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蛋白质分解代谢产物作为衰老生理学的血液生物标志物:犬类衰老项目的研究结果

Protein catabolites as blood-based biomarkers of aging physiology: Findings from the Dog Aging Project.

作者信息

Harrison Benjamin R, Partida-Aguilar Maria, Marye Abbey, Djukovic Danijel, Kauffman Mandy, Dunbar Matthew D, Mariner Blaise L, McCoy Brianah M, Algavi Yadid M, Muller Efrat, Baum Shiri, Bamberger Tal, Raftery Dan, Creevy Kate E, Avery Anne, Borenstein Elhanan, Snyder-Mackler Noah, Promislow Daniel E

机构信息

Department of Laboratory Medicine and Pathology, University of Washington, Seattle, WA, USA.

University of Utah, Department of Microbiology and Immunology, Salt Lake City, UT, USA.

出版信息

bioRxiv. 2024 Oct 21:2024.10.17.618956. doi: 10.1101/2024.10.17.618956.

Abstract

Our understanding of age-related physiology and metabolism has grown through the study of systems biology, including transcriptomics, single-cell analysis, proteomics and metabolomics. Studies in lab organisms in controlled environments, while powerful and complex, fall short of capturing the breadth of genetic and environmental variation in nature. Thus, there is now a major effort in geroscience to identify aging biomarkers and to develop aging interventions that might be applied across the diversity of humans and other free-living species. To meet this challenge, the Dog Aging Project (DAP) is designed to identify cross-sectional and longitudinal patterns of aging in complex systems, and how these are shaped by the diversity of genetic and environmental variation among companion dogs. Here we surveyed the plasma metabolome from the first year of sampling of the Precision Cohort of the DAP. By incorporating extensive metadata and whole genome sequencing information, we were able to overcome the limitations inherent in breed-based estimates of genetic and physiological effects, and to probe the physiological and dietary basis of the age-related metabolome. We identified a significant effect of age on approximately 40% of measured metabolites. Among other insights, we discovered a potentially novel biomarker of age in the post-translationally modified amino acids (ptmAAs). The ptmAAs, which can only be generated by protein hydrolysis, covaried both with age and with other biomarkers of amino acid metabolism, and in a way that was robust to diet. Clinical measures of kidney function mediated about half of the higher ptmAA levels in older dogs. This work identifies ptmAAs as robust indicators of age in dogs, and points to kidney function as a physiological mediator of age-associated variation in the plasma metabolome.

摘要

通过对系统生物学的研究,包括转录组学、单细胞分析、蛋白质组学和代谢组学,我们对与年龄相关的生理学和新陈代谢的理解不断加深。在受控环境中对实验生物进行的研究虽然强大且复杂,但仍无法涵盖自然界中遗传和环境变异的广度。因此,老年科学领域目前正在做出重大努力,以识别衰老生物标志物,并开发可能适用于人类和其他自由生活物种多样性的衰老干预措施。为了应对这一挑战,犬类衰老项目(DAP)旨在识别复杂系统中衰老的横断面和纵向模式,以及这些模式如何受到伴侣犬之间遗传和环境变异多样性的影响。在这里,我们调查了DAP精准队列第一年采样的血浆代谢组。通过纳入广泛的元数据和全基因组测序信息,我们能够克服基于品种的遗传和生理效应估计中固有的局限性,并探究与年龄相关的代谢组的生理和饮食基础。我们发现年龄对大约40%的测量代谢物有显著影响。在其他见解中,我们在翻译后修饰氨基酸(ptmAA)中发现了一种潜在的新型衰老生物标志物。ptmAA只能通过蛋白质水解产生,它与年龄以及氨基酸代谢的其他生物标志物都存在协变关系,并且这种关系不受饮食影响。老年犬较高的ptmAA水平中约有一半是由肾功能的临床指标介导的。这项工作将ptmAA确定为犬类年龄的可靠指标,并指出肾功能是血浆代谢组中与年龄相关变异的生理调节因子。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6603/11526923/ea4ca7530dd3/nihpp-2024.10.17.618956v1-f0001.jpg

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