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应用时间分辨荧光光谱学对人类免疫缺陷病毒 1 型(HIV-1)的 rev 进行表征。

Characterization of human immunodeficiency virus-1 (HIV-1) rev by (time-resolved) fluorescence spectroscopy.

机构信息

Sandoz Research Institute, ART, Brunnerstrasse 59, A-1235, Vienna, Austria.

出版信息

J Fluoresc. 1994 Dec;4(4):299-302. doi: 10.1007/BF01881444.

Abstract

Fluorescence spectroscopy has been applied to the single tryptophan-containing regulatory protein Rev of human immunodeficiency virus (HIV-1). The fluorescence emission was found to have a maximum at 336 nm which refers to a surrounding of the chromophore of intermediate polarity. Fluorescence transients recorded at the maximum of fluorescence were found to decay nonexponentially. A bimodal lifetime distribution is obtained from exponential series analysis (ESM) with centers at 1.7 and 4.5 ns. Two microenvironments for tryptophan are suggested to be responsible for the two lifetime distributions. No innerfilter effect occurred in a Rev solution up to a concentration of 40 μM. A data quality study of ESM analysis as function of collected counts in the peak channel maximum (CIM) showed that, for reliable reconvolution, at least 15,000 CIM are necessary. The widths of the two distributions are shown to be temperature dependent. The broadening of the lifetime distributions when the temperature is raised to 50°C is interpreted as extension of the number of conformational substates which do not interconvert on the fluorescence time scale. The thermal deactivation (temperature quenching) is reflected in a constant decrease in the center of the short-lived lifetime distribution.

摘要

荧光光谱法已应用于人类免疫缺陷病毒(HIV-1)的单个色氨酸调节蛋白 Rev。发现荧光发射的最大值在 336nm 处,这表明发色团周围的极性为中等。在荧光最大值处记录的荧光瞬变被发现是非指数衰减的。通过指数序列分析(ESM)获得双峰寿命分布,中心位于 1.7 和 4.5ns。两个微环境负责色氨酸的两个寿命分布。在高达 40μM 的 Rev 溶液中没有发生内滤效应。ESM 分析的数据分析质量研究作为峰通道最大值(CIM)中收集的计数的函数,表明为了可靠的卷积,至少需要 15000 个 CIM。两个分布的宽度显示为温度依赖性。当温度升高到 50°C 时,寿命分布的展宽被解释为不在荧光时间尺度上相互转换的构象亚状态数量的增加。热失活(温度猝灭)反映在短寿命分布的中心常数下降。

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