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Precise programming of multigene expression stoichiometry in mammalian cells by a modular and programmable transcriptional system.

Chenrui QinYanhui XiangJie LiuRuilin ZhangZiming LiuTingting LiZhi SunXiaoyi OuyangYeqing ZongHaoqian M ZhangQi OuyangLong QianChunbo Lou
Published in: Nature communications (2023)
Context-dependency of mammalian transcriptional elements has hindered the quantitative investigation of multigene expression stoichiometry and its biological functions. Here, we describe a host- and local DNA context-independent transcription system to gradually fine-tune single and multiple gene expression with predictable stoichiometries. The mammalian transcription system is composed of a library of modular and programmable promoters from bacteriophage and its cognate RNA polymerase (RNAP) fused to a capping enzyme. The relative expression of single genes is quantitatively determined by the relative binding affinity of the RNAP to the promoters, while multigene expression stoichiometry is predicted by a simple biochemical model with resource competition. We use these programmable and modular promoters to predictably tune the expression of three components of an influenza A virus-like particle (VLP). Optimized stoichiometry leads to a 2-fold yield of intact VLP complexes. The host-independent orthogonal transcription system provides a platform for dose-dependent control of multiple protein expression which may be applied for advanced vaccine engineering, cell-fate programming and other therapeutic applications.
Keyphrases
  • poor prognosis
  • gene expression
  • transcription factor
  • binding protein
  • dna methylation
  • long non coding rna
  • genome wide
  • cell fate
  • high resolution
  • oxidative stress
  • mass spectrometry
  • circulating tumor