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Enrichment of Collagen Fragments Using Dimeric Collagen Hybridizing Peptide for Urinary Collagenomics

机译:使用二聚体胶原杂交杂交尿蛋白酶富集胶原片的富集

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Collagen remodeling in normal and pathologic conditions releases numerous collagen fragments into biological fluids. Although a few collagen fragments have been tested as biomarkers for disease indication, most occur at trace levels, making them nearly impossible to detect even with modem analytical tools. Here we report a new way to enrich collagen fragments that allows complete peptidomic analysis of collagen fragments in urine. Enrichment is made possible by dimeric collagen hybridizing peptides (CHPs) that bind collagen fragments originating from the triple helical regions of all collagen types with minimal sequence bias. LC-MS/MS analysis of enriched mouse urine revealed an average of 383 collagenous peptide fragments per sample (compared to 34 for unenriched sample), which could be mapped to all types of mouse collagens in the SwissProt database including FACITs and MACITs. Hierarchical clustering of a selected panel of the detected fragments separated osteopenic mice from healthy mice. The results demonstrate dimeric CHP's ability to enrich collagen fragments from biological fluid and its potential to aid peptidomics-based disease detection and biomarker discovery.
机译:在正常和病理条件下重塑的胶原蛋白重塑将许多胶原碎片释放到生物流体中。虽然已经测试了少量胶原蛋白片段作为疾病指示的生物标志物,但大多数发生在痕量水平上,使它们几乎不可能通过调制解调器分析工具检测。在这里,我们报告了富含胶原蛋白片段的新方法,允许尿的胶原蛋白片段完全肽蛋白分析。通过二聚体胶原杂交肽(CHP)可以用最小序列偏压结合源自所有胶原类型的三重螺旋区域的胶原片段的富集。富集小鼠尿液的LC-MS / MS分析显示每个样品的平均383个胶原肽片段(与未成种样品相比的34相比),其可以映射到Swissprot数据库中的所有类型的小鼠胶原蛋白,包括Facits和Macits。检测到的片段的选定面板的分层聚类分离了来自健康小鼠的骨细胞。结果表明二聚体CHP富集生物流体的胶原蛋白片段的能力及其有助于帮助肽族病毒疾病检测和生物标志物发现。

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