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SEQUENCE-SPECIFIC DNA-BINDING DOMINATED BY DEHYDRATION

机译:脱水特异性测序的DNA结合

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qFluorescence spectroscopy and isothermal titration calorimetry were used to study the thermodynamics of binding of the glucocorticoid receptor DNA-binding domain to four different, but similar, DNA-binding sites. The binding sites are two naturally occurring sites that differ in the composition of one base pair, i.e., A . T to G . C mutation, and two sites containing chemical intermediates of these base pairs. The calorimetrically determined heat capacity change (Delta C-p degrees(obs)) for glucocorticoid receptor DNA-binding domain binding agrees with that calculated for dehydration or solvent-accessible surface areas. A dominating effect of dehydration or solvent reorganization on the thermodynamics is also consistent with an observed linear relationship between observed enthalpy change (Delta H degrees(obs)) and observed entropy change (Delta S degrees(obs)) with a slope close to the experimental temperature. Comparisons with structural data allow us to rationalize individual differences between Delta H degrees(obs) (and Delta S degrees(obs)) for the four complexes. For instance, we find that the removal of a methyl group at the DNA-protein interface is enthalpically favorable but entropically unfavorable, which is consistent with a replacement by an ordered water molecule. [References: 34]
机译:q荧光光谱法和等温滴定热法用于研究糖皮质激素受体DNA结合结构域与四个不同但相似的DNA结合位点结合的热力学。结合位点是两个天然存在的位点,它们在一个碱基对即A 1的组成上不同。 T到G。 C突变,两个位点包含这些碱基对的化学中间体。量热法确定的糖皮质激素受体DNA结合结构域结合的热容变化(ΔC-p度(obs))与针对脱水或溶剂可及表面积计算得出的热容变化一致。脱水或溶剂重组对热力学的主导作用还与观察到的焓变(ΔH度(obs))和观察到的熵变(ΔS度(obs))之间的线性关系一致,且斜率接近实验值温度。与结构数据的比较使我们能够合理化四个复合物的Delta H度(obs)(和Delta S度(obs))之间的个体差异。例如,我们发现在DNA-蛋白质界面处去除甲基在焓上是有利的,但在熵上是不利的,这与被有序的水分子替代是一致的。 [参考:34]

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