连接蛋白通道纳米孔结构和功能研究的生物物理方法

M. Bortolozzi, F. Mammano
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摘要

目的:连接蛋白是一种跨膜蛋白,在脊椎动物中形成细胞间连接通道,已知或怀疑参与多种生物过程,包括心脏发育和功能、听力、造血、再生、晶状体透明性、生育、免疫系统功能和氧化应激保护。连接蛋白突变可引起发育和生理缺陷,并与多种疾病有关。特别是,cAMP或肌醇-1,4,5-三磷酸(InsP3)通过连接蛋白通道的渗透缺陷分别与周围神经病变和耳聋有关。本文提出了一种估算单间隙结通道对第二信使的磁导率的方法。研究设计:以过表达野生型人连接蛋白26 (HCx26wt)的HeLa细胞为模型系统,结合对cAMP和InsP3选择性生物传感器的结导和荧光共振能量转移(FRET)发射比的测量。结果:对cAMP(47±15 × 10-3 μm3/s)和InsP3(60±12 × 10-3 μm3/s)的单一渗透率相似,但明显大于对路西法黄(LY;7±3 × 10-3 μm3/s),外源示踪剂。结论:该方法可以量化代谢偶联的缺陷,并可用于研究不同信号通路之间细胞间扩散和串扰的相互依赖性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A biophysical approach to the study of structure and function of connexin channel nanopores
Abstract Objective: Connexins are transmembrane proteins that form intercellular junctional channels in vertebrates and are known or suspected to be involved in a wide variety of biological processes including cardiac development and function, hearing, haematopoesis, regeneration, lens transparency, fertility, immune system function and protection from oxidative stress. Connexin mutations can cause developmental and physiological defects, and link to various diseases. In particular, defective permeation of cAMP or inositol-1,4,5-trisphosphate (InsP3) through connexin channels is associated with peripheral neuropathies and deafness, respectively. Here we present a method to estimate the permeability of single-gap junction channels to second messengers. Study design: Using HeLa cells that overexpressed wild-type human connexin 26 (HCx26wt) as a model system, we combined measurements of junctional conductance and fluorescence resonance energy transfer (FRET) emission ratio of biosensors selective for cAMP and InsP3. Results: The unitary permeabilities to cAMP (47 ± 15 × 10–3 μm3/s) and InsP3 (60 ± 12 × 10–3 μm3/s) were similar, but substantially larger than the unitary permeability to Lucifer Yellow (LY; 7 ± 3 × 10–3 μm3/s), an exogenous tracer. Conclusion: This method permits quantification of defects of metabolic coupling and can be used to investigate interdependence of intercellular diffusion and cross-talk between diverse signalling pathways.
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