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鞣花酸和单宁酸可保护新合成的弹性纤维,使其在真皮成纤维细胞培养中免受过早的酶降解。

Ellagic and tannic acids protect newly synthesized elastic fibers from premature enzymatic degradation in dermal fibroblast cultures.

作者信息

Jimenez Felipe, Mitts Thomas F, Liu Kela, Wang Yanting, Hinek Aleksander

机构信息

Research Department, Human Matrix Sciences, LLC, Visalia, California, USA.

出版信息

J Invest Dermatol. 2006 Jun;126(6):1272-80. doi: 10.1038/sj.jid.5700285.

Abstract

Progressive proteolytic degradation of cutaneous elastic fibers, that cannot be adequately replaced or repaired by adult dermal fibroblasts, constitutes a major feature of aging skin. Our present investigations, employing monolayer cultures of human dermal fibroblasts and organ cultures of skin biopsies, were aimed at testing whether the hydrophilic tannic acid (TA) and lipophilic ellagic acid (EA) would protect dermal elastin from exogenous and endogenous enzymatic degradation. Results from both culture systems indicated that dermal fibroblasts, maintained with TA or EA, deposit significantly more elastic fibers than untreated control cultures despite the fact that neither polyphenol enhanced transcription of elastin mRNA or cellular proliferation. Results of a pulse and chase experiment showed that pretreatment with both polyphenols enhanced biostability of tropoelastin and newly deposited elastin. Results of in vitro assays indicated that both polyphenols bound to purified elastin and significantly decreased its proteolytic degradation by elastolytic enzymes belonging to the serine proteinase, cysteine proteinase, and metallo-proteinase families. Importantly, both polyphenols also synergistically enhanced elastogenesis induced by selected elastogenic compounds in cultures of dermal fibroblasts. We propose that EA and TA may be useful for preventing proteolytic degradation of existing dermal elastic fibers and for enhancing more efficient elastogenesis in aged skin.

摘要

皮肤弹性纤维的渐进性蛋白水解降解是衰老皮肤的一个主要特征,而成人真皮成纤维细胞无法充分替代或修复这种降解。我们目前的研究采用人真皮成纤维细胞单层培养和皮肤活检组织块培养,旨在测试亲水性单宁酸(TA)和亲脂性鞣花酸(EA)是否能保护真皮弹性蛋白免受外源性和内源性酶解降解。两种培养系统的结果均表明,用TA或EA培养的真皮成纤维细胞沉积的弹性纤维明显多于未处理的对照培养物,尽管这两种多酚均未增强弹性蛋白mRNA的转录或细胞增殖。脉冲追踪实验结果表明,两种多酚预处理均增强了原弹性蛋白和新沉积弹性蛋白的生物稳定性。体外分析结果表明,两种多酚均与纯化的弹性蛋白结合,并显著降低其被丝氨酸蛋白酶、半胱氨酸蛋白酶和金属蛋白酶家族的弹性水解酶的蛋白水解降解。重要的是,两种多酚还协同增强了真皮成纤维细胞培养物中选定的促弹性生成化合物诱导的弹性生成。我们认为,EA和TA可能有助于预防现有真皮弹性纤维的蛋白水解降解,并在衰老皮肤中增强更有效的弹性生成。

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