Abstract
Treatment of confluent cultures of JAR human placental choriocarcinoma cells with cholera toxin or forskolin for 16 h markedly stimulated (2.4-fold) serotonin transport activity in these cells. Cycloheximide, an inhibitor of protein synthesis or actinomycin D, an inhibitor of mRNA synthesis effectively blocked this stimulation. Northern blot analysis revealed that treatment with cholera toxin resulted in severalfold increase in the concentrations of the three mRNA species (6.8, 4.9 and 3.0 kilobases in size) which hybridized to the human placental serotonin transporter cDNA. Under similar conditions, the concentrations of the mRNA species which hybridized to the human placental taurine transporter cDNA or to the human beta-actin cDNA were not affected. Analysis of paroxetine-sensitive binding of the cocaine analog 2 beta-carbomethoxy-3 beta-(4- [125I]iodophenyl)tropane to the membranes prepared from control and cholera toxin-treated cells indicated that the maximal binding capacity was increased 2.5-fold by cholera toxin, with no significant change in the binding affinity. Thus, stimulation of serotonin transporter activity in the placental choriocarcinoma cells following cholera toxin treatment is likely a result of an increase in cell surface density of the serotonin transporter protein as a consequence of increased steady state serotonin transporter mRNA levels.
Highlights
From the Departmentsof $Biochemistry and Molecular Biology and TPhysiology and Endocrinology, MedicaClollege of Georgia, Augusta, Georgia 30912-2100 and the1I..De.uartment of Anatomy andCell Biology, Emory University Schoolof Medicine, Atlanta, Georgia 30322
Treatment of confluent cultures of JAR human pla- ( l l ), r a t basophilic leukemia cells [12], and the human placental choriocarcinoma cells with cholera toxoirn for- centa [13], and comparison of amino acid sequences deduced skolin for 16 h markedly stimulated (2.4-fold) sero- from thecloned cDNAs indicates that serotonin transporters tonin transport activity in thesecells
Culture of Human Placental Choriocarcinoma Cells-The JAR human placentalchoriocarcinoma cell line was obtained from the Amerchemistry and Molecular Biology, Medical College of Georgia, Au-The abbreviation used is: RTI-55, 2/3-carbomethoxy-3~-(4-iodogusta, GA 30912-2100
Summary
Placental syncytiotrophoblastpossesses a high affinity transport system for serotonin (I), and the general properties of this transport system have been investigated in detail [2,3,4,5,6]. The biochemical and pharmacological characteristics of the placental serotonin transporter are strikingly similator those of the serotonin transport systems expressed in the plasma. 5-[1,2-3H]Hydroxytrytamin(eserotonin) binoxalate (specific radioactivity, 30.4 Ci/mmol), ~-[4,5-~H]leucin(sepecific radioactivity, 53Ci/mmol), [5,6-3H]uridine (specific radioactivity, 59 Ci/mmol), and [cu-32P]dCTP(specific radioactivity, 3000 Ci/mmol) were purchased from Du Pont-New England Nuclear. [‘z51]RTI-551(specific membrane of platelets [7,8] and serotonergic neurons[9, 10]. Radioactivity, 2200 Ci/mmol) was a gift from Dr.John W. The serotonin transporter habseen cloned from the rat brainNational Institute on DrAugbuse.
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