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极化的人支气管和结肠上皮细胞中的基底外侧储存式钙离子内流

Basolateral store-operated Ca(2+)-entry in polarized human bronchial and colonic epithelial cells.

作者信息

Kerstan D, Thomas J, Nitschke R, Leipziger J

机构信息

Physiologisches Institut, Albert-Ludwigs-Universität, Freiburg, Germany.

出版信息

Cell Calcium. 1999 Dec;26(6):253-60. doi: 10.1054/ceca.1999.0088.

Abstract

Bronchial epithelial cells respond to extracellular nucleotides from the luminal and basolateral side activating Cl- secretion via [Ca2+]i increase. In this study we investigated the differences of apically (ap) and basolaterally (bl) stimulated [Ca2+]i signals in polarized human bronchial epithelial cells (16HBE14o-). Specifically we investigated the localization of 'capacitative Ca2+ entry' (CCE). 16HBE14o- cells grown on permeable filters were mounted into an Ussing chamber built for the simultaneous measurement of Fura-2 fluorescence and electrical properties. Application of ATP from both sides induced a rapid [Ca2+]i increase and subsequent sustained [Ca2+]i plateau due to transmembraneous Ca(2+)-influx. The use of different nucleotides revealed the following rank order or potency which was very similar for addition from the apical or basolateral side: UTP (EC50 ap: 4 microM, bl: 5 microM) > ATP (EC50 ap: 4 microM, bl: 10 microM) > ADP (n = 4-7 from both sides). 2-MeS-ATP, AMP, adenosine and beta gamma-methylene ATP were ineffective (n = 3 from both sides). The ATP- (ap and bl) induced Ca2+ influx was only abolished by removal of basolateral Ca2+. This was also true for receptor-independent activation of Ca(2+)-influx by intracellular Ca(2+)-store depletion with 2,5 Di-(tert-butyl)-1,4-benzohydroquinone (BHQ) (10 microM). Also in polarized T84 cells the basolateral carbachol and BHQ activated Ca2+ plateau was exclusively sensitive to removal of basolateral Ca2+. We propose that in all polarized epithelial cells the CCE entry pathway is located in the basolateral membrane. We furthermore suggest that Ca2+[i elevating agonists acting from the apical side of the epithelium lead to the opening of a basolateral CCE pathway.

摘要

支气管上皮细胞对来自管腔侧和基底外侧的细胞外核苷酸作出反应,通过细胞内钙离子浓度([Ca2+]i)升高激活氯离子分泌。在本研究中,我们调查了极化的人支气管上皮细胞(16HBE14o-)中,顶端(ap)和基底外侧(bl)刺激引起的[Ca2+]i信号的差异。具体而言,我们研究了“容量性钙离子内流”(CCE)的定位。将生长在可渗透滤膜上的16HBE14o-细胞安装到一个用于同时测量Fura-2荧光和电特性的尤斯灌流小室中。从两侧施加ATP均诱导[Ca2+]i迅速升高,随后由于跨膜钙离子内流而出现持续的[Ca2+]i平台期。使用不同的核苷酸显示出以下效力排序,从顶端或基底外侧添加时非常相似:尿苷三磷酸(UTP,顶端EC50:4微摩尔,基底外侧:5微摩尔)>三磷酸腺苷(ATP,顶端EC(50):4微摩尔,基底外侧:10微摩尔)>二磷酸腺苷(ADP,两侧n = 4 - 7)。2 - 甲硫基 - ATP、单磷酸腺苷(AMP)、腺苷和βγ - 亚甲基ATP无效(两侧n = 3)。ATP(顶端和基底外侧)诱导的钙离子内流仅在去除基底外侧钙离子时被消除。用2,5 - 二 - (叔丁基) - 1,4 - 苯二酚(BHQ)(10微摩尔)使细胞内钙离子储存耗竭从而非受体依赖性激活钙离子内流时也是如此。同样在极化的T84细胞中,基底外侧的卡巴胆碱和BHQ激活的钙离子平台期仅对去除基底外侧钙离子敏感。我们提出,在所有极化上皮细胞中,CCE内流途径位于基底外侧膜。我们还进一步表明,从上皮顶端侧起作用的升高[Ca2+]i的激动剂会导致基底外侧CCE途径开放。

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