Release of 5‐hydroxytryptamine (serotonin) from the dog's gastro‐intestinal tract

Toh, Chee-Seng

doi:10.1113/jphysiol.1954.sp005206

Cited by 76 publications

(38 citation statements)

References 9 publications

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“…Hence, it can be assumed that under the 'Normal' and 'Niamid' conditions the endogenous 5-HT was released directly into the serosal fluid and that release into the lumen with subsequent absorption did not occur. The evidence that endogenous 5-HT is released into the serosal fluid adds further support to the view that blood 5-HT is derived from the intestine (Toh, 1954;Erspamer & Testini, 1959;Adams, 1960;Bertaccini, 1960;Stacey & Young, 1964).…”

Section: Discussionsupporting

confidence: 49%

“…The uptake of 5-HT by platelets in vivo has also been demonstrated (Erspamer, 1956;Weissbach, Bogdanski & Udenfriend, 1958). There is also considerable evidence that the gastrointestinal mucosa is the main, if not the only, source of platelet 5-HT (Toh, 1954;Haverback & Davidson, 1958;Rosenberg, Davis, Moran & Zimmermann, 1959;Bertaccini, 1960). The large amounts of 5-HT in the enterochromaffin cells and the elevation M. C. E. GWEE AND T. S. YEOH of blood 5-HT in patients with carcinoid tumours (Sjoerdsma, Weissbach & Udenfriend, 1956) indicate that platelet 5-HT has its origin in the enterochromaffin cells (Barter & Everson-Pearse, 1953, 1955Erspamer, 1955).…”

Section: Introductionmentioning

confidence: 96%

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The release of 5‐hydroxytryptamine from rabbit small intestine in vitro

Gwee¹,

Yeoh²

1968

The Journal of Physiology

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SUMMARY1. A method is described by which the lumen of intestinal segments may be perfused separately and simultaneously under identical conditions of perfusion pressure and temperature, and the rate of appearance of 5-hydroxytryptamine (5-HT) into the serosal fluid measured.2. 5-HT appeared in the serosal fluid from quiescent segments of rabbit intestine at a rate of about 4 0 ng/cm intestine/hr and about 14-0 ng/cm intestine/hr from segments performing active peristaltic movements.3. For both quiescent and active segments, when the perfusion fluid contained a monoamine oxidase inhibitor, nialamide (Niamid), the rate of appearance of 5-HT was increased and if, in addition, 5-HT was present in the perfusion fluid the rate of appearance of 5-HT in the serosal fluid was even greater.4. The rate of appearance of 5-HT from the intestine of rabbits pretreated with reserpine was about 08 ng/cm intestine/hr and Niamid only slightly increased this rate. However, if 5-HT as well as Niamid were present the rate of appearance of 5-HT was about 6-0 ng/cm intestine/hr. 5. Possible explanations for these findings are discussed.

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Section: Discussionsupporting

confidence: 49%

Section: Introductionmentioning

confidence: 96%

The release of 5‐hydroxytryptamine from rabbit small intestine in vitro

Gwee¹,

Yeoh²

1968

The Journal of Physiology

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“…Dopamine uptake by OCT1, although significant, is again unlikely to be germane to the liver because of the low circulating levels of this neurotransmitter. Serotonin, however, is found at high concentrations in the gut; consequently, portal blood levels are significantly higher than arterial blood, reportedly as much as 3-fold (Toh 1954;Gershon and Tack, 2007), making it the best candidate of the three neurotransmitters to be transported by OCT1 in vivo. Because of this, and the data suggesting that serotonin was the superior neurotransmitter substrate for OCT1, serotonin was selected as the model endogenous substrate for further study.…”

Section: Resultsmentioning

confidence: 99%

Common Drugs Inhibit Human Organic Cation Transporter 1 (OCT1)-Mediated Neurotransmitter Uptake

2014

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The human organic cation transporter 1 (OCT1) is a polyspecific transporter involved in the uptake of positively charged and neutral small molecules in the liver. To date, few endogenous compounds have been identified as OCT1 substrates; more importantly, the effect of drugs on endogenous substrate transport has not been examined. In this study, we established monoamine neurotransmitters as substrates for OCT1, specifically characterizing serotonin transport in human embryonic kidney 293 cells. Kinetic analysis yielded a K m of 197 micomolar and a V max of 561 pmol/mg protein/ minute for serotonin. Furthermore, we demonstrated that serotonin uptake was inhibited by diphenhydramine, fluoxetine, imatinib, and verapamil, with IC 50 values in the low micromolar range. These results were recapitulated in primary human hepatocytes, suggesting that OCT1 plays a significant role in hepatic elimination of serotonin and that xenobiotics may alter the elimination of endogenous compounds as a result of interactions at the transporter level.

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“…However platelets take up 5-HT from solution (Humphrey and Toh, 1954) and there are many sites (e.g., the intestinal tract; Toh, 1954) where the presence of large amounts of 5-hydroxytryptophan decarboxylase suggests that the circulating platelets may acquire their 5-HT. There is, however, no evidence that the 5-hydroxytryptophan is formed at the same sites at which it is decarboxylated.…”

mentioning

confidence: 99%