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睾酮和二甲双胍对生物年龄的糖基化年龄指数及IgG糖组组成的影响。

Effects of testosterone and metformin on the GlycanAge index of biological age and the composition of the IgG glycome.

作者信息

Vinicki Martina, Pribić Tea, Vučković Frano, Frkatović-Hodžić Azra, Plaza-Andrades Isaac, Tinahones Francisco, Raffaele Joseph, Fernández-García José Carlos, Lauc Gordan

机构信息

Glycoscience Research Laboratory, Genos Ltd, Borongajska Cesta 83H, Zagreb, Croatia.

Grupo de Oncología Traslacional, Centro de Investigación Médico-Sanitario (CIMES), Laboratorio Inmunobiota, Malaga, Spain.

出版信息

Geroscience. 2025 Apr;47(2):1777-1788. doi: 10.1007/s11357-024-01349-z. Epub 2024 Oct 4.

Abstract

With aging, the body's ability to maintain regular functions declines, increasing susceptibility to age-related diseases. Therapeutic interventions targeting the underlying biological changes of aging hold promise for preventing or delaying multiple age-related diseases. Metformin, a drug commonly used for diabetes treatment, has emerged as a potential gerotherapeutic agent due to its established safety record and preclinical and clinical data on its anti-aging effects. Glycosylation, one of the most common and complex co- and post-translational protein modifications, plays a crucial role in regulating protein function and has been linked to aging and various diseases. Changes in immunoglobulin G (IgG) glycosylation patterns have been observed with age, and these alterations may serve as valuable biomarkers for disease predisposition, diagnosis, treatment monitoring, and overall health assessment. In this study, we analyzed the IgG glycosylation patterns of white men from Europe, aged 29-45 years, under treatment with metformin, testosterone, metformin plus testosterone, and placebo (trial registration number NCT02514629, 2013/07/04), and investigated the longitudinal changes in glycosylation over time. We observed statistically significant differences in the IgG glycome composition between participants on testosterone therapy and placebo, with decreased agalactosylation and increased galactosylation and sialylation. However, metformin therapy did not result in statistically significant changes in glycosylation patterns. These findings contribute to our understanding of the impact of therapeutic interventions on IgG glycosylation and confirm the value of IgG glycosylation as a significant biomarker, capable of assessing biological age using the GlycanAge index and providing insight into overall health compared to chronological age.

摘要

随着年龄的增长,身体维持正常功能的能力下降,对与年龄相关疾病的易感性增加。针对衰老潜在生物学变化的治疗干预措施有望预防或延缓多种与年龄相关的疾病。二甲双胍是一种常用于治疗糖尿病的药物,由于其已确立的安全记录以及关于其抗衰老作用的临床前和临床数据,已成为一种潜在的老年治疗药物。糖基化是最常见和复杂的共翻译和翻译后蛋白质修饰之一,在调节蛋白质功能中起关键作用,并且与衰老和各种疾病有关。随着年龄的增长,已观察到免疫球蛋白G(IgG)糖基化模式的变化,这些改变可能作为疾病易感性、诊断、治疗监测和整体健康评估的有价值的生物标志物。在本研究中,我们分析了年龄在29 - 45岁之间接受二甲双胍、睾酮、二甲双胍加睾酮和安慰剂治疗的欧洲白人男性的IgG糖基化模式(试验注册号NCT02514629,2013/07/04),并研究了糖基化随时间的纵向变化。我们观察到接受睾酮治疗的参与者与接受安慰剂的参与者之间IgG糖组组成存在统计学上的显著差异,去半乳糖基化减少,半乳糖基化和唾液酸化增加。然而,二甲双胍治疗并未导致糖基化模式发生统计学上的显著变化。这些发现有助于我们理解治疗干预对IgG糖基化的影响,并证实IgG糖基化作为一种重要生物标志物的价值,它能够使用聚糖年龄指数评估生物学年龄,并与实际年龄相比洞察整体健康状况。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9d1b/11979073/4d4239fc213c/11357_2024_1349_Fig1_HTML.jpg

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