自体富血小板凝胶通过抑制噬铁蛋白加速糖尿病伤口愈合

Daoai Wu, Ping Zhu, Zhaoming Shi, Chen Li, Chenchen Wu, Weihua Sun, Jianmin Ran
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摘要

目的:研究自体富血小板凝胶(APG)治疗糖尿病伤口的疗效,并探讨 APG 与噬铁蛋白之间的关联。研究方法共纳入 32 名糖尿病足(DF)患者和 Wagner 1 至 2 级患者。在 APG 组中,DF 患者每周接受一次 APG 治疗。在非 APG 组中,DF 患者接受每日换药。流式细胞术量化了第 0 天和第 10 天外周血中内皮祖细胞 (EPC) 的比例。使用链脲佐菌素诱导糖尿病大鼠模型。大鼠背部有两个圆形皮肤伤口。正常血糖组每天更换伤口敷料。在糖尿病组中,左侧伤口每天换药,而右侧伤口每周用 APG 处理一次。皮肤损伤 7 天后检测 CD34 水平。14 天后对谷胱甘肽过氧化物酶 4 (GPX4)、核受体辅激活因子 4 (NCOA4)、轻链 3 (LC3) 和马森染色的水平进行量化。不分 DF 患者或糖尿病大鼠,分别测定损伤后 0 天和 14 天的伤口面积和伤口愈合率。结果显示无论 DF 患者还是糖尿病大鼠,APG 组的伤口愈合率均高于非 APG 组。APG 组 DF 患者的ΔEPCs%高于非 APG 组。在大鼠实验方面,APG 组的 NCOA4 和 LC3 表达水平较低,伤口愈合时间较短。然而,与非 APG 组相比,APG 组的 CD34 表达、GPX4 蛋白和胶原纤维水平更高。结论自体富血小板凝胶可加快糖尿病人群和大鼠的伤口愈合速度。自体富血小板凝胶促进了 EPCs 数量、胶原纤维体积和血管数量。自体富血小板凝胶降低了 LC3 和 NCOA4 的表达,但增加了 GPX4 蛋白的表达。可能的机制是抑制了噬铁蛋白。
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Autologous Platelet-Rich Gel Accelerates Diabetic Wound Healing Through Inhibition of Ferritinophagy.

Aims: The objective was to examine the efficacy of autologous platelet-rich gel (APG) in treating diabetic wound and investigate the association between APG and ferritinophagy. Methods: A total of 32 patients with diabetic foot (DF) and Wagner grade 1 to 2 were included. Within the APG group, individuals with DF received weekly APG treatment. In the non-APG group, DF patients received daily dressing changes. Flow cytometry quantified the proportion of endothelial progenitor cells (EPCs) in peripheral blood on days 0 and 10. The diabetic rat model was induced using Streptozotocin. Two circular skin wounds were created on the backs of rats. The normal glucose group received daily dressing changes on the wound. In the diabetic group, the left wound underwent daily dressing changes, whereas the right wound was treated with APG once a week. CD34 levels were tested 7 days after the skin damage. The levels of glutathione peroxidase 4 (GPX4), Nuclear Receptor Coactivator 4 (NCOA4), Light chain 3 (LC3), and Masson staining were quantified on 14 days. The wound area and wound healing rate were separately measured at 0 and 14 days after the injury, regardless of DF patients or diabetic rats. Results: The wound healing rate was higher in the APG group than in the non-APG group, regardless of DF patients or diabetic rats. The APG group had a greater ΔEPCs% in DF patients than the non-APG group. Regarding rat experiment, the APG group exhibited lower levels of NCOA4, and LC3 expressions and a shorter wound healing time. However, the APG group showed higher levels of CD34 expression, GPX4 protein, and collagen fibers than the non-APG group. Conclusions: Autologous platelet-rich gel accelerated the wound healing rate in diabetic populations and rats. Autologous platelet-rich gel promoted EPCs counts, collagen fiber volume, and vessel numbers. Autologous platelet-rich gel decreased LC3 and NCOA4 expression, but increased GPX4 protein expression. The possible mechanism was the inhibition of ferritinophagy.

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