Somatostatin: Regulation of Secretion

Arimura, Akira; Fishback, James B.

doi:10.1159/000123239

Cited by 53 publications

(19 citation statements)

References 55 publications

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“…When the islets were first incubated with 16.7 mmol/l glucose and then transferred to 3.3 mmol/l glucose (i.e., low-glucose stimulation), somatostatin secretion was significantly enhanced, corresponding to 147% of that with 16.7 mmol/l glucose throughout. Thus, high-and lowglucose stimulation enhanced somatostatin secretion, as has been observed in previous studies (3,15). Under similar assay conditions, the secretion of insulin and glucagon was enhanced by high-and low-glucose stimulation, respectively, indicating a well-known islet cellϪspecific response to glucose (Fig.…”

supporting

confidence: 85%

“…The inhibition is mediated through somatostatin receptor (SSTR)-1 and -5 in ␤-cells and SSTR-2 in ␣-cells (16 -18). Given that the mechanism underlying glucose sensing by ␦-cells is similar, if not identical, to that of ␤-cells, somatostatin secretion is upregulated by high blood glucose via cytosolic Ca 2ϩ and cAMP (3,15,19). Somewhat paradoxically, the lowering of blood glucose levels also enhances somatostatin secretion 1 and 3) and isolated islets (lanes 2 and 4).…”

mentioning

confidence: 99%

“…Somatostatin, a tetradecapeptide, is a potent paracrine modulator that inhibits the secretion of insulin and glucagon from islets (3,14,15). The inhibition is mediated through somatostatin receptor (SSTR)-1 and -5 in ␤-cells and SSTR-2 in ␣-cells (16 -18).…”

mentioning

confidence: 99%

“…The amplified product, which has the expected molecular weight, is indicated by an arrow. (15,20). Although somatostatin secreted under low-glucose conditions might be responsible for somatostatinevoked inhibition of glucagon secretion, it is unknown how low glucose enhances somatostatin secretion.…”

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A Novel Variant of Ionotropic Glutamate Receptor Regulates Somatostatin Secretion From δ-Cells of Islets of Langerhans

et al. 2004

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Many metabolic factors affect the secretion of insulin from ␤-cells and glucagon from ␣-cells of the islets of Langerhans to regulate blood glucose. Somatostatin from ␦-cells, considered a local inhibitor of islet function, reduces insulin and glucagon secretion by activating somatostatin receptors in islet cells. Somatostatin secretion from ␦-cells is increased by high glucose via glucose metabolism in a similar way to insulin secretion from ␤-cells. However, it is unknown how low glucose triggers somatostatin secretion. Because L-glutamate is cosecreted with glucagon from ␣-cells under low-glucose conditions and acts as a primary intercellular messenger, we hypothesized that glutamate signaling triggers the secretion of somatostatin. In this study, we showed that ␦-cells express GluR4c-flip, a newly identified splicing variant of GluR4, an (RS)-␣-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid (AMPA)-type ionotropic glutamate receptor of rat. After treatment with L-glutamate, AMPA, or kainate, secretion of somatostatin from isolated islets was significantly stimulated under low-glucose conditions. The glutamatedependent somatostatin secretion was Ca 2؉ dependent and blocked by 6-cyano-7-nitroquinoxaline-2,3-dione. Somatostatin in turn inhibited the secretion of L-glutamate and glucagon from ␣-cells. These results indicate that L-glutamate triggers somatostatin secretion from ␦-cells by way of the GluR4c-flip receptor under lowglucose conditions. The released somatostatin may complete the feedback inhibition of ␣-cells. Thus, ␣-and ␦-cells may communicate with each other through Lglutamate and somatostatin signaling.

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A Novel Variant of Ionotropic Glutamate Receptor Regulates Somatostatin Secretion From δ-Cells of Islets of Langerhans

et al. 2004

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“…Three mechanisms have been delineated for the influence of somatostatin on the secretory activity of the other endocrine cell types in the islets RcI et al, 1974;ORcI, 1976;UNGER and ORCI, 1976;FORSSMANN et al, 1978;UNGER et al, 1978;ORcI and PERRELET, 1979;EFENDIC et al, 1980;LARSSON, 1980;SCHAUDER, 1980;ARIMURA and FISHBACK, 1981;HONEY et al, 1981): a) membrane specializations (gap and tight junctions), b) secretion into the intercellular space, the "Parakrinie" of FEYRTER (1953), and c) secretion into the capillaries (endocrine route). The apparent interposition of D-cells between the A-cells and B-cells, at first reported in rodent islets and later on also for human islets, favored the hypothesis of a prevailing paracrine mode of action of D-cells (ORcI and UNGER,1975;LINGER andORcI, 1977, 1981a, b).…”

Section: Discussionmentioning

confidence: 99%

The microanatomy of human islets of Langerhans, with special reference to somatostatin (D-) cells.

Grube

Bohn

1983

Arch. Histol. Jap., Arch. Histol. Jpn

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Somatostatin in medullary thyroid cancer.In vitro andin vivo studies

Pacini

Elisei

Anelli

et al. 1989

Cancer

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The authors evaluated the presence of somatostatin (SRIF) in the plasma and in the tumor tissue of a total of 22 patients with medullary thyroid cancer (MTC) and studied the effect of exogenous SRIF administration on basal and pentagastrin (PG)-stimulated plasma calcitonin (CT) and carcinoembryonic antigen (CEA) levels. Mean plasma SRIF concentrations were significantly higher than those found in normal controls, with five of 15 patients having plasma SRIF levels above the mean + 2 SD of normal controls. High immunoreactive SRIF concentrations were found in the extract of three tumor tissues but not in one follicular thyroid cancer or in one toxic diffuse goiter. By immunoperoxidase staining seven of 11 (63.6%) primary MTC and five of 13 (38.5%) metastases expressed SRIF antigen in a low number of cells and with a weak degree of staining. As expected, CT was expressed in almost 100% of the cases with positivity in most of the cells and strong degree of staining. Patients with positive SRIF staining in the primary tumor had longer survival than SRIF negative patients. Infusion of synthetic SRIF (11 micrograms/minute/45 minutes) produced a significant reduction of plasma CT (but not CEA) levels in 12 of the 15 patients submitted to this test. Maximal percent decrease of plasma CT ranged from 10.8% to 72.7% of the basal value and was usually observed between 30 and 45 minutes from the beginning of the infusion. When infused together with the injection of PG, SRIF was able to significantly (P less than 0.05) inhibit the PG-induced CT release in five of six patients tested. These results demonstrate the following: SRIF is present in a few cells of many primary MTC and less frequently in their metastases; tentatively, the expression of SRIF antigen in the tumor seems to be associated with longer survival; increased SRIF concentrations are found in the plasma of some patients with metastatic involvement; and treatment with exogenous SRIF reduces the basal and PG-induced CT (but not CEA) release from the tumor.

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Somatostatin: Regulation of Secretion

Cited by 53 publications

References 55 publications

A Novel Variant of Ionotropic Glutamate Receptor Regulates Somatostatin Secretion From δ-Cells of Islets of Langerhans

A Novel Variant of Ionotropic Glutamate Receptor Regulates Somatostatin Secretion From δ-Cells of Islets of Langerhans

The microanatomy of human islets of Langerhans, with special reference to somatostatin (D-) cells.

Somatostatin in medullary thyroid cancer.In vitro andin vivo studies

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