Pivotal function for cytoplasmic protein FROUNT in CCR2-mediated monocyte chemotaxis.

Authors :: Terashima, Yuya
Onai, Nobuyuki
Murai, Masako
Enomoto, Masahiko
Poonpiriya, Vongsakorn
Hamada, Tsuyoshi
Motomura, Kazushi
Suwa, Makiko
Ezaki, Taichi
Haga, Tatsuya
Kanegasaki, Shiro
Matsushima, Kouji
Source :: Nature Immunology; Aug2005, Vol. 6 Issue 8, p827-835, 9p
Publication Year :: 2005
Abstract: Ligation of the chemokine receptor CCR2 on monocytes and macrophages with its ligand CCL2 results in activation of the cascade consisting of phosphatidylinositol-3-OH kinase (PI(3)K), the small G protein Rac and lamellipodium protrusion. We show here that a unique clathrin heavy-chain repeat homology protein, FROUNT, directly bound activated CCR2 and formed clusters at the cell front during chemotaxis. Overexpression of FROUNT amplified the chemokine-elicited PI(3)K–Rac–lamellipodium protrusion cascade and subsequent chemotaxis. Blocking FROUNT function by using a truncated mutant or antisense strategy substantially diminished signaling via CCR2. In a mouse peritonitis model, suppression of endogenous FROUNT markedly prevented macrophage infiltration. Thus, FROUNT links activated CCR2 to the PI(3)K–Rac–lamellipodium protrusion cascade and could be a therapeutic target in chronic inflammatory immune diseases associated with macrophage infiltration. [ABSTRACT FROM AUTHOR]

Subjects :: CHEMOTAXIS
MONOCYTES
LEUKOCYTES
KILLER cells
MEMBRANE proteins
HOMOLOGY (Biology)
PERITONEUM diseases

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