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Interaction of a mitochondrial presequence with lipid membranes: Role of helix formation for membrane binding and perturbation

机译:线粒体序列与脂质膜的相互作用:螺旋形成对膜结合和微扰的作用

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摘要

The binding of a peptide to a biological membrane is often accompanied by a transition from a random coil structure to an amphipathic cr-helix. Recently, we have presented a new approach which allows the determination of the thermodynamic parameters of membrane-induced helix formation [Wieprecht et al. (1999) J. Mol Biol. 294, 785]. It involves a systematic variation of the helix content of a given peptide by double D-substitution and a correlation of the binding parameters with the helicity: Here we have used this method to study membrane-induced helix formation for the presequence of rat mitochondrial rhodanese (RHD). The thermodynamic parameters of binding of the peptide RHD and of four of its double D-isomers were determined for 30 nm (SUVs) and 100 nm (LUVs) unilamellar vesicles composed of phosphatidylcholine/phosphatidylglycerol (3:1) using circular dichroism spectroscopy, fluorescence spectroscopy, and isothermal titration calorimetry. The incremental changes of the thermodynamic parameters of helix formation were found to be very similar for SUVs and LUVs. Membrane-induced helix formation of RHD entailed a negative enthalpy of DeltaH(helix) = -0.5 to -0.6 kcal/ mol/residue and was opposed by an entropy of about DeltaS(helix) = -1 to -1.4 cal/mol K/residue. The free energy of helix formation, DeltaG(helix), was about -0.2 kcal/mol, and helix formation accounted for 50-60% of the total free energy of membrane binding. Dye-release experiments were used to assess the role of helix formation for the membrane perturbation potential of the peptides. While helix formation plays a major role for membrane binding, it appears to have little importance for inducing membrane leakiness. [References: 45]
机译:肽与生物膜的结合通常伴随着从无规卷曲结构到两亲性cr-螺旋的转变。最近,我们提出了一种新方法,该方法可以确定膜诱导的螺旋形成的热力学参数[Wieprecht等。 (1999)J.Mol Biol。 294,785]。它涉及通过双D取代系统改变给定肽的螺旋含量,以及结合参数与螺旋度之间的相关性:在这里,我们已经使用此方法研究了膜诱导的螺旋形成,用于大鼠线粒体若丹松的先后顺序( RHD)。使用圆二色光谱,荧光法测定了30 nm(SUVs)和100 nm(LUVs)由磷脂酰胆碱/磷脂酰甘油(3:1)组成的单层囊泡中肽RHD及其四个双D异构体结合的热力学参数光谱和等温滴定热法。发现对于SUV和LUV,螺旋形成的热力学参数的增量变化非常相似。 RHD的膜诱导螺旋形成需要ΔH(螺旋)= -0.5至-0.6 kcal / mol /残基的负焓,并且被约DeltaS(螺旋)= -1至-1.4 cal / mol K /的熵所抵消。残留物。螺旋形成的自由能DeltaG(螺旋)约为-0.2kcal / mol,螺旋形成占膜结合总自由能的50-60%。染料释放实验用于评估螺旋形成对肽膜扰动潜力的作用。虽然螺旋的形成在膜结合中起主要作用,但对于诱导膜渗漏似乎并不重要。 [参考:45]

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