LTB₄ Is a Signal-Relay Molecule during Neutrophil Chemotaxis

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• 作者：Philippe  ; V. Afonso¹ ; ⁴ ; Mirkka Janka-Junttila¹ ; ⁴ ; Young  ; Jong Lee² ; Colin  ; P. McCann¹ ; ³ ; Charlotte  ; M. Oliver¹ ; Khaled  ; A. Aamer² ; Wolfgang Losert³ ; Marcus  ; T. Cicerone² ; Carole  ; A. Parent¹ ; ^{parentc@mail.nih.gov}
• 刊名：Developmental Cell
• 出版年：2012
• 期刊代码：10_15345807
• 类别：bio
• 出版时间：15 May, 2012
• 卷：22
• 期：5
• 页码：1079-1091
• 文件大小：1239 K

摘要

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class="h3">Summary

Neutrophil recruitment to inflammation sites purportedly depends on sequential waves of chemoattractants. Current models propose that leukotriene B₄ (LTB₄), a secondary chemoattractant secreted by neutrophils in response to primary chemoattractants such as formyl peptides, is important in initiating the聽inflammation process. In this study we demonstrate that LTB₄ plays a central role in neutrophil activation and migration to formyl peptides. We show that LTB₄聽production dramatically amplifies formyl peptide-mediated neutrophil polarization and chemotaxis by regulating specific signaling pathways acting upstream of actin polymerization and MyoII phosphorylation. Importantly, by analyzing the migration of neutrophils isolated from wild-type mice and mice lacking the formyl peptide receptor 1, we demonstrate that LTB₄ acts as a signal to relay information from cell to cell over long distances. Together, our findings imply that LTB₄ is a signal-relay molecule that exquisitely regulates neutrophil chemotaxis to formyl peptides, which are produced at the core of inflammation sites.