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在一项随机自身试验中观察到真皮再生后表皮 DNAH10 表达增加 - 对银屑病炎症的思考。

Discovery of increased epidermal DNAH10 expression after regeneration of dermis in a randomized with-in person trial - reflections on psoriatic inflammation.

机构信息

Helsinki Burn Centre, Department of Plastic Surgery, Helsinki University Hospital, University of Helsinki, Helsinki, Finland.

Department of Cell Biology, Institute of Molecular and Cell Biology, University of Tartu, Tartu, Estonia.

出版信息

Sci Rep. 2019 Dec 13;9(1):19136. doi: 10.1038/s41598-019-53874-z.

Abstract

Because molecular memories of past inflammatory events can persist in epidermal cells, we evaluated the long-term epidermal protein expression landscapes after dermal regeneration and in psoriatic inflammation. We first characterized the effects of two dermal regeneration strategies on transplants of indicator split-thickness skin grafts (STSGs) in ten adult patients with deep burns covering more than 20% of their body surface area. After fascial excision, three adjacent areas within the wound were randomized to receive a permanent dermal matrix, a temporary granulation-tissue-inducing dressing or no dermal component as control. Control areas were covered with STSG immediately, and treated areas after two-weeks of dermis formation. Epidermis-dermis-targeted proteomics of one-year-follow-up samples were performed for protein expression profiling. Epidermal expression of axonemal dynein heavy chain 10 (DNAH10) was increased 20-fold in samples having had regenerating dermis vs control. Given the dermal inflammatory component found in our dermal regeneration samples as well as in early psoriatic lesions, we hypothesized that DNAH10 protein expression also would be affected in psoriatic skin samples. We discovered increased DNAH10 expression in inflammatory lesions when compared to unaffected skin. Our results associate DNAH10 expression with cell proliferation and inflammation as well as with the epidermal memory resulting from the previous regenerative signals of dermis. This study (ISRCTN14499986) was funded by the Finnish Ministry of Defense and by government subsidies for medical research.

摘要

由于过去炎症事件的分子记忆可以在表皮细胞中持续存在,因此我们评估了真皮再生和银屑病炎症后长期的表皮蛋白表达谱。我们首先描述了两种真皮再生策略对十位深度烧伤面积超过 20%的成年患者的指示性分层皮肤移植物(STSG)移植的影响。在筋膜切除后,伤口内的三个相邻区域被随机分为永久性真皮基质、临时肉芽组织诱导敷料或无真皮成分的对照组。对照组立即用 STSG 覆盖,治疗组在形成真皮两周后进行治疗。对一年随访样本进行表皮-真皮靶向蛋白质组学研究,以进行蛋白质表达谱分析。与对照组相比,有再生真皮的样本中轴丝动力蛋白重链 10(DNAH10)的表皮表达增加了 20 倍。鉴于我们的真皮再生样本以及早期银屑病病变中存在真皮炎症成分,我们假设 DNAH10 蛋白表达也会受到银屑病皮肤样本的影响。与未受影响的皮肤相比,我们发现炎症病变中 DNAH10 的表达增加。我们的研究结果将 DNAH10 的表达与细胞增殖和炎症以及由先前真皮再生信号引起的表皮记忆联系起来。这项研究(ISRCTN14499986)由芬兰国防部和政府医疗研究补贴资助。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/df62/6910998/736cfdbc265e/41598_2019_53874_Fig1_HTML.jpg

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