AI Article Synopsis
- - Aging is a significant risk factor for cancer development, and both aging and tumor initiation involve changes in metabolism, which are not well understood in relation to the tumor microenvironment (TME).
- - Using a computational method called MMPC, researchers analyzed RNA sequencing data from 17 different cancer types and found notable metabolic differences in older patients, with increased activity in pathways like glycolysis but reduced function in immune cells like activated T cells and macrophages.
- - The study suggests that these age-related metabolic changes affect how glucose is utilized, altering immune responses and reshaping the TME, which could lead to new approaches for cancer treatment.
Article Abstract
Aging is an important risk factor for tumorigenesis. Metabolic reprogramming is a hallmark of both aging and tumor initiation. However, the manner in which the crosstalk between aging and metabolic reprogramming affects the tumor microenvironment (TME) to promote tumorigenesis was poorly explored. We utilized a computational approach proposed by our previous work, MMPC (Modeling Metabolic Plasticity by Pathway Pairwise Comparison), to characterize aging-related metabolic plasticity events using pan-cancer bulk RNA-seq data. Our analysis revealed a high degree of metabolically organized heterogeneity across 17 aging-related cancer types. In particular, a higher degree of several energy generation pathways, i.e., glycolysis and impaired oxidative phosphorylation, was observed in older patients. Similar phenomena were also found via single-cell RNA-seq analysis. Furthermore, those energy generation pathways were found to be weakened in activated T cells and macrophages, whereas they increased in exhausted T cells, immunosuppressive macrophages, and Tregs in older patients. It was suggested that aging-induced metabolic switches alter glucose utilization, thereby influencing immune function and resulting in the remodeling of the TME. This work offers new insights into the associations between tumor metabolism and the TME mediated by aging, linking with novel strategies for cancer therapy.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11506685 | PMC |
| http://dx.doi.org/10.3390/cells13201721 | DOI Listing |
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