Bidirectional effect of Wnt signaling antagonist DKK1 on the modulation of anthrax toxin uptake

被引:0
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作者
LiLi Qian
ChangZu Cai
PengFei Yuan
Sun-Young Jeong
XiaoZhou Yang
Venita DeAlmeida
James Ernst
Michael Costa
Stanley N. Cohen
WenSheng Wei
机构
[1] Peking University,College of Life Sciences and State Key Laboratory of Protein and Plant Gene Research
[2] Stanford University School of Medicine,Department of Genetics
[3] Stanford University School of Medicine,Department of Medicine
[4] Genentech,Department of Cancer Targets
[5] Inc.,Department of Protein Chemistry and Protein Engineering
[6] Genentech,undefined
[7] Inc.,undefined
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关键词
DKK1; anthrax toxin; LRP6; TALENs; internalization; Kremen2; receptor; Wnt;
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摘要
LRP6, a co-receptor for the morphogen Wnt, aids endocytosis of anthrax complexes. Here we report that Dickkopf1 (DKK1) protein, a secreted LRP6 ligand and antagonist, is also a modulator of anthrax toxin sensitivity. shRNA-mediated gene silencing or TALEN-mediated gene knockout of DKK1 reduced sensitivity of cells to PA-dependent hybrid toxins. However, unlike the solely inhibitory effect on Wnt signaling, the effects of DKK1 overexpression on anthrax toxicity were bidirectional, depending on its endogenous expression and cell context. Fluorescence microscopy and biochemical analyses showed that DKK1 facilitates internalization of anthrax toxins and their receptors, an event mediated by DKK1-LRP6-Kremen2 complex. Monoclonal antibodies against DKK1 provided dose-dependent protection to macrophages from killing by anthrax lethal toxin (LT). Our discovery that DKK1 forms ternary structure with LRP6 and Kremen2 in promoting PA-mediated toxin internalization provides a paradigm for bacterial exploitation of mechanisms that host cells use to internalize signaling proteins.
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页码:469 / 481
页数:12
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