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利用四环素染色荧光寿命成像显微镜观察视网膜色素上皮下羟磷灰石沉积。

Imaging hydroxyapatite in sub-retinal pigment epithelial deposits by fluorescence lifetime imaging microscopy with tetracycline staining.

机构信息

University of Maryland School of Medicine, Department of Biochemistry and Molecular Biology, Baltimo, United States.

Coppin State University, Department of Natural Sciences, Baltimore, United States.

出版信息

J Biomed Opt. 2020 Apr;25(4):1-11. doi: 10.1117/1.JBO.25.4.047001.

Abstract

SIGNIFICANCE

Recent evidence suggests that hydroxyapatite (HAP) in sub-retinal pigment epithelial (sub-RPE) deposits in aged human eyes may act to nucleate and contribute to their growth to clinically detectable size. Sub-RPE deposits such as drusen are clinical hallmarks of age-related macular degeneration (AMD), therefore enhanced and earlier detection is a clinical need. We found that tetracycline-family antibiotics, long known to stain HAP in teeth and bones, can also label the HAP in sub-RPE deposits. However, HAP-bound tetracycline fluorescence excitation and emission spectra overlap with the well-known autofluorescence of outer retinal tissues, making them difficult to resolve.

AIM

In this initial study, we sought to determine if the HAP-bound tetracyclines also exhibit enhanced fluorescence lifetimes, providing a useful difference in lifetime compared with the short lifetimes observed in vivo in the human retina by the pioneering work of Schweitzer, Zinkernagel, Hammer, and their colleagues, and thus a large enough effect size to resolve the HAP from background by fluorescence lifetime imaging.

APPROACH

We stained authentic HAP with tetracyclines and measured the lifetime(s) by phase fluorometry, and stained aged, fixed human cadaver retinas with drusen with selected tetracyclines and imaged them by fluorescence lifetime imaging microscopy (FLIM).

RESULTS

We found that chlortetracycline and doxycycline exhibited substantial increase in fluorescence lifetime compared to the free antibiotics and the retinal background, and the drusen were easily resolvable from the retinal background in these specimens by FLIM.

CONCLUSIONS

These findings suggest that FLIM imaging of tetracycline (and potentially other molecules) binding to HAP could become a diagnostic tool for the development and progression of AMD.

摘要

意义

最近的证据表明,老年人类眼睛的视网膜色素上皮下(sub-RPE)沉积物中的羟基磷灰石(HAP)可能起到成核作用,并促进其生长到可临床检测到的大小。sub-RPE 沉积物如玻璃膜疣是年龄相关性黄斑变性(AMD)的临床标志,因此增强和早期检测是临床需求。我们发现,四环素类抗生素长期以来已知可使牙齿和骨骼中的 HAP 染色,也可以标记 sub-RPE 沉积物中的 HAP。然而,HAP 结合的四环素荧光激发和发射光谱与外视网膜组织的已知自发荧光重叠,使得它们难以分辨。

目的

在这项初步研究中,我们试图确定 HAP 结合的四环素是否也表现出增强的荧光寿命,与 Schweitzer、Zinkernagel、Hammer 及其同事的开创性工作中在体内观察到的人类视网膜的短寿命相比,提供了有用的寿命差异,从而通过荧光寿命成像提供足够大的效应量来从背景中分辨 HAP。

方法

我们用四环素对真实的 HAP 进行染色,并通过相位荧光法测量寿命,并选择四环素对老年固定的人类尸体视网膜中的玻璃膜疣进行染色,并通过荧光寿命成像显微镜(FLIM)对其进行成像。

结果

我们发现金霉素和强力霉素与游离抗生素和视网膜背景相比,荧光寿命有显著增加,并且在这些标本中,FLIM 很容易将玻璃膜疣与视网膜背景区分开来。

结论

这些发现表明,FLIM 对四环素(和潜在的其他分子)与 HAP 结合的成像可能成为 AMD 发展和进展的诊断工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/74f3/7171513/4cc29161496a/JBO-025-047001-g001.jpg

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