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Determining Two-Photon Absorption Cross Sections via Non-resonant Multiphoton Photoacoustic Spectroscopy

机译:通过非共振多光子光声光谱法确定两个光子的吸收截面

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摘要

Multiphoton excitation of exogenous dyes and endogenous biochemical species has been used extensively for tissue diagnosis by fluorescence spectroscopy. Unfortunately, the majority of endogenous biochemical chromophores have low quantum yields, less than 0.2, therefore determining two-photon cross sections of weakly luminescencing molecules is difficult using two-photon fluorescence spectroscopy. Accurate determination of two-photon cross sections of these biochemicals could provide insight into fluorescence signal reduction caused by the absorption of excitation energy by non-target intracellular species. Non-resonant multiphoton photoacoustic spectroscopy (NMPPAS) is a novel technique we have developed for condensed matter measurements that has the potential for accurately determining two-photon absorption cross-sections of chemicals with small or non-existant fluorescence quantum yields. In this technique, near infrared light is used to generate an ultrasonic signal following a non-resonant two-photon excitation process. This ultrasonic wave is directly related to the non-radative relaxation of the chromophore of interest and is measured using a contact piezoelectric ultrasonic transducer. The signal from the ultrasonic transducer can then be used to calculate two-photon absorption cross sections. This paper will describe the validation of this technique by measuring the two-photon absorption cross-sections of well characterized chromophores such as rhodamine B and coumarin 1 in solution as well as riboflavin in a gelatin tissue phantom.
机译:外源性染料和内源性生化物种的多光子激发已广泛用于通过荧光光谱进行组织诊断。不幸的是,大多数内源生化生色团的量子产率很低,小于0.2,因此使用双光子荧光光谱法很难确定弱发光分子的双光子截面。准确测定这些生物化学物质的两个光子截面可以深入了解由非靶细胞内物质吸收激发能引起的荧光信号减少。非共振多光子光声光谱法(NMPPAS)是我们为凝结物测量开发的一种新技术,具有准确确定具有较小或不存在荧光量子产率的化学物质的双光子吸收截面的潜力。在该技术中,在非谐振双光子激发过程之后,近红外光用于生成超声信号。该超声波与感兴趣的生色团的非辐射弛豫直接相关,并使用接触式压电超声换能器进行测量。然后可以将来自超声换能器的信号用于计算双光子吸收截面。本文将通过测量溶液中特征明确的生色团(如若丹明B和香豆素1)以及明胶组织模型中的核黄素的双光子吸收截面来描述该技术的有效性。

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