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Showing 1–11 of 11 results
Advanced filters: Author: Hiran A. Prag Clear advanced filters

  • Giles et al. developed a method for noninvasive absorbance measurement of mitochondrial hemes to monitor the mitochondrial membrane potential in the perfused heart. They then applied this approach to show how the mitochondrial membrane potential changed during cardiac ischemia.

    • Abigail V. Giles
    • Raul Covian
    • Robert S. Balaban
    ResearchOpen Access
    Nature Cardiovascular Research
    Volume: 4, P: 1627-1641

  • The naked mole-rat exhibits extreme longevity, resistance to hypoxia and absence of cardiovascular disease. Here, Faulkes et al. identify mechanisms behind these traits by comparing cardiac metabolomes and transcriptomes of naked more-rats to other African mole-rat genera and evolutionary divergent mammals.

    • Chris G. Faulkes
    • Thomas R. Eykyn
    • Dunja Aksentijevic
    ResearchOpen Access
    Nature Communications
    Volume: 15, P: 1-13

  • Inhibition of the tricarboxylic acid cycle enzyme fumarate hydratase leads to deregulation of cytokine production in macrophages, which has implications in human diseases such as systemic lupus erythematosus.

    • Alexander Hooftman
    • Christian G. Peace
    • Luke A. J. O’Neill
    Research
    Nature
    Volume: 615, P: 490-498

  • Reactive oxygen species (ROS) production by reverse electron transfer (RET) through complex I is thought to cause tissue damage from heart attacks. Here, the authors combine in vivo work with biochemical and cryo-EM analyses to characterize the effects of a P25L mutation in the ND6 subunit of mitochondrial complex I. They observe that this mutation does not affect oxidative phosphorylation but renders complex I unable to generate ROS by RET: ND6-P25L mice are protected against cardiac ischaemia–reperfusion injury, thus providing evidence for the proposed role of ROS production in myocardial infarction.

    • Zhan Yin
    • Nils Burger
    • Judy Hirst
    ResearchOpen Access
    Nature Communications
    Volume: 12, P: 1-12

  • Mitochondrial DNA damage, metabolic disruption and aging have all been associated with cancer. These three threads are now woven together to show that aging-associated somatic mutations to mitochondrial DNA alter mitochondrial serine metabolism to support cell transformation and colon-cancer development.

    • Hiran A. Prag
    • Michael P. Murphy
    News & Views
    Nature Cancer
    Volume: 1, P: 941-942

  • Intermediate metabolites of the Krebs cycle serve bioenergetic and biosynthetic needs but have recently also been linked to signalling. The authors of this Review summarize such non-metabolic signalling functions of succinate, fumarate, itaconate, 2-hydroxyglutarate isomers and acetyl-CoA in both immune cells and cancer cells.

    • Dylan G. Ryan
    • Michael P. Murphy
    • Evanna L. Mills
    Reviews
    Nature Metabolism
    Volume: 1, P: 16-33