CTACK/CCL27 accelerates skin regeneration via accumulation of bone marrow-derived keratinocytes

被引:77
作者
Inokuma, Daisuke
Abe, Riichiro
Fujita, Yasuyuki
Sasaki, Mikako
Shibaki, Akihiko
Nakamura, Hideki
McMillan, James R.
Shimizu, Tadamichi
Shimizu, Hiroshi
机构
[1] Hokkaido Univ, Grad Sch Med, Dept Dermatol, Kita Ku, Sapporo, Hokkaido 0608638, Japan
[2] Toyama Univ, Fac Med, Dept Dermatol, Toyama 930, Japan
关键词
bone marrow-derived stem cell; CTACK/CCL27; CCR10; keratinocyte; wound healing;
D O I
10.1634/stemcells.2006-0264
中图分类号
Q813 [细胞工程];
学科分类号
摘要
Recent studies have suggested that bone marrow ( BM) cells transdifferentiate to regenerate a variety of cellular lineages. Due to the relatively small population of BM- derived cells in each organ, it is still controversial whether these BM- derived cells are really present in sufficient numbers for effective function. Conversely, it is speculated that chemokine/ chemokine receptor interactions mediate this migration of the tissue- specific precursor cells from BM into the target tissue. Here, we show that cutaneous T- cell attracting chemokine ( CTACK)/ CCL27 is the major regulator involved in the migration of keratinocyte precursor cells from BM into skin. By screening various chemokine expression patterns, we demonstrated that CTACK is constitutively expressed in normal skin and upregulated in wounds and that approximately 20% of CD34(+) BM cells expressed CCR10, the ligand for CTACK. Intradermal injection of CTACK/ CCL27 into the periphery of skin wounds significantly enhanced BM- derived keratinocyte ( BMDK) migration, and CTACK/ CCL27 neutralizing antibody inhibited this BMDK migration. Furthermore, increased BMDK migration caused by CTACK/ CCL27 significantly accelerated the wound- healing process without any influence over either angiogenesis or keratinocyte proliferation. These results provide direct evidence that recruitment of BM keratinocyte precursor cells to the skin is regulated by specific chemokine/ chemokine receptor interactions, making possible the development of new regenerative therapeutic strategies.
引用
收藏
页码:2810 / 2816
页数:7
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