AI Article Synopsis

  • Synthetic and native genes in cells compete for expression machinery, affecting how cellular processes work together due to shared resources.
  • A coarse-grained E. coli cell model is proposed to balance the complexity of metabolic regulation with the need for simplicity in biocircuit design, helping to understand the connection between resource availability and bacterial growth rates.
  • The model allows for effective prototyping of biocircuits and provides analytical insights that help in designing robust systems for managing ribosome availability in cells.

Article Abstract

Within a cell, synthetic and native genes compete for expression machinery, influencing cellular process dynamics through resource couplings. Models that simplify competitive resource binding kinetics can guide the design of strategies for countering these couplings. However, in bacteria resource availability and cell growth rate are interlinked, which complicates resource-aware biocircuit design. Capturing this interdependence requires coarse-grained bacterial cell models that balance accurate representation of metabolic regulation against simplicity and interpretability. We propose a coarse-grained E. coli cell model that combines the ease of simplified resource coupling analysis with appreciation of bacterial growth regulation mechanisms and the processes relevant for biocircuit design. Reliably capturing known growth phenomena, it provides a unifying explanation to disparate empirical relations between growth and synthetic gene expression. Considering a biomolecular controller that makes cell-wide ribosome availability robust to perturbations, we showcase our model's usefulness in numerically prototyping biocircuits and deriving analytical relations for design guidance.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10912777PMC
http://dx.doi.org/10.1038/s41467-024-46410-9DOI Listing

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