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新生儿短肠综合征的新兴仔猪模型

Emerging Piglet Models of Neonatal Short Bowel Syndrome.

作者信息

Lim David W, Turner Justine M, Wales Paul W

机构信息

Department of Surgery, University of Alberta, Edmonton, Alberta, Canada.

Department of Pediatrics, University of Alberta, Edmonton, Alberta, Canada Department of Agricultural, Food & Nutritional Science, University of Alberta, Edmonton, Alberta, Canada.

出版信息

JPEN J Parenter Enteral Nutr. 2015 Aug;39(6):636-43. doi: 10.1177/0148607114554621. Epub 2014 Oct 7.

Abstract

Short bowel syndrome (SBS) is a growing problem in the human neonatal population. In infants, SBS is the leading cause of intestinal failure, the state of being unable to absorb sufficient nutrients for growth and development. Neonates with SBS are dependent on long-term parenteral nutrition therapy, but many succumb to the complications of sepsis and liver disease. Research in neonatal SBS is challenged by the ethical limits of studying sick human neonates and the heterogeneous nature of the disease process. Outcomes in SBS vary depending on residual intestinal anatomy, intestinal length, patient age, and exposure to nutrition therapies. The neonatal piglet serves as an appropriate translational model of the human neonate because of similarities in gastrointestinal ontogeny, physiological maturity, and adaptive processes. Re-creating the disease process in a piglet model presents a unique opportunity for researchers to discover novel insights and therapies in SBS. Emerging piglet models of neonatal SBS now represent the entire spectrum of disease seen in human infants. This review aims to contextualize these emerging piglet models within the context of SBS as a heterogeneous disease. We first explore the factors that account for SBS heterogeneity and then explore the suitability of the neonatal piglet as an appropriate translational animal model. We then examine differences between the emerging piglet models of neonatal SBS and how these differences affect their translational potential to human neonates with SBS.

摘要

短肠综合征(SBS)在人类新生儿群体中是一个日益严重的问题。在婴儿中,SBS是肠衰竭的主要原因,肠衰竭是指无法吸收足够营养以支持生长发育的状态。患有SBS的新生儿依赖长期肠外营养治疗,但许多人会死于败血症和肝病等并发症。新生儿SBS的研究受到研究患病人类新生儿的伦理限制以及疾病过程异质性的挑战。SBS的预后因残余肠道解剖结构、肠长度、患者年龄以及营养治疗的接触情况而异。新生仔猪因其在胃肠道个体发生、生理成熟度和适应过程方面的相似性,成为人类新生儿合适的转化模型。在仔猪模型中重现疾病过程为研究人员发现SBS的新见解和治疗方法提供了独特机会。新出现的新生儿SBS仔猪模型现在涵盖了人类婴儿中所见疾病的整个范围。本综述旨在将这些新出现的仔猪模型置于SBS这种异质性疾病的背景下进行阐述。我们首先探讨导致SBS异质性的因素,然后探讨新生仔猪作为合适的转化动物模型的适用性。接着,我们研究新出现的新生儿SBS仔猪模型之间的差异,以及这些差异如何影响它们对患有SBS的人类新生儿的转化潜力。

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