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多事件病例对照前瞻性队列研究,以鉴定肥胖诱导的 30 岁加速老化的系统性、细胞性和分子性生物标志物:ObAGE 研究方案。

Multiple events case-control study in a prospective cohort to identify systemic, cellular, and molecular biomarkers of obesity-induced accelerated aging in 30-years-olds: the ObAGE study protocol.

机构信息

Institute of Nutrition & Food Technology, Universidad de Chile, Santiago, Chile.

Center for Integrative Biology, Universidad Mayor, Santiago, Chile.

出版信息

BMC Geriatr. 2022 May 2;22(1):387. doi: 10.1186/s12877-022-03032-4.

Abstract

BACKGROUND

Aging is characterized by a progressive loss of capacities linked to fundamental alterations/damage in multiple cellular and molecular pathways. It is the most significant risk factor for all non-communicable diseases (NCDs). Another contributing factor to the rise in NCDs is obesity. It has been suggested that obesity not only accelerates the onset of metabolic imbalances but also decreases lifespan and impacts cellular and molecular processes in a manner similar to aging. Obesity might accelerate the pace of aging. Guided by a lifecourse approach, we will explore how exposure to obesity in critical developmental stages disrupt homeostatic resilience mechanisms that preserve physiological integrity, inducing an early expression of aging phenotypes. Also, we will determine whether exposure to early psychosocial adversity influences vulnerability to obesity as a risk factor for accelerated aging.

METHODS

Multiple events case-control study embedded in a prospective cohort of Chileans at 30-31y, 50% females, of low- to-middle socioeconomic status, who participated in nutrition research since birth. At 23y, 25% had obesity and cardiometabolic risk was high. We will use a multi-layer approach including: anthropometric assessment; DXA scan for body composition; abdominal ultrasound of the liver; stool samples collection and sequencing of the ribosomal RNA 16S gene to characterize the gut microbiome; determination of age-related pro-inflammatory cytokynes and anti-inflammatory miokynes. For the first time in Chile, we will address age-related epigenetic changes using the Horvath´s epigenetic clock. In a subset we will conduct a controlled physical challenge to characterize physical resilience (autophagy).

DISCUSSION

ObAGE is in an excellent position to: approach aging as a process whose expression involves multiple factors from the early stages of a person's life; understand how longitudinal changes in health trajectories impact the biological mechanisms of aging; identify potential resilience mechanisms that help prevent unhealthy aging. Because SLS participants are still young, our research setting combined with advanced scientific techniques may identify individuals or groups at risk of early onset health issues. Results from ObAGE may pave the way to address the contribution of obesity to aging through lifespan from cells to systems and might be instrumental to developing interventions to improve health span in the Chilean population.

TRIAL REGISTRATION

The proposed study does not consider any health care intervention on human participants.

摘要

背景

衰老的特征是与多种细胞和分子途径的根本改变/损伤相关的能力逐渐丧失。它是所有非传染性疾病(NCDs)的最重要危险因素。NCDs 发病率上升的另一个促成因素是肥胖。有人认为,肥胖不仅加速了代谢失衡的发生,而且还缩短了寿命,并以类似于衰老的方式影响细胞和分子过程。肥胖可能会加速衰老的速度。本研究将以生命历程为指导,探讨在关键发育阶段暴露于肥胖如何破坏维持生理完整性的内稳态弹性机制,从而导致衰老表型的早期表达。此外,我们还将确定早期心理社会逆境暴露是否会影响肥胖作为加速衰老的危险因素的易感性。

方法

本研究是一项嵌套在智利人前瞻性队列中的多事件病例对照研究,该队列在 30-31 岁时入组,女性占 50%,社会经济地位处于中下水平,自出生以来一直参与营养研究。在 23 岁时,有 25%的人肥胖,且存在心血管代谢风险。我们将采用多层面的方法,包括:人体测量评估;双能 X 线吸收法(DXA)扫描用于身体成分分析;肝脏腹部超声检查;粪便样本收集和核糖体 RNA 16S 基因测序以表征肠道微生物组;测定与年龄相关的促炎细胞因子和抗炎细胞因子。智利将首次使用 Horvath 表观遗传时钟来解决与年龄相关的表观遗传变化。在一个亚组中,我们将进行受控的身体挑战以描述身体弹性(自噬)。

讨论

ObAGE 具有以下优势:将衰老视为一个过程,其表达涉及一个人生命早期的多个因素;了解健康轨迹的纵向变化如何影响衰老的生物学机制;确定潜在的弹性机制,有助于预防不健康的衰老。由于 SLS 参与者还很年轻,我们的研究环境结合先进的科学技术,可能会识别出有早期健康问题风险的个体或群体。ObAGE 的研究结果可能为通过从细胞到系统的寿命来解决肥胖对衰老的贡献铺平道路,并可能有助于制定改善智利人口健康寿命的干预措施。

试验注册

拟议的研究不考虑对人类参与者进行任何医疗保健干预。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7b33/9063300/684ed126b7f9/12877_2022_3032_Fig1_HTML.jpg

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