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Environment-specific virocell metabolic reprogramming.
Howard-Varona, Cristina; Lindback, Morgan M; Fudyma, Jane D; Krongauz, Azriel; Solonenko, Natalie E; Zayed, Ahmed A; Andreopoulos, William B; Olson, Heather M; Kim, Young-Mo; Kyle, Jennifer E; Glavina Del Rio, Tijana; Adkins, Joshua N; Tfaily, Malak M; Paul, Subhadeep; Sullivan, Matthew B; Duhaime, Melissa B.
Afiliação
  • Howard-Varona C; Department of Microbiology, The Ohio State University, 484 W 12th Ave, Columbus, OH 43210, United States.
  • Lindback MM; Department of Ecology and Evolutionary Biology, University of Michigan, 1105 North University Ave, Ann Arbor, MI 48109, United States.
  • Fudyma JD; Department of Environmental Science, University of Arizona, 1177 E 4th St, Tucson, AZ 85719, United States.
  • Krongauz A; Present address: Department of Plant Pathology, University of California, Davis, One Shields Avenue, Davis, CA 95616, United States.
  • Solonenko NE; Department of Statistics, The Ohio State University, 1958 Neil Ave, Columbus, OH 43210, United States.
  • Zayed AA; Department of Microbiology, The Ohio State University, 484 W 12th Ave, Columbus, OH 43210, United States.
  • Andreopoulos WB; Department of Microbiology, The Ohio State University, 484 W 12th Ave, Columbus, OH 43210, United States.
  • Olson HM; US Department of Energy Joint Genome Institute, 1 Cyclotron Road, Berkeley, CA 94720, United States.
  • Kim YM; Present address: Department of Computer Science, San Jose State University, One Washington Square, San Jose CA 95192, United States.
  • Kyle JE; Biological Sciences Division, Pacific Northwest National Laboratory, 902 Battelle Blvd, Richland, WA 99354, United States.
  • Glavina Del Rio T; Biological Sciences Division, Pacific Northwest National Laboratory, 902 Battelle Blvd, Richland, WA 99354, United States.
  • Adkins JN; Biological Sciences Division, Pacific Northwest National Laboratory, 902 Battelle Blvd, Richland, WA 99354, United States.
  • Tfaily MM; US Department of Energy Joint Genome Institute, 1 Cyclotron Road, Berkeley, CA 94720, United States.
  • Paul S; Biological Sciences Division, Pacific Northwest National Laboratory, 902 Battelle Blvd, Richland, WA 99354, United States.
  • Sullivan MB; Department of Biomedical Engineering, Oregon Health and Science University, Portland, OR 97239, United States.
  • Duhaime MB; Department of Environmental Science, University of Arizona, 1177 E 4th St, Tucson, AZ 85719, United States.
ISME J ; 18(1)2024 Jan 08.
Article em En | MEDLINE | ID: mdl-38552150
ABSTRACT
Viruses impact microbial systems through killing hosts, horizontal gene transfer, and altering cellular metabolism, consequently impacting nutrient cycles. A virus-infected cell, a "virocell," is distinct from its uninfected sister cell as the virus commandeers cellular machinery to produce viruses rather than replicate cells. Problematically, virocell responses to the nutrient-limited conditions that abound in nature are poorly understood. Here we used a systems biology approach to investigate virocell metabolic reprogramming under nutrient limitation. Using transcriptomics, proteomics, lipidomics, and endo- and exo-metabolomics, we assessed how low phosphate (low-P) conditions impacted virocells of a marine Pseudoalteromonas host when independently infected by two unrelated phages (HP1 and HS2). With the combined stresses of infection and nutrient limitation, a set of nested responses were observed. First, low-P imposed common cellular responses on all cells (virocells and uninfected cells), including activating the canonical P-stress response, and decreasing transcription, translation, and extracellular organic matter consumption. Second, low-P imposed infection-specific responses (for both virocells), including enhancing nitrogen assimilation and fatty acid degradation, and decreasing extracellular lipid relative abundance. Third, low-P suggested virocell-specific strategies. Specifically, HS2-virocells regulated gene expression by increasing transcription and ribosomal protein production, whereas HP1-virocells accumulated host proteins, decreased extracellular peptide relative abundance, and invested in broader energy and resource acquisition. These results suggest that although environmental conditions shape metabolism in common ways regardless of infection, virocell-specific strategies exist to support viral replication during nutrient limitation, and a framework now exists for identifying metabolic strategies of nutrient-limited virocells in nature.
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Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Assunto principal: Bacteriófagos Idioma: En Revista: ISME J Ano de publicação: 2024 Tipo de documento: Article
Texto completo
Imprimir
XML
PubMed Links
Buscar no Google

Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Assunto principal: Bacteriófagos Idioma: En Revista: ISME J Ano de publicação: 2024 Tipo de documento: Article