首页> 外文OA文献 >Human placental syncytiotrophoblast expresses two pharmacologically distinguishable types of Na(+)-H+ exchangers, NHE-1 in the maternal-facing (brush border) membrane and NHE-2 in the fetal-facing (basal) membrane.
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Human placental syncytiotrophoblast expresses two pharmacologically distinguishable types of Na(+)-H+ exchangers, NHE-1 in the maternal-facing (brush border) membrane and NHE-2 in the fetal-facing (basal) membrane.

机译:人胎盘合体滋养层细胞表达两种药理学上可区分的Na(+)-H +交换子类型,即面向母体(刷状边缘)的膜中的NHE-1和面向胎儿(基部)的膜中的NHE-2。

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摘要

We investigated whether highly purified preparations of basal (fetal-facing) membrane isolated from normal term human placentas possess Na(+)-H+ exchanger activity. Uptake of Na+ into basal membrane vesicles was stimulated many-fold by an outwardly directed H+ gradient. This H(+)-gradient-dependent uptake was inhibitable by amiloride and its analogues. Na+ uptake in these vesicles did not occur via a Na+ channel, as it was not influenced by changes in membrane potential and, in addition, was inhibited by benzamil only at high micromolar concentrations. The results indicate that the human placental basal membrane possesses Na(+)-H+ exchanger activity. We then studied whether this exchanger is similar to or distinct from the Na(+)-H+ exchanger described in brush border (maternal-facing) membrane preparations. For this purpose, we compared the pharmacological characteristics of the basal membrane Na(+)-H+ exchanger with those of the brush border membrane Na(+)-H+ exchanger. The basal membrane exchanger was about 20-fold less sensitive to inhibition by amiloride and about 70-fold less sensitive to inhibition by dimethylamiloride than was the brush border membrane exchanger. The exchanger activity in both membrane preparations was inhibitable by clonidine and cimetidine, but the inhibition patterns with these compounds were markedly different between basal and brush border membrane preparations. These data demonstrate that the basal membrane Na(+)-H+ exchanger is distinct from the brush border membrane Na(+)-H+ exchanger. The pharmacological profiles of these exchangers indicate that the human placental brush border membrane possesses the housekeeping or non-epithelial type Na(+)-H+ exchanger (NHE-1), whereas the basal membrane possesses the epithelial or apical type Na(+)-H+ exchanger (NHE-2).
机译:我们调查了从正常人胎盘中分离的基底膜(胎膜)的高纯度制剂是否具有Na(+)-H +交换子活性。向外定向的H +梯度可将Na +吸收到基底膜囊泡中。阿米洛利及其类似物可抑制这种H(+)梯度依赖性的摄取。这些囊泡中的Na +吸收没有通过Na +通道发生,因为它不受膜电位变化的影响,此外,仅在高微摩尔浓度下,苯扎米尔抑制了Na +的吸收。结果表明,人胎盘基底膜具有Na(+)-H +交换活性。然后,我们研究了该交换器是否类似于或与刷边界(面向母亲的)膜制备中所述的Na(+)-H +交换器相似或不同。为此,我们比较了基膜Na(+)-H +交换剂和刷状缘膜Na(+)-H +交换剂的药理特性。与刷缘膜交换器相比,基底膜交换器对阿米洛利的抑制敏感性低约20倍,对二甲基阿米洛利的抑制敏感性低约70倍。可乐定和西咪替丁对两种膜制剂的交换剂活性均具有抑制作用,但这些化合物的抑制模式在基底膜和刷状缘膜制剂之间明显不同。这些数据表明,基底膜Na(+)-H +交换剂不同于刷状边界膜Na(+)-H +交换剂。这些交换子的药理学特征表明,人胎盘刷状缘膜拥有管家型或非上皮型Na(+)-H +交换子(NHE-1),而基底膜具有上皮或根尖型Na(+)- H +交换器(NHE-2)。

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