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通过 Glucono-δ-内酯使胶原原纤维崩解:纤维化崩解的一个潜在线索。

Disintegration of collagen fibrils by Glucono-δ-lactone: An implied lead for disintegration of fibrosis.

机构信息

Bioorganic Chemistry Laboratory, Council of Scientific and Industrial Research (CSIR) - Central Leather Research Institute (CLRI), Adyar, Chennai 600020, India; Academy of Scientific and Innovative Research (AcSIR), CSIR-CLRI Campus, Chennai 600020, India.

Academy of Scientific and Innovative Research (AcSIR), CSIR-CLRI Campus, Chennai 600020, India; NMR laboratory (Inorganic & Physical Chemistry Department), Council of Scientific and Industrial Research (CSIR) - Central Leather Research Institute (CLRI), Adyar, Chennai 600020, India.

出版信息

Int J Biol Macromol. 2018 Feb;107(Pt A):175-185. doi: 10.1016/j.ijbiomac.2017.08.158. Epub 2017 Sep 1.

Abstract

Excess accumulation of collagen (fibrosis) undergoes self-aggregation, which leads to fibrillar collagen, on the extracellular matrix is the hallmark of a number of diseases such as keloids, hypertrophic scars, and systemic scleroderma. Direct inhibition or disintegration of collagen fibrils by small molecules offer a therapeutic approach to prevent or treat the diseases related to fibrosis. Herein, the anti-fibrotic property of Glucono-δ-lactone (GdL), known as acidifier, on the fibrillation and its disintegration of collagen was investigated. As collagen fibrillation is pH dependent, the pH modulation property of GdL is attractive to inhibit self-association of collagen. Optical density and microscopic data indicate that GdL elicits concentration-dependent fibril inhibition and also disintegrates pre-formed collagen fibrils. The simultaneous pH analysis showed that the modulation(lowering) of pH by GdL is the primary cause for its anti-fibrotic activity. The intact triple helical structure of collagen upon treatment of GdL suggests that collagen fibril disintegration can be achieved without affecting the native structure of collagen which is essential for any anti-fibrotic agents. Saturation transfer difference (STD) NMR result reveals that GdL is in proximity to collagen. The present results thus suggest that GdL provides a lead to design novel anti-fibrotic agents for the pathologies related to collagen deposition.

摘要

胶原(纤维)的过度积累会发生自聚集,导致细胞外基质中的纤维状胶原,这是许多疾病的特征,如瘢痕疙瘩、增生性瘢痕和系统性硬皮病。小分子对胶原纤维的直接抑制或分解为预防或治疗与纤维化相关的疾病提供了一种治疗方法。本文研究了作为酸化剂的葡萄糖酸-δ-内酯(GdL)对胶原纤维的纤维化及其分解的抗纤维化特性。由于胶原纤维的纤维化依赖于 pH 值,因此 GdL 的 pH 值调节特性很有吸引力,可以抑制胶原的自缔合。光密度和显微镜数据表明,GdL 能引发浓度依赖性的纤维抑制,还能分解预先形成的胶原纤维。同时进行的 pH 值分析表明,GdL 对 pH 值的调节(降低)是其抗纤维化活性的主要原因。GdL 处理后胶原保持完整的三螺旋结构,这表明胶原纤维的分解可以在不影响胶原天然结构的情况下实现,这对任何抗纤维化药物都是至关重要的。饱和转移差异(STD)NMR 结果表明 GdL 与胶原接近。因此,这些结果表明 GdL 为设计与胶原沉积相关的病理学的新型抗纤维化药物提供了线索。

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