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Effect of FGF10 monoclonal antibody on psoriasis-like model in guinea pigs

机译:FGF10单克隆抗体对豚鼠牛皮癣样模型的影响

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摘要

Objective: To investigate the therapeutical effect of topical application of FGF10 monoclonal antibody on the guinea pig model with psoriasis. Methods: Blank group, model group, hydrocortisone butyrate treatment group and high-dose (0.188mg/ml), middle-dose (0.094mg/ml) and low-dose (0.063mg/ml) FGF10 antibody group were set, respectively. After two-week treatment, pathological changes of psoriasis-like models were observed by HE staining, and the difference in VEGF and PCNA expression levels among different groups was observed by immunohistochemical staining. Results: All the test indicators of each treatment group were lower than those of the model group, and there was a significant difference (P<0.05). The inflammatory cell count of the high-dose FGF10 antibody group was not statistically different from those of the blank group (t=0.77, P=0.443), and the counts of the rest treatment groups were significantly higher than those of the blank group and the high-dose FGF10 antibody group (P<0.05). The epidermal thickness of each FGF10 antibody treatment group was significantly higher than that of hydrocortisone butyrate treatment group (P<0.05), while no statistical difference was found in the epidermal thickness among the FGF10 antibody treatment groups (P>0.05). FGF10 monoclonal antibodies can reduce the PCNA and VEGF expression in psoriasis-like model of guinea pig’s ear. Conclusion: FGF10 monoclonal antibodies can affect keratinocyte proliferation and division and can also significantly inhibit the inflammatory response in the psoriasis model. Meanwhile, FGF10 monoclonal antibodies can produce a therapeutic effect on psoriatic lesions by inhibiting the abnormal epidermis cell proliferation and neovascularization of the dermis in the psoriasis model.
机译:目的:探讨局部应用FGF10单克隆抗体对牛皮癣豚鼠的治疗作用。方法:分别设置空白组,模型组,丁酸氢化可的松治疗组,高剂量(0.188mg / ml),中剂量(0.094mg / ml)和低剂量(0.063mg / ml)FGF10抗体组。治疗两周后,HE染色观察牛皮癣样模型的病理变化,免疫组化染色观察不同组间VEGF和PCNA表达水平的差异。结果:各治疗组各项指标均低于模型组,差异有统计学意义(P <0.05)。大剂量FGF10抗体组的炎症细胞计数与空白组无统计学差异(t = 0.77,P = 0.443),其余治疗组的计数明显高于空白组和高剂量FGF10抗体组(P <0.05)。每个FGF10抗体治疗组的表皮厚度显着高于丁酸氢化可的松治疗组(P <0.05),而在FGF10抗体治疗组之间的表皮厚度无统计学差异(P> 0.05)。 FGF10单克隆抗体可以降低豚鼠银屑病样模型中PCNA和VEGF的表达。结论:FGF10单克隆抗体可影响牛皮癣模型角质形成细胞的增殖和分裂,并能明显抑制炎症反应。同时,FGF10单克隆抗体可通过抑制牛皮癣模型中异常的表皮细胞增殖和真皮的新血管形成来对牛皮癣病变产生治疗作用。

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