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代谢分区在小鼠肝脏中的功能后果:一个古老故事的新视角。

Functional Consequences of Metabolic Zonation in Murine Livers: Insights for an Old Story.

机构信息

Charité - Universitätsmedizin Berlin, corporate member of Freie Universität BerlinHumboldt-Universität zu Berlin, and Berlin Institute of HealthInstitute for Imaging Science and Computational Modelling in Cardiovascular MedicineBerlinGermany.

Rudolf-Schönheimer-Institute of BiochemistryFaculty of MedicineLeipzig UniversityLeipzigGermany.

出版信息

Hepatology. 2021 Feb;73(2):795-810. doi: 10.1002/hep.31274. Epub 2020 Nov 7.

Abstract

BACKGROUND AND AIMS

Zone-dependent differences in expression of metabolic enzymes along the portocentral axis of the acinus are a long-known feature of liver metabolism. A prominent example is the preferential localization of the enzyme, glutamine synthetase, in pericentral hepatocytes, where it converts potentially toxic ammonia to the valuable amino acid, glutamine. However, with the exception of a few key regulatory enzymes, a comprehensive and quantitative assessment of zonal differences in the abundance of metabolic enzymes and, much more important, an estimation of the associated functional differences between portal and central hepatocytes is missing thus far.

APPROACH AND RESULTS

We addressed this problem by establishing a method for the separation of periportal and pericentral hepatocytes that yields sufficiently pure fractions of both cell populations. Quantitative shotgun proteomics identified hundreds of differentially expressed enzymes in the two cell populations. We used zone-specific proteomics data for scaling of the maximal activities to generate portal and central instantiations of a comprehensive kinetic model of central hepatic metabolism (Hepatokin1).

CONCLUSIONS

The model simulations revealed significant portal-to-central differences in almost all metabolic pathways involving carbohydrates, fatty acids, amino acids, and detoxification.

摘要

背景与目的

沿肝小叶门腔轴,代谢酶的表达在区域上存在差异,这是肝脏代谢的一个众所周知的特征。一个突出的例子是酶谷氨酸合酶在中央周围肝细胞中的优先定位,它将潜在有毒的氨转化为有价值的氨基酸谷氨酰胺。然而,除了少数关键的调节酶外,目前还缺乏对代谢酶在区域上丰度的全面和定量评估,更重要的是,也缺乏对门脉和中央肝细胞之间相关功能差异的评估。

方法和结果

我们通过建立一种分离门周和中央肝细胞的方法来解决这个问题,该方法可得到两种细胞群体足够纯净的分数。定量shotgun 蛋白质组学鉴定了两种细胞群体中数百种差异表达的酶。我们使用区域特异性蛋白质组学数据对最大活性进行了标度,生成了中央肝代谢(Hepatokin1)的综合动力学模型的门脉和中央实例。

结论

模型模拟揭示了涉及碳水化合物、脂肪酸、氨基酸和解毒的几乎所有代谢途径中都存在显著的门脉到中央的差异。

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