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恒河猴一生中性别依赖性血清代谢组学模式的比较分析。

Comparative analysis of sex-dependent serum metabolomic patterns across the lifespan of rhesus macaques.

作者信息

Metzler Ludwig A P, Goy Robinson W, Metzger Jeanette M, Emborg Marina E, Kapoor Amita

机构信息

Wisconsin National Primate Research Center, University of Wisconsin, Madison, WI, United States.

Department of Medical Physics, University of Wisconsin, Madison, WI, United States.

出版信息

Front Genet. 2025 Aug 25;16:1655325. doi: 10.3389/fgene.2025.1655325. eCollection 2025.

Abstract

INTRODUCTION

Aging is accompanied by systemic metabolic changes that contribute to disease susceptibility and functional decline. Sex differences in aging have been reported in humans, yet their mechanistic basis remains poorly understood. Due to their physiological similarity to humans, rhesus macaques are a powerful translational model to investigate sex-specific metabolomic aging under controlled conditions.

METHODS

Targeted serum metabolomics were conducted in 58 rhesus (35 females, 23 males), ranging from 1.66 to 25.71 years of age, quantifying 513 metabolites spanning lipids, amino acids, and related compounds. Multivariate, univariate, and generalized additive model (GAM) analyses were performed to evaluate age-associated trajectories and test for sex differences.

RESULTS

Age-related changes in both sexes were identified in metabolites related to hormones (e.g., DHEAS), amino acid biosynthesis and catabolism (e.g., beta-alanine, sarcosine, t4-OH-pro), and energy metabolism (e.g., hexose). Sex affected age-related metabolic trajectories in lipids, amino acids and related compounds, and gut microbial species. Females demonstrated a profound increase in serum triglycerides (TGs), amino acids, and other small molecules, while males exhibited a heterogenous profile with changes in lipids, but no TGs were affected. Males also exhibited altered levels of amino acids and related metabolites, hormones, gut microbial metabolites, and energy-associated metabolites.

CONCLUSION

These results highlight pronounced sex differences in metabolomic aging trajectories in rhesus macaques, particularly in lipid and amino acid metabolism. These findings underscore the importance of incorporating sex as a biological variable in aging studies and support the utility of rhesus macaques for identifying conserved, sex-specific biomarkers of biological aging.

摘要

引言

衰老伴随着全身代谢变化,这些变化会导致疾病易感性和功能衰退。人类中已报道了衰老过程中的性别差异,但其机制基础仍知之甚少。由于恒河猴在生理上与人类相似,因此是在可控条件下研究性别特异性代谢组学衰老的有力转化模型。

方法

对58只年龄在1.66至25.71岁之间的恒河猴(35只雌性,23只雄性)进行靶向血清代谢组学分析,定量测定513种代谢物,包括脂质、氨基酸及相关化合物。进行多变量、单变量和广义相加模型(GAM)分析,以评估与年龄相关的轨迹并检测性别差异。

结果

在与激素(如硫酸脱氢表雄酮)、氨基酸生物合成和分解代谢(如β-丙氨酸、肌氨酸、t4-羟基脯氨酸)以及能量代谢(如己糖)相关的代谢物中,均发现了两性与年龄相关的变化。性别影响脂质、氨基酸及相关化合物和肠道微生物种类的与年龄相关的代谢轨迹。雌性血清甘油三酯(TGs)、氨基酸和其他小分子显著增加,而雄性则表现出脂质变化的异质性特征,但TGs未受影响。雄性还表现出氨基酸及相关代谢物、激素、肠道微生物代谢物和能量相关代谢物水平的改变。

结论

这些结果突出了恒河猴代谢组学衰老轨迹中明显的性别差异,特别是在脂质和氨基酸代谢方面。这些发现强调了将性别作为衰老研究中的生物学变量的重要性,并支持恒河猴在识别保守的、性别特异性生物衰老生物标志物方面的实用性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d45d/12414774/61f79720e479/fgene-16-1655325-g001.jpg

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