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蛋白质荧光衰减:离散成分还是寿命分布?真的无法摆脱困境吗?

Protein fluorescence decay: discrete components or distribution of lifetimes? Really no way out of the dilemma?

作者信息

Vix A, Lami H

机构信息

Laboratoire de Physique, Université Louis Pasteur, Illkirch, France.

出版信息

Biophys J. 1995 Mar;68(3):1145-51. doi: 10.1016/S0006-3495(95)80290-0.

Abstract

A new methodology of fluorescence decay analysis by iterative reconvolution is presented. It is based on the recent finding that the statistics of single-photon time-correlated data are best described by a compound Poisson law and requires the recording of a sample of at least 20 decays. Application of multivariate statistical methods to the analysis of the recovered decay parameters results in improved accuracy and better estimation of the uncertainties of mono- and multiexponential decays. If it is, of course, not possible to distinguish unambiguously between discrete components and a continuous distribution of lifetimes, it is, however, possible to determine a higher limit of the width of such a distribution should it be present. With our methodology, the presence of a distribution of lifetimes with a width of approximately 20% of its center value inevitably leads to a failure in the deconvolution procedure, a fact of crucial importance in protein conformational studies, for example.

摘要

本文提出了一种通过迭代反卷积进行荧光衰减分析的新方法。该方法基于最近的一项发现,即单光子时间相关数据的统计特性最好用复合泊松定律来描述,并且需要记录至少20次衰减的样本。将多元统计方法应用于对恢复的衰减参数的分析,可提高单指数和多指数衰减的不确定性估计的准确性和精度。当然,如果无法明确区分离散成分和寿命的连续分布,那么如果存在这样的分布,就有可能确定其宽度的上限。使用我们的方法,例如在蛋白质构象研究中,寿命分布的宽度约为其中心值的20%时,必然会导致反卷积过程失败,这一事实至关重要。

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