Decreased liver B vitamin-related enzymes as a metabolic hallmark of cancer cachexia

Author:

Kojima YasushiORCID,Mishiro-Sato EmiORCID,Fujishita TeruakiORCID,Satoh Kiyotoshi,Kajino-Sakamoto RieORCID,Oze IsaoORCID,Nozawa Kazuki,Narita Yukiya,Ogata Takatsugu,Matsuo KeitaroORCID,Muro Kei,Taketo Makoto Mark,Soga TomoyoshiORCID,Aoki MasahiroORCID

Abstract

AbstractCancer cachexia is a complex metabolic disorder accounting for ~20% of cancer-related deaths, yet its metabolic landscape remains unexplored. Here, we report a decrease in B vitamin-related liver enzymes as a hallmark of systemic metabolic changes occurring in cancer cachexia. Metabolomics of multiple mouse models highlights cachexia-associated reductions of niacin, vitamin B6, and a glycine-related subset of one-carbon (C1) metabolites in the liver. Integration of proteomics and metabolomics reveals that liver enzymes related to niacin, vitamin B6, and glycine-related C1 enzymes dependent on B vitamins decrease linearly with their associated metabolites, likely reflecting stoichiometric cofactor-enzyme interactions. The decrease of B vitamin-related enzymes is also found to depend on protein abundance and cofactor subtype. These metabolic/proteomic changes and decreased protein malonylation, another cachexia feature identified by protein post-translational modification analysis, are reflected in blood samples from mouse models and gastric cancer patients with cachexia, underscoring the clinical relevance of our findings.

Funder

The Hori Science and Arts Foundation, Project Mirai Cancer Research Grants The Takeda Science Foundation

MEXT | Japan Society for the Promotion of Science

Suzuken Memorial Foundation

Nagono Medical Foundation

Daiwa Securities Health Foundation

Foundation for Promotion of Cancer Research

Japan Agency for Medical Research and Development

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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