Extensive rewiring of the EGFR network in colorectal cancer cells expressing transforming levels of KRASG13D

SA Kennedy; MA Jarboui; S Srihari; C Raso; K Bryan; L Dernayka; T Charitou; M Bernal-Llinares; C Herrera-Montavez; A Krstic; D Matallanas; M Kotlyar; I Jurisica; J Curak; V Wong; I Stagljar; T LeBihan; L Imrie; P Pillai; MA Lynn; E Fasterius; C Al-Khalili Szigyarto; J Breen; C Kiel; L Serrano; N Rauch; O Rukhlenko; BN Kholodenko; LF Iglesias-Martinez; CJ Ryan; R Pilkington; P Cammareri; O Sansom; S Shave; M Auer; N Horn; F Klose; M Ueffing; K Boldt; DJ Lynn; W Kolch

Journal article

Extensive rewiring of the EGFR network in colorectal cancer cells expressing transforming levels of KRASG13D

SA Kennedy, MA Jarboui, S Srihari, C Raso, K Bryan, L Dernayka, T Charitou, M Bernal-Llinares, C Herrera-Montavez, A Krstic, D Matallanas, M Kotlyar, I Jurisica, J Curak, V Wong, I Stagljar, T LeBihan, L Imrie, P Pillai, MA Lynn Show all

Nature Communications | Published : 2020

DOI: 10.1038/s41467-019-14224-9

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Abstract

Protein-protein-interaction networks (PPINs) organize fundamental biological processes, but how oncogenic mutations impact these interactions and their functions at a network-level scale is poorly understood. Here, we analyze how a common oncogenic KRAS mutation (KRASG13D) affects PPIN structure and function of the Epidermal Growth Factor Receptor (EGFR) network in colorectal cancer (CRC) cells. Mapping >6000 PPIs shows that this network is extensively rewired in cells expressing transforming levels of KRASG13D (mtKRAS). The factors driving PPIN rewiring are multifactorial including changes in protein expression and phosphorylation. Mathematical modelling also suggests that the binding dynam..

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