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血液来源的小Dot细胞可减少伤口愈合中的疤痕形成。

Blood-derived small Dot cells reduce scar in wound healing.

作者信息

Kong Wuyi, Li Shaowei, Longaker Michael T, Lorenz H Peter

机构信息

Children's Surgical Research Laboratory, Stanford University School of Medicine, 257 Campus Drive, Stanford, California 94305-5148, USA.

出版信息

Exp Cell Res. 2008 Apr 15;314(7):1529-39. doi: 10.1016/j.yexcr.2008.01.022. Epub 2008 Feb 9.

Abstract

Wounds in fetal skin heal without scar, however the mechanism is unknown. We identified a novel group of E-cadherin positive cells in the blood of fetal and adult mice and named them "Dot cells". The percentage of Dot cells in E16.5 fetal mice blood is more than twenty times higher compared to adult blood. Dot cells also express integrin beta1, CD184, CD34, CD13low and Sca1low, but not CD45, CD44, and CD117. Dot cells have a tiny dot shape between 1 and 7 microm diameters with fast proliferation in vitro. Most of the Dot cells remain positive for E-cadherin and integrin beta1 after one month in culture. Transplantation of Dot cells to adult mice heals skin wounds with less scar due to reduced smooth muscle actin and collagen expression in the repair tissue. Tracking GFP-positive Dot cells demonstrates that Dot cells migrate to wounds and differentiate into dermal cells, which also express strongly to FGF-2, and later lose their GFP expression. Our results indicate that Dot cells are a group of previously unidentified cells that have strong wound healing effect. The mechanism of scarless wound healing in fetal skin is due to the presence of a large number of Dot cells.

摘要

胎儿皮肤伤口愈合后不留疤痕,但其机制尚不清楚。我们在胎儿和成年小鼠的血液中发现了一组新的E-钙黏蛋白阳性细胞,并将其命名为“点状细胞”。与成年小鼠血液相比,E16.5胎儿小鼠血液中点状细胞的百分比高出二十多倍。点状细胞还表达整合素β1、CD184、CD34、CD13低表达和Sca1低表达,但不表达CD45、CD44和CD117。点状细胞呈微小的点状,直径在1至7微米之间,在体外增殖迅速。大多数点状细胞在培养一个月后仍对E-钙黏蛋白和整合素β1呈阳性。将点状细胞移植到成年小鼠身上可使皮肤伤口愈合后疤痕减少,这是因为修复组织中平滑肌肌动蛋白和胶原蛋白的表达降低。追踪绿色荧光蛋白阳性的点状细胞表明,点状细胞迁移到伤口并分化为真皮细胞,这些真皮细胞也强烈表达FGF-2,随后失去绿色荧光蛋白表达。我们的结果表明,点状细胞是一组先前未被识别的具有强大伤口愈合作用的细胞。胎儿皮肤无疤痕愈合的机制是由于存在大量的点状细胞。

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