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首页> 外文期刊>Proceedings of the Nutrition Society >Understanding susceptibility and targeting treatment in non-alcoholic fatty liver disease in children; moving the fulcrum
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Understanding susceptibility and targeting treatment in non-alcoholic fatty liver disease in children; moving the fulcrum

机译:了解儿童非酒精脂肪肝病的易感性和靶向治疗; 移动支点

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Non-alcoholic fatty liver disease (NAFLD) is the most common cause of paediatric liver disease, affecting 10% of school-aged children and 44–70% of obese children and young people (CYP) in the western world. Encompassing a spectrum from simple steatosis to steatohepatitis and progressive fibrosis, the disease is rapidly becoming the most common indication for liver transplantation. The molecular pathogenesis of NAFLD remains only partially understood. Development and progression of NAFLD is influenced by genetic and nutritional factors, insulin resistance, oxidative stress, gut microbiome, bile acid metabolism and lipid/glucose handling and is closely associated with overweight and obesity. Lifestyle change is the only proven effective treatment for paediatric NAFLD, however this is difficult to achieve in many. Given that moderate or severe fibrosis is already present in 30–50% of children with NAFLD at the time of presentation, progression in CYP may be more rapid, though adequate outcome data do not yet exist in this cohort. CYP with NAFLD are an excellent population in which to study underlying mechanisms and interventions to correct disease progression as they are largely unaffected by other environmental influences such as alcohol and may represent the more severe end of the spectrum in terms of early onset. Undoubtedly genetic and epigenetic mechanisms determine a large proportion of susceptibility to the disease and potentially, identification of individuals at risk may allow for targeted therapy. This review with give a clinical perspective of paediatric NAFLD focused on identifying those at risk of progressive disease and what to consider in attempting to modify risk.
机译:非酒精性脂肪肝病(NAFLD)是儿科肝病最常见的原因,影响了10%的学龄儿童和44-70%的肥胖儿童和青年人(CYP)。包括一种从简单的脂肪变性到脂肪性肝炎和渐进式纤维化的光谱,这种疾病正在迅速成为肝移植的最常见的迹象。 NAFLD的分子发病机制仅部分地理解。 NAFLD的开发和进展受遗传和营养因素的影响,胰岛素抵抗,氧化应激,肠道微生物组,胆汁酸代谢和脂质/葡萄糖处理,与超重和肥胖密切相关。生活方式改变是唯一可获得儿科NAFLD的有效处理,但很难在许多方面实现。鉴于中度或严重的纤维化已经存在于30-50%的NAFLD在介绍时的儿童中,CYP的进展可能更加迅速,但在这队列中尚未存在足够的结果数据。与NAFLD的CYP是一种优秀的人群,用于研究潜在的机制和干预措施,以纠正疾病的进展,因为它们主要不受酒精等其他环境影响的影响,并且可以代表早期发病方面的频谱的更严重结束。无疑遗传和表观遗传机制决定了对疾病的大部分易感性,潜在地,鉴定风险的个体可能允许靶向治疗。本综述借助小儿NAFLD的临床观点,重点是识别患有渐进疾病风险的临床观点以及需要考虑修改风险的内容。

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