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在动脉和组织培养中,鉴定来自平滑肌细胞、成纤维细胞和内皮细胞的不同钠区室。

Identification of different sodium compartments from smooth muscle cells, fibroblasts and endothelial cells, in arteries and tissue culture.

作者信息

Garay R P, Moura A M, Osborne-Pellegrin M J, Papadimitriou A, Worcel M

出版信息

J Physiol. 1979 Feb;287:213-29. doi: 10.1113/jphysiol.1979.sp012655.

DOI:10.1113/jphysiol.1979.sp012655
PMID:571018
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1281491/
Abstract
  1. The (22)Na efflux curve from the rat tail artery, at 35 degrees C, can be analysed as the sum of three distinct components, from 0 to 90 min of washout. After an initial diffusional component the two late exponential components Be(-kBt) and Ce(-kCt) have the following values: B = 3.03 +/- 0.15 m-mole/kg wet wt. and C = 0.56 +/- 0.04; k(B) = 0.145 +/- 0.005 min(-1) and k(C) = 0.015 +/- 0.007.2. In order to identify the cellular origin of the different compartments we compared the (22)Na efflux curve from the rat tail artery with the curves obtained from whole rabbit aortal strips, rabbit aortal medial or adventitial strips; and primary cultures from rabbit aorta medial smooth muscle cells, cultures of a non-fusing muscle cell line (BC(3)H1), fibroblasts and endothelial cells.3. It is possible to identify under these experimental conditions the cellular compartments from which the different exponential components of the efflux from the whole arteries originate. Fibroblasts and endothelial cultures, as well as adventitial strips exchange (22)Na slowly with exponential constants resembling k(C). Their efflux rate constants are: fibroblast cultures 0.010 +/- 0.002 min(-1), endothelial cells 0.015 +/- 0.003 min(-1) and adventitia 0.019 +/- 0.007 min(-1). Smooth muscle cells are exclusively responsible for the intermediate component Be(-kBt), but they present also a slow component, indistinguishible from the slow exponential component from the other types of cells in the artery. The rate constants for muscle cells are: rabbit aortic media k(B) 0.25 +/- 0.09 min(-1) and k(C) = 0.013 +/- 0.004 min(-1); medial cultures k(B) = 0.202 +/- 0.005 min(-1) and k(C1) = 0.020 +/- 0.003 min(-1); and BC(3)H1 cell culture k(B) = 0.205 +/- 0.083 min(-1) and k(C) = 0.016 +/- 0.003 min(-1).4. The efflux from compartment B of smooth muscle cells is inhibited by ouabain and in the absence of extracellular K(+). The efflux from compartment C is inhibited only by ouabain but not by the suppression of extracellular K(+).5. We propose a distribution of Na(+) in smooth muscle cells in two intracellular compartments: (1) Na(+) freely dissolved in the sarcoplasm, exchanging with the kinetics of compartment B and (2) a second cellular compartment which could be contained in the sarcoplasmic reticulum exchanging with the kinetics of compartment C.6. On the basis of the previous model of Na(+) distribution, considering our values, and without any correction, the estimated sarcoplasmic concentration of Na(+) is 9.6 mM, compatible with the direct measurements obtained in skeletal and heart muscle. The Na(+) concentration in the sarcoplasmic reticulum would be 4-10 times higher than in the cytoplasm. In order to increase the accuracy of our calculations it would be necessary to account for the interdiffusion and back diffusion of Na(+) between compartments. It is not possible to attain this goal at the present time.
摘要
  1. 在35摄氏度下,大鼠尾动脉的(22)钠流出曲线,在洗脱0至90分钟内,可分析为三个不同成分的总和。在初始扩散成分之后,两个晚期指数成分Be(-kBt)和Ce(-kCt)具有以下值:B = 3.03±0.15毫摩尔/千克湿重,C = 0.56±0.04;k(B) = 0.145±0.005分钟(-1),k(C) = 0.015±0.007。

  2. 为了确定不同区室的细胞来源,我们将大鼠尾动脉的(22)钠流出曲线与从全兔主动脉条、兔主动脉中膜或外膜条获得的曲线进行了比较;以及兔主动脉中膜平滑肌细胞的原代培养物、非融合肌肉细胞系(BC(3)H1)的培养物、成纤维细胞和内皮细胞。

  3. 在这些实验条件下,可以确定全动脉流出的不同指数成分所源自的细胞区室。成纤维细胞和内皮细胞培养物,以及外膜条以类似于k(C)的指数常数缓慢交换(22)钠。它们的流出速率常数为:成纤维细胞培养物0.010±0.002分钟(-1),内皮细胞0.015±0.003分钟(-1),外膜0.019±0.007分钟(-1)。平滑肌细胞专门负责中间成分Be(-kBt),但它们也呈现出一个缓慢成分,与动脉中其他类型细胞的缓慢指数成分无法区分。肌肉细胞的速率常数为:兔主动脉中膜k(B) 0.25±0.09分钟(-1),k(C) = 0.013±0.004分钟(-1);中膜培养物k(B) = 0.202±0.005分钟(-1),k(C1) = 0.020±0.003分钟(-1);以及BC(3)H1细胞培养物k(B) = 0.205±0.083分钟(-1),k(C) = 0.016±0.003分钟(-1)。

  4. 平滑肌细胞B区室的流出受到哇巴因抑制,且在无细胞外钾(+)的情况下。C区室的流出仅受哇巴因抑制,而不受细胞外钾(+)抑制的影响。

  5. 我们提出平滑肌细胞中钠(+)分布在两个细胞内区室:(1)自由溶解在肌浆中的钠(+),以B区室的动力学进行交换;(2)第二个细胞区室,可能包含在肌浆网中,以C区室的动力学进行交换。

  6. 根据先前的钠(+)分布模型,考虑到我们的值,且未经任何校正,估计的肌浆中钠(+)浓度为9.6毫摩尔/升,与在骨骼肌和心肌中获得的直接测量值相符。肌浆网中的钠(+)浓度将比细胞质中的高4至10倍。为了提高我们计算的准确性,有必要考虑钠(+)在区室之间的相互扩散和反向扩散。目前无法实现这一目标。

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