ceh-23;isp-1

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Genetic mutants with ceh-23, isp-1 alterations

Names of genes are ordered alphabetically. For the order of interventions, please see the specific paper.

Temperature °C
20
Diet
OP50
Lifespan (days)
23.31
Lifespan change (compared to wild type)
31.03%
Phenotype
isp-1(qm150) mutants exhibited longer mean lifespan than ceh-23(ms23);isp-1(qm150) mutants. Loss of ceh-23 decreased the lifespan of isp-1 mutant by ~20%.
Lifespan comparisons
Double mutant ceh-23(ms23);isp-1(qm150) has a lifespan of 23.31 days, while single mutant isp-1(qm150) has a lifespan of 25.43 days, single mutant ceh-23(ms23) has a lifespan of 19.16 days and wild type has a lifespan of 17.79 days.
Type of interaction
See methods
Dependent
Citation
View abstract
Walter L et al., 2011, The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans. PLoS Biol. 9(6):e1001084 21713031 Click here to select all mutants from this PubMed ID in the graph
Abstract
Recent findings indicate that perturbations of the mitochondrial electron transport chain (METC) can cause extended longevity in evolutionarily diverse organisms. To uncover the molecular basis of how altered METC increases lifespan in C. elegans, we performed an RNAi screen and revealed that three predicted transcription factors are specifically required for the extended longevity of mitochondrial mutants. In particular, we demonstrated that the nuclear homeobox protein CEH-23 uniquely mediates the longevity but not the slow development, reduced brood size, or resistance to oxidative stress associated with mitochondrial mutations. Furthermore, we showed that ceh-23 expression levels are responsive to altered METC, and enforced overexpression of ceh-23 is sufficient to extend lifespan in wild-type background. Our data point to mitochondria-to-nucleus communications to be key for longevity determination and highlight CEH-23 as a novel longevity factor capable of responding to mitochondrial perturbations. These findings provide a new paradigm for how mitochondria impact aging and age-dependent diseases.

Temperature °C
20
Diet
OP50
Lifespan (days)
21.4
Lifespan change (compared to wild type)
20.29%
Phenotype
isp-1(qm150) mutants exhibited longer mean lifespan than ceh-23(ms23);isp-1(qm150) mutants. Loss of ceh-23 decreased the lifespan of isp-1 mutant by ~20%.
Lifespan comparisons
Double mutant ceh-23(ms23);isp-1(qm150) has a lifespan of 21.4 days, while single mutant isp-1(qm150) has a lifespan of 25.43 days, single mutant ceh-23(ms23) has a lifespan of 19.16 days and wild type has a lifespan of 17.79 days.
Type of interaction
See methods
Dependent
Citation
View abstract
Walter L et al., 2011, The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans. PLoS Biol. 9(6):e1001084 21713031 Click here to select all mutants from this PubMed ID in the graph
Abstract
Recent findings indicate that perturbations of the mitochondrial electron transport chain (METC) can cause extended longevity in evolutionarily diverse organisms. To uncover the molecular basis of how altered METC increases lifespan in C. elegans, we performed an RNAi screen and revealed that three predicted transcription factors are specifically required for the extended longevity of mitochondrial mutants. In particular, we demonstrated that the nuclear homeobox protein CEH-23 uniquely mediates the longevity but not the slow development, reduced brood size, or resistance to oxidative stress associated with mitochondrial mutations. Furthermore, we showed that ceh-23 expression levels are responsive to altered METC, and enforced overexpression of ceh-23 is sufficient to extend lifespan in wild-type background. Our data point to mitochondria-to-nucleus communications to be key for longevity determination and highlight CEH-23 as a novel longevity factor capable of responding to mitochondrial perturbations. These findings provide a new paradigm for how mitochondria impact aging and age-dependent diseases.

Temperature °C
20
Diet
OP50
Lifespan (days)
20.66
Lifespan change (compared to wild type)
16.13%
Phenotype
isp-1(qm150) mutants exhibited longer mean lifespan than ceh-23(ms23);isp-1(qm150) mutants. Loss of ceh-23 decreased the lifespan of isp-1 mutant by ~20%.
Lifespan comparisons
Double mutant ceh-23(ms23);isp-1(qm150) has a lifespan of 20.66 days, while single mutant isp-1(qm150) has a lifespan of 25.43 days, single mutant ceh-23(ms23) has a lifespan of 19.16 days and wild type has a lifespan of 17.79 days.
Type of interaction
See methods
Dependent
Citation
View abstract
Walter L et al., 2011, The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans. PLoS Biol. 9(6):e1001084 21713031 Click here to select all mutants from this PubMed ID in the graph
Abstract
Recent findings indicate that perturbations of the mitochondrial electron transport chain (METC) can cause extended longevity in evolutionarily diverse organisms. To uncover the molecular basis of how altered METC increases lifespan in C. elegans, we performed an RNAi screen and revealed that three predicted transcription factors are specifically required for the extended longevity of mitochondrial mutants. In particular, we demonstrated that the nuclear homeobox protein CEH-23 uniquely mediates the longevity but not the slow development, reduced brood size, or resistance to oxidative stress associated with mitochondrial mutations. Furthermore, we showed that ceh-23 expression levels are responsive to altered METC, and enforced overexpression of ceh-23 is sufficient to extend lifespan in wild-type background. Our data point to mitochondria-to-nucleus communications to be key for longevity determination and highlight CEH-23 as a novel longevity factor capable of responding to mitochondrial perturbations. These findings provide a new paradigm for how mitochondria impact aging and age-dependent diseases.

Temperature °C
20
Diet
OP50
Lifespan (days)
20.0
Lifespan change (compared to wild type)
12.42%
Phenotype
isp-1(qm150) mutants exhibited longer mean lifespan than ceh-23(ms23);isp-1(qm150) mutants. Loss of ceh-23 decreased the lifespan of isp-1 mutant by ~20%.
Lifespan comparisons
Double mutant ceh-23(ms23);isp-1(qm150) has a lifespan of 20.0 days, while single mutant isp-1(qm150) has a lifespan of 25.43 days, single mutant ceh-23(ms23) has a lifespan of 19.16 days and wild type has a lifespan of 17.79 days.
Type of interaction
See methods
Dependent
Citation
View abstract
Walter L et al., 2011, The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans. PLoS Biol. 9(6):e1001084 21713031 Click here to select all mutants from this PubMed ID in the graph
Abstract
Recent findings indicate that perturbations of the mitochondrial electron transport chain (METC) can cause extended longevity in evolutionarily diverse organisms. To uncover the molecular basis of how altered METC increases lifespan in C. elegans, we performed an RNAi screen and revealed that three predicted transcription factors are specifically required for the extended longevity of mitochondrial mutants. In particular, we demonstrated that the nuclear homeobox protein CEH-23 uniquely mediates the longevity but not the slow development, reduced brood size, or resistance to oxidative stress associated with mitochondrial mutations. Furthermore, we showed that ceh-23 expression levels are responsive to altered METC, and enforced overexpression of ceh-23 is sufficient to extend lifespan in wild-type background. Our data point to mitochondria-to-nucleus communications to be key for longevity determination and highlight CEH-23 as a novel longevity factor capable of responding to mitochondrial perturbations. These findings provide a new paradigm for how mitochondria impact aging and age-dependent diseases.

Temperature °C
20
Diet
OP50
Lifespan (days)
21.07
Lifespan change (compared to wild type)
18.44%
Phenotype
isp-1(qm150) mutants exhibited longer mean lifespan than ceh-23(ms23);isp-1(qm150) mutants. Loss of ceh-23 decreased the lifespan of isp-1 mutant by ~20%.
Lifespan comparisons
Double mutant ceh-23(ms23);isp-1(qm150) has a lifespan of 21.07 days, while single mutant isp-1(qm150) has a lifespan of 25.43 days, single mutant ceh-23(ms23) has a lifespan of 19.16 days and wild type has a lifespan of 17.79 days.
Type of interaction
See methods
Dependent
Citation
View abstract
Walter L et al., 2011, The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans. PLoS Biol. 9(6):e1001084 21713031 Click here to select all mutants from this PubMed ID in the graph
Abstract
Recent findings indicate that perturbations of the mitochondrial electron transport chain (METC) can cause extended longevity in evolutionarily diverse organisms. To uncover the molecular basis of how altered METC increases lifespan in C. elegans, we performed an RNAi screen and revealed that three predicted transcription factors are specifically required for the extended longevity of mitochondrial mutants. In particular, we demonstrated that the nuclear homeobox protein CEH-23 uniquely mediates the longevity but not the slow development, reduced brood size, or resistance to oxidative stress associated with mitochondrial mutations. Furthermore, we showed that ceh-23 expression levels are responsive to altered METC, and enforced overexpression of ceh-23 is sufficient to extend lifespan in wild-type background. Our data point to mitochondria-to-nucleus communications to be key for longevity determination and highlight CEH-23 as a novel longevity factor capable of responding to mitochondrial perturbations. These findings provide a new paradigm for how mitochondria impact aging and age-dependent diseases.

Temperature °C
20
Diet
OP50
Lifespan (days)
20.4
Lifespan change (compared to wild type)
8.97%
Phenotype
isp-1(qm150) mutants exhibited longer mean lifespan than ceh-23(ms23);isp-1(qm150) mutants. Loss of ceh-23 decreased the lifespan of isp-1 mutant by ~20%.
Lifespan comparisons
Double mutant ceh-23(ms23);isp-1(qm150) has a lifespan of 20.4 days, while single mutant isp-1(qm150) has a lifespan of 25.5 days, single mutant ceh-23(ms23) has a lifespan of 18.57 days and wild type has a lifespan of 18.72 days.
Type of interaction
See methods
Opposite lifespan effects of single mutants
Citation
View abstract
Walter L et al., 2011, The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans. PLoS Biol. 9(6):e1001084 21713031 Click here to select all mutants from this PubMed ID in the graph
Abstract
Recent findings indicate that perturbations of the mitochondrial electron transport chain (METC) can cause extended longevity in evolutionarily diverse organisms. To uncover the molecular basis of how altered METC increases lifespan in C. elegans, we performed an RNAi screen and revealed that three predicted transcription factors are specifically required for the extended longevity of mitochondrial mutants. In particular, we demonstrated that the nuclear homeobox protein CEH-23 uniquely mediates the longevity but not the slow development, reduced brood size, or resistance to oxidative stress associated with mitochondrial mutations. Furthermore, we showed that ceh-23 expression levels are responsive to altered METC, and enforced overexpression of ceh-23 is sufficient to extend lifespan in wild-type background. Our data point to mitochondria-to-nucleus communications to be key for longevity determination and highlight CEH-23 as a novel longevity factor capable of responding to mitochondrial perturbations. These findings provide a new paradigm for how mitochondria impact aging and age-dependent diseases.

Temperature °C
20
Diet
OP50
Lifespan (days)
19.04
Lifespan change (compared to wild type)
1.71%
Phenotype
isp-1(qm150) mutants exhibited longer mean lifespan than ceh-23(ms23);isp-1(qm150) mutants. Loss of ceh-23 decreased the lifespan of isp-1 mutant by ~20%.
Lifespan comparisons
Double mutant ceh-23(ms23);isp-1(qm150) has a lifespan of 19.04 days, while single mutant isp-1(qm150) has a lifespan of 25.5 days, single mutant ceh-23(ms23) has a lifespan of 18.57 days and wild type has a lifespan of 18.72 days.
Type of interaction
See methods
Opposite lifespan effects of single mutants
Citation
View abstract
Walter L et al., 2011, The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans. PLoS Biol. 9(6):e1001084 21713031 Click here to select all mutants from this PubMed ID in the graph
Abstract
Recent findings indicate that perturbations of the mitochondrial electron transport chain (METC) can cause extended longevity in evolutionarily diverse organisms. To uncover the molecular basis of how altered METC increases lifespan in C. elegans, we performed an RNAi screen and revealed that three predicted transcription factors are specifically required for the extended longevity of mitochondrial mutants. In particular, we demonstrated that the nuclear homeobox protein CEH-23 uniquely mediates the longevity but not the slow development, reduced brood size, or resistance to oxidative stress associated with mitochondrial mutations. Furthermore, we showed that ceh-23 expression levels are responsive to altered METC, and enforced overexpression of ceh-23 is sufficient to extend lifespan in wild-type background. Our data point to mitochondria-to-nucleus communications to be key for longevity determination and highlight CEH-23 as a novel longevity factor capable of responding to mitochondrial perturbations. These findings provide a new paradigm for how mitochondria impact aging and age-dependent diseases.

Temperature °C
20
Diet
OP50
Lifespan (days)
18.76
Lifespan change (compared to wild type)
0.21%
Phenotype
isp-1(qm150) mutants exhibited longer mean lifespan than ceh-23(ms23);isp-1(qm150) mutants. Loss of ceh-23 decreased the lifespan of isp-1 mutant by ~20%.
Lifespan comparisons
Double mutant ceh-23(ms23);isp-1(qm150) has a lifespan of 18.76 days, while single mutant isp-1(qm150) has a lifespan of 25.5 days, single mutant ceh-23(ms23) has a lifespan of 18.57 days and wild type has a lifespan of 18.72 days.
Type of interaction
See methods
Opposite lifespan effects of single mutants
Citation
View abstract
Walter L et al., 2011, The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans. PLoS Biol. 9(6):e1001084 21713031 Click here to select all mutants from this PubMed ID in the graph
Abstract
Recent findings indicate that perturbations of the mitochondrial electron transport chain (METC) can cause extended longevity in evolutionarily diverse organisms. To uncover the molecular basis of how altered METC increases lifespan in C. elegans, we performed an RNAi screen and revealed that three predicted transcription factors are specifically required for the extended longevity of mitochondrial mutants. In particular, we demonstrated that the nuclear homeobox protein CEH-23 uniquely mediates the longevity but not the slow development, reduced brood size, or resistance to oxidative stress associated with mitochondrial mutations. Furthermore, we showed that ceh-23 expression levels are responsive to altered METC, and enforced overexpression of ceh-23 is sufficient to extend lifespan in wild-type background. Our data point to mitochondria-to-nucleus communications to be key for longevity determination and highlight CEH-23 as a novel longevity factor capable of responding to mitochondrial perturbations. These findings provide a new paradigm for how mitochondria impact aging and age-dependent diseases.

Temperature °C
20
Diet
OP50
Lifespan (days)
17.86
Lifespan change (compared to wild type)
-4.59%
Phenotype
isp-1(qm150) mutants exhibited longer mean lifespan than ceh-23(ms23);isp-1(qm150) mutants. Loss of ceh-23 decreased the lifespan of isp-1 mutant by ~20%.
Lifespan comparisons
Double mutant ceh-23(ms23);isp-1(qm150) has a lifespan of 17.86 days, while single mutant isp-1(qm150) has a lifespan of 25.5 days, single mutant ceh-23(ms23) has a lifespan of 18.57 days and wild type has a lifespan of 18.72 days.
Type of interaction
See methods
Opposite lifespan effects of single mutants
Citation
View abstract
Walter L et al., 2011, The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans. PLoS Biol. 9(6):e1001084 21713031 Click here to select all mutants from this PubMed ID in the graph
Abstract
Recent findings indicate that perturbations of the mitochondrial electron transport chain (METC) can cause extended longevity in evolutionarily diverse organisms. To uncover the molecular basis of how altered METC increases lifespan in C. elegans, we performed an RNAi screen and revealed that three predicted transcription factors are specifically required for the extended longevity of mitochondrial mutants. In particular, we demonstrated that the nuclear homeobox protein CEH-23 uniquely mediates the longevity but not the slow development, reduced brood size, or resistance to oxidative stress associated with mitochondrial mutations. Furthermore, we showed that ceh-23 expression levels are responsive to altered METC, and enforced overexpression of ceh-23 is sufficient to extend lifespan in wild-type background. Our data point to mitochondria-to-nucleus communications to be key for longevity determination and highlight CEH-23 as a novel longevity factor capable of responding to mitochondrial perturbations. These findings provide a new paradigm for how mitochondria impact aging and age-dependent diseases.

Temperature °C
20
Diet
OP50
Lifespan (days)
21.24
Lifespan change (compared to wild type)
13.46%
Phenotype
isp-1(qm150) mutants exhibited longer mean lifespan than ceh-23(ms23);isp-1(qm150) mutants. Loss of ceh-23 decreased the lifespan of isp-1 mutant by ~20%.
Lifespan comparisons
Double mutant ceh-23(ms23);isp-1(qm150) has a lifespan of 21.24 days, while single mutant isp-1(qm150) has a lifespan of 25.5 days, single mutant ceh-23(ms23) has a lifespan of 18.57 days and wild type has a lifespan of 18.72 days.
Type of interaction
See methods
Opposite lifespan effects of single mutants
Citation
View abstract
Walter L et al., 2011, The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans. PLoS Biol. 9(6):e1001084 21713031 Click here to select all mutants from this PubMed ID in the graph
Abstract
Recent findings indicate that perturbations of the mitochondrial electron transport chain (METC) can cause extended longevity in evolutionarily diverse organisms. To uncover the molecular basis of how altered METC increases lifespan in C. elegans, we performed an RNAi screen and revealed that three predicted transcription factors are specifically required for the extended longevity of mitochondrial mutants. In particular, we demonstrated that the nuclear homeobox protein CEH-23 uniquely mediates the longevity but not the slow development, reduced brood size, or resistance to oxidative stress associated with mitochondrial mutations. Furthermore, we showed that ceh-23 expression levels are responsive to altered METC, and enforced overexpression of ceh-23 is sufficient to extend lifespan in wild-type background. Our data point to mitochondria-to-nucleus communications to be key for longevity determination and highlight CEH-23 as a novel longevity factor capable of responding to mitochondrial perturbations. These findings provide a new paradigm for how mitochondria impact aging and age-dependent diseases.

Temperature °C
20
Diet
OP50
Lifespan (days)
23.95
Lifespan change (compared to wild type)
42.90%
Phenotype
isp-1(qm150) mutants exhibited longer mean lifespan than ceh-23(ms23);isp-1(qm150) mutants. Loss of ceh-23 decreased the lifespan of isp-1 mutant by ~20%.
Lifespan comparisons
Double mutant ceh-23(ms23);isp-1(qm150) has a lifespan of 23.95 days, while single mutant isp-1(qm150) has a lifespan of 25.15 days, single mutant ceh-23(ms23) has a lifespan of 19.7 days and wild type has a lifespan of 16.76 days.
Type of interaction
See methods
Dependent
Citation
View abstract
Walter L et al., 2011, The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans. PLoS Biol. 9(6):e1001084 21713031 Click here to select all mutants from this PubMed ID in the graph
Abstract
Recent findings indicate that perturbations of the mitochondrial electron transport chain (METC) can cause extended longevity in evolutionarily diverse organisms. To uncover the molecular basis of how altered METC increases lifespan in C. elegans, we performed an RNAi screen and revealed that three predicted transcription factors are specifically required for the extended longevity of mitochondrial mutants. In particular, we demonstrated that the nuclear homeobox protein CEH-23 uniquely mediates the longevity but not the slow development, reduced brood size, or resistance to oxidative stress associated with mitochondrial mutations. Furthermore, we showed that ceh-23 expression levels are responsive to altered METC, and enforced overexpression of ceh-23 is sufficient to extend lifespan in wild-type background. Our data point to mitochondria-to-nucleus communications to be key for longevity determination and highlight CEH-23 as a novel longevity factor capable of responding to mitochondrial perturbations. These findings provide a new paradigm for how mitochondria impact aging and age-dependent diseases.

Temperature °C
20
Diet
OP50
Lifespan (days)
22.57
Lifespan change (compared to wild type)
34.67%
Phenotype
isp-1(qm150) mutants exhibited longer mean lifespan than ceh-23(ms23);isp-1(qm150) mutants. Loss of ceh-23 decreased the lifespan of isp-1 mutant by ~20%.
Lifespan comparisons
Double mutant ceh-23(ms23);isp-1(qm150) has a lifespan of 22.57 days, while single mutant isp-1(qm150) has a lifespan of 25.15 days, single mutant ceh-23(ms23) has a lifespan of 19.7 days and wild type has a lifespan of 16.76 days.
Type of interaction
See methods
Dependent
Citation
View abstract
Walter L et al., 2011, The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans. PLoS Biol. 9(6):e1001084 21713031 Click here to select all mutants from this PubMed ID in the graph
Abstract
Recent findings indicate that perturbations of the mitochondrial electron transport chain (METC) can cause extended longevity in evolutionarily diverse organisms. To uncover the molecular basis of how altered METC increases lifespan in C. elegans, we performed an RNAi screen and revealed that three predicted transcription factors are specifically required for the extended longevity of mitochondrial mutants. In particular, we demonstrated that the nuclear homeobox protein CEH-23 uniquely mediates the longevity but not the slow development, reduced brood size, or resistance to oxidative stress associated with mitochondrial mutations. Furthermore, we showed that ceh-23 expression levels are responsive to altered METC, and enforced overexpression of ceh-23 is sufficient to extend lifespan in wild-type background. Our data point to mitochondria-to-nucleus communications to be key for longevity determination and highlight CEH-23 as a novel longevity factor capable of responding to mitochondrial perturbations. These findings provide a new paradigm for how mitochondria impact aging and age-dependent diseases.

Temperature °C
20
Diet
OP50
Lifespan (days)
19.01
Lifespan change (compared to wild type)
21.78%
Phenotype
isp-1(qm150) mutants exhibited longer mean lifespan than ceh-23(ms23);isp-1(qm150) mutants. Loss of ceh-23 decreased the lifespan of isp-1 mutant by ~20%.
Lifespan comparisons
Double mutant ceh-23(ms23);isp-1(qm150) has a lifespan of 19.01 days, while single mutant isp-1(qm150) has a lifespan of 19.63 days, single mutant ceh-23(ms23) has a lifespan of 15.4 days and wild type has a lifespan of 15.61 days.
Type of interaction
See methods
Opposite lifespan effects of single mutants
Citation
View abstract
Walter L et al., 2011, The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans. PLoS Biol. 9(6):e1001084 21713031 Click here to select all mutants from this PubMed ID in the graph
Abstract
Recent findings indicate that perturbations of the mitochondrial electron transport chain (METC) can cause extended longevity in evolutionarily diverse organisms. To uncover the molecular basis of how altered METC increases lifespan in C. elegans, we performed an RNAi screen and revealed that three predicted transcription factors are specifically required for the extended longevity of mitochondrial mutants. In particular, we demonstrated that the nuclear homeobox protein CEH-23 uniquely mediates the longevity but not the slow development, reduced brood size, or resistance to oxidative stress associated with mitochondrial mutations. Furthermore, we showed that ceh-23 expression levels are responsive to altered METC, and enforced overexpression of ceh-23 is sufficient to extend lifespan in wild-type background. Our data point to mitochondria-to-nucleus communications to be key for longevity determination and highlight CEH-23 as a novel longevity factor capable of responding to mitochondrial perturbations. These findings provide a new paradigm for how mitochondria impact aging and age-dependent diseases.

Temperature °C
20
Diet
OP50
Lifespan (days)
18.47
Lifespan change (compared to wild type)
18.32%
Phenotype
isp-1(qm150) mutants exhibited longer mean lifespan than ceh-23(ms23);isp-1(qm150) mutants. Loss of ceh-23 decreased the lifespan of isp-1 mutant by ~20%.
Lifespan comparisons
Double mutant ceh-23(ms23);isp-1(qm150) has a lifespan of 18.47 days, while single mutant isp-1(qm150) has a lifespan of 19.63 days, single mutant ceh-23(ms23) has a lifespan of 15.4 days and wild type has a lifespan of 15.61 days.
Type of interaction
See methods
Opposite lifespan effects of single mutants
Citation
View abstract
Walter L et al., 2011, The homeobox protein CEH-23 mediates prolonged longevity in response to impaired mitochondrial electron transport chain in C. elegans. PLoS Biol. 9(6):e1001084 21713031 Click here to select all mutants from this PubMed ID in the graph
Abstract
Recent findings indicate that perturbations of the mitochondrial electron transport chain (METC) can cause extended longevity in evolutionarily diverse organisms. To uncover the molecular basis of how altered METC increases lifespan in C. elegans, we performed an RNAi screen and revealed that three predicted transcription factors are specifically required for the extended longevity of mitochondrial mutants. In particular, we demonstrated that the nuclear homeobox protein CEH-23 uniquely mediates the longevity but not the slow development, reduced brood size, or resistance to oxidative stress associated with mitochondrial mutations. Furthermore, we showed that ceh-23 expression levels are responsive to altered METC, and enforced overexpression of ceh-23 is sufficient to extend lifespan in wild-type background. Our data point to mitochondria-to-nucleus communications to be key for longevity determination and highlight CEH-23 as a novel longevity factor capable of responding to mitochondrial perturbations. These findings provide a new paradigm for how mitochondria impact aging and age-dependent diseases.

Search genes: ceh-23 isp-1

Entrez ID
Symbol
GenAge
Wormbase ID

176096
ceh-23
View on GenAge (ceh-23)
WBGene00000446

Homeobox protein ceh-23

Locus: CELE_ZK652.5

Wormbase description: ceh-23 encodes a homeodomain protein required for a specific differentiated trait of the thermosensory interneuron AIY; a ceh-23::gfp promoter fusion is expressed in nine pairs of head neurons, including seven amphid sensory neurons, the BAG sensory neurons, AIY interneurons, and the CAN neurons that are in close association with the excretory canal.

Entrez ID
Symbol
GenAge
Wormbase ID

177609
isp-1
View on GenAge (isp-1)
WBGene00002162

Cytochrome b-c1 complex subunit Rieske, mitochondrial

Locus: CELE_F42G8.12

Wormbase description: isp-1 encodes a Rieske iron sulphur protein (ISP) which is a subunit of the mitochondrial complex III in the mitochondrial membrane; the subunits are highly conserved in all mitochondria and aerobic bacteria; mitochondrial complex III catalyses electron transport from ubiquinol to cytochrome c; isp-1 mutants show low oxygen consumption, a decreased sensitivity to reactive oxygen species and increased lifespan suggesting that mitochondrial electron transport is a key factor affecting life span; isp-1 affects the rates of physiological processes like reproduction and development and also affects behavior.

Orthologs of ceh-23;isp-1 in SynergyAge

Show in SynergyAge
Species	Gene

Not in SynergyAge
Species	Gene

Orthologs of ceh-23 in SynergyAge

Show in SynergyAge
Species	Gene

Not in SynergyAge
Species	Gene
Drosophila melanogaster	exex

Orthologs of isp-1 in SynergyAge

Show in SynergyAge
Species	Gene

Not in SynergyAge
Species	Gene
Mus musculus	Uqcrfs1