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一种用于研究杜普伊特伦挛缩症分子发病机制的综合蛋白质组学方法。

An integrated proteomics approach for studying the molecular pathogenesis of Dupuytren's disease.

作者信息

Kraljevic Pavelic Sandra, Sedic Mirela, Hock Karlo, Vucinic Srdan, Jurisic Davor, Gehrig Peter, Scott Mike, Schlapbach Ralph, Cacev Tamara, Kapitanovic Sanja, Pavelic Kresimir

机构信息

Division of Molecular Medicine, Rudjer Boskovic Institute, Bijenicka Cesta 54, 10000 Zagreb, Croatia.

出版信息

J Pathol. 2009 Mar;217(4):524-33. doi: 10.1002/path.2483.

Abstract

Dupuytren's disease (DD) is a fibromatosis characterized by non-malignant transformation of palmar fascia leading to permanent contraction of one or more fingers. Despite the extensive knowledge of its clinical pathogenesis, the aetiology of this disease remains obscure. In the present paper, we report for the first time on the proteomic profiling of diseased versus unaffected patient-matched palmar fasciae tissues from DD patients using two-dimensional gel electrophoresis coupled with mass spectrometry analysis. The herein identified proteins were then used to create the protein-protein interaction network (interactome). Such an integrated approach revealed the involvement of several different molecular processes related to DD progression, including extra- and intra-cellular signalling, oxidative stress, cytoskeletal changes, and alterations in cellular metabolism. In particular, autocrine regulation through ERBB-2 and IGF-1R receptors and the Akt signalling pathway have emerged as novel components of pro-survival signalling in Dupuytren's fibroblasts and thus might provide a basis for a new therapeutic strategy in Dupuytren's disease.

摘要

掌腱膜挛缩症(DD)是一种纤维瘤病,其特征是掌腱膜发生非恶性转化,导致一个或多个手指永久性挛缩。尽管对其临床发病机制已有广泛了解,但该疾病的病因仍不清楚。在本文中,我们首次报告了使用二维凝胶电泳结合质谱分析对DD患者患病与未患病的配对掌腱膜组织进行蛋白质组分析的结果。然后,利用本文鉴定出的蛋白质构建蛋白质-蛋白质相互作用网络(相互作用组)。这种综合方法揭示了与DD进展相关的几个不同分子过程的参与,包括细胞外和细胞内信号传导、氧化应激、细胞骨架变化以及细胞代谢改变。特别是,通过ERBB-2和IGF-1R受体的自分泌调节以及Akt信号通路已成为掌腱膜成纤维细胞中促生存信号的新成分,因此可能为掌腱膜挛缩症的新治疗策略提供基础。

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