A mix-and-read drop-based in vitro two-hybrid method for screening high-affinity peptide binders

نویسندگان

  • Naiwen Cui
  • Huidan Zhang
  • Nils Schneider
  • Ye Tao
  • Haruichi Asahara
  • Zhiyi Sun
  • Yamei Cai
  • Stephan A. Koehler
  • Tom F. A. de Greef
  • Alireza Abbaspourrad
  • David A. Weitz
  • Shaorong Chong
چکیده

Drop-based microfluidics have recently become a novel tool by providing a stable linkage between phenotype and genotype for high throughput screening. However, use of drop-based microfluidics for screening high-affinity peptide binders has not been demonstrated due to the lack of a sensitive functional assay that can detect single DNA molecules in drops. To address this sensitivity issue, we introduced in vitro two-hybrid system (IVT2H) into microfluidic drops and developed a streamlined mix-and-read drop-IVT2H method to screen a random DNA library. Drop-IVT2H was based on the correlation between the binding affinity of two interacting protein domains and transcriptional activation of a fluorescent reporter. A DNA library encoding potential peptide binders was encapsulated with IVT2H such that single DNA molecules were distributed in individual drops. We validated drop-IVT2H by screening a three-random-residue library derived from a high-affinity MDM2 inhibitor PMI. The current drop-IVT2H platform is ideally suited for affinity screening of small-to-medium-sized libraries (10(3)-10(6)). It can obtain hits within a single day while consuming minimal amounts of reagents. Drop-IVT2H simplifies and accelerates the drop-based microfluidics workflow for screening random DNA libraries, and represents a novel alternative method for protein engineering and in vitro directed protein evolution.

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عنوان ژورنال:

دوره 6  شماره 

صفحات  -

تاریخ انتشار 2016