与基质金属蛋白酶介导的细胞外基质重塑相关的病理中多糖碎片化。

Federica Genovese, Natasha Barascuk, Lise Larsen, Martin Røssel Larsen, Arkadiusz Nawrocki, Yili Li, Qinlong Zheng, Jianxia Wang, Sanne Skovgård Veidal, Diana Julie Leeming, Morten Asser Karsdal
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The scope of the present study was to develop a novel enzyme-linked immunosorbent assay (ELISA) for the measurement of a MMP-9 and MMP-12-generated biglycan neo-epitope and to test its biological validity in a rat model of RA and in two rat models of liver fibrosis, chosen as models of ECMR.</p><p><strong>Results: </strong>Biglycan was cleaved in vitro by MMP-9 and -12 and the 344'YWEVQPATFR'353 peptide (BGM) was chosen as a potential neo-epitope. A technically sound competitive ELISA for the measurement of BGM was generated and the assay was validated in a bovine cartilage explant culture (BEX), in a collagen induced model of rheumatoid arthritis (CIA) and in two different rat models of liver fibrosis: the carbon tetrachloride (CCL4)-induced fibrosis model, and the bile duct ligation (BDL) model. 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引用次数: 53

摘要

背景:蛋白多糖多糖(BGN)参与胶原原纤维的组装,其断裂可能与细胞外基质重塑(ECMR)失调疾病(如类风湿关节炎(RA)和肝纤维化)发病过程中的胶原周转有关。本研究的范围是开发一种新的酶联免疫吸附试验(ELISA),用于测量MMP-9和mmp -12产生的高聚糖新表位,并在RA大鼠模型和两种肝纤维化大鼠模型中测试其生物学有效性,这两种模型被选为ECMR模型。结果:Biglycan被MMP-9和-12体外切割,344'YWEVQPATFR'353肽(BGM)被选为潜在的新表位。生成了一种技术上合理且具有竞争力的测定BGM的ELISA,并在牛软骨外植体培养(BEX)、胶原诱导的类风湿性关节炎模型(CIA)和两种不同的大鼠肝纤维化模型(四氯化碳(CCL4)诱导的纤维化模型和胆管结扎(BDL)模型中进行了验证。与对照组相比,CIA大鼠血清BGM显著升高,与对照组相比,CCL4治疗16周和20周的大鼠血清BGM显著升高,与假手术组相比,BDL治疗各组大鼠血清BGM显著升高。此外,血清BGM水平与CCL4模型肝切片天狼星红染色测定的肝纤维化程度有显著相关性。结论:我们证明了mmp降解大聚糖的特异性组织重塑产物,即新表位BGM,与病理ECMR相关。该检测既代表了ECM转换的新标志物,也代表了一种潜在的新工具,可以阐明biglycan在ECMR相关病理过程中的作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Biglycan fragmentation in pathologies associated with extracellular matrix remodeling by matrix metalloproteinases.

Background: The proteoglycan biglycan (BGN) is involved in collagen fibril assembly and its fragmentation is likely to be associated with collagen turnover during the pathogenesis of diseases which involve dysregulated extracellular matrix remodeling (ECMR), such as rheumatoid arthritis (RA) and liver fibrosis. The scope of the present study was to develop a novel enzyme-linked immunosorbent assay (ELISA) for the measurement of a MMP-9 and MMP-12-generated biglycan neo-epitope and to test its biological validity in a rat model of RA and in two rat models of liver fibrosis, chosen as models of ECMR.

Results: Biglycan was cleaved in vitro by MMP-9 and -12 and the 344'YWEVQPATFR'353 peptide (BGM) was chosen as a potential neo-epitope. A technically sound competitive ELISA for the measurement of BGM was generated and the assay was validated in a bovine cartilage explant culture (BEX), in a collagen induced model of rheumatoid arthritis (CIA) and in two different rat models of liver fibrosis: the carbon tetrachloride (CCL4)-induced fibrosis model, and the bile duct ligation (BDL) model. Significant elevation in serum BGM was found in CIA rats compared to controls, in rats treated with CCL4 for 16 weeks and 20 weeks compared to the control groups as well as in all groups of rats subject to BDL compared with sham operated groups. Furthermore, there was a significant correlation of serum BGM levels with the extent of liver fibrosis determined by the Sirius red staining of liver sections in the CCL4 model.

Conclusion: We demonstrated that the specific tissue remodeling product of MMPs-degraded biglycan, namely the neo-epitope BGM, is correlated with pathological ECMR. This assay represents both a novel marker of ECM turnover and a potential new tool to elucidate biglycan role during the pathological processes associated with ECMR.

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