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有证据表明外向整流性氯离子通道是心脏中容量调节性氯电流的基础。

Evidence that outwardly rectifying Cl- channels underlie volume-regulated Cl- currents in heart.

作者信息

Duan D, Hume J R, Nattel S

机构信息

Department of Pharmacology and Therapeutics, McGill University, Montreal, Canada.

出版信息

Circ Res. 1997 Jan;80(1):103-13. doi: 10.1161/01.res.80.1.103.

Abstract

Swelling-induced Cl- current (ICl.swell) is present in most cardiac tissues, but the unitary channel underlying ICls.well is unknown. We used the cell-attached patch-clamp technique to assess the properties of single channels underlying ICls.well and the basally active Cl- current (ICl.b) in rabbit atrial myocytes. Under isotonic conditions, single outwardly rectifying Cl- channels (ORCCs) with a slope conductance of 28 +/- 1 pS at the reversal potential were observed in 21 (5.7%) of 367 patches. Unconditional kinetic analysis revealed at least three open and four closed-channel states. Hypotonic superfusion-induced swelling resulted in the appearance of active channels in 41 (15.5%) of 265 patches without channel activity under isotonic conditions and caused a second active channel to appear in 3 of 14 patches showing a single channel under isotonic conditions. Overall, channels were seen in 54 of 336 patches under hypotonic conditions (16.1%, P < .001 versus isotonic conditions). The current-voltage relations, reversal potential-[Cl-]o relations, open probability, and kinetics of swelling-induced channels were indistinguishable from those of ORCCs under isotonic conditions. Unitary ORCCs, ICl.b, and ICl.swell were strongly and similarly inhibited by tamoxifen. Swelling-induced increases in macroscopic Cl- current were attributable to an increase in the number of active ORCCs with no significant effects on single-channel amplitude or open probability. Estimated macroscopic currents based on cell surface area, patch dimensions, single-channel ORCC current amplitude, open probability, and density were consistent with measured values of ICl.b and ICl.swell. We conclude that ORCCs underlie volume-regulated basal and swelling-induced Cl- currents in isolated rabbit atrial myocytes.

摘要

肿胀诱导的氯离子电流(ICl.swell)存在于大多数心脏组织中,但ICl.swell所对应的单通道情况尚不清楚。我们采用细胞贴附式膜片钳技术评估兔心房肌细胞中ICl.swell所对应的单通道特性以及基础活性氯离子电流(ICl.b)。在等渗条件下,在367个膜片中的21个(5.7%)观察到了单向外整流氯离子通道(ORCCs),其在反转电位下的斜率电导为28±1 pS。无条件动力学分析揭示了至少三个开放和四个关闭通道状态。低渗灌流诱导的肿胀导致在等渗条件下无通道活性的265个膜片中的41个(15.5%)出现活性通道,并使在等渗条件下显示单通道的14个膜片中的3个出现第二个活性通道。总体而言,在低渗条件下336个膜片中的54个观察到了通道(16.1%,与等渗条件相比P <.001)。肿胀诱导通道的电流 - 电压关系、反转电位 - [Cl-]o关系、开放概率和动力学与等渗条件下的ORCCs无法区分。单一的ORCCs、ICl.b和ICl.swell受到他莫昔芬的强烈且相似的抑制。肿胀诱导的宏观氯离子电流增加归因于活性ORCCs数量的增加,而对单通道幅度或开放概率无显著影响。基于细胞表面积、膜片尺寸、单通道ORCC电流幅度、开放概率和密度估计的宏观电流与ICl.b和ICl.swell的测量值一致。我们得出结论,ORCCs是分离的兔心房肌细胞中容量调节的基础和肿胀诱导的氯离子电流的基础。

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