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Proteomic analysis of the interaction of Bifidobacterium longum NCC2705 with the intestine cells Caco-2 and identification of plasminogen receptors

机译:长双歧杆菌NCC2705与肠细胞Caco-2相互作用的蛋白质组学分析和纤溶酶原受体的鉴定

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摘要

To identify proteins with a potential role in the interaction of Bifidobacterium longum with intestinal epithelial cells, we profiled the protein response of B. longum NCC2705 following interaction with Caco-2 cells. Thirty-one protein spots, belonging to a total of 23 proteins, which exhibited a change in abundance of at least 3-fold were identified in B. longum NCC2705 following co-culture with Caco-2 cells, and were subsequently identified. Changes in expression were confirmed at the transcriptional level for a selection of these proteins. Enolase (Eno) and elongation factor Tu (EF-Tu) were amongst the proteins that showed the most prominent increase in abundance. Interaction of these proteins with plasminogen (Pig) was analyzed by Pig overlay assays, glutathione S-transferase (GST)-pull down, and western blot analysis. The results suggested that EF-Tu and Eno serve as surface receptors for B. longum NCC2705 binding to human plasminogen. Purified GST-EF-Tu and GST-Eno inhibited adhesion of B. longum NCC2705 to Caco-2 cells. Collectively, our data suggest that Eno and EF-Tu moonlight as adhesions, and are possibly involved in the protective role played by B. longum NCC2705 in defense against enteric pathogens.
机译:为了鉴定在长双歧杆菌与肠上皮细胞相互作用中具有潜在作用的蛋白质,我们在与Caco-2细胞相互作用后对长双歧杆菌NCC2705的蛋白质​​反应进行了分析。与Caco-2细胞共培养后,在长双歧杆菌NCC2705中鉴定了31个蛋白质斑点,该蛋白质斑点总共显示23种蛋白质,其丰度变化至少3倍,随后被鉴定。在选择这些蛋白质的转录水平上证实了表达的变化。烯醇化酶(Eno)和延伸因子Tu(EF-Tu)是蛋白质中丰度增加最明显的蛋白质。这些蛋白与纤溶酶原(Pig)的相互作用通过Pig覆盖分析,谷胱甘肽S-转移酶(GST)-下拉和Western blot分析进行了分析。结果表明EF-Tu和Eno作为长双歧杆菌NCC2705与人纤溶酶原结合的表面受体。纯化的GST-EF-Tu和GST-Eno抑制长双歧杆菌NCC2705与Caco-2细胞的粘附。总体而言,我们的数据表明Eno和EF-Tu月光为粘连,并且可能参与了长双歧杆菌NCC2705在防御肠道病原体中的保护作用。

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