Quantitative analysis of lipids: a higher-throughput LC-MS/MS-based method and its comparison to ELISA

Adarsh S Gandhi; David Budac; Tanzilya Khayrullina; Roland Staal; Gamini Chandrasena

doi:10.4155/fsoa-2016-0067

Quantitative analysis of lipids: a higher-throughput LC-MS/MS-based method and its comparison to ELISA

Future Sci OA. 2017 Jan 16;3(1):FSO157. doi: 10.4155/fsoa-2016-0067. eCollection 2017 Mar.

Authors

Adarsh S Gandhi¹, David Budac¹, Tanzilya Khayrullina², Roland Staal², Gamini Chandrasena¹

Affiliations

¹ Molecular Pharmacology, Bioanalysis & Operations, Lundbeck Research USA, 215 College Road, Paramus, NJ, USA; Molecular Pharmacology, Bioanalysis & Operations, Lundbeck Research USA, 215 College Road, Paramus, NJ, USA.
² Neuroinflammation Disease Biology Unit, In Vitro Biology, Lundbeck Research USA, 215 College Road, Paramus, NJ, USA; Neuroinflammation Disease Biology Unit, In Vitro Biology, Lundbeck Research USA, 215 College Road, Paramus, NJ, USA.

Abstract

Aim: Lipids such as prostaglandins, leukotrienes and thromboxanes are released as a result of an inflammatory episode in pain (central and peripheral).

Methodology & results: To measure these lipids as potential mechanistic biomarkers in neuropathic pain models, we developed a higher-throughput LC-MS/MS-based method with simultaneous detection of PGE2, PGD2, PGF2α, LTB4, TXB2 and 2-arachidonoyl glycerol in brain and spinal cord tissues. We also demonstrate that the LC-MS/MS method was more sensitive and specific in differentiating PGE2 levels in CNS tissues compared with ELISA.

Conclusion: The ability to modify the LC-MS/MS method to accommodate numerous other lipids in one analysis, demonstrates that the presented method offers a cost-effective and more sensitive alternative to ELISA method useful in drug discovery settings.

Keywords: ELISA; LC–MS/MS; higher-throughput; lipids; neuropathic pain.