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KMID : 0613820150250050585
Journal of Life Science
2015 Volume.25 No. 5 p.585 ~ p.593
Alteration of Stress Fiber in Fibroblastic Reticular Cells via Lymphotoxin ¥â Receptor Stimulation is Associated with Myosin
Kim Min-Hwan

Kim Yeon-Hee
Choi Woo-Bong
Lee Jong-Hwan
Abstract
Stress fiber (SF) alteration is mediated by cellular receptors, which, upon interaction with the extracellular counterpart, signal to the actin cytoskeleton for remodeling. This association is mediated by a variety of scaffold and signaling factors, which control the mechanical and signaling activities of the interaction site. The heterotrimeric transmembrane lymphotoxin ¥á1¥â2 (LT¥á1¥â2), a member of the tumor necrosis factor (TNF) family of cytokines, including soluble homotrimeric lymphotoxin (LT¥á), plays an important role in lymphoid tissue architecture. Ligation between LT¥á1¥â2 and the lymphotoxin ¥â receptor (LT¥âR) activates signal-cascade in fibroblastic reticular cells (FRCs). We found LT¥âR stimulation using an agonistic anti-LT¥âR antibody alone or combined with LT¥á or TNF¥á induced changes in the actin and plasticity of cells. To clarify the involvement of myosin underlying the alteration, we analyzed the effect of myosin light chain kinase (MLCK) with an MLCK inhibitor (ML7), the phosphorylation level of myosin light chains (MLC), and the level of phospho-myosin phosphatase target subunit 1 (MYPT1) after treatment with an agonistic anti-LT¥âR antibody for cytoskeleton reorganization in FRCs. The inhibition of MLCK activity induced changes in the actin cytoskeleton organization and cell morphology in FRC. In addition, we showed the phosphorylation of MLC and MYPT1 was reduced by LT¥âR stimulation in cells. A DNA chip revealed the LT¥âR stimulation of FRC down-regulated transcripts of myosin and actin components. Collectively, these results suggest LT¥âR stimulation is linked to myosin regarding SF alteration in FRC.
KEYWORD
Fibroblastic reticular cell (FRC), lymphotoxin ¥â receptor (LT¥âR), myosin, stress fiber
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