Resolution of inflammation: the beginning programs the end

CN Serhan, J Savill - Nature immunology, 2005 - nature.com
CN Serhan, J Savill
Nature immunology, 2005nature.com
Acute inflammation normally resolves by mechanisms that have remained somewhat
elusive. Emerging evidence now suggests that an active, coordinated program of resolution
initiates in the first few hours after an inflammatory response begins. After entering tissues,
granulocytes promote the switch of arachidonic acid–derived prostaglandins and
leukotrienes to lipoxins, which initiate the termination sequence. Neutrophil recruitment thus
ceases and programmed death by apoptosis is engaged. These events coincide with the …
Abstract
Acute inflammation normally resolves by mechanisms that have remained somewhat elusive. Emerging evidence now suggests that an active, coordinated program of resolution initiates in the first few hours after an inflammatory response begins. After entering tissues, granulocytes promote the switch of arachidonic acid–derived prostaglandins and leukotrienes to lipoxins, which initiate the termination sequence. Neutrophil recruitment thus ceases and programmed death by apoptosis is engaged. These events coincide with the biosynthesis, from omega-3 polyunsaturated fatty acids, of resolvins and protectins, which critically shorten the period of neutrophil infiltration by initiating apoptosis. Consequently, apoptotic neutrophils undergo phagocytosis by macrophages, leading to neutrophil clearance and release of anti-inflammatory and reparative cytokines such as transforming growth factor-β1. The anti-inflammatory program ends with the departure of macrophages through the lymphatics. Understanding these and further details of the mechanism required for inflammation resolution may underpin the development of drugs that can resolve inflammatory processes in directed and controlled ways.
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