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Fucosylated IgG linked to adipose tissue dysfunction in aging

04.26.26 | Higher Education Press

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Role of fucosylated IgG in eWAT dysfunction and aging.
(a) Experimental design of the fucosylated and nonfucosylated IgGin vivomodel in B-cell-depleted aged mice. (b–d) qRT-PCR analysis of the expression of key genes related to (b) adipogenesis, (c) inflammation, and (d) fibrosis in eWAT (n= 4 for each group). The data are presented as the means ± SDs. *P Credit: Jingyu Wang, Wei Su et al.

A study published in Engineering has identified fucosylated immunoglobulin G (IgG) as a key mediator contributing to adipose tissue dysfunction during aging, offering insights into age-related metabolic disorders and potential therapeutic targets.

Researchers from North China University of Science and Technology and Capital Medical University conducted transcriptomic and glycoproteomic analyses on epididymal white adipose tissue (eWAT) from young and aged mice. RNA-sequencing results showed significant downregulation of adipogenic genes in aged eWAT, accompanied by elevated expression of inflammatory and fibrotic markers, which were validated by quantitative polymerase chain reaction. Comprehensive N- and O-glycoproteomic profiling revealed widespread glycosylation changes in aged adipose tissue, with differentially glycosylated proteins mainly located in the extracellular space and involved in innate immune responses, transport, signal transduction, and extracellular matrix–receptor interaction pathways.

Notably, IgG glycosylation levels were significantly increased in aged mice. The N-fucosylation of IgG1, IgG2a, and IgG3 was elevated, while only IgG2a showed increased O-fucosylation, indicating N-fucosylation as a common age-related modification across IgG subtypes. In vivo experiments demonstrated that B-cell depletion-induced IgG reduction enhanced adipogenic gene expression and suppressed fibrotic marker expression in aged mice. These effects were reversed by repletion with either fucosylated or nonfucosylated IgG. Compared with nonfucosylated IgG, fucosylated IgG exacerbated inflammation and fibrosis while more strongly inhibiting adipogenesis, confirming its role in driving age‑related adipose dysfunction.

The findings link IgG fucosylation to metabolic decline, chronic inflammation, and fibrosis in aging adipose tissue. Modulating IgG fucosylation may represent a potential strategy to alleviate age-related metabolic disorders and improve health in older populations.

The paper “Fucosylated IgG Contributes to Adipose Tissue Dysfunction During Aging,” is authored by Jingyu Wang, Wei Su, Haotian Wang, Licui Liu, Jinlong Li, Youxin Wang. Full text of the open access paper: https://doi.org/10.1016/j.eng.2025.10.008 . For more information about Engineering , visit the website at https://www.sciencedirect.com/journal/engineering .

Engineering

10.1016/j.eng.2025.10.008

Fucosylated IgG Contributes to Adipose Tissue Dysfunction During Aging

17-Feb-2026

Keywords

Health and Medicine

Article Information

Journal
Engineering
DOI
10.1016/j.eng.2025.10.008
Article Publication Date
2026-02-17
Article Title
Fucosylated IgG Contributes to Adipose Tissue Dysfunction During Aging

Contact Information

Rong Xie
Higher Education Press
xierong@hep.com.cn

How to Cite This Article

APA:
Higher Education Press. (2026, April 26). Fucosylated IgG linked to adipose tissue dysfunction in aging. Brightsurf News. https://www.brightsurf.com/news/8X5Y0GM1/fucosylated-igg-linked-to-adipose-tissue-dysfunction-in-aging.html
MLA:
"Fucosylated IgG linked to adipose tissue dysfunction in aging." Brightsurf News, Apr. 26 2026, https://www.brightsurf.com/news/8X5Y0GM1/fucosylated-igg-linked-to-adipose-tissue-dysfunction-in-aging.html.