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通过傅里叶变换红外光谱法进行胶原类型分析与鉴别

Collagen types analysis and differentiation by FTIR spectroscopy.

作者信息

Belbachir Karima, Noreen Razia, Gouspillou Gilles, Petibois Cyril

机构信息

Université Victor Segalen Bordeaux 2, 146 rue Léo Saignat, 33076, Bordeaux-Cedex, France.

出版信息

Anal Bioanal Chem. 2009 Oct;395(3):829-37. doi: 10.1007/s00216-009-3019-y. Epub 2009 Aug 16.

DOI:10.1007/s00216-009-3019-y
PMID:19685340
Abstract

Abnormal formation and organization of collagen network is commonly observed in many organ pathologies, but analytical techniques able to reveal the collagen biodistribution are still lacking. In this study, Fourier-transform infrared (FTIR) spectroscopy has been used to analyze type I, III, IV, V, and VI collagens, the most important compounds of connective tissues. A robust classification of 30 FTIR spectra per collagen type could be obtained by using a combination of four spectral intervals [nu(C=O) absorption of amide I (1,700-1,600 cm(-1)), delta(CH(2)), and delta(CH(3)) absorptions (1,480-1,350 cm(-1)), nu(C-N), and delta(N-H) absorptions of amide III (1,300-1,180 cm(-1)), and nu(C-O) and nu(C-O-C) absorptions of carbohydrate moieties (1,100-1,005 cm(-1))]. Then, a submolecular justification of this classification model was sought using a curve fitting analysis of the four spectral intervals. Results demonstrated that every spectral interval used for the classification contained highly discriminant absorption bands between all collagen types (multivariate analysis of variance, p < 0.01; Dunnett's T3 post hoc test, p < 0.05). All conditions seem thus joined to make FTIR spectroscopy and imaging major tools for implementing innovative methods in the field of molecular histology, which would be very helpful for the diagnosis of a wide range of pathologies.

摘要

在许多器官病变中,常可观察到胶原网络的异常形成和组织紊乱,但仍缺乏能够揭示胶原生物分布的分析技术。在本研究中,傅里叶变换红外(FTIR)光谱已被用于分析I型、III型、IV型、V型和VI型胶原,这些是结缔组织中最重要的化合物。通过使用四个光谱区间的组合[酰胺I的ν(C=O)吸收(1700 - 1600 cm⁻¹)、δ(CH₂)和δ(CH₃)吸收(1480 - 1350 cm⁻¹)、酰胺III的ν(C - N)和δ(N - H)吸收(1300 - 1180 cm⁻¹)以及碳水化合物部分的ν(C - O)和ν(C - O - C)吸收(1100 - 1005 cm⁻¹)],可以对每种胶原类型的30个FTIR光谱进行可靠分类。然后,通过对这四个光谱区间进行曲线拟合分析,寻求该分类模型的亚分子依据。结果表明,用于分类的每个光谱区间在所有胶原类型之间都包含高度判别性的吸收带(多变量方差分析,p < 0.01;Dunnett's T3事后检验,p < 0.05)。因此,所有条件似乎都表明FTIR光谱和成像将成为在分子组织学领域实施创新方法的主要工具,这对多种病变的诊断非常有帮助。

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