A Systematic Mammalian Genetic Interaction Map Reveals Pathways Underlying Ricin Susceptibility

نویسندگان

  • Michael C. Bassik
  • Martin Kampmann
  • Robert Jan Lebbink
  • Shuyi Wang
  • Marco Y. Hein
  • Ina Poser
  • Jimena Weibezahn
  • Max A. Horlbeck
  • Siyuan Chen
  • Matthias Mann
  • Anthony A. Hyman
  • Emily M. LeProust
  • Michael T. McManus
  • Jonathan S. Weissman
چکیده

Genetic interaction (GI) maps, comprising pairwise measures of how strongly the function of one gene depends on the presence of a second, have enabled the systematic exploration of gene function in microorganisms. Here, we present a two-stage strategy to construct high-density GI maps in mammalian cells. First, we use ultracomplex pooled shRNA libraries (25 shRNAs/gene) to identify high-confidence hit genes for a given phenotype and effective shRNAs. We then construct double-shRNA libraries from these to systematically measure GIs between hits. A GI map focused on ricin susceptibility broadly recapitulates known pathways and provides many unexpected insights. These include a noncanonical role for COPI, a previously uncharacterized protein complex affecting toxin clearance, a specialized role for the ribosomal protein RPS25, and functionally distinct mammalian TRAPP complexes. The ability to rapidly generate mammalian GI maps provides a potentially transformative tool for defining gene function and designing combination therapies based on synergistic pairs.

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عنوان ژورنال:
  • Cell

دوره 152  شماره 

صفحات  -

تاریخ انتشار 2013