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一种用于在时间和波长维度联合分析荧光发射的非参数方法。

A nonparametric method for analysis of fluorescence emission in combined time and wavelength dimensions.

作者信息

Ivanova Olga V, Marcu Laura, Khoo Michael C K

机构信息

Department of Biomedical Engineering, University of Southern California, Los Angeles, CA 90089, USA.

出版信息

Ann Biomed Eng. 2005 Apr;33(4):531-44. doi: 10.1007/s10439-005-2512-5.

Abstract

We report a method for accurate recovery of tissue intrinsic fluorescence emission characteristics, including fluorescence lifetimes and spectral profiles, from complex two-dimensional (spectro-temporal) emission waveforms. Most algorithms for analysis of fluorescence data address separately the characteristics of either spectral emission or fluorescence relaxation time. We developed a novel nonparametric analytical method that allows for identification and estimation of the intrinsic Fluorescent Impulse Response Kernel (FIRK) simultaneously in time and wavelength dimensions. Modeling of FIRK was based on the characteristics of spectro-temporal fluorescence waveforms. Due to the decaying behavior of the fluorescence, a linear combination of discrete Laguerre functions was used to model the fluorescence response in time. To address the large variability of spectral profiles of distinct fluorophores, a discrete Fourier series expansion was used to model the variation of fluorescence intensity across wavelength. The proposed method was validated on synthetic fluorescence data and data measured from fluorescence lifetime standards and tissue endogenous fluorescent biomolecules. We determined that this method provides a direct recovery of the two-dimensional FIRK and accurate estimation (residual error < 6%) of a broad range of fluorescence lifetimes including the sub-nanosecond range. The FIRK retrieved using this method can further facilitate modeling and recognition of pathological and physiological conditions in tissues.

摘要

我们报告了一种从复杂的二维(光谱-时间)发射波形中准确恢复组织固有荧光发射特性的方法,包括荧光寿命和光谱轮廓。大多数用于分析荧光数据的算法分别处理光谱发射或荧光弛豫时间的特性。我们开发了一种新颖的非参数分析方法,该方法允许在时间和波长维度上同时识别和估计固有荧光脉冲响应核(FIRK)。FIRK的建模基于光谱-时间荧光波形的特性。由于荧光的衰减行为,使用离散拉盖尔函数的线性组合来对时间上的荧光响应进行建模。为了解决不同荧光团光谱轮廓的巨大变异性,使用离散傅里叶级数展开来对荧光强度在波长上的变化进行建模。所提出的方法在合成荧光数据以及从荧光寿命标准品和组织内源性荧光生物分子测量的数据上得到了验证。我们确定该方法能够直接恢复二维FIRK,并能准确估计包括亚纳秒范围在内的广泛荧光寿命(残余误差<6%)。使用该方法检索到的FIRK可进一步促进对组织中病理和生理状况的建模与识别。

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