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肠衰竭相关肝病的病理生理学、预防、治疗及预后

Pathophysiology, prevention, treatment, and outcomes of intestinal failure-associated liver disease.

作者信息

Al-Shahwani Noora H, Sigalet David L

机构信息

Department of Pediatric Surgery, Hamad Medical Corporation, Doha, Qatar.

Chair of Surgery, Sidra Medical and Research Center, PO Box 26999, Doha, Qatar.

出版信息

Pediatr Surg Int. 2017 Apr;33(4):405-411. doi: 10.1007/s00383-016-4042-7. Epub 2016 Dec 27.

Abstract

BACKGROUND

Intestinal failure-associated liver disease (IFALD) remains a serious problem in the treatment of infants with nutritional problems and short bowel syndrome.

METHODS

A review of the recent literature from 2010 to 2016, concentrating on articles related to the pathophysiology of IFALD and to outcomes of novel nutritional and pharmacological therapies for neonatal cholestasis in the post-surgical neonate.

RESULTS

The pathophysiology of IFALD relates to an increase sensitivity of the neonatal liver to cholestasis in the non-fed state; prolonged cholestasis almost inevitably results in liver damage which will progress from fibrosis to cirrhosis. Clinically discerned risk factors include premature birth, inflammation, sepsis, disruption of the enterohepatic circulation by creation of a proximal stoma, and the duration and type of parenteral nutritional support. Within the hepatocyte, the regulatory enzyme farsanoid receptor X (FXR) appears to play a pivotal role in the development of cholestasis. Recent studies have shown that its activity is suppressed by sepsis, and by plant phytosterols found in soy-based lipid preparations. This paradigm is reflected in the emerging consensus for the care of post-surgical neonates, which is based around a multi-disciplinary team approach. Using an algorithm-driven approach, an appropriate balance between caloric support and prevention of IFALD can be achieved.

CONCLUSIONS

Further prospective studies are required to further refine the optimal sequence of use of these therapies and the long-term effects on neurological development and hepatic function. However, with optimal care, the number of IF patients progressing to end-stage liver disease because of IFALD should be very low.

摘要

背景

在患有营养问题和短肠综合征的婴儿治疗中,肠衰竭相关肝病(IFALD)仍然是一个严重问题。

方法

回顾2010年至2016年的近期文献,重点关注与IFALD病理生理学以及新生儿胆汁淤积症术后新生儿新型营养和药物治疗结果相关的文章。

结果

IFALD的病理生理学与新生儿肝脏在非喂养状态下对胆汁淤积敏感性增加有关;长期胆汁淤积几乎不可避免地导致肝损伤,肝损伤将从纤维化发展为肝硬化。临床上可识别的危险因素包括早产、炎症、败血症、近端造口导致肠肝循环中断以及肠外营养支持的持续时间和类型。在肝细胞内,调节酶法尼醇X受体(FXR)似乎在胆汁淤积的发展中起关键作用。最近的研究表明,其活性受到败血症以及大豆脂质制剂中植物甾醇的抑制。这种模式反映在针对术后新生儿护理的新共识中,该共识基于多学科团队方法。使用算法驱动的方法,可以在热量支持和预防IFALD之间实现适当的平衡。

结论

需要进一步的前瞻性研究来进一步完善这些治疗方法的最佳使用顺序以及对神经发育和肝功能的长期影响。然而,通过最佳护理,因IFALD进展为终末期肝病的IF患者数量应该非常少。

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