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用植物血凝素处理的人血淋巴细胞中的钾转运

Potasssium transport in human blood lymphocytes treated with phytohemagglutinin.

作者信息

Segel G B, Lichtman M A

出版信息

J Clin Invest. 1976 Dec;58(6):1358-69. doi: 10.1172/JCI108591.

Abstract

We have confirmed that phytohemagglutinin (PHA) rapidly enhances the uptake of potassium (K+) by human blood lymphocytes. PHA, however, did not produce an increase in lymphocyte K+ concentration. The apparent steady-state of cell K+ concentration despite the marked increase in uptake of 42K+ could be explained by either an increase in K+-K+ exchange or an increase in concentrative (active) K+ accumulation in association with an increase in the leak of K+ from the cell. We compared, therefore, the uptake of 42K+ with the decrement in cellular K+ content when active transport was inhibited by ouabain. These studies established that K+-K+ exchange was negligible in human blood lymphocytes and that the increase in 42K+ uptake after PHA treatment represented concentrative transport. Our studies did indicate that 42K+ exodus from PHA treated lymphocytes increased markedly from 19 to 38 mmol-1 cell water-1-h-1. Within the same time period K+ influx into PHA-treated lymphocytes increased from 20 to 38 mmol-1 cell water-1-h-1. Thus, PHA produces a marked increase in the permeability of the lymphocyte membrane to K+, and the increase in active K+ influx in PHA-treated lymphocytes may represent a homeostatic response by the membrane K+ transport system to the increase in K+ efflux. Increased K+ turnover was observed at the lowest concentrations of PHA which produced an observable increase in [3H]thymidine incorporation into DNA. Thus, PHA produces an increase in K+ permeability that closely parallels its mitogenic effect. The rapid increase in K+ influx preceding blastogenesis and mitogenesis is required, therefore, to maintain normal intracellular K+ concentration. An adequate intracellular K+ concentration is essential for the synthetic processes required for cell transformation or division.

摘要

我们已经证实,植物血凝素(PHA)能迅速增强人血淋巴细胞对钾(K+)的摄取。然而,PHA并未使淋巴细胞K+浓度升高。尽管42K+摄取量显著增加,但细胞K+浓度的明显稳态可能是由于K+-K+交换增加,或者是与细胞K+泄漏增加相关的浓缩(主动)K+积累增加所致。因此,我们比较了哇巴因抑制主动转运时42K+的摄取与细胞K+含量的减少情况。这些研究表明,人血淋巴细胞中的K+-K+交换可忽略不计,PHA处理后42K+摄取量的增加代表浓缩转运。我们的研究确实表明,PHA处理的淋巴细胞中42K+外流从19 mmol·细胞水-1·小时-1显著增加到38 mmol·细胞水-1·小时-1。在同一时间段内,K+流入PHA处理的淋巴细胞从20 mmol·细胞水-1·小时-1增加到38 mmol·细胞水-1·小时-1。因此,PHA使淋巴细胞膜对K+的通透性显著增加,PHA处理的淋巴细胞中主动K+流入的增加可能代表膜K+转运系统对K+外流增加的一种稳态反应。在产生可观察到的[3H]胸苷掺入DNA增加的最低PHA浓度下,观察到K+周转率增加。因此,PHA使K+通透性增加,这与其促有丝分裂作用密切平行。因此,在芽殖和有丝分裂之前K+流入的迅速增加是维持正常细胞内K+浓度所必需的。足够的细胞内K+浓度对于细胞转化或分裂所需的合成过程至关重要。

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