羊膜上皮细胞培养中水通道蛋白3在人胎膜中的表达及环磷酸腺苷对其上调的影响。

Shengbiao Wang, Fataneh Amidi, Marie Beall, Lizhen Gui, Michael G Ross
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引用次数: 40

摘要

目的:细胞膜水通道蛋白水通道蛋白(AQPs)可能在调节羊水(AF)的膜内吸收途径中起重要作用。本研究的目的是确定水通道蛋白3 (AQP3)是否在人胎膜中表达,并进一步确定AQP3在原代人羊膜细胞培养中的表达是否受第二信使环磷酸腺苷(cAMP)的调节。方法:采用逆转录聚合酶链反应(RT-PCR)和免疫组化(IHC)技术检测正常足月妊娠人胎膜中AQP3的表达。为了确定cAMP对AQP3表达的影响,我们将原代人羊膜细胞培养物分别置于单独的热灭活培养基(对照)或热灭活培养基中处理:(1)SP-cAMP,一种膜渗透性和抗磷酸二酯酶的cAMP激动剂,或(2)福斯可林,一种腺苷酸环化酶刺激剂。提取总RNA,采用多重实时RT-PCR技术相对定量AQP3的表达。结果:采用RT-PCR检测胎盘、绒毛膜和羊膜中AQP3的表达。通过免疫组化,我们鉴定了AQP3蛋白在胎盘合胞滋养细胞和细胞滋养细胞、绒毛膜细胞滋养细胞和羊膜上皮中的表达。在原代羊膜上皮细胞培养中,AQP3 mRNA在福斯可林或SP-cAMP治疗后2小时显著升高,在福斯可林治疗后10小时保持升高,并在治疗后20小时恢复到基线水平。结论:本研究提供了AQP3在人胎膜中表达的证据,并证明了AQP3在人原代羊膜细胞培养中被第二信使cAMP上调表达。由于AQP3对水、尿素和甘油具有渗透性,因此其在胎膜中的表达调节可能有助于心房颤动的稳态。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Aquaporin 3 expression in human fetal membranes and its up-regulation by cyclic adenosine monophosphate in amnion epithelial cell culture.

Objective: The cell membrane water channel protein aquaporins (AQPs) may be important in regulating the intramembranous (IM) pathway of amniotic fluid (AF) resorption. The objective of the present study was to determine whether aquaporin 3 (AQP3) is expressed in human fetal membranes and to further determine if AQP3 expression in primary human amnion cell culture is regulated by second-messenger cyclic adenosine monophosphate (cAMP).

Methods: AQP3 expression in human fetal membranes of normal term pregnancy was studied by reverse transcription polymerase chain reaction (RT-PCR) and immunohistochemistry (IHC). To determine the effect of cAMP on AQP3 expression, primary human amnion cell cultures were treated in either heat-inactivated medium alone (control), or heat-inactivated medium containing: (1) SP-cAMP, a membrane-permeable and phosphodiesterase resistant cAMP agonist, or (2) forskolin, an adenylate cyclase stimulator. Total RNA was isolated and multiplex real-time RT-PCR employed for relative quantitation of AQP3 expression.

Results: We detected AQP3 expression in placenta, chorion, and amnion using RT-PCR. Using IHC, we identified AQP3 protein expression in placenta syncytiotrophoblasts and cytotrophoblasts, chorion cytotrophoblasts, and amnion epithelia. In primary amnion epithelial cell culture, AQP3 mRNA significantly increased at 2 hours following forskolin or SP-cAMP, remained elevated at 10 hours following forskolin, and returned to baseline levels by 20 hours following treatment.

Conclusion: This study provides evidence of AQP3 expression in human fetal membranes and demonstrates that AQP3 expression in primary human amnion cell culture is up-regulated by second-messenger cAMP. As AQP3 is permeable to water, urea, and glycerol, modulation of its expression in fetal membranes may contribute to AF homeostasis.

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