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钙通道阻滞剂、类固醇和干扰素治疗增生性瘢痕中核心蛋白聚糖和基质金属蛋白酶13基因表达的比较:一项携带人瘢痕的动物模型研究。

A Comparison of Gene Expression of Decorin and MMP13 in Hypertrophic Scars Treated With Calcium Channel Blocker, Steroid, and Interferon: A Human-Scar-Carrying Animal Model Study.

作者信息

Yang Shih-Yi, Yang Jui-Yung, Hsiao Yen-Chang, Chuang Shiow-Shuh

机构信息

Department of Plastic Surgery, Linkou Burn Center, Chang Gung Memorial Hospital, Chang Gung University, Taipei, Taiwan.

出版信息

Dermatol Surg. 2017 Jan;43 Suppl 1:S37-S46. doi: 10.1097/DSS.0000000000000990.

Abstract

BACKGROUND

The formation of hypertrophic scaring (HSc) is an abnormal wound-healing response. In a previous study, an animal model with human scar tissue implanted into nude mice (BALB/c) has been successfully established. The effects of verapamil as well as combination therapy with verapamil and kenacort have been studied and compared.

OBJECTIVE

To treat persistent hypertrophic scars, local injection of drugs composed of steroids, calcium channel blockers (CCBs), and interferon might be a good method. What is the best dose of the regimen and what are the mechanisms are also a worthwhile study.

MATERIALS AND METHODS

Scar specimens were harvested from patients with HSc or Keloid resulting from burn injury, and then implanted to BALB/c-nu nude mice for 4 weeks. Before implantation, the specimen was either injected with or without drugs such as steroids (kenacort), CCBs (verapamil), and interferons (INFα2b), respectively. After the removal of implants, quantitative gene expressions of decorin and collagenase (MMP13) were measured using a real-time polymerase chain reaction to detect their mRNAs. Two way-ANOVA and Post Hoc were used for statistical analysis using the software SPSS 15.0.

RESULTS

All drug-treated groups increased the expressions of decorin and MMP13 in comparison with those in noninjected group (p < .001) in a dose-dependent manner. Comparing equal amounts of individual drugs, gene expression of decorin was increased with increasing injection amount, and the best result in low amount of injection (0.02 mL of each) was shown in the group injected with INFα2b followed by kenacort and verapamil. However, the results were changed while injection amount was up to 0.04 mL and the strongest decorin gene expression was found in kenacort injection. Regarding MMP-13 expression, low-amount injection (0.02 mL) of INFα2b has strongest gene expression followed by kenacort and verapamil, but in the large-amount regimes (0.04 mL), verapamil had strongest gene expression followed by INFα2b and kenacort.

CONCLUSION

This study showed that the kenacort, verapamil, and INFα2b all inhibited HSc in a dose-dependent manner through the evidence of gene expression of decorin and MMP13. In comparison with the injections between small amounts of drugs, INFα2b potentiated the strongest decorin and MMP13 expression. On the contrary, among the large-amount injection regimes, kenacrot was more effective on decorin expression as verapamil to MMP13 expression. To decrease side effects from the drugs and produce promising results for the clinical practice, it is suggested to maintain the dose of INFα2b along with an increased dose of verapamil for HSc improvement.

摘要

背景

增生性瘢痕(HSc)的形成是一种异常的伤口愈合反应。在先前的一项研究中,已成功建立了将人瘢痕组织植入裸鼠(BALB/c)的动物模型。研究并比较了维拉帕米以及维拉帕米与康宁克通联合治疗的效果。

目的

局部注射由类固醇、钙通道阻滞剂(CCB)和干扰素组成的药物可能是治疗持续性增生性瘢痕的一种好方法。该方案的最佳剂量以及作用机制也是一项值得研究的内容。

材料与方法

从烧伤后出现增生性瘢痕或瘢痕疙瘩的患者身上采集瘢痕标本,然后植入BALB/c-nu裸鼠体内4周。植入前,标本分别注射或不注射类固醇(康宁克通)、CCB(维拉帕米)和干扰素(INFα2b)等药物。取出植入物后,使用实时聚合酶链反应测量核心蛋白聚糖和胶原酶(MMP13)的定量基因表达,以检测它们的mRNA。使用SPSS 15.0软件进行双向方差分析和事后检验进行统计分析。

结果

与未注射组相比,所有药物治疗组核心蛋白聚糖和MMP13的表达均呈剂量依赖性增加(p <.001)。比较等量的单一药物,核心蛋白聚糖的基因表达随注射量增加而增加,在低注射量(每种0.02 mL)时,注射INFα2b组的效果最佳,其次是康宁克通和维拉帕米组。然而,当注射量达到0.04 mL时结果发生变化,康宁克通注射组核心蛋白聚糖基因表达最强。关于MMP-13表达,低注射量(0.02 mL)的INFα2b基因表达最强,其次是康宁克通和维拉帕米,但在高注射量(0.04 mL)时,维拉帕米基因表达最强,其次是INFα2b和康宁克通。

结论

本研究表明,根据核心蛋白聚糖和MMP13的基因表达证据,康宁克通、维拉帕米和INFα2b均以剂量依赖性方式抑制增生性瘢痕。与少量药物注射相比,INFα2b增强核心蛋白聚糖和MMP13的表达最强。相反,在高注射量方案中,康宁克通对核心蛋白聚糖表达的效果比维拉帕米对MMP13表达的效果更好。为减少药物副作用并在临床实践中产生良好效果,建议维持INFα2b的剂量并增加维拉帕米的剂量以改善增生性瘢痕。

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