Mass Spec Roundup: Hidden Origins and Cellular States - Summary - MDSpire
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Mass Spec Roundup: Hidden Origins and Cellular States
New studies separate host and microbial metabolites, trace secreted proteins, identify a pro-regenerative cardiomyocyte state, and map macrophage lipid metabolism
To explore the origins of metabolites and cellular states using advanced mass spectrometry techniques.
Approach:
Microbiome Metabolites: Isotope tracing was used to determine the production of indole and phenol metabolites by mammalian cells, distinguishing between host and microbial contributions.
Secretome Analysis: An in vivo proximity-labeling platform was developed to trace secreted proteins back to specific cell types and analyze changes across metabolic states.
Cardiac Regeneration: Single-cell proteomic analysis linked Myc expression to metabolic reprogramming in cardiomyocytes, identifying a pro-regenerative cell population.
Macrophage Phenotypes: Cell-resolved MALDI imaging differentiated macrophage phenotypes and highlighted phospholipid metabolism as a key factor.
Key Findings:
Mammalian cells can produce several circulating indole and phenol metabolites independently of the gut microbiome, as shown by isotope tracing.
The TurboID platform enabled the identification of low-abundance secreted proteins and their changes during metabolic states.
Myc expression in cardiomyocytes shifted metabolic pathways from fatty acid oxidation to glycolysis, indicating a pro-regenerative state.
M1 macrophages synthesized more phospholipids than M2 macrophages, suggesting a functional role in their antitumor activity.
Interpretation:
The studies highlight the need to distinguish between host and microbial contributions to metabolite production and the metabolic states of cells.
Limitations:
The study on microbiome metabolites may not account for all variables influencing metabolite levels.
The secretome analysis may not capture all secreted proteins due to detection limits.
The findings on cardiac regeneration are based on mouse models and may not directly translate to human physiology.
Conclusion:
These findings provide insights into the metabolic origins of key metabolites and cellular states.