Modulation of Inflammatory Platelet-activating Factor (PAF) Receptor by the Acyl Analogue of PAF

Overview

Journal J Lipid Res

Publisher Elsevier

Specialty Biochemistry

Date 2018 Aug 25

PMID 30139761

Citations 11

Authors

Vyala Hanumanthareddy Chaithra

Shancy Petsel Jacob

Chikkamenahalli Lakshminarayana Lakshmikanth

Mosale Seetharam Sumanth

Kandahalli Venkataranganayaka Abhilasha

Chu-Huang Chen

Anita Thyagarajan

Ravi P Sahu

Jeffery Bryant Travers

Thomas M McIntyre

Kempaiah Kemparaju

Gopal Kedihithlu Marathe

Affiliations

Soon will be listed here.

Abstract

Platelet-activating factor (PAF) is a potent inflammatory mediator that exerts its actions via the single PAF receptor (PAF-R). Cells that biosynthesize alkyl-PAF also make abundant amounts of the less potent PAF analogue acyl-PAF, which competes for PAF-R. Both PAF species are degraded by the plasma form of PAF acetylhydrolase (PAF-AH). We examined whether cogenerated acyl-PAF protects alkyl-PAF from systemic degradation by acting as a sacrificial substrate to enhance inflammatory stimulation or as an inhibitor to dampen PAF-R signaling. In ex vivo experiments both PAF species are prothrombotic in isolation, but acyl-PAF reduced the alkyl-PAF-induced stimulation of human platelets that express canonical PAF-R. In Swiss albino mice, alkyl-PAF causes sudden death, but this effect can also be suppressed by simultaneously administering boluses of acyl-PAF. When PAF-AH levels were incrementally elevated, the protective effect of acyl-PAF on alkyl-PAF-induced death was serially decreased. We conclude that, although acyl-PAF in isolation is mildly proinflammatory, in a pathophysiological setting abundant acyl-PAF suppresses the action of alkyl-PAF. These studies provide evidence for a previously unrecognized role for acyl-PAF as an inflammatory set-point modulator that regulates both PAF-R signaling and hydrolysis.

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