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小叶内涎腺导管膜囊泡中的钠离子通道

Na+ channels in membrane vesicles from intralobular salivary ducts.

作者信息

Moran A, Davis V H, Turner R J

机构信息

Department of Physiology, Faculty of Health Sciences, Ben-Gurion University, Beer-Sheva, Israel.

出版信息

Am J Physiol. 1995 Feb;268(2 Pt 1):C350-5. doi: 10.1152/ajpcell.1995.268.2.C350.

Abstract

Electrical potential-driven 22Na+ fluxes were measured in membrane vesicles prepared from male and female rat submandibular intralobular ducts. A relatively temperature-independent (Q10 = 1.45 +/- 0.15), amiloride-inhibitable (mean affinity constant approximately 1 microM), rheogenic Na+ transport pathway was observed. The relative potency of amiloride analogues for inhibition of this pathway was amiloride > ethylisopropyl-amiloride > phenamil, similar to that of the "low-amiloride-affinity" Na+ channel recently observed in a number of other tissues. These results are consistent with the existence of the apical Na+ channel thought to be involved in intralobular ductal salt reabsorption. No significant difference was found in the magnitude or pharmacology of electrogenic Na+ fluxes in vesicles prepared from male and female rat intralobular ducts, suggesting that the sexual dimorphism observed in this tissue is not reflected at the level of the apical membrane Na+ channel. Amiloride-sensitive 22Na+ fluxes in intralobular ductal membranes were of the same magnitude as 22Na+ fluxes measured in similarly prepared and assayed vesicles from the toad bladder, a tissue thought to be a rich source of amiloride-sensitive Na+ channels.

摘要

在从雄性和雌性大鼠下颌下腺小叶内导管制备的膜囊泡中测量了电势驱动的22Na+通量。观察到一种相对不依赖温度(Q10 = 1.45 +/- 0.15)、可被氨氯吡咪抑制(平均亲和常数约为1 microM)、产生电流的Na+转运途径。氨氯吡咪类似物对该途径抑制的相对效力为氨氯吡咪>乙基异丙基氨氯吡咪>非那明,类似于最近在许多其他组织中观察到的“低氨氯吡咪亲和力”Na+通道。这些结果与被认为参与小叶内导管盐重吸收的顶端Na+通道的存在一致。在从雄性和雌性大鼠小叶内导管制备的囊泡中,电生性Na+通量的大小或药理学没有发现显著差异,这表明在该组织中观察到的性二态性在顶端膜Na+通道水平上没有体现。小叶内导管膜中对氨氯吡咪敏感的22Na+通量与在从蟾蜍膀胱制备并测定的类似囊泡中测量的22Na+通量大小相同,蟾蜍膀胱被认为是氨氯吡咪敏感Na+通道的丰富来源。

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