4.7 Article

Isopropanol extraction for cerebrospinal fluid lipidomic profiling analysis

期刊

TALANTA
卷 195, 期 -, 页码 619-627

出版社

ELSEVIER SCIENCE BV
DOI: 10.1016/j.talanta.2018.11.101

关键词

Cerebrospinal fluid; Lipidomic; UHPLC-MS; Isopropanol; Chloroform-methanol; Lipid extraction

资金

  1. Department of Economic Promotion, Rural Areas and Territorial Balance of the Provincial Government of Gipuzkoa [124/16]
  2. Department of Health of the Basque Government [2016111096]
  3. Institute de Salud Carlos III (PN de I + D + I 2013-2016) [PI15/00919]
  4. Basque Government (AIJ) [RBFI-2015-1-0231]
  5. Ministerio de Economia y Competitividad
  6. Basque Country Government
  7. Kutxa-Fundazioa

向作者/读者索取更多资源

The cerebrospinal fluid (CSF) lipidome is attracting increasing attention due to the importance of lipids in brain molecular signaling and their involvement in several neurological diseases. Different solvent systems have been used for the extraction of multiple lipid classes from CSF but no comparative study of the effectiveness of these protocols has been carried out. To optimize CSF lipid extraction for lipidomic measurements by untargeted ultra-high performance liquid chromatography - mass spectrometry, we evaluate and compare two sample preparation protocols, one involving protein precipitation with isopropanol (IPA) and other consisting of a liquid liquid extraction with chloroform-methanol. For that purpose, human CSF from neurologically healthy and normolipidemic volunteers was used. The criteria established to compare these two methods were based on four critical aspects of sample preparation: simplicity, lipid coverage, reproducibility and recovery efficiencies. We found that both methods were highly reproducible techniques ( > 75% of the lipids with coefficient of variation (CV) < 30%). In terms of recovery, the single-step IPA procedure yielded better values for most of the lipid classes and it was less toxic and simpler than the liquid-liquid extraction method. In relation to lipid coverage, variation in selectivity was observed between methods, providing evidence that IPA was more selective for polar lipids. Overall, IPA precipitation provides excellent results in terms of simplicity of execution, lipid coverage, reproducibility and recovery. We conclude that it is a choice procedure for large-scale, untargeted lipid profiling using UHPLC-MS in CSF analysis.

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