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LSm4与质膜相关联,并在细胞体积调节中作为辅助因子发挥作用。

LSm4 associates with the plasma membrane and acts as a co-factor in cell volume regulation.

作者信息

Gandini Rosaria, Dossena Silvia, Vezzoli Valeria, Tamplenizza Margherita, Salvioni Elisabetta, Ritter Markus, Paulmichl Markus, Furst Johannes

机构信息

Department of Physiology and Medical Physics, Division of Physiology, Innsbruck Medical University, Innsbruck, Austria.

出版信息

Cell Physiol Biochem. 2008;22(5-6):579-90. doi: 10.1159/000185542. Epub 2008 Dec 9.

Abstract

ICln is a ubiquitous, multifunctional protein with functions in cell volume regulation and RNA processing, and is thus part of an intricate protein network critically involved in the homoeostasis of cells. To better understand this vital protein network in health and disease it is fundamental to characterize the interactions between the physiological pathways in which ICln is involved, as well as the spatio-temporal regulation of these interactions. In this study, we focused on the interaction between the two best studied pathways in which ICln is involved--regulatory volume decrease and RNA processing--and asked, whether or not the RNA processing factor and ICln interaction partner LSm4 may also have a function in cell volume regulation in NIH3T3 fibroblasts or HEK293 Phoenix cells. To address this question, we studied in isotonic and hypotonic conditions by FRET, biochemistry and electrophysiology, the intracellular distribution of the RNA processing factor LSm4, its interaction with ICln, as well as the involvement of LSm4 in the activation of the swelling dependent anion and osmolyte channel IClswell. In isotonic conditions, LSm4 associates with ICln, and the plasma membrane. Hypotonic cell swelling leads to the dissociation of LSm4 from the plasma membrane, and from ICln. Over-expression of LSm4 affects the translocation of ICln to the cell membrane and markedly inhibits the activation kinetics and current density of IClswell. These findings indicate that LSm4 not only acts in RNA processing, but also as a co-factor in cell volume regulation.

摘要

ICln是一种普遍存在的多功能蛋白质,在细胞容积调节和RNA加工中发挥作用,因此是一个复杂蛋白质网络的一部分,该网络对细胞的稳态至关重要。为了更好地理解健康和疾病状态下这个重要的蛋白质网络,表征ICln所涉及的生理途径之间的相互作用以及这些相互作用的时空调节至关重要。在本研究中,我们聚焦于ICln所涉及的两个研究最为深入的途径——调节性容积减小和RNA加工——之间的相互作用,并探究RNA加工因子以及ICln相互作用伴侣LSm4是否也在NIH3T3成纤维细胞或HEK293 Phoenix细胞的细胞容积调节中发挥作用。为解决这个问题,我们通过荧光共振能量转移(FRET)、生物化学和电生理学方法,在等渗和低渗条件下研究了RNA加工因子LSm4的细胞内分布、它与ICln的相互作用,以及LSm4在肿胀依赖性阴离子和渗透溶质通道IClswell激活中的作用。在等渗条件下,LSm4与ICln以及质膜结合。低渗性细胞肿胀导致LSm4从质膜和ICln上解离。LSm4的过表达影响ICln向细胞膜的转位,并显著抑制IClswell的激活动力学和电流密度。这些发现表明,LSm4不仅在RNA加工中发挥作用,还作为细胞容积调节的辅助因子。

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