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. Author manuscript; available in PMC: 2021 Mar 12.
Published in final edited form as: J Med Chem. 2019 Sep 26;63(5):2139–2180. doi: 10.1021/acs.jmedchem.9b00826

Table 1.

Structure-activity relationships for N-(4-methoxybenzyl)-substituted aminopyrazoles, exploring variation of the resorcylate amide with methyl- and phenyl-substitution at R2. Fold-selectivity > 5 for any compound is highlighted in red.

graphic file with name nihms-1055611-t0010.jpg
Entry Compound X R2 C. neoformans
EC50a (μM)
C. neoformans
fold-
selectivityb
C. albicans
EC50c (μM)
C. albicans
fold-
selectivityb
1 20 graphic file with name nihms-1055611-t0011.jpg CH3 0.040 0.8 0.011 0.9
2 21 Ph 0.877 2.5 0.511 2.2


3 22 graphic file with name nihms-1055611-t0012.jpg CH3 0.087 1.2 0.184 0.4
4 23 Ph 0.142 4.0 0.068 6.2


5 24 graphic file with name nihms-1055611-t0013.jpg CH3 0.063 1.7 0.157 0.5
6 25 Ph 0.121 2.7 0.063 3.9


7 26 graphic file with name nihms-1055611-t0014.jpg CH3 0.109 0.6 0.117 0.4
8 27 Ph 0.787 2.2 1.089 1.2


9 28 graphic file with name nihms-1055611-t0015.jpg CH3 0.592 0.1 0.054 0.5
10 29 Ph 0.705 2.7 1.043 1.3


11 30 graphic file with name nihms-1055611-t0016.jpg CH3 1.330 5.8 > 9 -
12 31 Ph > 9 - > 9 -


13 32 graphic file with name nihms-1055611-t0017.jpg CH3 0.096 1.0 0.171 0.4
14 33 Ph 0.146 0.8 0.023 1.8


15 34 graphic file with name nihms-1055611-t0018.jpg CH3 0.086 1.2 0.115 0.7
16 35 Ph 0.091 0.8 0.014 1.7


17 36 graphic file with name nihms-1055611-t0019.jpg CH3 0.115 0.9 0.143 0.6


18 37 graphic file with name nihms-1055611-t0020.jpg CH3 4.814 1.6 > 6 0.0


19 38 graphic file with name nihms-1055611-t0021.jpg Ph 0.464 2.1 0.282 1.2


20 39 graphic file with name nihms-1055611-t0022.jpg Ph >10 - >10 -

EC50 values were determined by FP-based equilibrium competition assay performed in 384-well format using whole cell lysates prepared from C. neoformans (a) and C. albicans (c) and serial compound dilutions. All determinations were performed in duplicate. To calculate fold-selectivity (b), the EC50 value determined in human HepG2 cell lysate was divided by the EC50 value determined in fungal cell lysate. The resulting ratio was then normalized to values determined in the same assay for the non-selective inhibitor geldanamycin using lysate of each cell type. Results for key selective compounds were confirmed by repeat assay (see Supplemental Table 1).