在伤口愈合过程中，表皮整合素β-1 和 p75NTR 阳性细胞增殖和迁移，产生各种生长因子，而慢性皮肤溃疡患者的 p75NTR 表达降低。

The epidermal Integrin beta-1 and p75NTR positive cells proliferating and migrating during wound healing produce various growth factors, while the expression of p75NTR is decreased in patients with chronic skin ulcers.

机构信息

Department of Dermatology, Fujita Health University School of Medicine, 1-98 Kutsukake-cho, Toyoake, Aichi 470-1192, Japan.

出版信息

J Dermatol Sci. 2013 Aug;71(2):122-9. doi: 10.1016/j.jdermsci.2013.04.006. Epub 2013 Apr 17.

DOI:10.1016/j.jdermsci.2013.04.006

PMID:23642664

Abstract

BACKGROUND

More effective treatment strategies are needed for the chronic skin ulcers. Recently, it has been reported that clinical application of stem cells improve wound healing.

OBJECTIVE

We aimed to determine the dynamic time-course movement of epidermal stem cell markers especially p75 neurotrophin receptor (p75NTR) and Integrin beta-1 in wound healing process. Furthermore, we also investigated the presence of these markers in human.

METHODS

Epidermal Integrin beta-1(+) and p75NTR(+) cells were counted in wound healing process in mice. Both cells were also counted in human skin specimen obtained from chronic skin ulcers and healthy controls. Growth factor gene expression levels by purified mouse epidermal p75NTR(+) cells were also analyzed using real-time RT-PCR.

RESULTS

Integrin beta-1(+) and p75NTR(+) cells were proliferated from 3 days after wounding. Reepithelization was completed 7 days after wounding, and the numbers of cells were returned to the baseline levels by 14 days after wounding. Integrin beta-1(+) cells were proliferated in the basal layer, and p75NTR(+) cells were proliferated in the upper layer of epidermis. In human skin, Integrin beta-1(+) and p75NTR(+) cells were 81%±12% and 36%±15% of the basal cells, respectively. In patients with chronic skin ulcers, the percentage of Integrin beta-1(+) cells in the epidermis was identical to healthy controls. Surprisingly, p75NTR(+) cells were significantly decreased in chronic skin ulcer patients (1.2%±2.6%; p<0.0005) compared to healthy controls. Purified mouse epidermal p75NTR(+) cells expressed higher transforming growth factor-beta2 and vascular endothelial growth factor-alpha transcripts and lower epidermal growth factor transcripts than p75NTR(-) cells.

CONCLUSION

These results suggest that Integrin beta-1(+) and p75NTR(+) cells play an important role in wound healing process, and that p75NTR may be a key molecule and a candidate for new therapeutic target besides preexisting molecules for chronic skin ulcer patients.

摘要

背景

需要更有效的治疗策略来治疗慢性皮肤溃疡。最近有报道称，干细胞的临床应用可改善伤口愈合。

目的

本研究旨在确定表皮干细胞标志物，尤其是 p75 神经营养素受体（p75NTR）和整合素β-1 在伤口愈合过程中的动态时间过程运动。此外，我们还研究了这些标志物在人类中的存在。

方法

在小鼠伤口愈合过程中计算表皮整合素β-1（+）和 p75NTR（+）细胞的数量。还对慢性皮肤溃疡和健康对照组获得的人皮肤标本中的这些标志物进行计数。还使用实时 RT-PCR 分析了纯化的小鼠表皮 p75NTR（+）细胞中生长因子基因的表达水平。

结果

整合素β-1（+）和 p75NTR（+）细胞在创伤后 3 天开始增殖。创伤后 7 天完成再上皮化，创伤后 14 天细胞数量恢复到基线水平。整合素β-1（+）细胞在基底层增殖，p75NTR（+）细胞在表皮上层增殖。在人类皮肤中，整合素β-1（+）和 p75NTR（+）细胞分别占基底层细胞的 81%±12%和 36%±15%。在慢性皮肤溃疡患者中，表皮中整合素β-1（+）细胞的百分比与健康对照组相同。令人惊讶的是，与健康对照组相比，慢性皮肤溃疡患者的 p75NTR（+）细胞显著减少（1.2%±2.6%；p<0.0005）。与 p75NTR（-）细胞相比，纯化的小鼠表皮 p75NTR（+）细胞表达更高的转化生长因子-β2 和血管内皮生长因子-α转录物，而表达更低的表皮生长因子转录物。