LEGO‐Inspired Drug Design: Unveiling a Class of Benzo[d]thiazoles Containing a 3,4‐Dihydroxyphenyl Moiety as Plasma Membrane H⁺‐ATPase Inhibitors

Abstract: The fungal plasma membrane H+‐ATPase (Pma1p) is a potential target for the discovery of new antifungal agents. Surprisingly, no structure–activity relationship studies for small molecules targeting Pma1p have been reported. Herein, we disclose a LEGO‐inspired fragment assembly strategy for the design, synthesis, and discovery of benzo[d]thiazoles containing a 3,4‐dihydroxyphenyl moiety as potential Pma1p inhibitors. A series of 2‐(benzo[d]thiazol‐2‐ylthio)‐1‐(3,4‐dihydroxyphenyl)ethanones was found to inhibit … Show more

“…For over 25 years, only 17 notable studies of chemical agents targeting Pma1 for antifungal purposes were reported. Thioether: possible oxidation in the cell [34]…”

“…In 2018, our group has reported an alternative drug design method based on the LEGO concept called: HFSA-SDOS (from hypothesis-based fragment selection and assembly (HFSA), specific biological relevant scaffold-based diversity-oriented synthesis (SDOS) to rational design) (Figure 17). [34] In this research, the combination of privileged-scaffolds selection and diversity-oriented synthesis has led to the identification of the series of benzo[d]thiazoles containing a 3,4dihydroxyphenyl moiety as potent Pma1 inhibitors. 16 compounds (68-83) were synthesized with IC 50 values ranging from 8 μM to 36 μM (Table 5).…”

“…In 2018, our group has reported an alternative drug design method based on the LEGO concept called: HFSA‐SDOS (from hypothesis‐based fragment selection and assembly (HFSA), specific biological relevant scaffold‐based diversity‐oriented synthesis (SDOS) to rational design) (Figure 17). [34] …”

“…IC 50 values for compounds 68-83 determined from Pma1 ATPase activity measurements. Reproduced from ref [34]. with permission.…”

Drug Discovery and Development on Pma1, Where Are We Now? A Critical Review from 1995 to 2022

“…For over 25 years, only 17 notable studies of chemical agents targeting Pma1 for antifungal purposes were reported. Thioether: possible oxidation in the cell [34]…”

“…In 2018, our group has reported an alternative drug design method based on the LEGO concept called: HFSA-SDOS (from hypothesis-based fragment selection and assembly (HFSA), specific biological relevant scaffold-based diversity-oriented synthesis (SDOS) to rational design) (Figure 17). [34] In this research, the combination of privileged-scaffolds selection and diversity-oriented synthesis has led to the identification of the series of benzo[d]thiazoles containing a 3,4dihydroxyphenyl moiety as potent Pma1 inhibitors. 16 compounds (68-83) were synthesized with IC 50 values ranging from 8 μM to 36 μM (Table 5).…”

“…In 2018, our group has reported an alternative drug design method based on the LEGO concept called: HFSA‐SDOS (from hypothesis‐based fragment selection and assembly (HFSA), specific biological relevant scaffold‐based diversity‐oriented synthesis (SDOS) to rational design) (Figure 17). [34] …”

“…IC 50 values for compounds 68-83 determined from Pma1 ATPase activity measurements. Reproduced from ref [34]. with permission.…”

Drug Discovery and Development on Pma1, Where Are We Now? A Critical Review from 1995 to 2022

“…Azolium heterocycles are not only present in natural products, but also in countless substances of technical and medicinal importance. [16][17][18][19][20][21][22] The 2-thionated derivatives show valuable biological, e.g. anti-thyroid, properties.…”

2-Mercaptoimidazolium halides: structural diversity, stability and spontaneous racemisation

One pot synthesis of 2‐substituted thiobenzoazoles containing α‐sulfenylated aromatic ketones under transition metal‐free conditions