4.5 Article

Quantitative prediction of conditional vulnerabilities in regulatory and metabolic networks using PRIME

Journal

NPJ SYSTEMS BIOLOGY AND APPLICATIONS
Volume 7, Issue 1, Pages -

Publisher

NATURE PORTFOLIO
DOI: 10.1038/s41540-021-00205-6

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Funding

  1. Bill and Melinda Gates Foundation [INV-009322]
  2. National Institute of Allergy and Infectious Diseases of the National Institutes of Health [R01AI141953, R01AI128215, U19AI135976]
  3. National Science Foundation [NSF IIBR RoL 2042948]

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The ability of Mycobacterium tuberculosis to adopt heterogeneous physiological states is crucial for its immune system evasion and antibiotic resistance. Developing new TB therapeutics requires a systems-level approach to understand the complexity of network-based adaptations of Mtb.
The ability of Mycobacterium tuberculosis (Mtb) to adopt heterogeneous physiological states underlies its success in evading the immune system and tolerating antibiotic killing. Drug tolerant phenotypes are a major reason why the tuberculosis (TB) mortality rate is so high, with over 1.8 million deaths annually. To develop new TB therapeutics that better treat the infection (faster and more completely), a systems-level approach is needed to reveal the complexity of network-based adaptations of Mtb. Here, we report a new predictive model called PRIME (Phenotype of Regulatory influences Integrated with Metabolism and Environment) to uncover environment-specific vulnerabilities within the regulatory and metabolic networks of Mtb. Through extensive performance evaluations using genome-wide fitness screens, we demonstrate that PRIME makes mechanistically accurate predictions of context-specific vulnerabilities within the integrated regulatory and metabolic networks of Mtb, accurately rank-ordering targets for potentiating treatment with frontline drugs.

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