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Label-free, rapid and quantitative phenotyping of stress response in E. coli via ramanome

  • Lin Teng
  • , Xian Wang
  • , Xiaojun Wang
  • , Honglei Gou
  • , Lihui Ren
  • , Tingting Wang
  • , Yun Wang
  • , Yuetong Ji
  • , Wei E. Huang
  • , Jian Xu
  • Chinese Academy of Sciences
  • University of Chinese Academy of Sciences
  • University of Oxford

Research output: Contribution to journalArticlepeer-review

96 Scopus citations

Abstract

Rapid profiling of stress-response at single-cell resolution yet in a label-free, non-disruptive and mechanism-specific manner can lead to many new applications. We propose a single-cell-level biochemical fingerprinting approach named "ramanome", which is the collection of Single-cell Raman Spectra (SCRS) from a number of cells randomly selected from an isogenic population at a given time and condition, to rapidly and quantitatively detect and characterize stress responses of cellular population. SCRS of Escherichia coli cells are sensitive to both exposure time (eight time points) and dosage (six doses) of ethanol, with detection time as early as 5 min and discrimination rate of either factor over 80%. Moreover, the ramanomes upon six chemical compounds from three categories, including antibiotics of ampicillin and kanamycin, alcohols of ethanol and n-butanol and heavy metals of Cu2+ and Cr6+, were analyzed and 31 marker Raman bands were revealed which distinguish stress-responses via cytotoxicity mechanism and variation of inter-cellular heterogeneity. Furthermore, specificity, reproducibility and mechanistic basis of ramanome were validated by tracking stress-induced dynamics of metabolites and by contrasting between cells with and without genes that convey stress resistance. Thus ramanome enables rapid prediction and mechanism-based screening of cytotoxicity and stress-response programs at single-cell resolution.

Original languageEnglish
Article number34359
JournalScientific Reports
Volume6
DOIs
StatePublished - 19 Oct 2016
Externally publishedYes

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