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    Home»Health»Can We Slow Down Aging? New Biomarker Shows Promise
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    Can We Slow Down Aging? New Biomarker Shows Promise

    By Chinese Academy of Sciences HeadquartersNovember 17, 20241 Comment4 Mins Read
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    A team from the Chinese Academy of Sciences and BGI Research has identified how immunoglobulins contribute to aging by mapping high-precision cellular changes across multiple organs. Their study reveals that IgG buildup triggers aging processes, and a potential intervention using antisense oligonucleotides could slow aging.

    Scientists from CAS and BGI Research found that immunoglobulins are both drivers and markers of aging, with IgG accumulation inducing aging across tissues.

    A research team from the Chinese Academy of Sciences (CAS) and BGI Research has unveiled the complex mechanisms through which immunoglobulins impact the aging process, a discovery that could transform our understanding of aging.

    This research, published in Cell on November 4, not only charts a high-precision map of aging across various organs but also reveals the dual-edged sword of immunoglobulins in systemic aging.

    The quest for systemic biomarkers and key drivers of aging has been a long-standing puzzle in the field of gerontology. This study, a collaborative effort between Guanghui Liu’s team from the Institute of Zoology (IOZ) of CAS, Ying Gu’s team from BGI Research, Weiqi’s Zhang team from the Beijing Institute of Genomics of CAS, and Jing Qu’s team also from IOZ, has provided compelling answers.

    By meticulously analyzing millions of spatial spots across nine organs in male mice, the team created high-precision spatial transcriptomic maps. These maps detailed the spatial distribution of over 70 cell types, offering a vivid picture of aging’s spatial characteristics.

    Gerontological Geography and Aging Hallmarks

    The transcriptomic landscape, dubbed Gerontological Geography (GG), exposes the common threads of tissue structural disorder and loss of cellular identity as hallmarks of aging.

    “This landscape is a significant step forward, pinpointing the epicenters of aging within multiple organs and uncovering the accumulation of immunoglobulins as a key aging characteristic and driver,” said Professor LIU, one of the corresponding authors of the study.

    Using the novel method of organizational structure entropy (OSE) analysis, the researchers discovered that increased spatial structural disorder and loss of cellular identity are universal signs of systemic aging, suggesting that spatial structural damage may be a primary cause of organ functional decline during aging.

    The team also identified senescence-sensitive spots (SSS), which are structural regions in different tissues more susceptible to aging’s effects. They found that areas closer to SSS exhibit higher tissue structural entropy and greater loss of cellular identity, indicating that SSS could be the nucleus of organ aging.

    Role of Immunoglobulins in Aging

    Notably, in immune organs, plasma cells, which are responsible for antibody synthesis, and cells with specific structures and functions, are the main components of the SSS microenvironment. The expression levels of immunoglobulin-related genes in these cells increase around SSS.

    The study further discovered that immunoglobulin G (IgG) accumulates in multiple tissues and organs during aging in humans and mice, suggesting that IgG levels could serve as a new biomarker for aging. Moreover, IgG was found to directly induce aging in human and mouse macrophages and microglia, releasing inflammatory factors. Intriguingly, injecting IgG into young mice induced aging in multiple tissues and organs, demonstrating its potent aging effects.

    In a promising development, the team developed an intervention strategy using antisense oligonucleotides (ASO) to reduce IgG content in mouse tissues, thereby delaying the aging of multiple organs.

    This study is the first to map the spatial transcriptome of pan-organ aging in mammals, revealing tissue structural disorder and loss of cellular identity as key aging hallmarks and precisely locating the core regions and microenvironmental characteristics of aging sensitivity.

    The Immunoglobulin-associated Senescence Phenotype (IASP) proposed by the study expands the frontiers of aging science and opens new avenues for delaying aging and preventing related diseases.

    Reference: “Spatial transcriptomic landscape unveils immunoglobin-associated senescence as a hallmark of aging” by Shuai Ma, Zhejun Ji, Bin Zhang, Lingling Geng, Yusheng Cai, Chao Nie, Jiaming Li, Yuesheng Zuo, Yuzhe Sun, Gang Xu, Beibei Liu, Jiaqi Ai, Feifei Liu, Liyun Zhao, Jiachen Zhang, Hui Zhang, Shuhui Sun, Haoyan Huang, Yiyuan Zhang, Yanxia Ye, Yanling Fan, Fangshuo Zheng, Jinghao Hu, Baohu Zhang, Jingyi Li, Xin Feng, Feng Zhang, Yuan Zhuang, Tianjie Li, Yang Yu, Zhaoshi Bao, Sipei Pan, Concepcion Rodriguez Esteban, Zhili Liu, Haohao Deng, Feng Wen, Moshi Song, Si Wang, Guodong Zhu, Jiayin Yang, Tao Jiang, Weihong Song, Juan Carlos Izpisua Belmonte, Jing Qu, Weiqi Zhang, Ying Gu and Guang-Hui Liu, 4 November 2024, Cell.
    DOI: 10.1016/j.cell.2024.10.019

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    Aging Antibodies Cell Biology Chinese Academy of Sciences Gerontology Immunology Popular
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    1 Comment

    1. John Bayer on November 19, 2024 9:26 pm

      Antisense! Yeah, that’s the ticket!

      Maybe nonsense would be easier, though…

      Reply
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