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旨在阐明 SirT1 在骨关节炎中的作用。

Towards elucidating the role of SirT1 in osteoarthritis.

机构信息

Head Laboratory of Cartilage Biology, Institute of Dental Sciences, Faculty of Dental Medicine, Hebrew University- Hadassah Ein Kerem P. O. Box 12272, Jerusalem 91120, Israel.

出版信息

Front Biosci (Landmark Ed). 2013 Jan 1;18(1):343-55. doi: 10.2741/4105.

Abstract

Osteoarthritis (OA) is a degenerative joint disease particularly affecting the elderly population. Although several genetic features have been characterized as risk factors for OA susceptibility, a growing body of evidence indicates that epigenetic effectors may also modulate gene expression and thus contribute to OA pathology. One such epigenetic regulator of particular relevance to OA is Silent Information Regulator 2 type 1 (SirT1) which has been linked to aging and caloric intake, Consistently, SirT1 has been also connected with various age-associated diseases such as diabetes type II, Alzheimers and osteoporosis. Recent reports show that OA is linked to changes in SirT1 activity or levels within cartilage. In human chondrocytes, SirT1 plays a role in cartilage extracellular matrix (ECM) synthesis and promotes cell survival, even under proinflammatory stress. It appears that SirT1 fine tunes many cellular biochemical processes through its capacity to interact and modify various histone and non-histone proteins. Taken together these investigations demonstrate that SirT1 is involved in cartilage biology and could potentially serve as novel drug target in treating OA even at its premature stages, thereby possibly reversing mechanical-stress induced cartilage degeneration.

摘要

骨关节炎(OA)是一种退行性关节疾病,尤其影响老年人群体。尽管已经确定了一些遗传特征是 OA 易感性的风险因素,但越来越多的证据表明,表观遗传效应物也可能调节基因表达,从而导致 OA 病理学发生。沉默信息调节因子 2 型 1(SirT1)是一种与衰老和热量摄入有关的表观遗传调节剂,与 OA 特别相关。一直以来,SirT1 与各种与年龄相关的疾病有关,如 2 型糖尿病、阿尔茨海默病和骨质疏松症。最近的报告表明,OA 与软骨内 SirT1 活性或水平的变化有关。在人软骨细胞中,SirT1 在外基质(ECM)合成和促进细胞存活中发挥作用,即使在促炎应激下也是如此。SirT1 似乎通过与各种组蛋白和非组蛋白蛋白相互作用和修饰来微调许多细胞生化过程。总之,这些研究表明,SirT1 参与软骨生物学,并且可能作为治疗 OA 的新型药物靶点,甚至在早期阶段,从而可能逆转机械应激诱导的软骨退化。

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