscle in vivo (31). It has also been suggested that somatostatin may antagonize the suppressive effect of oral glucose on GH secretion (8), and it is worth noting that the difference in GH levels in our study was mainly present during the OGTT.…”

Section: Discussionmentioning

confidence: 99%

“…In addition, slightly elevated GH levels in the presence of normalized IGF1 levels may be an early predictor of disease recurrence (10), but cases of persistent disease despite very low GH levels (and elevated IGF1 levels) also exist (7,11). Furthermore, somatostatin acts not only at the pituitary level to suppress GH release, but also exhibits inhibitory effects on GH signaling and thus GH receptor (GHR)-mediated clearance of GH (12). In addition, somatostatin suppresses insulin secretion (13), which may lower hepatic IGF1 production and hence also the circulating levels of IGF1 (14).…”

Section: Introductionmentioning

confidence: 99%

Conventional and novel biomarkers of treatment outcome in patients with acromegaly: discordant results after somatostatin analog treatment compared with surgery

Rubeck

Madsen²,

Andreasen³

et al. 2010

European Journal of Endocrinology

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Context: Control of disease activity in acromegaly is critical, but the biochemical definitions remain controversial. Objective: To compare traditional and novel biomarkers and health status in patients with acromegaly treated with either surgery alone or somatostatin analog (SA). Design and methods: Sixty-three patients in long-term remission based on normalized total IGF1 levels after surgery alone (nZ36) or SA (nZ27) were studied in a cross-sectional manner. The groups were comparable at diagnosis regarding demographic and biochemical variables. Each subject underwent 3 h of serum sampling including a 2-h oral glucose tolerance test (OGTT). Health status was measured by two questionnaires: EuroQoL and Acrostudy (Patient-assessed-Acromegaly symptom questionnaire (PASQ)). Results: Total and bioactive IGF1 (mg/l) levels were similar (total: 185G10 (SA) versus 171G8 (surgery) (PZ0.28); bioactive: 1.9G0.2 vs 1.9G0.1 (PZ0.70)). Suppression of total and free GH (mg/l) during OGTT was blunted in the SA group (total GH nadir : 0.59G0.08 (SA) versus 0.34G0.06 (surgery) (PZ0.01); free GH nadir : 0.43G0.06 vs 0.19G0.04 (P!0.01)). The insulin response to OGTT was delayed, and the 2-h glucose level was elevated during SA treatment (PZ0.02). Disease-specific health status was better in patients after surgery (PZ0.02). Conclusions: i) Despite similar and normalized IGF1 levels, SA treatment compared with surgery alone was associated with less suppressed GH levels and less symptom relief; ii) this discordance may be due to specific suppression of hepatic IGF1 production by SA; iii) we suggest that biochemical assessment during SA treatment should include both GH and IGF1.

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“…They inhibit pituitary GH release and sst2 and sst5 are the subtypes primary involved in this effect. They also inhibit hepatic GH-induced IGF-I production via sst2-and/or sst3-mediated activation of a tyrosine phosphatase leading to dephosphorylation of STAT5b and to a decrease in IGF-I gene transcription (Murray et al, 2004).…”

Section: Indirect Antitumor Effects Of Somatostatinmentioning

confidence: 99%

“…Tumor angiogenesis is essential for tumor growth, invasion and metastasis. Several experimental results indicate that somatostatin analogs inhibit angiogenesis in vitro and in vivo (Murray et al, 2004). Overexpression of peritumoral vascular somatostatin receptors with high-affinity for sst2-preferring analog octreotide has been reported in human primary colorectal carcinomas, small cell lung carcinoma, breast cancer, renal carcinoma and malignant lymphoma.…”

Section: Indirect Antitumor Effects Of Somatostatinmentioning

confidence: 99%

Antitumor effects of somatostatin

Pyronnet

Bousquet

Najib

et al. 2008

Molecular and Cellular Endocrinology

159

118

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SummarySince its discovery three decades ago as an inhibitor of GH release from the pituitary gland, somatostatin has attracted much attention because of its functional role in the regulation of a wide variety of physiological functions in the brain, pituitary, pancreas, gastrointestinal tract, adrenals, thyroid, kidney and immune system. In addition to its negative role in the control of endocrine and exocrine secretions, somatostatin and analogs also exert inhibitory effects on the proliferation and survival of normal and tumor cells. Over the past 15 years, studies have begun to reveal some of the molecular mechanisms underlying the antitumor activity of somatostatin. This review covers the present knowledge in the antitumor effect of somatostatin and analogs and discusses the perspectives of novel clinical strategies based on somatostatin receptor sst2 gene transfer therapy.

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Central and peripheral actions of somatostatin on the growth hormone–IGF-I axis

Cited by 139 publications

References 60 publications

Rainbow trout somatostatin receptor subtypes SSTR1A, SSTR1B, and SSTR2 differentially activate the extracellular signal-regulated kinase and phosphatidylinositol 3-kinase signaling pathways in transfected cells

Rainbow trout somatostatin receptor subtypes SSTR1A, SSTR1B, and SSTR2 differentially activate the extracellular signal-regulated kinase and phosphatidylinositol 3-kinase signaling pathways in transfected cells

Conventional and novel biomarkers of treatment outcome in patients with acromegaly: discordant results after somatostatin analog treatment compared with surgery

Antitumor effects of somatostatin

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