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"Isomeric lipid signatures reveal compartmentalized fatty acid metaboli" by Reuben S.E. Young, Andrew P. Bowman et al.

The cellular energy and biomass demands of cancer drive a complex dynamic between uptake of extracellular FAs and their de novo synthesis. Given that oxidation of de novo synthesized FAs for energy would result in net-energy loss, there is an implication that FAs from these two sources must have distinct metabolic fates; however, hitherto, all FAs have been considered part of a common pool. To probe potential metabolic partitioning of cellular FAs, cancer cells were supplemented with stable isotope-labeled FAs. Structural analysis of the resulting glycerophospholipids revealed that labeled FAs from uptake were largely incorporated to canonical (sn-) positions on the glycerol backbone. Surprisingly, labeled FA uptake also disrupted canonical isomer patterns of the unlabeled lipidome and induced repartitioning of n-3 and n-6 PUFAs into glycerophospholipid classes. These structural changes support the existence of differences in the metabolic fates of FAs derived from uptake or de novo so ....

Fa Transport , Maging Ms , Ipid Isomers , Ipolysis And Fa Metabolism , Ozone Induced Dissociation , Hospholipid Metabolism , Hospholipids Phosphatidylcholine , Table Isotope Tracing ,