Linder, T., Liu, R., Atanasov, A., Li, Y., Geyrhofer, S., Schwaiger, S., Stuppner, H., Schnürch, M., Dirsch, V., & Mihovilovic, M. (2019). Leoligin-inspired synthetic lignans with selectivity for cell-type and bioactivity relevant for cardiovascular disease. Chemical Science, 10(22), 5815–5820. https://doi.org/10.1039/c9sc00446g
Recently, a natural compound leoligin, a furan-type lignan, was discovered as an interesting hit compound with an anti-inflammatory pharmacological activity profile. We developed a modular and stereoselective approach for the synthesis of the edelweiss-derived lignan leoligin and used the synthetic route to rapidly prepare leoligin analogs even on the gram scale. Proof of concept of this approach together with cell-based bio-assays gained structural analogs with increased selectivity towards vascular smooth muscle versus endothelial cell proliferation inhibition, a major benefit in fighting vascular neointima formation. In addition, we identified the structural features of leoligin analogs that define their ability to
inhibit the pro-inflammatory NF-kB pathway. Results are discussed in the context of structural modification of these novel synthetic lignans.
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