A. Seitova scite author profile

A. Seitova

2Publications

66Citation Statements Received

77Citation Statements Given

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Oklahoma Medical Research Foundation, University of Oklahoma

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Thrombomodulin Tightens the Thrombin Active Site Loops To Promote Protein C Activation

et al. 2005

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Thrombomodulin (TM) forms a 1:1 complex with thrombin. Whereas thrombin alone cleaves fibrinogen to make the fibrin clot, the thrombin-TM complex cleaves protein C to initiate the anticoagulant pathway. Crystallographic investigations of the complex between thrombin and TMEGF456 did not show any changes in the thrombin active site. Therefore, research has focused recently on how TM may provide a docking site for the protein C substrate. Previous work, however, showed that when the thrombin active site was occupied with substrate analogues labeled with fluorophores, the fluorophores responded differently to active (TMEGF1-6) versus inactive (TMEGF56) fragments of TM. To investigate this further, we have carried out amide H/(2)H exchange experiments on thrombin in the presence of active (TMEGF45) and inactive (TMEGF56) fragments of TM. Both on-exchange and off-exchange experiments show changes in the thrombin active site loops, some of which are observed only when the active TM fragment is bound. These results are consistent with the previously observed fluorescence changes and point to a mechanism by which TM changes the thrombin substrate specificity in favor of protein C cleavage.

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287 The discovery and optimization of small molecule antagonists of the WDR5–MLL interaction

Al-Awar¹,

Getlik²,

Smil³

et al. 2014

European Journal of Cancer

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A. Seitova

Thrombomodulin Tightens the Thrombin Active Site Loops To Promote Protein C Activation

287 The discovery and optimization of small molecule antagonists of the WDR5–MLL interaction

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