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黏弹性物质通过触发 syndecan-4 途径和形成 annexin A1/S100A11 复合物来诱导角质形成细胞的激活。

Mesoglycan induces keratinocyte activation by triggering syndecan-4 pathway and the formation of the annexin A1/S100A11 complex.

机构信息

Department of Pharmacy, University of Salerno, Salerno, Italy.

Department of Primary Care, Wound Care Service, Health Local Agency Naples 3 South, Napoli, Italy.

出版信息

J Cell Physiol. 2019 Nov;234(11):20174-20192. doi: 10.1002/jcp.28618. Epub 2019 Apr 8.

DOI:10.1002/jcp.28618
PMID:30963564
Abstract

Wound healing is a dynamic process comprising multiple events, such as inflammation, re-epithelialization, and tissue remodeling. Re-epithelialization phase is characterized by the engagement of several cell populations, mainly of keratinocytes that sequentially go through cycles of migration, proliferation, and differentiation to restore skin functions. Troubles can arise during the re-epithelialization phase of skin wound healing particularly in keratinocyte migration, resulting in chronic non-healing lesions, which represent a serious clinical problem. Over the last decades, the efforts aimed to find new pharmacological approaches for wound care were made, yet almost all current therapeutic strategies used remain inadequate or even ineffective. As such, it is crucial to identify new drugs that can enable a proper regeneration of the epithelium in wounded skin. Here, we have investigated the effects of the fibrinolytic drug mesoglycan, a glycosaminoglycans mixture derived from porcine intestinal mucosa on HaCaT human keratinocytes that were used as in vitro experimental model of skin re-epithelialization. We found that mesoglycan induces keratinocyte migration and early differentiation by triggering the syndecan-4/PKCα pathway and that these effects were at least in part, because of the formation of the annexin A1/S100A11 complex. Our data suggest that mesoglycan may be useful as a new pro-healing drug for skin wound care.

摘要

伤口愈合是一个动态的过程,包括多个事件,如炎症、再上皮化和组织重塑。再上皮化阶段的特点是涉及多个细胞群体,主要是角质形成细胞,它们依次经历迁移、增殖和分化的循环,以恢复皮肤功能。在皮肤伤口愈合的再上皮化阶段可能会出现问题,特别是在角质形成细胞迁移方面,导致慢性不愈合的病变,这是一个严重的临床问题。在过去的几十年中,人们努力寻找新的伤口护理药物治疗方法,但几乎所有目前使用的治疗策略仍然不够有效。因此,识别能够使受伤皮肤适当再生上皮的新药至关重要。在这里,我们研究了纤维蛋白溶解药物黏多糖,一种从猪肠黏膜中提取的糖胺聚糖混合物对 HaCaT 人角质形成细胞的影响,HaCaT 细胞被用作皮肤再上皮化的体外实验模型。我们发现黏多糖通过触发 syndecan-4/PKCα 通路诱导角质形成细胞迁移和早期分化,并且这些作用至少部分是由于 annexin A1/S100A11 复合物的形成。我们的数据表明,黏多糖可用作皮肤伤口护理的新的促愈合药物。

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