Argonautes Promote Male Fertility and Provide a Paternal Memory of Germline Gene Expression in C. elegans

Conine, Colin C.; Moresco, James J.; Gu, Weifeng; Shirayama, Masaki; Conte, Darryl; Yates, John R.; Mello, Craig C.

doi:10.1016/j.cell.2013.11.032

Cited by 167 publications

(293 citation statements)

References 60 publications

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“…RNAi inheritance has been implicated in trans-generational epigenetic inheritance in several species [17]. In C. elegans, exogenous and endogenous RNAi pathways require the argonaute genes rde-1 and ergo-1, respectively [18,19], although additional argonautes do exist and could be required for specific RNA inheritance events [20]. We found that, similar to the progressive fertility defects [6], the trans-generationally extended longevity of spr-5 mutant worms was independent of the main exogenous (Supplementary information, Figure S3A) and endogenous (Supplementary information, Figure S3B) RNAi pathways mediated by these argonautes.…”

Section: Transgenerational Longevity Of Spr-5(by101) Mutant Worms Is mentioning

confidence: 99%

“…In this paper mutant worms were backcrossed: jmjd-2(tm2966): 2 times, daf-12(m20): 3 times, rde-1(ne219): 3 times, set-17(n5017): 2-7 times, set-30(gk315): 2-8 times, damt-1(gk961032): 5 times, ergo-1(tm1860): 7 times, and eap-1(ok3432): 2-13 times. Generation 1 spr-5 mutant worms were obtained by crossing later generation (generation [10][11][12][13][14][15][16][17][18][19][20] homozygous mutant worms with WT males to obtain P0 heterozygous mutants. Individual P0 heterozygous mutants were picked to plates and allowed to lay generation 1 progeny after which the P0 heterozygous mutant genotype was confirmed by single worm PCR genotyping.…”

Section: Worm Strainsmentioning

confidence: 99%

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Mutation of C. elegans demethylase spr-5 extends transgenerational longevity

et al. 2015

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Complex organismal properties such as longevity can be transmitted across generations by non-genetic factors. Here we demonstrate that deletion of the C. elegans histone H3 lysine 4 dimethyl (H3K4me2) demethylase, spr-5, causes a trans-generational increase in lifespan. We identify a chromatin-modifying network, which regulates this lifespan extension. We further show that this trans-generational lifespan extension is dependent on a hormonal signaling pathway involving the steroid dafachronic acid, an activator of the nuclear receptor DAF-12. These findings suggest that loss of the demethylase SPR-5 causes H3K4me2 mis-regulation and activation of a known lifespan-regulating signaling pathway, leading to trans-generational lifespan extension.

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Section: Transgenerational Longevity Of Spr-5(by101) Mutant Worms Is mentioning

confidence: 99%

Section: Worm Strainsmentioning

confidence: 99%

Mutation of C. elegans demethylase spr-5 extends transgenerational longevity

et al. 2015

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“…In order to understand the potential molecular mechanism by which endogenous RNAi is required for pheromone sensation, we sought to identify candidate genes involved in sensory signaling that are expressed in ASI, ASJ, and ADL neurons, and exhibit a daf-d phenotype when mutated. The CSR-1 pathway has been shown to positively regulate the transcription of endogenous genes (Avgousti et al 2012;Conine et al 2013) through interactions with RNA polymerase II (Cecere et al 2014), and maintenance of a euchromatic chromatin state at target gene loci (Claycomb et al 2009;Seth et al 2013;Wedeles et al 2013). Thus, we hypothesize that gene expression of CSR-1 targets required for dauer formation would be downregulated in the mut-16 and csr-1 hypomorph strains, resulting in their observed daf-d phenotype.…”

Section: Csr-1 Promotes Expression Of G Proteins Required For Dauer Fmentioning

confidence: 99%

Endogenous RNAi Pathways Are Required in Neurons for Dauer Formation in Caenorhabditis elegans

Bharadwaj¹,

Hall

2017

Genetics

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Animals can adapt to unfavorable environments through changes in physiology or behavior. In the nematode, Caenorhabditis elegans, environmental conditions perceived early in development determine whether the animal enters either the reproductive cycle, or enters into an alternative diapause stage named dauer. Here, we show that endogenous RNAi pathways play a role in dauer formation in crowding (high pheromone), starvation, and high temperature conditions. Disruption of the Mutator proteins or the nuclear Argonaute CSR-1 result in differential dauer-deficient phenotypes that are dependent upon the experienced environmental stress. We provide evidence that the RNAi pathways function in chemosensory neurons for dauer formation, upstream of the TGF-b and insulin signaling pathways. In addition, we show that Mutator MUT-16 expression in a subset of individual pheromone-sensing neurons is sufficient for dauer formation in high pheromone conditions, but not in starvation or high temperature conditions. Furthermore, we also show that MUT-16 and CSR-1 are required for expression of a subset of G proteins with functions in the detection of pheromone components. Together, our data suggest a model where Mutator-amplified siRNAs that associate with the CSR-1 pathway promote expression of genes required for the detection and signaling of environmental conditions to regulate development and behavior in C. elegans. This study highlights a mechanism whereby RNAi pathways mediate the link between environmental stress and adaptive phenotypic plasticity in animals.

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“…While the aforementioned studies utilized the powerful context of transgenes to illustrate a role for CSR-1 in opposing the piRNA pathway to promote gene expression, Conine, et al 28 provided evidence that the CSR-1 pathway is involved in transmitting a heritable memory of paternal gene expression established in sperm by the ALG-3/4 small RNA pathway. Previous work had demonstrated that ALG-3/4 associate with 26G-RNAs to regulate the expression of transcripts important for male fertility and spermatogenesis.…”

Section: Multiple C Elegans Argonautes Promote the Expression Of Spementioning

confidence: 99%

“…While rare, small RNA pathways have previously been linked to promoting the expression of targeted loci in mammalian cell culture, through mechanisms that remain largely unclear. 25 Together, these observations set the stage for three papers published in late 2013, Seth, et al, 26 Wedeles, et al, 27 and Conine, et al, 28 which demonstrated a role for the AGO, CSR-1, in promoting the expression of germline transcripts.…”

Section: Introductionmentioning

confidence: 99%