| Literature DB >> 20714413 |
Hidenori Hattori1, Kulandayan K Subramanian, Jiro Sakai, Hongbo R Luo.
Abstract
Neutrophil chemotaxis is a critical component in innate immunity. Recently, using a small-molecule functional screening, we identified NADPHoxidase- dependent Reactive Oxygen Species (ROS) as key regulators of neutrophil chemotactic migration. Neutrophils depleted of ROS form more frequent multiple pseudopodia and lost their directionality as they migrate up a chemoattractant concentration gradient. Here, we further studied the role of ROS in neutrophil chemotaxis and found that multiple pseudopodia formation induced by NADPH inhibitor diphenyleneiodonium chloride (DPI) was more prominent in relatively shallow chemoattractant gradient. It was reported that, in shallow chemoattractant gradients, new pseudopods are usually generated when existing ones bifurcate. Directional sensing is mediated by maintaining the most accurate existing pseudopod, and destroying pseudopods facing the wrong direction by actin depolymerization. We propose that NADPH-mediated ROS production may be critical for disruption of misoriented pseudopods in chemotaxing neutrophils. Thus, inhibition of ROS production will lead to formation of multiple pseudopodia.Entities:
Keywords: NADPH oxidase; cell migration; chemokines; chronic granulomatous disease; innate immunity; signal transduction
Year: 2010 PMID: 20714413 PMCID: PMC2918776 DOI: 10.4161/cib.3.3.11559
Source DB: PubMed Journal: Commun Integr Biol ISSN: 1942-0889