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KMID : 0620920080400010059
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Experimental & Molecular Medicine
2008 Volume.40 No. 1 p.59 ~ p.70
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RANKL stimulates proliferation, adhesion and IL-7 expression of thymic epithelial cells
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Lee Hee-Woo
Yoon Sik
Lee Choong-Won
Na Yong-Jin
Kim Chi-Dae
Kim Bong-Seon
Kim Jae-Bong
Park Hye-Kyung
Lee Jung-Hoon
Moon Jeon-Ok
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Abstract
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In many clinical situations which cause thymic involution and thereby result in immune deficiency, T cells are the most often affected, leading to a prolonged deficiency of T cells. Since only the thymic-dependent T cell production pathway secures stable regeneration of fully mature T cells, seeking strategies to enhance thymic regeneration should be a key step in developing therapeutic methods for the treatment of these significant clinical problems. This study clearly shows that receptor activator of NF-¥êB ligand (RANKL) stimulates mouse thymic epithelial cell activities including cell proliferation, thymocyte adhesion to thymic epithelial cells, and the expression of cell death regulatory genes favoring cell survival, cell adhesion molecules such as ICAM-1 and VCAM-1, and thymopoietic factors including IL-7. Importantly, RANKL exhibited a significant capability to facilitate thymic regeneration in mice. In addition, this study demonstrates that RANKL acts directly on the thymus to activate thymus regeneration regardless of its potential influences on thymic regeneration through an indirect or systemic effect. In light of this, the present study provides a greater insight into the development of novel therapeutic strategies for effective thymus repopulation using RANKL in the design of therapies for many clinical conditions in which immune reconstitution is required.
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KEYWORD
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cell adhesion molecules, RANK ligand, regeneration, thymopoietins, thymus gland
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