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Literature DB >> 26430544

Searching for the elusive mitochondrial longevity signal in C. elegans.

Christopher F Bennett¹, Haeri Choi², Matt Kaeberlein².

Abstract

There is a growing list of examples where perturbed mitochondrial function is associated with increased longevity, yet the exact mechanisms have remained elusive. This phenomenon was first documented, and has been studied most extensively, in C. elegans. One prominent model proposed that lifespan extension resulting from electron transport chain inhibition is due to induction of the mitochondrial unfolded protein response. This model requires revision in light of recent data showing that the mitochondrial unfolded protein response, as defined by the field, is neither necessary nor sufficient for lifespan extension in C. elegans. Several additional factors have been proposed to underlie this lifespan extension, which is likely to be multifactorial and complex.

Entities: Species

Keywords: ATFS-1; aging; electron transport chain; hsp-6; lifespan; longevity; mitochondrial unfolded protein response

Year: 2014 PMID： 26430544 PMCID： PMC4588544 DOI： 10.4161/21624046.2014.959404

Source DB: PubMed Journal: Worm ISSN： 2162-4046

42 in total

1. Role of the ubiquitin-like protein Hub1 in splice-site usage and alternative splicing.

Authors: Shravan Kumar Mishra; Tim Ammon; Grzegorz M Popowicz; Marcin Krajewski; Roland J Nagel; Manuel Ares; Tad A Holak; Stefan Jentsch
Journal: Nature Date: 2011-05-25 Impact factor: 49.962

2. The cell-non-autonomous nature of electron transport chain-mediated longevity.

Authors: Jenni Durieux; Suzanne Wolff; Andrew Dillin
Journal: Cell Date: 2011-01-07 Impact factor: 41.582

3. Reversible inactivation of HIF-1 prolyl hydroxylases allows cell metabolism to control basal HIF-1.

Authors: Huasheng Lu; Clifton L Dalgard; Ahmed Mohyeldin; Thomas McFate; A Sasha Tait; Ajay Verma
Journal: J Biol Chem Date: 2005-10-13 Impact factor: 5.157

4. The intrinsic apoptosis pathway mediates the pro-longevity response to mitochondrial ROS in C. elegans.

Authors: Callista Yee; Wen Yang; Siegfried Hekimi
Journal: Cell Date: 2014-05-08 Impact factor: 41.582

5. The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans.

Authors: Ludivine Walter; Aiswarya Baruah; Hsin-Wen Chang; Heather Mae Pace; Siu Sylvia Lee
Journal: PLoS Biol Date: 2011-06-21 Impact factor: 8.029

3. New functional and biophysical insights into the mitochondrial Rieske iron-sulfur protein from genetic suppressor analysis in C. elegans.

Authors: Gholamali Jafari; Brian M Wasko; Matt Kaeberlein; Antony R Crofts
Journal: Worm Date: 2016-04-11

3 in total

Searching for the elusive mitochondrial longevity signal in C. elegans.

1. Role of the ubiquitin-like protein Hub1 in splice-site usage and alternative splicing.

2. The cell-non-autonomous nature of electron transport chain-mediated longevity.

3. Reversible inactivation of HIF-1 prolyl hydroxylases allows cell metabolism to control basal HIF-1.

4. The intrinsic apoptosis pathway mediates the pro-longevity response to mitochondrial ROS in C. elegans.

5. The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans.

6. Protective coupling of mitochondrial function and protein synthesis via the eIF2α kinase GCN-2.

7. The HIF-1 hypoxia-inducible factor modulates lifespan in C. elegans.

8. Surveillance-activated defenses block the ROS-induced mitochondrial unfolded protein response.

9. Genome-Wide RNAi Longevity Screens in Caenorhabditis elegans.

10. Activation of the mitochondrial unfolded protein response does not predict longevity in Caenorhabditis elegans.

1. The mysterious relationship between reproduction and longevity.

Review 2. Biochemical Genetic Pathways that Modulate Aging in Multiple Species.

3. New functional and biophysical insights into the mitochondrial Rieske iron-sulfur protein from genetic suppressor analysis in C. elegans.