posted on 2024-11-16, 03:09authored byGeraud Sansom, Nicholas Kirk, Christopher Guise, Robert Anderson, Jeff Smaill, Adam Patterson, Michael Kelso
Amide- and ester-linked kinase inhibitor-cytotoxin conjugates were rationally designed and synthesised as prototype hypoxia-activated anticancer mutual prodrugs. Chemical reduction of an aryl nitro trigger moiety was shown to initiate a spontaneous cyclisation/fragmentation reaction that simultaneously released the kinase inhibitor semaxanib (SU5416) and the amine- or alcohol-linked cytotoxin from the prodrugs. Preliminary cell testing and reduction potential measurements support optimisation of the compounds towards tumour-selective mutual prodrugs.
Funding
Repurposing Amiloride into Breast Cancer Drugs with a Dual-Targeting Mechanism
Sansom, G. N., Kirk, N. S., Guise, C. P., Anderson, R. F., Smaill, J. B., Patterson, A. V. & Kelso, M. J. (2019). Prototyping kinase inhibitor-cytotoxin anticancer mutual prodrugs activated by tumour hypoxia: A chemical proof of concept study. Bioorganic and Medicinal Chemistry Letters, 29 (10), 1215-1219.