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    Date Issued2021 (1)2020 (2)AuthorGiese, Gabrielle E. (3)Li, Xuhang (3)Ponomarova, Olga (3)Walhout, Albertha J. M. (3)Walker, Melissa D. (3)View MoreUMass Chan AffiliationGraduate School of Biomedical Sciences (3)Program in Molecular Medicine (3)Program in Systems Biology (3)Document TypeJournal Article (2)Preprint (1)KeywordCellular and Molecular Physiology (3)metabolism (3)Biochemical Phenomena, Metabolism, and Nutrition (2)C. elegans (2)Computational Biology (2)View MoreJournalbioRxiv (1)eLife (1)Genetics (1)

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    WormPaths: Caenorhabditis elegans metabolic pathway annotation and visualization

    Walker, Melissa D.; Giese, Gabrielle E.; Holdorf, Amy D.; Bhattacharya, Sushila; Diot, Cedric; Garcia-Gonzalez, Aurian; Horowitz, Brent; Lee, Yong-Uk; Leland, Thomas; Li, Xuhang; et al. (2021-06-12)
    In our group, we aim to understand metabolism in the nematode Caenorhabditis elegans and its relationships with gene expression, physiology and the response to therapeutic drugs. Visualization of the metabolic pathways that comprise the metabolic network is extremely useful for interpreting a wide variety of experiments. Detailed annotated metabolic pathway maps for C. elegans is mostly limited to pan-organismal maps, many with incomplete or inaccurate pathway and enzyme annotations. Here we present WormPaths, which is composed of two parts: 1) the careful manual annotation of metabolic genes into pathways, categories and levels, and 2) 62 pathway maps that include metabolites, metabolite structures, genes, reactions, and pathway connections between maps. These maps are available on the WormFlux website. We show that WormPaths provides easy-to-navigate maps and that the different levels in WormPaths can be used for metabolic pathway enrichment analysis of transcriptomic data. In the future we envision further developing these maps to be more interactive, with an analogy of road maps that are available on mobile devices.
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    WormPaths: Caenorhabditis elegans metabolic pathway annotation and visualization [preprint]

    Walker, Melissa D.; Giese, Gabrielle E.; Holdorf, Amy D.; Bhattacharya, Sushila; Diot, Cedric; Garcia-Gonzalez, Aurian; Horowitz, Brent; Lee, Yong-Uk; Leland, Thomas; Li, Xuhang; et al. (2020-12-23)
    In our group, we aim to understand metabolism in the nematode Caenorhabditis elegans and its relationships with gene expression, physiology and the response to therapeutic drugs. On March 15, 2020, a stay-at-home order was put into effect in the state of Massachusetts, USA, to flatten the curve of the spread of the novel SARS-CoV2 virus that causes COVID-19. For biomedical researchers in our state, this meant putting a hold on experiments for nine weeks until May 18, 2020. To keep the lab engaged and productive, and to enhance communication and collaboration, we embarked on an in-lab project that we all found important but that we never had the time for: the detailed annotation and drawing of C. elegans metabolic pathways. As a result, we present WormPaths, which is composed of two parts: 1) the careful manual annotation of metabolic genes into pathways, categories and levels, and 2) 66 pathway maps that include metabolites, metabolite structures, genes, reactions, and pathway connections between maps. These maps are available on our WormFlux website. We show that WormPaths provides easy-to-navigate maps and that the different levels in WormPaths can be used for metabolic pathway enrichment analysis of transcriptomic data. In the unfortunate event of additional lockdowns, we envision further developing these maps to be more interactive, with an analogy of road maps that are available on mobile devices.
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    Caenorhabditis elegans methionine/S-adenosylmethionine cycle activity is sensed and adjusted by a nuclear hormone receptor

    Giese, Gabrielle E.; Walker, Melissa D.; Ponomarova, Olga; Zhang, Hefei; Li, Xuhang; Minevich, Gregory; Walhout, Albertha J. M. (2020-10-05)
    Vitamin B12 is an essential micronutrient that functions in two metabolic pathways: the canonical propionate breakdown pathway and the methionine/S-adenosylmethionine (Met/SAM) cycle. In Caenorhabditis elegans, low vitamin B12, or genetic perturbation of the canonical propionate breakdown pathway results in propionate accumulation and the transcriptional activation of a propionate shunt pathway. This propionate-dependent mechanism requires nhr-10 and is referred to as 'B12-mechanism-I'. Here, we report that vitamin B12 represses the expression of Met/SAM cycle genes by a propionate-independent mechanism we refer to as 'B12-mechanism-II'. This mechanism is activated by perturbations in the Met/SAM cycle, genetically or due to low dietary vitamin B12. B12-mechanism-II requires nhr-114 to activate Met/SAM cycle gene expression, the vitamin B12 transporter, pmp-5, and adjust influx and efflux of the cycle by activating msra-1 and repressing cbs-1, respectively. Taken together, Met/SAM cycle activity is sensed and transcriptionally adjusted to be in a tight metabolic regime.
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