Chemical genetic screen identifies lithocholic acid as an anti-aging compound that extends yeast chronological life span in a TOR-independent manner, by modulating housekeeping longevity assurance processes

Goldberg, Alexander A.; Richard, Vincent; Kyryakov, Pavlo; Bourque, Simon D.; Beach, Adam; Burstein, Michelle T.; Glebov, Anastasia; Koupaki, Olivia; Boukh‐Viner, Tatiana; Gregg, Christopher; Juneau, Mylène; English, Ann M.; Thomas, David Y.; Titorenko, Vladimir I.

doi:10.18632/aging.100168

Cited by 101 publications

(227 citation statements)

References 76 publications

(150 reference statements)

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“…The former is regarded as a model for dividing mammalian cells (i.e., stem cells), while the latter can be utilized as a model for non-dividing mammalian cells (i.e., neurons). 29,30 We found that, compared with the WT, replicative lifespan is significantly reduced in Δmgm1 cells (Δmgm1: 11 generations vs. WT: 23 generations) (Fig. 4A).…”

Section: Resultsmentioning

confidence: 89%

Unopposed mitochondrial fission leads to severe lifespan shortening

Scheckhuber¹,

Wanger²,

Mignat³

et al. 2011

Cell Cycle

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Section: Resultsmentioning

confidence: 89%

Unopposed mitochondrial fission leads to severe lifespan shortening

Scheckhuber¹,

Wanger²,

Mignat³

et al. 2011

Cell Cycle

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“…This pathway stimulates transcription of the RSB1 gene; the resulting increased abundance of Rsb1p promotes further reduction of PE in the outer leaflet of the PM by (1) enhancing a stimulating effect of Rsb1p on the Lem3p-dependent transport of PE from the outer leaflet to the inner (intracellular) leaflet of the PM; and (2) amplifying an inhibitory effect of Rsb1p on the Yor1p-dependent transport of PE within the PM bilayer in the opposite direction. An ensuing depletion of PE in the outer leaflet of the PM elevates the permeability of this cellular membrane for small molecules (such as propidium iodide 1,71 ), thereby contributing to the commitment of yeast to liponecrotic PCD.…”

Section: Discussionmentioning

confidence: 99%

Mechanism of liponecrosis, a distinct mode of programmed cell death

Richard¹,

Beach²,

Piano³

et al. 2014

Cell Cycle

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“…[3][4][5][6]16,20,25,31,33,56 Of note, we found that a treatment of yeast cells with LCA alters the agerelated chronology of these mitochondrial processes. 5,36,38,[68][69][70] We therefore hypothesized that LCA may impact not only the levels of numerous mitochondrial proteins but also the levels of proteins in cellular locations outside mitochondria. To validate our hypothesis, we used quantitative mass spectrometry to compare proteins that were recovered in total lysates of WT cells cultured in the presence of LCA or in its absence.…”

Section: Lca Elicits Age-related Changes In Mitochondrial Proteomementioning

confidence: 99%

“…These cellular processes include the following: (1) glycogen degradation; (2) the glycolytic pathway; (3) the pentose phosphate pathway; (4) pyruvate conversion to acetyl-CoA; (5) the maintenance of redox balance between NAD and NADH with the help of carnitine and glycerol-3-phosphate shuttles; (6) ROS detoxification; (7) stress response; (8) glutathione synthesis; (9) gluconeogenesis; (10) ethanol formation; (11) the synthesis and hydrolytic degradation of triacylglycerols (TAG) and ergosteryl esters (EE), the 2 major neutral lipids; (12) the synthesis of various amino acids; (13) nucleotide synthesis; (14) the assembly of the 40S and 60S ribosomal subunits from numerous protein components whose levels were altered by LCA; and (15) proteasomal and vacuolar protein degradation. 4,5,39,41,38,71,72 We then subjected cellular proteins whose levels were changed in yeast grown in a medium supplemented with LCA to bioinformatic analysis with the help of the SPELL online search engine, 51 as described above for mitochondrial proteins. Just as our bioinformatic analysis of mitochondrial proteins revealed (see above), we found that each of the cellular proteins whose level was altered in yeast cultured with LCA belongs to the following 2 multi-clustered regulons: (1) the PMD regulon, which consisted of the rho 0 (Rtg2p governed) cluster, S1 cluster, general TCA cycle dysfunction cluster, kgd1D, kgd2D or lpd1D cluster, yme1Dmdl1D Figure 2.…”

Section: Lca Elicits Age-related Changes In Mitochondrial Proteomementioning

confidence: 99%

“…Yeast cells for these experiments were cultured under caloric restriction (CR) conditions on 0.2% glucose rather than under non-CR conditions on 2% glucose. We chose CR conditions for the following reasons: (1) mitochondria, the organelles whose LCA-driven ability to operate as signaling compartments in yeast chronological aging we investigated in this study, are significantly more abundant and functionally active in yeast cells limited in calorie supply than they are in yeast cells on a high-calorie diet; 37,38 …”

Section: Introductionmentioning

confidence: 99%

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