Abstract
The anti-apoptotic protein survivin is highly expressed in most human cancer cells, but has very low expression in normal differentiated cells. Thus survivin is considered as an attractive cancer drug target. Herein we report the design and synthesis of a series of novel survivin inhibitors based on the oxyquinoline scaffold from our recently identified hit compound UC-112. These new analogs were tested against a panel of cancer cell lines including one with multidrug-resistant phenotype. Eight of these new UC-112 analogs showed IC50 values in the nanomole range in anti-proliferative assays. The best three compounds among them along with UC-112 were submitted for NCI-60 cancer cell line screening. The results indicated that structural modification from UC-112 to our best compound 4g has improved activity by four folds (2.2 μM for UC-112 vs. 0.5 μM for 4g, average GI50 values over all cancer cell lines in the NCI-60 panel).Western blot analyses demonstrated the new compounds maintained high selectivity for survivin inhibition over other members in the inhibition of apoptosis protein family. When tested in an A375 human melanoma xenograft model, the most active compound 4g effectively suppressed tumor growth and strongly induced cancer cell apoptosis in tumor tissues. This novel scaffold is promising for the development of selective survivin inhibitors as potential anticancer agents.
Highlights
Survivin is a unique member of inhibitor of apoptosis protein (IAP) family.[1]
Ethers 3b-3e and ethers 3h-3l were synthesized using step b in which substituted benzyl alcohols were allowed to react with salt 2 in the presence of sodium hydride in anhydrous THF
[22] Compounds 6a-6g with the C ring moiety in UC-112 replaced by different function groups were prepared as Fig 3 shown
Summary
Survivin is a unique member of inhibitor of apoptosis protein (IAP) family.[1] It is overexpressed in most human cancer cells, but is rarely expressed in adult differentiated tissues.[2,3,4,5] This attribute distinguishes survivin from other IAPs which are usually expressed in both cancer and normal cells. Survivin promotes cell proliferation and inhibits apoptosis,[3, 6,7,8,9] facilitates angiogenesis in tumors,[10,11,12] and its expression has been shown to strongly correlate. Novel Small Molecule Survivin Inhibitors for Cancer to Eurofins Panlabs for profiling its drug-like properties. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript
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