Discriminating Capacity of Indole Markers in the Diagnosis of Carcinoid Tumors

Meijer, Wim G.; Kema, Ido P.; Volmer, Marcel; Willemse, Pax H.B.; Vries, Elisabeth G.E. de

doi:10.1093/clinchem/46.10.1588

Cited by 119 publications

(59 citation statements)

References 28 publications

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“…In a later study, the same group reported that patients with midgut carcinoid tumors had median platelet 5‐HT levels of 23.8 (nmol/10 9 platelets) as compared to 3.4 in normal controls (7.0‐fold increase) 70 . A similar 8.6‐fold increase in platelet 5‐HT was reported by others 71 . Robiolio et al 67 reported that patients with carcinoid syndrome and VHD had higher serum and platelet 5‐HT levels than carcinoid patients without VHD.…”

Section: Discussionsupporting

confidence: 60%

Serotonin (5‐HT) Transporter Ligands Affect Plasma 5‐HT in Rats

Rothman

Żółkowska

Baumann

2008

Annals of the New York Academy of Sciences

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Dual dopamine (DA)/serotonin (5-HT)-releasing agents are promising candidate medications for stimulant addiction and other disorders. However, certain 5-HT transporter (SERT) substrates are associated with development of idiopathic pulmonary arterial hypertension (IPAH) and valvular heart disease (VHD). According to the "5-HT hypothesis," SERT substrates increase the risk for developing IPAH and VHD by increasing plasma 5-HT. To test this hypothesis directly, we determined the effects of acute and chronic fenfluramine, and other SERT ligands, on plasma 5-HT in male rats. For acute treatments, rats received i.v. vehicle or test drug (0.3 and 1.0 mg/kg), and serial blood samples were withdrawn. For chronic treatments, vehicle or test drug was infused via osmotic minipump (3 and 10 mg/kg/d) for 2 weeks. On the last day of infusion, rats received i.v. fenfluramine challenge (1 mg/kg), and serial blood samples were withdrawn. Plasma 5-HT was measured using ex vivo microdialysis in whole-blood samples. Baseline plasma 5-HT was <1.0 nM. Acute injection of fenfluramine or other SERT substrates caused large (up to 24-fold) dose-dependent increases in plasma 5-HT. Chronic fenfluramine at 3 and 10 mg/kg/d produced 1.7- and 3.5-fold increases in baseline plasma 5-HT, while chronic fluoxetine had no effect. Chronic infusions of fenfluramine or fluoxetine diminished the ability of acute fenfluramine to elevate dialysate 5-HT, and both drugs markedly reduced whole-blood 5-HT. Acute fenfluramine increases plasma 5-HT to concentrations that are below the micromolar levels necessary to produce adverse cardiovascular effects. Chronic fenfluramine and fluoxetine have minimal effects on plasma 5-HT, suggesting that the increased risk for IPAH associated with fenfluramine does not depend upon elevations in plasma 5-HT.

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Section: Discussionsupporting

confidence: 60%

Serotonin (5‐HT) Transporter Ligands Affect Plasma 5‐HT in Rats

Rothman

Żółkowska

Baumann

2008

Annals of the New York Academy of Sciences

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“…Darüber hinaus werden für das Karzinoid-Syndrom neben Serotonin auch die Sekretion weiterer Tachykinine wie Substanz P und Neurokinin A verantwortlich gemacht, sodass in seltenen Fällen die 5-HIES-Ausscheidung auch beim Vorhandensein eines Karzinoid-Syndroms unauffällig sein kann, insbesondere wenn keine Durchfälle bestehen [68]. Durch Absenken des Grenzwerts auf 2,8 mmol/mol Kreatinin kann die Sensitivität auf 68 % angehoben werden (bei 89 % Spezifität), während bei einem hohen Grenzwert von 6,7 mmol/mol Kreatinin die Sensitivität bei nur 52 % liegt, aber die Spezifität bei 98 % [70]. Es besteht keine gute Korrelation zwischen der Höhe der 5-HIES-Spiegel und dem Schweregrad der Symptome, was wahrscheinlich auf eine fluktuierende Serotoninsekretion durch den Tumor und zusätzliche Mediatoren des Karzinoid-Syndroms zurückzuführen ist.…”

Section: Starke Empfehlung Konsensunclassified

S2k-Leitlinie Neuroendokrine Tumore

Gastroenterologie¹,

Tumoren²,

e.V.³

et al. 2018

Z Gastroenterol

127

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“…Sometimes serotonin‐secreting PNETs are classified with use of tissue samples (serotonin staining); however, this does not always reflect clinical functionality of the tumour as assessed by determining the 24‐hours urinary 5‐hydroxyindoleacetic acid (5‐HIAA) excretion . In gastrointestinal NETs, 24‐hours urinary 5‐HIAA excretion has a high sensitivity and specificity for detecting metastatic midgut NETs, but it is less useful for predicting survival during follow‐up . In PNETs, the incidence and the effect of elevated 24‐hours urinary 5‐HIAA excretion on survival is unknown.…”

Section: Introductionmentioning

confidence: 99%