CDC20 interacts with conductin and induces its proteosomal degradation

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CDC20 interacts with conductin and induces its proteosomal degradation. CDC20 interacts with conductin and induces its proteosomal degradation. (A) WB of lysates from 293T cells co‐transfected with Flag‐conductin alone or with GFP‐CDC20 and treated with proteosomal inhibitors MG132 and ALLN or control ALLM for 1 h before lysis. (B) WB of lysates from 293T cells co‐transfected with Flag‐conductin and increasing amounts of GFP‐CDC20, a CDC20 mutant lacking the WD40 repeats (GFP‐N‐159), or GFP‐CDH1 as indicated. GFP plasmid was used to keep total DNA amounts equal. (C) WB for HA‐Ub and Flag‐expressed proteins after Flag IP from lysates of 293T cells transfected with indicated plasmids in the presence or absence of proteosomal inhibitor MG132. Ubiquitin chains (HA‐Ub), as well as antibody heavy/light chains (asterisks), are indicated. (D) WB for endogenous conductin and CDC20 after IP with antibodies against conductin, CDC20 or control (IgG) from lysates of mitotic SW480. (E) Western blotting for endogenous conductin, CDC20 and β‐actin in lysates of SW480 and HCT116 colon cancer cells, transfected with siRNAs against CDC20 or GFP, 1 h after release from nocodazole‐induced mitotic arrest. CDC20, cell division cycle 20; GFP, green fluorescent protein; HA‐Ub, HA‐Ubiquitin; IP, immunoprecipitation; WB, western blot. Michel V Hadjihannas et al. EMBO Rep. 2012;13:347-354 © as stated in the article, figure or figure legend