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多柔比星对MDR1/P-糖蛋白的选择降低了MES-SA细胞中肿胀激活的钾离子和氯离子电流。

Doxorubicin selection for MDR1/P-glycoprotein reduces swelling-activated K+ and Cl- currents in MES-SA cells.

作者信息

Luckie D B, Krouse M E, Law T C, Sikic B I, Wine J J

机构信息

Cystic Fibrosis Research Laboratory, Stanford University, California 94305, USA.

出版信息

Am J Physiol. 1996 Apr;270(4 Pt 1):C1029-36. doi: 10.1152/ajpcell.1996.270.4.C1029.

Abstract

To test the hypothesis that P-glycoprotein enhances swelling currents through regulation of volume-sensitive Cl- channels [recently termed VSOAC (volume-sensitive osmolyte and anion channel)], a human uterine sarcoma cell line (MES-SA) and its doxorubicin-selected counterpart (Dx5) were studied. P-glycoprotein mRNA and protein levels were detected only in Dx5 cells. However, whole cell patch-clamp experiments showed that swollen Dx5 cells (n = 5) produced smaller VSOAC currents than MES-SA cells (n = 4; 106 +/- 26 pA/pF vs. 232 +/- 76 pA/pF at 90 mV). In radioisotopic efflux experiments, both swelling-activated 125I (Cl-) currents (n = 15) and 86Rb (K+) currents (n = 8) were found to be two-to fourfold smaller in the Dx5 (high P-glycoprotein) cells. Inhibitors of P-glycoprotein showed no specificity for the doxorubicin-selected cells (Dx5). Dideoxyforskolin (100 microM) blocked swelling-activated 125I efflux equally in both cell lines, whereas 100 microM verapamil had no effect. Thus, in this cell line, selection for P-glycoprotein expression is associated with reduced swelling currents. These findings suggest that P-glycoprotein expression does not directly facilitate VSOAC.

摘要

为了验证P-糖蛋白通过调节容积敏感性氯离子通道(最近称为VSOAC,即容积敏感性渗透物和阴离子通道)增强肿胀电流这一假说,对一种人子宫肉瘤细胞系(MES-SA)及其经阿霉素筛选的对应细胞系(Dx5)进行了研究。仅在Dx5细胞中检测到P-糖蛋白的mRNA和蛋白水平。然而,全细胞膜片钳实验表明,肿胀的Dx5细胞(n = 5)产生的VSOAC电流比MES-SA细胞(n = 4;在90 mV时为106±26 pA/pF对232±76 pA/pF)小。在放射性同位素外流实验中,发现肿胀激活的125I(Cl-)电流(n = 15)和86Rb(K+)电流(n = 8)在Dx5(高P-糖蛋白)细胞中均小两到四倍。P-糖蛋白抑制剂对经阿霉素筛选的细胞(Dx5)没有特异性。双脱氧福司可林(100 μM)在两种细胞系中均同等程度地阻断肿胀激活的125I外流,而100 μM维拉帕米则无作用。因此,在该细胞系中,对P-糖蛋白表达的选择与肿胀电流降低相关。这些发现表明,P-糖蛋白的表达并不直接促进VSOAC。

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