首页> 外文期刊>Nucleic Acids Research >What matters for lac repressor search in vivo-sliding, hopping, intersegment transfer, crowding on DNA or recognition?
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What matters for lac repressor search in vivo-sliding, hopping, intersegment transfer, crowding on DNA or recognition?

机译:对于紫胶阻遏物在体内滑动,跳跃,节间转移,DNA拥挤或识别的搜索有什么意义?

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We have investigated which aspects of transcription factor DNA interactions are most important to account for the recent in vivo search time measurements for the dimeric lac repressor. We find the best agreement for a sliding model where non-specific binding to DNA is improbable at first contact and the sliding LacI protein binds at high probability when reaching the specific O-sym operator. We also find that the contribution of hopping to the overall search speed is negligible although physically unavoidable. The parameters that give the best fit reveal sliding distances, including hopping, close to what has been proposed in the past, i.e. similar to 40 bp, but with an unexpectedly high 1D diffusion constant on non-specific DNA sequences. Including a mechanism of inter-segment transfer between distant DNA segments does not bring down the 1D diffusion to the expected fraction of the in vitro value. This suggests a mechanism where transcription factors can slide less hindered in vivo than what is given by a simple viscosity scaling argument or that a modification of the model is needed. For example, the estimated diffusion rate constant would be consistent with the expectation if parts of the chromosome, away from the operator site, were inaccessible for searching.
机译:我们已经调查了转录因子DNA相互作用的哪些方面对于解释二聚体lac阻遏物的最新体内搜索时间测量最重要。我们找到了一种滑动模型的最佳协议,在这种模型中,第一次接触时不可能与DNA发生非特异性结合,并且当到达特定的O-sym操纵子时,滑动LacI蛋白很可能结合。我们还发现,跳跳对整体搜索速度的贡献可以忽略不计,尽管这在物理上是不可避免的。提供最佳拟合的参数揭示了包括跳变在内的滑动距离,其接近于过去已经提出的距离,即类似于40bp,但是在非特异性DNA序列上具有出乎意料的高一维扩散常数。包括远距离DNA片段之间的片段间转移机制,不会使1D扩散降低到体外值的预期分数。这提示了一种机制,其中转录因子在体内的滑动受阻碍的程度要比简单的粘度缩放论证所给出的机制或需要对模型进行修改的机制要好。例如,如果染色体的远离操作者部位的部分无法进行搜索,则估计的扩散速率常数将与预期一致。

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