Anthrax lethal factor causes proteolytic inactivation of mitogen- activated protein kinase kinase

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ABL-Basic Research Program, Division of Basic Sciences, NCI-FCRDC, Frederick, MD, United States [1 ]
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J. Appl. Microbiol. | / 2卷 / 289-293期
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Diseases - Enzyme activity - Recombinant proteins;
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A search of the National Cancer Institute's Anti-Neoplastic Drug Screen for compounds with an inhibitory profile similar to that of the mitogen- activated protein kinase kinase (MAPKK) inhibitor PD098059 yielded anthrax lethal toxin. Anthrax lethal factor was found to inhibit progesterone-induced meiotic maturation of frog oocytes by preventing the phosphorylation and activation of mitogen-activated protein kinase (MAPK). Similarly, lethal toxin prevented the activation of MAPK in serum stimulated, ras-transformed NIH3T3 cells. In vitro analyses using recombinant proteins indicated that lethal factor proteolytically modified the NH2-terminus of both MAPKK1 and 2, rendering them inactive and hence incapable of activating MAPK. The consequences of this inactivation upon meiosis and transformed cells are also discussed.
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