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Query: UNIPROT:P61278 (
somatostatin
)
22,083
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Immunocytochemical quantitative studies on the development of rat thyroid calcitonin (C) cells have been performed. In neonatal rat pups up to day 6 nearly 90% of all calcitonin cells are also
somatostatin
immunoreactive and 45% of these cells also show immunoreactivity to a C-terminal gastrin/cholecystokinin antiserum (
CCK-4
-like immunoreactivity). Already at day 8 the frequency of
somatostatin
immunoreactive calcitonin cells has dropped to 25%, whereas half of the calcitonin cells still display
CCK-4
-like immunoreactivity. In adult rats, less than 1% of the calcitonin cells are
somatostatin
immunoreactive, whereas 90% of the calcitonin cells display
CCK-4
-like immunoreactivity. These data show that between day 6-8 a pronounced change in the peptide repertoire of rat thyroid C cells occur and that these cells, prior to this time, mainly contain calcitonin and
somatostatin
immunoreactivity and after this time mainly contain calcitonin and
CCK-4
-like immunoreactivity. The time course of the change in the C cell peptides is similar to that observed with changes in transitory peptides of neonatal rat pancreas and duodenum, suggesting that possible hormonal mechanisms during this period act to change the peptide repertoire of several endocrine cell types simultaneously. It is possible that many of the transitory peptides exert actions in the developing individual that are necessary for growth and differentiation. Interestingly, many of these transitory peptides reappear in tumours, where theoretically they could exert similar actions.
...
PMID:Differential changes in calcitonin, somatostatin and gastrin/cholecystokinin-like immunoreactivities in rat thyroid parafollicular cells during ontogeny. 286 84
It is known that cholecystokinin (CCK) stimulates islet hormone secretion under a variety of experimental conditions. Since CCK occurs in several different molecular forms, with 58, 39, 33, 12, 8, or 4 amino acid residues, the question has evolved as to which is the shortest active form of CCK. We therefore investigated the influences of the C-terminal octapeptide of CCK, CCK-8 (sulfated form) and of the C-terminal tetrapeptide,
CCK-4
, on the secretion of insulin, glucagon, and
somatostatin
from the pig pancreas in vivo by infusing each of the two peptides into the superior pancreatic artery. We found that islet hormone secretion increased promptly upon infusion of both CCK-8 and
CCK-4
. Thus, the secretion of insulin was stimulated from 51 +/- 12 to 295 +/- 70 microU/min during the first 2 min after injection of CCK-8 and from 40 +/- 12 to 240 +/- 78 microU/min after injection of
CCK-4
. Similarly, the secretion of glucagon was stimulated from 240 +/- 45 to 357 +/- 38 pg/min after CCK-8 and from 282 +/- 44 to 335 +/- 43 pg/min after
CCK-4
, and
somatostatin
secretion was stimulated from 112 +/- 7 to 226 +/- 12 pg/min by CCK-8 and from 105 +/- 11 to 246 +/- 16 pg/min by
CCK-4
. With regard to the efficiency to stimulate the secretion of these three islet hormones, CCK-8 and
CCK-4
were equipotent. We conclude that in pigs, CCK-8 and
CCK-4
both stimulate the secretion of insulin, glucagon, and
somatostatin
from the pancreas in vivo.(ABSTRACT TRUNCATED AT 250 WORDS)
...
PMID:Cholecystokinin (CCK)-4 and CCK-8 stimulate islet hormone secretion in vivo in the pig. 289 79
Rats were trained to discriminate vehicle injections from intraperitoneal injections of 3 micrograms/kg caerulein, a cholecystokinin (CCK) neuropeptide analog. The reward that reinforced correct choices was an electrical brain stimulation self-administered by bar pressing. Dose-response quantitative generalization was obtained by using 1 and 2 micrograms/kg caerulein. Qualitative generalization to the vehicle occurred after injecting 10, 20 and 200 micrograms/kg unsulfated CCK-8, 10, 20 and 200 micrograms/kg
CCK-4
, 5 micrograms/kg CCK-8 and 1 microgram/kg caerulein, neurotensin or bombesin and 200 micrograms/kg apomorphine or 320 micrograms/kg amphetamine. Total generalization to the caerulein cue was obtained with 20 micrograms/kg sulfated CCK-8 or gastrin 2-17, 25 micrograms/kg
somatostatin
, 50 micrograms/kg haloperidol and 2 mg/kg chlorpromazine. The previous 5 mg/kg injection of an antiemetic drug such as chlorhydrate of trimethobenzamide did not eliminate the discriminative properties of a subsequent injection of caerulein. Our data thus tend to show that IP injection of caerulein produces effects similar to those of IP neuroleptics.
...
PMID:Neuroleptic-like properties of cholecystokinin analogs: distinctive mechanisms underlying similar behavioral profiles depending on the route of administration. 290 29
Using cultures of dissociated neurons from the lower brainstem of 14- to 15-day-old rat embryos, we studied a site of action of a brain-gut peptide by determining whether neuronal responses to a test peptide are abolished or not after replacement of normal medium with low Ca2+- high Mg2+ medium. VIP, secretin and
CCK-4
may act on the postsynaptic membrane, while motilin and neurotensin may act on the presynaptic terminal.
Somatostatin
and bombesin may work either presynaptically or postsynaptically.
...
PMID:Sites of action of brain-gut peptides in cultured neurons of rat brainstem. 299 59
A study was made of the action of C-terminal tetrapeptide cholecystokinin (
CCK-4
) on the secretory function of A-, B- and D-cells of the islets of Langerhans and on the lactotropic function of the hypophysis. Intravenous injection into rats of
CCK-4
in doses of 5 and 50 micrograms/kg bw resulted within 2 min in increased blood immunoreactive insulin. Tetrapeptide also exerted a stimulant dose-dependent action on the function of insulin-, glucagon- and
somatostatin
-secreting pancreatic cells of the pancreatic islets in culture at concentrations ranging within 10(-9)-10(-6)M. When given in the same doses
CCK-4
did not affect basal or dopamine-inhibited prolactin secretion by cultured adenohypophyseal cells. It is concluded that
CCK-4
stimulates insulin, glucagon and
somatostatin
secretion by direct contact with target cells.
...
PMID:[Effect of C-terminal tetrapeptide cholecystokinin (CCK-4) on the function of the islands of Langerhans and the adenohypophysis]. 614 60
Studies were performed to investigate the effects of neurotransmitters and neurotransmitter candidates (substance P, VIP,
somatostatin
, Met-enkephalin, gastrin-17,
CCK-4
and -8, neurotensin and TRH) of the newly discovered peptidergic nervous system on lower oesophageal sphincter pressure in anaesthetized pigs. All neuropeptides were infused over 2 min periods in 6 different doses, separated by resting periods of at least 1 min, directly into the arterial supply of the lower oesophageal sphincter. Substance P caused a dose-dependent increase in lower oesophageal shpincter pressure; the threshold dose was 9 pmol . kg-1 . min-1 and half maximal response occurred at 72 pmol . kg-1 . min-1. None of the other polypeptides, however, influenced the resting lower oesophageal sphincter. These studies show that substance P is a potent stimulant of smooth muscle in the lower oesophageal sphincter, suggesting that this peptide may be an important regulator of lower oesophageal sphincter pressure.
...
PMID:Effects of regulatory peptides on the porcine lower oesophageal sphincter. 618 84
Since VIP occurs in intrathyroidal nerves its role in thyroid hormone secretion has been investigated. It has been found that VIP is a stimulator of iodothyronine secretion in mice. In this respect VIP has a weaker potency than TSH, but shows a similar time characteristic. Also, VIP and TSH potentiate each others effects. In contrast to the effect of TSH, that of VIP is uninfluenced by alpha-adrenoceptor blockade. VIP, like TSH, stimulates thyroid cyclic AMP production. Thus, VIP nerves might, together with TSH, adrenergic and cholinergic nerves and other peptides such as
somatostatin
, participate in the complex regulation of iodothyronine secretion. Beside this, VIP has also been found to stimulate calcitonin secretion in rats. Other intrathyroidal neuropeptides, such as substance P and
CCK-4
, have been found to be without effects on iodothyronine secretion, but, like VIP, to stimulate calcitonin secretion.
...
PMID:Influence of VIP on thyroid hormone secretion. 647 58
Endocrine cells containing gastrin/cholecystokinin (CCK)-like immunoreactivity were localized to the islet tissue in the pancreas of the spiny dogfish. Most of these cells were located in the 'intestinal' lobe of the pancreas; only occasional cells were observed in the 'splenic' lobe. The gastrin/CCK-like immunoreactive cells were often co-localized with the 'classical' pancreas hormones (insulin, glucagon and
somatostatin
). Radioimmunoassay of water extracts with a C-terminally directed antiserum revealed high levels of immunoreactive material in the intestinal part (48.6 +/- 19.9 pmol/g) and lower levels (4.5 +/- 0.6 pmol/g) in the splenic part. Acetic acid extracts of the intestinal lobe contained low levels (6.8 +/- 3.3 pmol/g) of gastrin/CCK-like immunoreactivity, whereas corresponding extracts of the splenic part showed no immunoreactivity. When the extracts were subjected to DEAE ion-exchange chromatography the gastrin/CCK-like peptides eluted as a major peak. After Sephadex gel filtration, pooled immunoreactive material from the main DEAE chromatographic peak eluted at a position close to that of
CCK4
. Further characterization by ion-exchange and reversed-phase HPLC showed that, in general, the immunoreactive material behaved like the shorter forms of the gastrin/CCK family (
CCK4
/G5 and CCK8/Cae 3-10).
...
PMID:Endocrine cells with gastrin/cholecystokinin-like immunoreactivity in the pancreas of the spiny dogfish, Squalus acanthias. 1250 16
