治疗性 TNF 抑制剂在加速皮肤伤口愈合方面表现出不同程度的功效

Yonghao Cao , Bohdan P. Harvey , Liang Jin , Susan Westmoreland , Jing Wang , Munish Puri , Yingli Yang , Holly M. Robb , Sultan Tanriverdi , Chenqi Hu , Xue Wang , Xiaofeng Xin , Yingchun Liu , Michael P. Macoritto , Kathleen M. Smith , Yu Tian , Kevin White , Timothy R.D.J. Radstake , Zehra Kaymakcalan
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引用次数: 0

摘要

据报道,阿达木单抗(adalimumab)但依那西普(etanercept)和certolizumab-pegol都不能通过调节巨噬细胞分化和基质金属蛋白酶的表达在体外诱导伤口愈合,这可能是各种TNF-α抑制剂对慢性炎症性皮肤病--化脓性扁桃体炎患者伤口愈合受损的疗效存在差异的原因。为了研究和比较各种 TNF 抑制剂对体内皮肤伤口愈合的疗效,我们建立了人类 TNF 基因敲入 Leprdb/db 小鼠模型,以模拟化脓性扁平苔藓患者受损的皮肤伤口愈合。模型中的载体组表现出严重的皮肤伤口愈合障碍。与此相反,阿达木单抗能显著加速伤口愈合,这一点已通过组织学评估和独特的愈合转录谱得到证实。此外,阿达木单抗和英夫利昔单抗显示出相似的疗效,但戈利木单抗以及依那西普和certolizumab-pegol的疗效较差。与组织学评估结果一致的是,对暴露于各种TNF抑制剂的愈合伤口进行的蛋白质组学分析显示了不同的伤口愈合特征,这可能是这些抑制剂在加速皮肤伤口愈合方面不同疗效的原因。综上所述,这些数据显示 TNF 抑制剂在体内伤口愈合受损模型中加速皮肤伤口愈合方面表现出不同程度的功效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Therapeutic TNF Inhibitors Exhibit Differential Levels of Efficacy in Accelerating Cutaneous Wound Healing

Adalimumab but neither etanercept nor certolizumab-pegol has been reported to induce a wound-healing profile in vitro by regulating macrophage differentiation and matrix metalloproteinase expression, which may underlie the differences in efficacy between various TNF-α inhibitors in impaired wound healing in patients with hidradenitis suppurativa, a chronic inflammatory skin disease. To examine and compare the efficacy of various TNF inhibitors in cutaneous wound healing in vivo, a human TNF knock-in Leprdb/db mouse model was established to model the impaired cutaneous wound healing as seen in hidradenitis suppurativa. The vehicle group exhibited severe impairments in cutaneous wound healing. In contrast, adalimumab significantly accelerated healing, confirmed by both histologic assessment and a unique healing transcriptional profile. Moreover, adalimumab and infliximab showed similar levels of efficacy, but golimumab was less effective, along with etanercept and certolizumab-pegol. In line with histologic assessments, proteomics analyses from healing wounds exposed to various TNF inhibitors revealed distinct and differential wound-healing signatures that may underlie the differential efficacy of these inhibitors in accelerating cutaneous wound healing. Taken together, these data revealed that TNF inhibitors exhibited differential levels of efficacy in accelerating cutaneous wound healing in the impaired wound-healing model in vivo.

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