血小板反应蛋白-1 和肌成纤维细胞在角膜伤口修复过程中的定位。
Localization of thrombospondin-1 and myofibroblasts during corneal wound repair.
机构信息
The Schepens Eye Research Institute and Department of Ophthalmology, Harvard Medical School, 20 Staniford Street, Boston, MA 02114, USA.
出版信息
Exp Eye Res. 2011 Oct;93(4):534-40. doi: 10.1016/j.exer.2011.06.018. Epub 2011 Jul 2.
Thrombospondin-1 (TSP-1) is a multifunctional matrix protein that has recently been examined in various wound processes, primarily for its ability to activate the latent complex of transforming growth factor-beta (TGF-β). TGF-β has been shown to play a major role in stimulating mesenchymal cells to synthesize extracellular matrix. After injury, corneal keratocytes become activated and transform into fibroblasts and myofibroblasts. Our hypothesis is that TSP-1 regulates the transformation of keratocytes into myofibroblasts (MF) via TGF-β. In the current study, we examined the expression of TSP-1 and α-smooth muscle actin (SMA), a marker of MF, during rat corneal wound healing. Three-mm keratectomy or debridement wounds were made in the central rat cornea and allowed to heal from 8 hours to 8 weeks in vivo. Unwounded rat corneas served as controls. Expression of TSP-1, SMA and Ki67, a marker of proliferating cells, were examined by indirect-immunofluorescence microscopy. In unwounded corneas, TSP-1 expression was observed primarily in the endothelium. No expression was seen in the stroma, and only low levels were detected in the epithelium. Ki67 was localized in the epithelial basal cells and no SMA was present in the central cornea of unwounded eyes. After keratectomy wounds, TSP-1 expression was seen 24 h after wounding in the stroma immediately subjacent to the wound-healing epithelium. The expression of TSP-1 increased daily and peaked 7-8 days after wounding. SMA expression, however, was not observed until 3-4 days after wounding. Interestingly, SMA-positive cells were almost exclusively seen in the stromal zone expressing TSP-1. Peak expression of SMA-positive cells was observed 7-8 days after wounding. Ki67-expressing cells were seen both in the area expressing TSP-1 and the adjacent area. In the debridement wounds, no SMA expressing cells were observed at any time point. TSP-1 was localized in the basement membrane zone from 2 to 5 days after wounding, and the localization did not appear to penetrate into the stroma. These data are in agreement with our hypothesis that TSP-1 localization in the stromal matrix is involved in the transformation of keratocytes into myofibroblasts.
血小板反应蛋白 1(TSP-1)是一种多功能基质蛋白,最近在各种伤口过程中进行了研究,主要是因为它能够激活转化生长因子-β(TGF-β)的潜伏复合物。TGF-β 在刺激间充质细胞合成细胞外基质方面发挥着重要作用。受伤后,角膜成纤维细胞被激活并转化为成纤维细胞和肌成纤维细胞。我们的假设是,TSP-1 通过 TGF-β 调节角膜成纤维细胞向肌成纤维细胞(MF)的转化。在目前的研究中,我们检查了血小板反应蛋白 1(TSP-1)和α-平滑肌肌动蛋白(SMA)的表达,α-平滑肌肌动蛋白是 MF 的标志物,在大鼠角膜伤口愈合过程中。在大鼠中央角膜上进行 3mm 的角膜切除术或清创术,并在体内从 8 小时到 8 周的时间内愈合。未受伤的大鼠角膜作为对照。通过间接免疫荧光显微镜检查 TSP-1、SMA 和增殖细胞标志物 Ki67 的表达。在未受伤的角膜中,TSP-1 的表达主要在内皮细胞中观察到。在基质中未观察到表达,在上皮中仅检测到低水平的表达。Ki67 位于上皮基底层,在未受伤眼睛的中央角膜中不存在 SMA。在角膜切除术伤口后,TSP-1 的表达在伤口愈合上皮下方的基质中在受伤后 24 小时可见。TSP-1 的表达每天增加,在受伤后 7-8 天达到峰值。然而,直到受伤后 3-4 天才观察到 SMA 的表达。有趣的是,SMA 阳性细胞几乎仅在表达 TSP-1 的基质区域中可见。SMA 阳性细胞的表达峰值出现在受伤后 7-8 天。Ki67 表达细胞可见于表达 TSP-1 的区域和相邻区域。在清创伤口中,在任何时间点都未观察到表达 SMA 的细胞。TSP-1 在受伤后 2-5 天定位于基底膜区,并且定位似乎未穿透到基质中。这些数据与我们的假设一致,即 TSP-1 在基质基质中的定位参与了角膜成纤维细胞向肌成纤维细胞的转化。
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