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Swelling-Activated Anion Channels Are Essential for Volume Regulation of Mouse Thymocytes

Ranokhon Sh. KurbannazarovaDepartment of Biophysics, National University, Tashkent 100174, Vuzgorodok, UzbekistanS. V. BessonovaDepartment of Cell Physiology, National Institute for Physiological Sciences, Okazaki 444-8585, JapanYasunobu OkadaDepartment of Cell Physiology, National Institute for Physiological Sciences, Okazaki 444-8585, JapanRavshan Z. SabirovDepartment of Biophysics, National University, Tashkent 100174, Vuzgorodok, Uzbekistan
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Аннотация

Channel-mediated trans-membrane chloride movement is a key process in the active cell volume regulation under osmotic stress in most cells. However, thymocytes were hypothesized to regulate their volume by activating a coupled K-Cl cotransport mechanism. Under the patch-clamp, we found that osmotic swelling activates two types of macroscopic anion conductance with different voltage-dependence and pharmacology. At the single-channel level, we identified two types of events: one corresponded to the maxi-anion channel, and the other one had characteristics of the volume-sensitive outwardly rectifying (VSOR) chloride channel of intermediate conductance. A VSOR inhibitor, phloretin, significantly suppressed both macroscopic VSOR-type conductance and single-channel activity of intermediate amplitude. The maxi-anion channel activity was largely suppressed by Gd(3+) ions but not by phloretin. Surprisingly, [(dihydroindenyl)oxy] alkanoic acid (DIOA), a known antagonist of K-Cl cotransporter, was found to significantly suppress the activity of the VSOR-type single-channel events with no effect on the maxi-anion channels at 10 μM. The regulatory volume decrease (RVD) phase of cellular response to hypotonicity was mildly suppressed by Gd(3+) ions and was completely abolished by phloretin suggesting a major impact of the VSOR chloride channel and modulatory role of the maxi-anion channel. The inhibitory effect of DIOA was also strong, and, most likely, it occurred via blocking the VSOR Cl(-) channels.

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