Replacement of phenyl substituents at phosphorus by hexyl ones in 2-(2-hydroxyaryl)vinylphosphonium salts can tune the nature of the induced proton transport through lipid membranes

IF 2.8 3区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Tatyana I. Rokitskaya , Ljudmila S. Khailova , Anna G. Strelnik , Elena A. Kotova , Vladimir F. Mironov , Dmitry A. Tatarinov , Yuri N. Antonenko
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Abstract

2-(2-hydroxyaryl)vinylphosphonium salts are zwitterionic protonophores previously shown to induce proton transport across lipid membranes via cyclic deprotonation and protonation of the hydroxyl group. Here, we examine the impact of the kind of substituents at phosphorus on the protonophoric activity of these compounds. In particular, replacement of all the three phenyl groups at the phosphorus atom of the 2-(2-hydroxyaryl)vinyl(triphenyl)phosphonium salt (2HVPPh3) by hexyl chains (2HVPHex3) led to a tremendous increase in electric current induced by the phosphonium salt across planar bilayer lipid membranes (BLM). Remarkably, the BLM conductance quadratically increased with increasing 2HVPHex3 concentration, whereas a linear concentration dependence of the BLM current was observed for 2HVPPh3, 2HVPHexPh2 ((hexyl)diphenyl) and 2HVPHex2Ph ((dihexyl)phenyl), i.e., in the presence of at least one phenyl substituent at the phosphorus atom. Proton selectivity of the 2HVPHex3-induced electric current was close to perfect in membranes formed of diphytanylphosphatidylcholine with the decreased dipole potential, but rather low in membranes formed of the usual synthetic lipid – diphytanoylphosphatidylcholine. We hypothesize that the proton transport across BLM is carried out by 2HVPHex3 dimers. By contrast, the uncoupling activity of 2HVPHex3 in isolated rat liver mitochondria was observed at similar concentrations, as found for the compounds with phenyl substituents, thereby indicating that dimers do not play a key role in the uncoupling process. At the same time, the rate of 2HVPHex3-induced mitochondrial swelling under the deenergized conditions in potassium acetate medium, reflecting the protonophoric activity of the compound in mitochondria, significantly exceeded that for other compounds.

Abstract Image

在2-(2-羟乙基)乙烯基磷酸盐中用己基取代磷上的苯基取代基可以调节诱导质子通过脂质膜转运的性质
2-(2-羟酰基)乙烯基磷酸盐是两性离子质子载体,先前证明可以通过羟基的环去质子化和质子化诱导质子在脂质膜上的转运。在这里,我们研究了磷取代基的种类对这些化合物的亲质子活性的影响。特别是,2-(2-羟基)乙烯基(三苯基)磷盐(2HVPPh3)磷原子上的三个苯基被己基链(2HVPHex3)取代,导致磷盐在平面双层脂质膜(BLM)上产生的电流急剧增加。值得注意的是,随着2HVPHex3浓度的增加,BLM电导呈二次增长,而对于2HVPPh3、2HVPHexPh2((己基)二苯基)和2HVPHex2Ph((二己基)苯基),即在磷原子上存在至少一个苯基取代基时,BLM电流呈线性依赖关系。在偶极电势降低的二植烷酰磷脂酰胆碱膜中,2hvphex3诱导电流的质子选择性接近完美,而在通常的合成脂质-二植烷酰磷脂酰胆碱膜中,质子选择性较低。我们假设质子通过BLM的输运是由2HVPHex3二聚体进行的。相比之下,2HVPHex3在离体大鼠肝脏线粒体中具有相似浓度的解偶联活性,与苯基取代基化合物相似,这表明二聚体在解偶联过程中不起关键作用。同时,在醋酸钾培养基中失电条件下,2hvphex3诱导的线粒体肿胀率明显超过其他化合物,反映了该化合物在线粒体中的亲原活性。
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来源期刊
Biochimica et biophysica acta. Biomembranes
Biochimica et biophysica acta. Biomembranes 生物-生化与分子生物学
CiteScore
8.20
自引率
5.90%
发文量
175
审稿时长
2.3 months
期刊介绍: BBA Biomembranes has its main focus on membrane structure, function and biomolecular organization, membrane proteins, receptors, channels and anchors, fluidity and composition, model membranes and liposomes, membrane surface studies and ligand interactions, transport studies, and membrane dynamics.
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