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皮肤细胞和组织在低度炎症条件下对交联透明质酸的反应。

Skin Cell and Tissue Responses to Cross-Linked Hyaluronic Acid in Low-Grade Inflammatory Conditions.

作者信息

Sanchez Benjamin, Ferraro Sandra, Josset-Lamaugarny Audrey, Pagnon Aurélie, Hee Charlie K, Nakab Lauren, Sigaudo-Roussel Dominique, Fromy Bérengère

机构信息

Laboratoire Biologie Tissulaire et Ingénierie Thérapeutique, Centre national de la recherche scientifique (CNRS), UMR 5305, LBTI, 7 Passage du Vercors, F-69367 Lyon cedex 7, France.

University of Lyon 1, UMR 5305, LBTI, 7 Passage du Vercors, F-69367 Lyon cedex 7, France.

出版信息

Int J Inflam. 2023 Aug 26;2023:3001080. doi: 10.1155/2023/3001080. eCollection 2023.

Abstract

Hyaluronic acid (HA), used in a variety of medical applications, is associated in rare instances to long-term adverse effects. Although the aetiology of these events is unknown, a number of hypotheses have been proposed, including low molecular weight of HA (LMW-HA) in the filler products. We hypothesized that cross-linked HA and its degradation products, in a low-grade inflammatory microenvironment, could impact immune responses that could affect cell behaviours in the dermis. Using two different cross-linking technologies VYC-15L and HYC-24L+, and their hyaluronidase-induced degradation products, we observed for nondegraded HA, VYC-15L and HYC-24L+, a moderate and transient increase in IL-1, TNF- in M1 macrophages under low-grade inflammatory conditions. Endothelial cells and fibroblasts were preconditioned using inflammatory medium produced by M1 macrophages. 24 h after LMW-HA fragments and HA stimulation, no cytokine was released in these preconditioned cells. To further characterize HA responses, we used a novel murine model exhibiting a systemic low-grade inflammatory phenotype. The intradermal injection of VYC-15L and its degradation products induced an inflammation and cell infiltration into the skin that was more pronounced than those by HYC-24L+. This acute cutaneous inflammation was likely due to mechanical effects due to filler injection and tissue integration rather than its biological effects on inflammation. VYC-15L and its degradation product potentiated microvascular response to acetylcholine in the presence of a low-grade inflammation. The different responses with 2D cell models and mouse model using the two tested cross-linking HA technologies showed the importance to use integrative complex model to better understand the effects of HA products according to inflammatory state.

摘要

透明质酸(HA)被用于多种医学应用中,在罕见情况下与长期不良反应相关。尽管这些事件的病因尚不清楚,但已经提出了一些假设,包括填充产品中低分子量HA(LMW-HA)的作用。我们假设,在低度炎症微环境中,交联HA及其降解产物可能会影响免疫反应,进而影响真皮中的细胞行为。使用两种不同的交联技术VYC-15L和HYC-24L+及其透明质酸酶诱导的降解产物,我们观察到,在低度炎症条件下,未降解的HA、VYC-15L和HYC-24L+会使M1巨噬细胞中的IL-1、TNF出现适度且短暂的增加。内皮细胞和成纤维细胞使用M1巨噬细胞产生的炎性培养基进行预处理。在LMW-HA片段和HA刺激24小时后,这些预处理细胞中未释放细胞因子。为了进一步表征HA的反应,我们使用了一种表现出系统性低度炎症表型的新型小鼠模型。皮内注射VYC-15L及其降解产物会引起皮肤炎症和细胞浸润,比HYC-24L+引起的更明显。这种急性皮肤炎症可能是由于填充剂注射和组织整合产生的机械效应,而非其对炎症的生物学效应。在低度炎症存在的情况下VYC-15L及其降解产物增强了微血管对乙酰胆碱的反应。使用两种测试的交联HA技术,二维细胞模型和小鼠模型呈现出不同的反应,这表明使用综合复杂模型对于根据炎症状态更好地理解HA产品的效果非常重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/994e/10474960/3f832d71cc98/IJI2023-3001080.001.jpg

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