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Merck
  • Fatty acid chain length drives lysophosphatidylserine-dependent immunological outputs.

Fatty acid chain length drives lysophosphatidylserine-dependent immunological outputs.

Cell chemical biology (2021-02-12)
Neha Khandelwal, Minhaj Shaikh, Amol Mhetre, Shubham Singh, Theja Sajeevan, Alaumy Joshi, Kithiganahalli Narayanaswamy Balaji, Harinath Chakrapani, Siddhesh S Kamat
摘要

In humans, lysophosphatidylserines (lyso-PSs) are potent lipid regulators of important immunological processes. Given their structural diversity and commercial paucity, here we report the synthesis of methyl esters of lyso-PS (Me-lyso-PSs) containing medium- to very-long-chain (VLC) lipid tails. We show that Me-lyso-PSs are excellent substrates for the lyso-PS lipase ABHD12, and that these synthetic lipids are acted upon by cellular carboxylesterases to produce lyso-PSs. Next, in macrophages we demonstrate that VLC lyso-PSs orchestrate pro-inflammatory responses and in turn neuroinflammation via a Toll-like receptor 2 (TLR2)-dependent pathway. We also show that long-chain (LC) lyso-PSs robustly induce intracellular cyclic AMP production, cytosolic calcium influx, and phosphorylation of the nodal extracellular signal-regulated kinase to regulate macrophage activation via a TLR2-independent pathway. Finally, we report that LC lyso-PSs potently elicit histamine release during the mast cell degranulation process, and that ABHD12 is the major lyso-PS lipase in these immune cells.

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Sigma-Aldrich
组胺, ≥97.0%
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伴刀豆球蛋白A 来源于洋刀豆 (刀豆), Type IV-S, lyophilized powder, γ-irradiated, BioReagent, suitable for cell culture
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干细胞因子 来源于小鼠, SCF, recombinant, expressed in E. coli, powder, suitable for cell culture