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激光诱导自体荧光在医学诊断中的应用。

Laser-induced autofluorescence for medical diagnosis.

机构信息

Institute of Lasertechnology in Medicine, Ulm, Germany.

出版信息

J Fluoresc. 1994 Mar;4(1):17-40. doi: 10.1007/BF01876650.

Abstract

The naturally occurring autofluorescence of cells and tissues is based on biomolecules containing intrinsic fluorophores, such as porphyrins, the amino acids tryptophan and tyrosine, and the coenzymes NADH, NADPH, and flavins. Coenzymes fluoresce in the blue/green spectral region (fluorecence lifetimes: 0.5-6 ns) and are highly sensitive indicators of metabolic function. Steadystate and time-resolved blue-green autofluorescence is, therefore, an appropriate measure of the function of the respiratory chain as well as of cellular and tissue damage. Autofluorescence in the yellow/red spectral region is based mainly on endogenous porphyrins and metalloporphyrins, such as coproporphyrin, protoporphyrin (fluorescence lifetime of porphyrin monomers: >10 ns), and Zn-protoporphyrin (2 ns). Various pathological microorganisms such asPropionibacterium acnes, Pseudomonas aeruginosa, Actinomyces odontolyticus, Bacteroides intermedius, andSaccharomyces cerevisiae are able to synthesize large amounts of these fluorophores and can therefore be located. This permits fluorescence-based detection of a variety of diseases, including early-stage dental caries, dental plaque, acne vulgaris, otitis externa, and squamous cell carcinoma. The sensitivity of noninvasive autofluorescence diagnostics can be enhanced by time-gated fluorescence measurements using an appropriate time delay between ultrashort laser excitation and detection. For example, videocameras with ultrafast shutters, in the nanosecond region, can be used to create "caries images" of the teeth. Alternatively, autofluorescence can be enhanced by stimulating protoporphyrin biosynthesis with the exogenously administered porphyrin precursor 5-aminolevulinic acid (ALA). The fluorophore protoporphyrin IX (PP IX) is photolabile and photodynamically active. Irradiation of PP IX-containing tissue results in cytotoxic reactions which correlate with modifications in fluorescence due to photobleaching and singlet oxygen-dependent photoproduct formation. Therefore, on-line autofluorescence measurements during the phototreatment can yield information on the efficiency of ALA-based photodynamic therapy.

摘要

细胞和组织的自发荧光基于含有内源性荧光团的生物分子,如卟啉、色氨酸和酪氨酸等氨基酸以及 NADH、NADPH 和黄素等辅酶。辅酶在蓝/绿光区(荧光寿命:0.5-6ns)内荧光,是代谢功能的高度敏感指标。因此,稳态和时间分辨的蓝绿光自发荧光是呼吸链功能以及细胞和组织损伤的适当测量方法。基于内源性卟啉和金属卟啉(如粪卟啉、原卟啉(卟啉单体荧光寿命:>10ns)和 Zn-原卟啉(2ns))的黄/红光区自发荧光主要基于内源性卟啉和金属卟啉(如粪卟啉、原卟啉(卟啉单体荧光寿命:>10ns)和 Zn-原卟啉(2ns))。各种病理微生物,如痤疮丙酸杆菌、铜绿假单胞菌、解糖放线菌、中间型拟杆菌和酿酒酵母,能够大量合成这些荧光团,因此可以定位。这使得能够基于荧光检测多种疾病,包括早期龋齿、牙菌斑、寻常痤疮、外耳炎和鳞状细胞癌。通过使用适当的超短激光激发和检测之间的时间延迟来进行时间门控荧光测量,可以增强非侵入性自发荧光诊断的灵敏度。例如,可以使用纳秒级超快快门的摄像机来创建牙齿的“龋齿图像”。或者,可以通过用外源性卟啉前体 5-氨基酮戊酸(ALA)刺激原卟啉生物合成来增强自发荧光。荧光团原卟啉 IX(PP IX)是光不稳定的并且光动力活跃的。含有 PP IX 的组织的辐照会导致细胞毒性反应,这些反应与由于光漂白和单线态氧依赖性光产物形成而导致的荧光变化相关。因此,在光治疗过程中进行在线自发荧光测量可以提供有关基于 ALA 的光动力疗法效率的信息。

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