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同一组织切片中元素和脂质多模态质谱成像联合工作流程的评估

Evaluation of combined workflows for multimodal mass spectrometry imaging of elements and lipids from the same tissue section.

作者信息

Sarretto Tassiani, Westerhausen Mika T, Mckinnon Jayden C, Bishop David P, Ellis Shane R

机构信息

Molecular Horizons and School of Chemistry and Molecular Bioscience, University of Wollongong, Wollongong, Australia.

Hyphenated Mass Spectrometry Laboratory, University of Technology Sydney, Ultimo, Sydney, NSW, Australia.

出版信息

Anal Bioanal Chem. 2025 Feb;417(4):705-719. doi: 10.1007/s00216-024-05696-w. Epub 2025 Jan 20.

Abstract

The wide range of mass spectrometry imaging (MSI) technologies enables the spatial distributions of many analyte classes to be investigated. However, as each approach is best suited to certain analytes, combinations of different MSI techniques are increasingly being explored to obtain more chemical information from a sample. In many cases, performing a sequential analysis of the same tissue section is ideal to enable a direct correlation of multimodal data. In this work, we explored different workflows that allow sequential lipid and elemental imaging on the same tissue section using atmospheric pressure laser desorption/ionisation-plasma post-ionisation-MSI (AP-MALDI-PPI-MSI) and laser ablation-inductively coupled plasma-MSI (LA-ICP-MSI), respectively. It is found that performing lipid imaging first using matrix-coated samples, followed by elemental imaging on matrix-coated samples, provides high-quality MSI datasets for both lipids and elements, with the resulting distributions being similar to those obtained when each is performed in isolation. The effect of matrix removal prior to elemental imaging, and of performing elemental imaging first were also investigated but found to generally yield lower quality elemental imaging data but comparable lipid imaging data. Finally, we used the ability to acquire both elemental and lipid imaging data from the same section to investigate the spatial correlations between different lipids (including ceramides, phosphatidylethanolamine, and hexosylceramides) and elements within mouse brain tissue.

摘要

广泛的质谱成像(MSI)技术能够研究多种分析物类别的空间分布。然而,由于每种方法都最适合某些分析物,因此人们越来越多地探索不同MSI技术的组合,以便从样品中获取更多化学信息。在许多情况下,对同一组织切片进行顺序分析非常理想,能够实现多模态数据的直接关联。在这项工作中,我们探索了不同的工作流程,分别使用常压激光解吸/电离-等离子体后电离-MSI(AP-MALDI-PPI-MSI)和激光烧蚀-电感耦合等离子体-MSI(LA-ICP-MSI),在同一组织切片上进行脂质和元素的顺序成像。结果发现,首先使用涂覆基质的样品进行脂质成像,然后对涂覆基质的样品进行元素成像,可为脂质和元素提供高质量的MSI数据集,所得分布与单独进行每种成像时获得的分布相似。还研究了在元素成像之前去除基质的效果以及首先进行元素成像所产生的影响,结果发现通常会产生质量较低的元素成像数据,但脂质成像数据相当。最后,我们利用从同一组织切片获取元素和脂质成像数据的能力,研究了小鼠脑组织中不同脂质(包括神经酰胺、磷脂酰乙醇胺和己糖神经酰胺)与元素之间的空间相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ade8/11772510/b6ad3bc70cbb/216_2024_5696_Fig1_HTML.jpg

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