C. elegans orthologs MUT-7/CeWRN-1 of Werner syndrome protein regulate neuronal plasticity

Hsu, Tsung-Yuan; Zhang, Bo; L’Étoile, Noëlle D.; Juang, Bi-Tzen

doi:10.7554/elife.62449

Cited by 7 publications

(10 citation statements)

References 41 publications

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“…Olfactory learning requires downregulation of the expression of a guanylyl cyclase, ODR-1, by endogenous odr-1 siRNA. The production of this siRNA is modulated by MUT-7 in the cytoplasm, and this siRNA is required for the formation of the complex with chromatin-associated heterochromatin protein 1 (HP1) homolog HPL-2 in the nucleus; HPL-2 binds to odr-1 mRNA to silence ODR-1 expression in a negative feedback loop [ 54 , 55 ]. These findings suggest that the WRN exonuclease is critical for the installation of epigenetic modifications that regulate gene expression.…”

Section: Roles Of the Wrn Exonuclease In Gene Regulationmentioning

confidence: 99%

“…This behavioral state is termed long-term olfactory learning and requires the accumulation of EGL-4 in the nucleus of AWC neurons [ 68 , 69 ]. When EGL-4 accumulates in the nucleus, MUT-7 acts specifically in the cytoplasm to promote the synthesis of 22G siRNA [ 54 , 55 ]. Endogenous 22G siRNAs are 22 nucleotides long and have a guanosine at the 5′ end [ 63 ].…”

Section: Separate Functional Domains Of the Wrn Ortholog In C Elegansmentioning

confidence: 99%

“…The nuclear argonaute protein NRDE-3 acts as a shuttle to carry these 22G siRNAs from the cytoplasm to the nucleus [ 70 ]. The entrance of the 22G siRNAs into the nucleus induces nuclear EGL-4 to phosphorylate nuclear MUT-7 [ 54 ]. Activated MUT-7 is required for the association between HPL-2 and CeWRN-1 and their loading on the siRNA-targeted locus odr-1 [ 54 ].…”

Section: Separate Functional Domains Of the Wrn Ortholog In C Elegansmentioning

confidence: 99%

“…The entrance of the 22G siRNAs into the nucleus induces nuclear EGL-4 to phosphorylate nuclear MUT-7 [ 54 ]. Activated MUT-7 is required for the association between HPL-2 and CeWRN-1 and their loading on the siRNA-targeted locus odr-1 [ 54 ]. This results in a reduction in the mRNA level of odr-1 , which encodes the guanylyl cyclase ODR-1 that generates the second messenger cGMP; it is this reduction that is highly correlated with the adaptation of the odor-seeking response [ 54 , 55 ].…”

Section: Separate Functional Domains Of the Wrn Ortholog In C Elegansmentioning

confidence: 99%

“…Activated MUT-7 is required for the association between HPL-2 and CeWRN-1 and their loading on the siRNA-targeted locus odr-1 [ 54 ]. This results in a reduction in the mRNA level of odr-1 , which encodes the guanylyl cyclase ODR-1 that generates the second messenger cGMP; it is this reduction that is highly correlated with the adaptation of the odor-seeking response [ 54 , 55 ]. These findings support the idea that the 3′-5′ exonuclease of MUT-7 is required for siRNA synthesis and suggest that the import of siRNA into the AWC neuron nucleus is required for CeWRN-1-dependent olfactory learning ( Figure 3 ).…”

Section: Separate Functional Domains Of the Wrn Ortholog In C Elegansmentioning

confidence: 99%

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MUT-7 Provides Molecular Insight into the Werner Syndrome Exonuclease

Hsu

Chen

et al. 2021

Cells

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Werner syndrome (WS) is a rare recessive genetic disease characterized by premature aging. Individuals with this disorder develop normally during childhood, but their physiological conditions exacerbate the aging process in late adolescence. WS is caused by mutation of the human WS gene (WRN), which encodes two main domains, a 3′-5′ exonuclease and a 3′-5′ helicase. Caenorhabditis elegans expresses human WRN orthologs as two different proteins: MUT-7, which has a 3′-5′ exonuclease domain, and C. elegans WRN-1 (CeWRN-1), which has only helicase domains. These unique proteins dynamically regulate olfactory memory in C. elegans, providing insight into the molecular roles of WRN domains in humans. In this review, we specifically focus on characterizing the function of MUT-7 in small interfering RNA (siRNA) synthesis in the cytoplasm and the roles of siRNA in directing nuclear CeWRN-1 loading onto a heterochromatin complex to induce negative feedback regulation. Further studies on the different contributions of the 3′-5′ exonuclease and helicase domains in the molecular mechanism will provide clues to the accelerated aging processes in WS.

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Section: Roles Of the Wrn Exonuclease In Gene Regulationmentioning

confidence: 99%

Section: Separate Functional Domains Of the Wrn Ortholog In C Elegansmentioning

confidence: 99%

Section: Separate Functional Domains Of the Wrn Ortholog In C Elegansmentioning

confidence: 99%

Section: Separate Functional Domains Of the Wrn Ortholog In C Elegansmentioning

confidence: 99%

Section: Separate Functional Domains Of the Wrn Ortholog In C Elegansmentioning

confidence: 99%

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MUT-7 Provides Molecular Insight into the Werner Syndrome Exonuclease

Hsu

Chen

et al. 2021

Cells

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Mechanisms of epigenetic regulation by C. elegans nuclear RNA interference pathways

Seroussi

Sundby

et al. 2022

Seminars in Cell & Developmental Biology

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Validation of metaxin-2 deficient C. elegans as a model for MandibuloAcral Dysplasia associated to mtx-2 (MADaM) syndrome

Talarmin-Gas,

Smolyakov,

Parisi

et al. 2024

Commun Biol

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MandibuloAcral Dysplasia associated to MTX2 gene (MADaM) is a recently described progeroid syndrome (accelerated aging disease) whose clinical manifestations include skin abnormalities, growth retardation, and cardiovascular diseases. We previously proposed that mtx-2 -deficient C. elegans could be used as a model for MADaM and to support this, we present here our comprehensive phenotypic characterization of these worms using atomic force microscopy (AFM), transcriptomic, and oxygen consumption rate analyses. AFM analysis showed that young mtx-2 -less worms had a significantly rougher, less elastic cuticle which becomes significantly rougher and less elastic as they age, and abnormal mitochondrial morphology. mtx-2 C. elegans displayed slightly delayed development, decreased pharyngeal pumping, significantly reduced mitochondrial respiratory capacities, and transcriptomic analysis identified perturbations in the aging, TOR, and WNT-signaling pathways. The phenotypic characteristics of mtx-2 worms shown here are analogous to many of the human clinical presentations of MADaM and we believe this validates their use as a model which will allow us to uncover the molecular details of the disease and develop new therapeutics and treatments.

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C. elegans orthologs MUT-7/CeWRN-1 of Werner syndrome protein regulate neuronal plasticity

Cited by 7 publications

References 41 publications

MUT-7 Provides Molecular Insight into the Werner Syndrome Exonuclease

MUT-7 Provides Molecular Insight into the Werner Syndrome Exonuclease

Mechanisms of epigenetic regulation by C. elegans nuclear RNA interference pathways

Validation of metaxin-2 deficient C. elegans as a model for MandibuloAcral Dysplasia associated to mtx-2 (MADaM) syndrome

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