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Potential of an Interorgan Network Mediated by Toxic Advanced Glycation End-Products in a Rat Model

机译:在大鼠模型中由有毒的先进糖糖末端产品介导的中同知网络介导的潜力

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摘要

Excessive intake of glucose and fructose in beverages and foods containing high-fructose corn syrup (HFCS) plays a significant role in the progression of lifestyle-related diseases (LSRD). Glyceraldehyde-derived advanced glycation end-products (AGEs), which have been designated as toxic AGEs (TAGE), are involved in LSRD progression. Understanding of the mechanisms underlying the effects of TAGE on gene expression in the kidneys remains limited. In this study, DNA microarray analysis and quantitative real-time polymerase chain reaction (PCR) were used to investigate whether HFCS-consuming Wister rats generated increased intracellular serum TAGE levels, as well as the potential role of TAGE in liver and kidney dysfunction. HFCS consumption resulted in significant accumulation of TAGE in the serum and liver of rats, and induced changes in gene expression in the kidneys without TAGE accumulation or upregulation of receptor for AGEs (RAGE) upregulation. Changes in specific gene expression profiles in the kidney were more correlated with TAGE levels in the liver tissue than in the serum. These findings suggest a direct or indirect interaction may be present between the liver and kidneys that does not involve serum TAGE or RAGE. The involvement of internal signal transduction factors such as exosomes or cytokines without IL-1β and TNF-α is suggested to contribute to the observed changes in kidney gene expression.
机译:在饮料和含有高果糖玉米糖浆(HFC)的饮料和食物中过度摄入葡萄糖和果糖在生活方式相关疾病(LSRD)的进展中起着重要作用。甘油醛衍生的先进糖糖末期产品(年龄)被指定为有毒年龄(Tage),参与了LSRD进展。理解肾脏在肾脏基因表达对基因表达的影响仍然有限。在该研究中,使用DNA微阵列分析和定量实时聚合酶链反应(PCR)来研究HFCS消费的饮料大鼠是否产生增加的细胞内血清支架水平,以及造成肝肾功能障碍的潜在作用。 HFCS消费导致大鼠血清和肝脏造成的造成的显着积累,并且肾脏中基因表达的变化,没有Tage积累或受体的上调(RAGE)上调。肾脏中特定基因表达谱的变化与肝组织中的磁性水平更相关,而不是在血清中。这些发现表明,肝脏和肾脏之间可能存在直接或间接的相互作用,其不涉及血清支架或愤怒的肝脏。内部信号转导因子如外泌体或细胞因子的累积,建议有助于肾基因表达的观察变化。

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