Ageing hallmarks exhibit organ-specific temporal signatures

老化 生物 计算生物学 进化生物学 遗传学
作者
Nicholas Schaum,Benoit Lehallier,Oliver Hãhn,Róbert Pálovics,Shayan Hosseinzadeh,Song Eun Lee,Rene Sit,Davis P. Lee,Patricia Morán Losada,Macy E. Zardeneta,Tobias Fehlmann,James T. Webber,Aaron McGeever,Kruti Calcuttawala,Hui Zhang,Daniela Berdnik,Vidhu Mathur,Weilun Tan,Alexander Zee,Michelle Tan,Nicole Almanzar,Jane Antony,Ankit S. Baghel,Isaac Bakerman,Ishita Bansal,Ben A. Barres,Philip A. Beachy,Daniela Berdnik,Biter Bilen,Douglas Brownfield,Corey J. Cain,Charles K. F. Chan,Michelle B. Chen,Michael F. Clarke,Stephanie D. Conley,Spyros Darmanis,Aaron Demers,Kubilay Demir,Antoine de Morrée,Tessa Divita,Haley du Bois,Hamid Ebadi,F. Hernán Espinoza,Matt Fish,Qiang Gan,Benson M. George,Astrid Gillich,Rafael Gómez-Sjöberg,Foad Green,Geraldine Genetiano,Xueying Gu,Gunsagar S. Gulati,Oliver Hãhn,Michael S. Haney,Yan Hang,Lincoln Harris,Mu He,Shayan Hosseinzadeh,Albin Huang,Kerwyn Casey Huang,Tal Iram,Taichi Isobe,Feather Ives,Robert C. Jones,Kevin S. Kao,Jim Karkanias,Guruswamy Karnam,Andreas Keller,Aaron M. Kershner,Nathalie Khoury,Seung K. Kim,Bernhard Kiss,William Kong,Mark A. Krasnow,Maya E. Kumar,Christin S. Kuo,Jonathan Y. Lam,Davis P. Lee,Song Eun Lee,Benoit Lehallier,Olivia Leventhal,Guang Li,Qingyun Li,Ling Liu,Annie Lo,Wan-Jin Lu,Maria Lugo-Fagundo,Anoop Manjunath,Andrew P. May,Ashley Maynard,Aaron McGeever,Marina McKay,M. Windy McNerney,Bryan D. Merrill,Ross J. Metzger,Marco Mignardi,Dullei Min,Ahmad N. Nabhan,Norma Neff,Katharine M. Ng,Patricia K. Nguyen,Joseph Noh,Roel Nusse,Róbert Pálovics,Rasika Patkar,Weng Chuan Peng,Lolita Penland,Angela Oliveira Pisco,Katherine S. Pollard,Robert Puccinelli,Zhen Qi,Stephen R. Quake,Thomas A. Rando,Eric Rulifson,Nicholas Schaum,Joe M. Segal,Shaheen S. Sikandar,Rahul Sinha,Rene Sit,Justin L. Sonnenburg,Daniel Staehli,Krzysztof Szade,Michelle Tan,Weilun Tan,Cristina M. Tato,Krissie Tellez,Laughing Bear Torrez Dulgeroff,Kyle J. Travaglini,Carolina Tropini,Margaret Tsui,Lucas Waldburger,Bruce M. Wang,Linda J. van Weele,Kenneth I. Weinberg,Irving L. Weissman,Michael N. Wosczyna,Sean M. Wu,Tony Wyss‐Coray,Jinyi Xiang,Soso Xue,Kevin A. Yamauchi,Andrew C. Yang,Lakshmi Yerra,Justin Youngyunpipatkul,Brian Yu,Fabio Zanini,Macy E. Zardeneta,Alexander Zee,Chunyu Zhao,Fan Zhang,Hui Zhang,Martin Jinye Zhang,Lu Zhou,James Zou,Angela Oliveira Pisco,Jim Karkanias,Norma Neff,Andreas Keller,Spyros Darmanis,Stephen R. Quake,Tony Wyss‐Coray
出处
期刊:Nature [Springer Nature]
卷期号:583 (7817): 596-602 被引量:413
标识
DOI:10.1038/s41586-020-2499-y
摘要

Ageing is the single greatest cause of disease and death worldwide, and understanding the associated processes could vastly improve quality of life. Although major categories of ageing damage have been identified—such as altered intercellular communication, loss of proteostasis and eroded mitochondrial function1—these deleterious processes interact with extraordinary complexity within and between organs, and a comprehensive, whole-organism analysis of ageing dynamics has been lacking. Here we performed bulk RNA sequencing of 17 organs and plasma proteomics at 10 ages across the lifespan of Mus musculus, and integrated these findings with data from the accompanying Tabula Muris Senis2—or 'Mouse Ageing Cell Atlas'—which follows on from the original Tabula Muris3. We reveal linear and nonlinear shifts in gene expression during ageing, with the associated genes clustered in consistent trajectory groups with coherent biological functions—including extracellular matrix regulation, unfolded protein binding, mitochondrial function, and inflammatory and immune response. Notably, these gene sets show similar expression across tissues, differing only in the amplitude and the age of onset of expression. Widespread activation of immune cells is especially pronounced, and is first detectable in white adipose depots during middle age. Single-cell RNA sequencing confirms the accumulation of T cells and B cells in adipose tissue—including plasma cells that express immunoglobulin J—which also accrue concurrently across diverse organs. Finally, we show how gene expression shifts in distinct tissues are highly correlated with corresponding protein levels in plasma, thus potentially contributing to the ageing of the systemic circulation. Together, these data demonstrate a similar yet asynchronous inter- and intra-organ progression of ageing, providing a foundation from which to track systemic sources of declining health at old age. Bulk RNA sequencing of organs and plasma proteomics at different ages across the mouse lifespan is integrated with data from the Tabula Muris Senis, a transcriptomic atlas of ageing mouse tissues, to describe organ-specific changes in gene expression during ageing.
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