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甘氨酰酪氨酸在苯丙酮尿症患者中的应用:系统评价和荟萃分析。

The Use of Glycomacropeptide in Patients with Phenylketonuria: A Systematic Review and Meta-Analysis.

机构信息

Departamento de Biomedicina, Unidade de Bioquímica, Faculdade de Medicina, Universidade do Porto, 4200-319 Porto, Portugal.

Department of Dietetics, Birmingham Children's Hospital, Birmingham B4 6NH, UK.

出版信息

Nutrients. 2018 Nov 18;10(11):1794. doi: 10.3390/nu10111794.

Abstract

In phenylketonuria (PKU), synthetic protein derived from L-amino acids (AAs) is essential in a low-phenylalanine (Phe) diet. Glycomacropeptide (GMP), an intact protein, is very low in Phe in its native form. It has been modified and adapted for PKU to provide an alternative protein source through supplementation with rate-limiting amino acids (GMP-AAs), although it still contains residual Phe. This review aims to systematically evaluate published intervention studies on the use of GMP-AAs in PKU by considering its impact on blood Phe control (primary aim) and changes in tyrosine control, nutritional biomarkers, and patient acceptability or palatability (secondary aims). Four electronic databases were searched for articles published from 2007 to June 2018. Of the 274 studies identified, only eight were included. Bias risk was assessed and a quality appraisal of the body of evidence was completed. A meta-analysis was performed with two studies with adequate comparable methodology which showed no differences between GMP-AAs and AAs for any of the interventions analysed. This work underlines the scarcity and nature of studies with GMP-AAs interventions. All were short-term with small sample sizes. There is a need for better-designed studies to provide the best evidence-based recommendations.

摘要

在苯丙酮尿症(PKU)中,来源于 L-氨基酸(AA)的合成蛋白在低苯丙氨酸(phe)饮食中是必不可少的。糖巨肽(GMP)是一种完整的蛋白质,在其天然形式中phe 含量非常低。它已经经过修饰和适应 PKU,通过补充限速氨基酸(GMP-AA)来提供替代蛋白质来源,尽管它仍然含有残留的phe。本综述旨在通过考虑其对血液phe 控制的影响(主要目标)以及酪氨酸控制、营养生物标志物以及患者接受性或可接受性(次要目标)的变化,系统地评估已发表的关于 GMP-AA 在 PKU 中应用的干预研究。从 2007 年到 2018 年 6 月,四个电子数据库都对发表的文章进行了搜索。在确定的 274 项研究中,只有 8 项被纳入。对偏倚风险进行了评估,并对证据进行了质量评估。对两项具有足够可比性方法学的研究进行了荟萃分析,结果显示,在分析的任何干预措施中,GMP-AA 和 AA 之间没有差异。这项工作强调了 GMP-AA 干预研究的稀缺性和性质。所有研究都是短期的,样本量小。需要设计更好的研究来提供最佳的循证建议。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ed9e/6266274/f533e397dc56/nutrients-10-01794-g001.jpg

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