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基因背景和性别对小鼠脂肪、骨骼肌和肝脏组织代谢组的独立及交互作用

Independent and Interactive Effects of Genetic Background and Sex on Tissue Metabolomes of Adipose, Skeletal Muscle, and Liver in Mice.

作者信息

Wells Ann E, Barrington William T, Dearth Stephen, Milind Nikhil, Carter Gregory W, Threadgill David W, Campagna Shawn R, Voy Brynn H

机构信息

UT-ORNL Graduate School of Genome Science and Technology, University of Tennessee-Knoxville, Knoxville, TN 37996, USA.

The Jackson Laboratory, 600 Main Street, Bar Harbor, ME 04609, USA.

出版信息

Metabolites. 2022 Apr 8;12(4):337. doi: 10.3390/metabo12040337.

Abstract

Genetics play an important role in the development of metabolic diseases. However, the relative influence of genetic variation on metabolism is not well defined, particularly in tissues, where metabolic dysfunction that leads to disease occurs. We used inbred strains of laboratory mice to evaluate the impact of genetic variation on the metabolomes of tissues that play central roles in metabolic diseases. We chose a set of four common inbred strains that have different levels of susceptibility to obesity, insulin resistance, and other common metabolic disorders. At the ages used, and under standard husbandry conditions, these lines are not overtly diseased. Using global metabolomics profiling, we evaluated water-soluble metabolites in liver, skeletal muscle, and adipose from A/J, C57BL/6J, FVB/NJ, and NOD/ShiLtJ mice fed a standard mouse chow diet. We included both males and females to assess the relative influence of strain, sex, and strain-by-sex interactions on metabolomes. The mice were also phenotyped for systems level traits related to metabolism and energy expenditure. Strain explained more variation in the metabolite profile than did sex or its interaction with strain across each of the tissues, especially in liver. Purine and pyrimidine metabolism and pathways related to amino acid metabolism were identified as pathways that discriminated strains across all three tissues. Based on the results from ANOVA, sex and sex-by-strain interaction had modest influence on metabolomes relative to strain, suggesting that the tissue metabolome remains largely stable across sexes consuming the same diet. Our data indicate that genetic variation exerts a fundamental influence on tissue metabolism.

摘要

遗传学在代谢性疾病的发展中起着重要作用。然而,遗传变异对代谢的相对影响尚未明确界定,尤其是在发生导致疾病的代谢功能障碍的组织中。我们使用近交系实验小鼠来评估遗传变异对在代谢性疾病中起核心作用的组织代谢组的影响。我们选择了一组对肥胖、胰岛素抵抗和其他常见代谢紊乱具有不同易感性水平的四种常见近交系。在所使用的年龄以及标准饲养条件下,这些品系没有明显疾病。通过全局代谢组学分析,我们评估了喂食标准小鼠饲料的A/J、C57BL/6J、FVB/NJ和NOD/ShiLtJ小鼠肝脏、骨骼肌和脂肪中的水溶性代谢物。我们纳入了雄性和雌性小鼠以评估品系、性别以及品系与性别的相互作用对代谢组的相对影响。这些小鼠还针对与代谢和能量消耗相关的系统水平特征进行了表型分析。在每个组织中,品系比性别或其与品系的相互作用能解释代谢物谱中更多的变异,尤其是在肝脏中。嘌呤和嘧啶代谢以及与氨基酸代谢相关的途径被确定为在所有三个组织中区分品系的途径。基于方差分析的结果,相对于品系,性别以及性别与品系的相互作用对代谢组的影响较小,这表明在食用相同饮食的不同性别中,组织代谢组在很大程度上保持稳定。我们的数据表明遗传变异对组织代谢具有根本性影响。

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