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去除嵌入组织中的最佳切割温度(O.C.T.)复合物,用于 MALDI 成像脂质。

Removal of optimal cutting temperature (O.C.T.) compound from embedded tissue for MALDI imaging of lipids.

机构信息

South Australian Health and Medical Research Institute (SAHMRI), North Terrace, Adelaide, South Australia, 5000, Australia.

The University of Adelaide Medical School, North Terrace, Adelaide, South Australia, 5005, Australia.

出版信息

Anal Bioanal Chem. 2021 Apr;413(10):2695-2708. doi: 10.1007/s00216-020-03128-z. Epub 2021 Feb 9.

Abstract

Matrix-assisted laser desorption/ionisation mass spectrometry imaging (MALDI-MSI) is a common molecular imaging modality used to characterise the abundance and spatial distribution of lipids in situ. There are several technical challenges predominantly involving sample pre-treatment and preparation which have complicated the analysis of clinical tissues by MALDI-MSI. Firstly, the common embedding of samples in optimal cutting temperature (O.C.T.), which contains high concentrations of polyethylene glycol (PEG) polymers, causes analyte signal suppression during mass spectrometry (MS) by competing for available ions during ionisation. This suppressive effect has constrained the application of MALDI-MSI for the molecular mapping of clinical tissues. Secondly, the complexity of the mass spectra is obtained by the formation of multiple adduct ions. The process of analyte ion formation during MALDI can generate multiple m/z peaks from a single lipid species due to the presence of alkali salts in tissues, resulting in the suppression of protonated adduct formation and the generation of multiple near isobaric ions which produce overlapping spatial distributions. Presented is a method to simultaneously remove O.C.T. and endogenous salts. This approach was applied to lipid imaging in order to prevent analyte suppression, simplify data interpretation, and improve sensitivity by promoting lipid protonation and reducing the formation of alkali adducts.

摘要

基质辅助激光解吸/电离质谱成像(MALDI-MSI)是一种常用的分子成像方式,用于原位表征脂质的丰度和空间分布。主要涉及样品预处理和准备的几个技术挑战,使得 MALDI-MSI 分析临床组织变得复杂。首先,样品通常嵌入最佳切割温度(O.C.T.)中,其中含有高浓度的聚乙二醇(PEG)聚合物,在离子化过程中会与可用离子竞争,从而抑制质谱(MS)中的分析物信号。这种抑制作用限制了 MALDI-MSI 在临床组织分子图谱中的应用。其次,通过形成多个加合物离子获得复杂的质谱。由于组织中存在碱盐,MALDI 过程中分析物离子的形成会导致单个脂质物种产生多个 m/z 峰,从而抑制质子化加合物的形成并产生多个近等排离子,从而产生重叠的空间分布。本文提出了一种同时去除 O.C.T. 和内源性盐的方法。该方法应用于脂质成像,以防止分析物抑制,简化数据解释,并通过促进脂质质子化和减少碱加合物的形成来提高灵敏度。

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