Effects of vasoactive autacoids on the human umbilical‐fetal placental vasculature

Mak, K. K.-W.; Gude, Neil M; Walters, W.A.W.; Boura, A. L. A.

doi:10.1111/j.1471-0528.1984.tb05890.x

Cited by 125 publications

(50 citation statements)

References 26 publications

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“…Koren et al (1966) have shown that the 5-HT content of the placenta gradually increases as pregnancy advances; this is consistent with the lack of 5-HT immunoreactivity in endothelial cells from early pregnancy observed in this study. Various authors have demonstrated that placental vessels are much less sensitive to 5-HT than umbilical arteries (Panigel 1962;Mak et al 1984;MacLean et al 1992); this implies that the main role for 5-HT lies in the umbilical vessels. Responses to 5-HT in the feto-placental circulation have been demonstrated by several authors (McGrath et al 1990;Breslin 1991).…”

Section: Discussionmentioning

confidence: 98%

Electron-microscopic immunolabelling of vasoactive substances in human umbilical endothelial cells and their actions in early and late pregnancy

Sexton

Loesch

Turmaine

et al. 1996

Cell and Tissue Research

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Human umbilical vessels are devoid of nerves and therefore endothelial cells may play an important role in the control of feto-placental blood flow. The pharmacological effects of 5-hydroxytryptamine, histamine and endothelin were examined in umbilical arteries and veins from legal terminations (gestational age 8-17 weeks, n=12) and normal term vaginal deliveries (gestational age 38-41, n=12). Immunocytochemistry of human unbilical vessels indicated that 5-hydroxytryptamine, histamine and endothelin were localised in subpopulations of endothelial cells of both artery and vein in late, but not early, pregnancy. 5-Hydroxytryptamine (10 nM-30 microM) caused sustained concentration-dependent contractions in all vessels from early and late pregnancy. Histamine (0.1 microM-30 mM) also caused sustained contractions in all vessels from late pregnancy but only 27% of arteries and 41% of veins from early pregnancy responded. Endothelin (10 pM-30 nM) caused slow long-lasting contractions in all vessels from early and late pregnancy. Atrial natriuretic peptide and neuropeptide Y did not alter vascular tone. The endothelium may thus play an autocrine/paracrine role, by synthesizing and releasing the above reactive substances in late pregnancy to influence feto-placental blood flow.

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Section: Discussionmentioning

confidence: 98%

Electron-microscopic immunolabelling of vasoactive substances in human umbilical endothelial cells and their actions in early and late pregnancy

Sexton

Loesch

Turmaine

et al. 1996

Cell and Tissue Research

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“…Maximal activation of TxAz receptors in the human placental fetal vasculature with the TxAz-mimetic U466 19 can cause complete occlusion of the fetal circulation, emphasizing the adverse effects this autacoid can have on blood flow when liberated in excessive amounts during disease. Similar degrees of maximal vasoconstriction can also be caused by high concentrations of PGFzn and PGEz, although these autacoids are approximately I00 and 3000 times, respectively, less potent than U46619 (Mak et al 1984). Prostacyclin, the physiological antagonist of TxAz, has also been indirectly identified as its stable metabolic product 6-ketoPGF1,.…”

Section: Effects Of Passage Through the Placenta On The Activities Ofmentioning

confidence: 99%

Autacoids and Control of Human Placental Blood Flow

Boura

Walters

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et al. 1994

Clin Exp Pharma Physio

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SUMMARY1. Humans have a haemochorial, villous placenta. Uterine blood passes through maternal sinuses, bathing placental villi through which fetal blood circulates. Blood flow through each circulation is high and vascular resistance low. This haemodynamic situation is essential for efficient placental function.2. The low placental vascular resistance is due to a lack of nervous influences together with pregnancy-induced changes promoting vasodilatation. Increases occur in output of the vasodilators prostacyclin and nitric oxide and also in membrane sodium pump activity.3. Many autacoids are present in umbilical blood. Fetal vessels of the placenta develop intense vasoconstriction in the presence of some autacoids, such as thromboxane A2 and prostaglandins Fza and E2, and respond weakly to others, such as angiotensin I1 and 5-hydroxytryptamine. Nevertheless, vasodilator influences predominate.4. The diseases of pre-eclampsia and fetal growth retardation are associated with reduced output of nitric oxide and prostacyclin and with increased production of thromboxane A2 and endothelin-1 . These changes promote vasoconstriction, increased vascular sensitivity to vasoconstrictor stimuli, platelet aggregation and intravascular coagulation, retarding blood flow and fetoplacental growth.5. Aspirin and glyceryl trinitrate have been investigated for possible therapeutic use in preeclampsia and fetal growth retardation. Improved drug therapy is likely as knowledge increases of the importance of autacoids in normal placental function and in the changes that occur during disease.

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“…or inhaled 70% N20 and 30% 02. These drugs have no apparent effects on responses of the foetal vascular tissues under the conditions used (Mak et al, 1984 tration causing a threshold effect, the concentration was increased by approximately 0.5 log10 intervals, after each effect obtained became constant. The highest concentration used was either that causing a maximal response or that which could be achieved due to the constraint of lack of sufficient solubility in the solution being infused.…”

Section: Collection Ofplacentaementioning

confidence: 99%

Vascular actions of purines in the foetal circulation of the human placenta

Read

Boura

Walters

1993

British J Pharmacology

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1 The vasoactive effects of adenosine triphosphate (ATP), adenosine and other purines in the foetal circulation of the human placenta were examined. Single lobules of the placenta were bilaterally perfused in vitro with Krebs buffer (maternal and foetal sides 5 ml min' each, 95% 02:5% CO2, 37°C). Changes in foetal vascular tone were assessed by recording perfusion pressure during constant infusion of each purine. To allow recording of the vasodilator effects, submaximal vasoconstriction was induced by concomitant infusion of prostaglandin F20, (0.7-2.0 ytmolI 1).2 ATP (1.0-1001amoll-1) usually caused concentration-dependent reductions in perfusion pressure.However, biphasic with initial transient increases, or only increases in pressure were sometimes observed. Falls in pressure caused by ATP were significantly reduced by addition to the perfusate of N0-nitro-Larginine (L-NOARG) (100 jamol 1-') but not N0-nitro-D-arginine (D-NOARG) (100 tLmol 1). They were not influenced by addition of indomethacin (I0 lmolI 1) or L-arginine (100 gmol 1').

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Effects of vasoactive autacoids on the human umbilical‐fetal placental vasculature

Cited by 125 publications

References 26 publications

Electron-microscopic immunolabelling of vasoactive substances in human umbilical endothelial cells and their actions in early and late pregnancy

Electron-microscopic immunolabelling of vasoactive substances in human umbilical endothelial cells and their actions in early and late pregnancy

Autacoids and Control of Human Placental Blood Flow

Vascular actions of purines in the foetal circulation of the human placenta

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