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The enthalpy of the alanine peptide helix measured by isothermal titration calorimetry using metal-binding to induce helix formation

机译:用金属结合诱导螺旋形成的等温滴定热法测量丙氨酸肽螺旋的焓

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摘要

The goal of this study is to use the model system described earlier to make direct measurements of the enthalpy of helix formation at different temperatures. For this we studied model alanine peptides in which helix formation can be triggered by metal (La3+) binding. The heat of La3+ interaction with the peptides at different temperatures is measured by isothermal titration calorimetry. Circular dichroism spectroscopy is used to follow helix formation. Peptides of increasing length (12-, 16-, and 19-aa residues) that contain a La3+-binding loop followed by helices of increasing length, are used to separate the heat of metal binding from the enthalpy of helix formation. We demonstrate that (i) the enthalpy of helix formation is −0.9 ± 0.1 kcal/mol; (ii) the enthalpy of helix formation is independent of the peptide length; (iii) the enthalpy of helix formation does not depend significantly on temperature in the range from 5 to 45°C, suggesting that the heat capacity change on helix formation is very small. Thus, the use of metal binding to induce helix formation has an enormous potential for measuring various thermodynamic properties of α-helices.
机译:这项研究的目的是使用前面描述的模型系统直接测量不同温度下螺旋形成的焓。为此,我们研究了模型丙氨酸肽,其中可以通过金属(La 3 + )结合触发螺旋形成。通过等温滴定量热法测定La 3 + 在不同温度下与多肽相互作用的热量。圆二色光谱用于追踪螺旋的形成。包含La 3 + 结合环的长度增加的肽段(12、16、19和19-aa残基)和随后增加长度的螺旋用于分离金属结合热和螺旋形成的焓。我们证明(i)螺旋形成的焓为-0.9±0.1 kcal / mol; (ii)螺旋形成的焓与肽长度无关; (iii)螺旋形成的焓在5至45℃的范围内不显着依赖于温度,这表明螺旋形成时的热容变化很小。因此,使用金属结合来诱导螺旋形成具有用于测量α-螺旋的各种热力学性质的巨大潜力。

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