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2型糖尿病小鼠的肝脏糖原呈随机分支状,形成增大的聚集体,葡萄糖释放减弱。

Liver glycogen in type 2 diabetic mice is randomly branched as enlarged aggregates with blunted glucose release.

作者信息

Besford Quinn Alexander, Zeng Xiao-Yi, Ye Ji-Ming, Gray-Weale Angus

机构信息

School of Chemistry, University of Melbourne, Victoria, 3010, Australia.

School of Health Sciences, RMIT University, Victoria, 3083, Australia.

出版信息

Glycoconj J. 2016 Feb;33(1):41-51. doi: 10.1007/s10719-015-9631-5. Epub 2015 Oct 31.

Abstract

Glycogen is a vital highly branched polymer of glucose that is essential for blood glucose homeostasis. In this article, the structure of liver glycogen from mice is investigated with respect to size distributions, degradation kinetics, and branching structure, complemented by a comparison of normal and diabetic liver glycogen. This is done to screen for differences that may result from disease. Glycogen α-particle (diameter ∼ 150 nm) and β-particle (diameter ∼ 25 nm) size distributions are reported, along with in vitro γ-amylase degradation experiments, and a small angle X-ray scattering analysis of mouse β-particles. Type 2 diabetic liver glycogen upon extraction was found to be present as large loosely bound, aggregates, not present in normal livers. Liver glycogen was found to aggregate in vitro over a period of 20 h, and particle size is shown to be related to rate of glucose release, allowing a structure-function relationship to be inferred for the tissue specific distribution of particle types. Application of branching theories to small angle X-ray scattering data for mouse β-particles revealed these particles to be randomly branched polymers, not fractal polymers. Together, this article shows that type 2 diabetic liver glycogen is present as large aggregates in mice, which may contribute to the inflexibility of interconversion between glucose and glycogen in type 2 diabetes, and further that glycogen particles are randomly branched with a size that is related to the rate of glucose release.

摘要

糖原是一种重要的高度分支的葡萄糖聚合物,对血糖稳态至关重要。在本文中,研究了小鼠肝脏糖原的大小分布、降解动力学和分支结构,并与正常和糖尿病肝脏糖原进行了比较,以筛选可能由疾病导致的差异。报告了糖原α颗粒(直径约150纳米)和β颗粒(直径约25纳米)的大小分布,以及体外γ淀粉酶降解实验和小鼠β颗粒的小角X射线散射分析。发现2型糖尿病肝脏糖原提取后以大的松散结合聚集体形式存在,而正常肝脏中不存在。发现肝脏糖原在体外20小时内会聚集,并且颗粒大小与葡萄糖释放速率相关,从而可以推断出颗粒类型的组织特异性分布的结构-功能关系。将分支理论应用于小鼠β颗粒的小角X射线散射数据表明,这些颗粒是随机分支的聚合物,而不是分形聚合物。总之,本文表明2型糖尿病肝脏糖原在小鼠中以大聚集体形式存在,这可能导致2型糖尿病中葡萄糖和糖原之间相互转化的不灵活性,并且进一步表明糖原颗粒是随机分支的,其大小与葡萄糖释放速率相关。

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