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Profiling IgG N-glycans as potential biomarker of chronological and biological ages A community-based study in a Han Chinese population

机译:分析IgG N-聚糖作为年代和生物年龄的潜在生物标记物一项基于汉族人群的社区研究

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As an important post-translation modifying process, glycosylation significantly affects the structure and function of immunoglobulin G (IgG) molecules and is essential in many steps of the inflammatory cascade. Studies have demonstrated the potential of using glycosylation features of IgG as a component of predictive biomarkers for chronological age in several European populations, whereas no study has been reported in Chinese. Herein, we report various patterns of changes in IgG glycosylation associated with age by analyzing IgG glycosylation in 701 community-based Han Chinese (244 males, 457 females; 23-68 years old). Eleven IgG glycans, including FA2B, A2G1, FA2[6]G1, FA2[3]G1, FA2[6]BG1, FA2[3]BG1, A2G2, A2BG2, FA2G2, FA2G2S1, and FA2G2S2, change considerably with age and specific combinations of these glycan features can explain 23.3% to 45.4% of the variance in chronological age in this population. This indicates that these combinations of glycan features provide more predictive information than other single markers of biological age such as telomere length. In addition, the clinical traits such as fasting plasma glucose and aspartate aminotransferase associated with biological age are strongly correlated with the combined glycan features. We conclude that IgG glycosylation appears to correlate with both chronological and biological ages, and thus its possible role in the aging process merits further study.
机译:作为重要的翻译后修饰过程,糖基化会显着影响免疫球蛋白G(IgG)分子的结构和功能,并且在炎症级联反应的许多步骤中都至关重要。研究表明,在多个欧洲人群中,将IgG的糖基化功能用作预测生物标志物的时间顺序的潜力,而中国尚未有研究报道。本文中,我们通过分析701位社区汉族(244位男性,457位女性; 23-68岁)的IgG糖基化来报告与年龄相关的IgG糖基化变化的各种模式。 11种IgG聚糖,包括FA2B,A2G1,FA2 [6] G1,FA2 [3] G1,FA2 [6] BG1,FA2 [3] BG1,A2G2,A2BG2,FA2G2,FA2G2S1和FA2G2S2随年龄和特定因素而变化很大这些聚糖特征的组合可以解释该人群按时间顺序的年龄变化的23.3%至45.4%。这表明这些聚糖特征的组合比生物学年龄的其他单个标记(例如端粒长度)提供了更多的预测信息。另外,与生物年龄相关的诸如空腹血糖和天冬氨酸转氨酶等临床特征与综合的聚糖特征密切相关。我们得出结论,IgG糖基化似乎与年代和生物学年龄相关,因此它在衰老过程中的可能作用值得进一步研究。

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