Nucleotide reverse transcriptase inhibitors, such as tenofovir and emtricitabine, are key components of HIV treatment and HIV Pre-exposure Prophylaxis. These drugs are prodrugs and require phosphorylation by kinases within host cells in order to become activated. This talk will discuss the impact of genetic variation in kinases including adenylate and creatine kinases on the activation of clinically important nucleotide reverse transcriptase inhibitors.

Many anticancer agents in current clinical use lack the desired tumor selectivity and are associated with systemic side effects. Prodrug design is one approach that could potentially improve the target-selectivity of anticancer agents. This talk will discuss the design of anticancer prodrugs for site-specific activation in tumor tissues through bioreduction and proteolysis

Anti-COVID-19 prodrugs (e.g., remdesivir) are activated by specific drug-metabolizing enzymes. This talk, co-presented by Drs Hao-Jie Zhu and Joy Feng, will discuss the proteomics of the activating enzymes in various organs related to the pharmacokinetics and pharmacodynamics of anti-COVID-19 prodrugs and the strategy of using the information to improve the design of anti-COVID-19 prodrugs.

Anti-COVID-19 prodrugs (e.g., remdesivir) are activated by specific drug-metabolizing enzymes. This talk, co-presented by Drs Hao-Jie Zhu and Joy Feng, will discuss the proteomics of the activating enzymes in various organs related to the pharmacokinetics and pharmacodynamics of anti-COVID-19 prodrugs and the strategy of using the information to improve the design of anti-COVID-19 prodrugs.