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在伤口成熟过程中,血管生成与血清白蛋白的片段化相关,但与铜蓝蛋白、转铁蛋白或触珠蛋白无关。

Vascularity during wound maturation correlates with fragmentation of serum albumin but not ceruloplasmin, transferrin, or haptoglobin.

机构信息

Department of Oral Pathology and Oral Medicine, University of Sydney, Westmead Centre for Oral Health, Westmead Hospital, Westmead, NSW, Australia.

出版信息

Wound Repair Regen. 2010 Mar-Apr;18(2):211-22. doi: 10.1111/j.1524-475X.2010.00572.x. Epub 2010 Mar 12.

DOI:10.1111/j.1524-475X.2010.00572.x
PMID:20409147
Abstract

Reduced vascularity during wound maturation is mediated by endothelial apoptosis. Albumin has an anti-apoptotic activity for endothelium, which increases up to 100-fold on albumin fragmentation (AF). We now report that levels of AF correlate with changing vascularity during wound maturation. Both scarring and adipogenic wound-healing models were established in mice. Western blots of granulation tissue revealed AF concurrent with periods of high vascularity as determined by thin-section microscopy, with reduced AF on wound maturation (p<0.02). In profiling AF, the levels of 27.5 and 39 kDa fragments were reduced on maturation of both scarring and adipogenic wounds (p<0.005), as were the levels of an additional 17.5 kDa fragment prominent only in adipogenic wounds (p<0.001). A 49 kDa albumin fragment was found to be reduced during maturation of scarring (p<0.001) but not adipogenic wounds. For comparison, we probed for transferrin, ceruloplasmin, and haptoglobin fragmentation on the basis that like albumin, these are considered acute-phase transport proteins. Minimal fragmentation of transferrin and ceruloplasmin was seen, along with partial dissociation of haptoglobin subunits, but these did not correlate with AF or vascularity. Our findings are consistent with a role for AF in regulating granulation tissue vascularity during healing.

摘要

血管生成减少在伤口成熟过程中是由内皮细胞凋亡介导的。白蛋白对内皮细胞具有抗凋亡活性,在白蛋白片段化(AF)时增加高达 100 倍。我们现在报告说,AF 的水平与伤口成熟过程中血管生成的变化相关。在小鼠中建立了瘢痕和脂肪生成性伤口愈合模型。肉芽组织的 Western blot 显示,AF 与通过薄切片显微镜确定的高血管期同时存在,在伤口成熟时 AF 减少(p<0.02)。在分析 AF 时,在瘢痕和脂肪生成性伤口的成熟过程中,27.5 和 39 kDa 片段的水平降低(p<0.005),而仅在脂肪生成性伤口中突出的另外 17.5 kDa 片段的水平也降低(p<0.001)。发现 49 kDa 白蛋白片段在瘢痕形成过程中减少(p<0.001),但在脂肪生成性伤口中则不然。作为比较,我们探测了转铁蛋白、铜蓝蛋白和触珠蛋白的片段化,因为像白蛋白一样,这些被认为是急性期转运蛋白。转铁蛋白和铜蓝蛋白的片段化很少见,同时触珠蛋白亚基部分解离,但这些与 AF 或血管生成无关。我们的发现与 AF 在调节愈合过程中肉芽组织血管生成中的作用一致。

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