A nude mouse model of hypertrophic scar shows morphologic and histologic characteristics of human hypertrophic scar

病理 增生性瘢痕 疤痕 H&E染色 免疫组织化学 染色 苏木精 三色 医学 多糖 裸鼠 马森三色染色 人体皮肤 植皮术 组织学 解剖 生物 外科 内科学 癌症 蛋白多糖 遗传学 软骨
作者
Moein Momtazi,Peter Kwan,Jie Ding,Colin C. Anderson,Dariush Honardoust,Serge Goekjian,Edward E. Tredget
出处
期刊:Wound Repair and Regeneration [Wiley]
卷期号:21 (1): 77-87 被引量:59
标识
DOI:10.1111/j.1524-475x.2012.00856.x
摘要

Hypertrophic scar (HSc) is a fibroproliferative disorder that occurs following deep dermal injury. Lack of a relevant animal model is one barrier toward better understanding its pathophysiology. Our objective is to demonstrate that grafting split-thickness human skin onto nude mice results in survival of engrafted human skin and murine scars that are morphologically, histologically, and immunohistochemically consistent with human HSc. Twenty nude mice were xenografted with split-thickness human skin. Animals were euthanized at 30, 60, 120, and 180 days postoperatively. Eighteen controls were autografted with full-thickness nude mouse skin and euthanized at 30 and 60 days postoperatively. Scar biopsies were harvested at each time point. Blinded scar assessment was performed using a modified Manchester Scar Scale. Histologic analysis included hematoxylin and eosin, Masson's trichrome, toluidine blue, and picrosirius red staining. Immunohistochemistry included anti-human human leukocyte antigen-ABC, α-smooth muscle actin, decorin, and biglycan staining. Xenografted mice developed red, shiny, elevated scars similar to human HSc and supported by blinded scar assessment. Autograft controls appeared morphologically and histologically similar to normal skin. Xenografts survived up to 180 days and showed increased thickness, loss of hair follicles, adnexal structures and rete pegs, hypercellularity, whorled collagen fibers parallel to the surface, myofibroblasts, decreased decorin and increased biglycan expression, and increased mast cell density. Grafting split-thickness human skin onto nude mice results in persistent scars that show morphologic, histologic, and immunohistochemical consistency with human HSc. Therefore, this model provides a promising technique to study HSc formation and to test novel treatment options.
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