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1. Quantifying redox transcription factor dynamics as a tool to investigate redox signalling.

2. Computational models as catalysts for investigating redoxin systems.

3. Atypical network topologies enhance the reductive capacity of pathogen thiol antioxidant defense networks.

4. Modelling the Decamerisation Cycle of PRDX1 and the Inhibition-like Effect on Its Peroxidase Activity.

5. Can thiol-based redox systems be utilized as parts for synthetic biology applications?

6. Analyzing biological models and data sets using Jupyter notebooks as an alternate to laboratory-based exercises during COVID-19.

7. The thioredoxin redox potential and redox charge are surrogate measures for flux in the thioredoxin system.

8. Hyperoxidation of Peroxiredoxins: Gain or Loss of Function?

9. Quantitative measures for redox signaling.

10. The thioredoxin system and not the Michaelis-Menten equation should be fitted to substrate saturation datasets from the thioredoxin insulin assay.

11. The Development of Computational Biology in South Africa: Successes Achieved and Lessons Learnt.

12. The glutaredoxin mono- and di-thiol mechanisms for deglutathionylation are functionally equivalent: implications for redox systems biology.

13. From top-down to bottom-up: computational modeling approaches for cellular redoxin networks.

14. The logic of kinetic regulation in the thioredoxin system.

15. Enzymes or redox couples? The kinetics of thioredoxin and glutaredoxin reactions in a systems biology context.

16. Cathepsin B stability, but not activity, is affected in cysteine:cystine redox buffers.

17. Endolysosomal proteolysis and its regulation.

18. Use of 2-methylpropan-2-ol to inhibit proteolysis and other protein interactions in a tissue homogenate: an illustrative application to the extraction of cathepsins B and L from liver tissue.

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