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1. Mechanism of O2 diffusion and reduction in FeFe hydrogenases

2. Reactivity of the Excited States of the H-Cluster of FeFe Hydrogenases

4. Mechanism of O2 diffusion and reduction in FeFe hydrogenases

5. Reactivity of the Excited States of the H-Cluster of FeFe Hydrogenases

6. Genome-Wide Transcription Start Site Mapping and Promoter Assignments to a Sigma Factor in the Human Enteropathogen Clostridioides difficile .

7. Clostridium difficile Biofilm: Remodeling Metabolism and Cell Surface to Build a Sparse and Heterogeneously Aggregated Architecture.

8. Mechanism of O 2 diffusion and reduction in FeFe hydrogenases.

9. Reactivity of the Excited States of the H-Cluster of FeFe Hydrogenases.

10. A Recombination Directionality Factor Controls the Cell Type-Specific Activation of σK and the Fidelity of Spore Development in Clostridium difficile.

11. Electrochemical Measurements of the Kinetics of Inhibition of Two FeFe Hydrogenases by O2 Demonstrate That the Reaction Is Partly Reversible.

12. The regulatory network controlling spore formation in Clostridium difficile.

13. Genome-wide identification of regulatory RNAs in the human pathogen Clostridium difficile.

14. The spore differentiation pathway in the enteric pathogen Clostridium difficile.

15. Genome-wide analysis of cell type-specific gene transcription during spore formation in Clostridium difficile.

16. The key sigma factor of transition phase, SigH, controls sporulation, metabolism, and virulence factor expression in Clostridium difficile.

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