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使用拉曼微光谱研究人类细胞系中的化学固定效应。

Studies of chemical fixation effects in human cell lines using Raman microspectroscopy.

机构信息

School of Physics, Dublin Institute of Technology, Kevin Street, Dublin, Ireland.

出版信息

Anal Bioanal Chem. 2010 Mar;396(5):1781-91. doi: 10.1007/s00216-009-3411-7. Epub 2010 Jan 20.

Abstract

The in vitro study of cellular species using Raman spectroscopy has proven a powerful non-invasive modality for the analysis of cell constituents and processes. This work uses micro-Raman spectroscopy to study the chemical fixation mechanism in three human cell lines (normal skin, normal bronchial epithelium, and lung adenocarcinoma) employing fixatives that preferentially preserve proteins (formalin), and nucleic acids (Carnoy's fixative and methanol-acetic acid). Spectral differences between the mean live cell spectra and fixed cell spectra together with principal components analysis (PCA), and clustering techniques were used to analyse and interpret the spectral changes. The results indicate that fixation in formalin produces spectral content that is closest to that in the live cell and by extension, best preserves the cellular integrity. Nucleic acid degradation, protein denaturation, and lipid leaching were observed with all fixatives and for all cell lines, but to varying degrees. The results presented here suggest that the mechanism of fixation for short fixation times is complex and dependent on both the cell line and fixative employed. Moreover, important spectral changes occur with all fixatives that have consequences for the interpretation of biochemical processes within fixed cells. The study further demonstrates the potential of vibrational spectroscopy in the characterization of complex biochemical processes in cells at a molecular level.

摘要

使用拉曼光谱对细胞种类进行的体外研究已被证明是分析细胞成分和过程的一种强大的非侵入性方法。本工作使用微拉曼光谱研究了三种人类细胞系(正常皮肤、正常支气管上皮和肺腺癌)的化学固定机制,使用优先保存蛋白质(福尔马林)和核酸(卡诺氏固定剂和甲醇-乙酸)的固定剂。活细胞光谱和固定细胞光谱之间的平均光谱差异以及主成分分析(PCA)和聚类技术用于分析和解释光谱变化。结果表明,福尔马林固定产生的光谱内容最接近活细胞的光谱,因此可以最好地保持细胞完整性。所有固定剂和所有细胞系都观察到核酸降解、蛋白质变性和脂质浸出,但程度不同。这里提出的结果表明,短时间固定的固定机制很复杂,取决于所使用的细胞系和固定剂。此外,所有固定剂都会发生重要的光谱变化,这对固定细胞内生化过程的解释有影响。该研究进一步证明了振动光谱在细胞内复杂生化过程的分子水平表征中的潜力。

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