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. 2021 May 24;16(15):2366–2374. doi: 10.1002/cmdc.202100118

Table 1.

In vitro biological activity of 312.

ID

Structure

EC50(FXR)[a] (efficacy)

IC50(LTA4H)[b] (max. inhib.)

3

graphic file with name CMDC-16-2366-g022.jpg

0.026±0.001 μM (34±1 %)

0.54±0.07 μM (97.2±0.4 %)

4

graphic file with name CMDC-16-2366-g004.jpg

15±3 μM (27±1 %)

1.6±0.2 μM (82.6±0.8 %)

5

graphic file with name CMDC-16-2366-g002.jpg

inactive (50 μM)

15±2 μM (80±5 %)

6

graphic file with name CMDC-16-2366-g012.jpg

0.19±0.02 μM (26±1 %)

5.5±0.5 μM (85±2 %)

7

graphic file with name CMDC-16-2366-g016.jpg

0.014±0.001 μM (29±1 %)

0.37±0.02 μM (97.8±0.1 %)

8

graphic file with name CMDC-16-2366-g011.jpg

0.029±0.006 μM (22±1 %)

0.14±0.01 μM (98.8±0.1 %)

9

graphic file with name CMDC-16-2366-g009.jpg

0.15±0.02 μM (56±1 %)

0.61±0.06 μM (96.0±0.2 %)

10

graphic file with name CMDC-16-2366-g021.jpg

0.009±0.001 μM (20±1 %)

1.1±0.1 μM (94.9±0.2 %)

11

graphic file with name CMDC-16-2366-g025.jpg

0.0010±0.0003 μM (35±1 %)

0.55±0.06 μM (98.2±0.1 %)

12

graphic file with name CMDC-16-2366-g017.jpg

0.3±0.1 μM (14±1 %)

5.2±0.6 μM (81.1±0.6 %)

[a] FXR modulation was determined in a full‐length FXR reporter gene assay based on the human FXR response element from the BSEP promoter. Efficacy refers to maximum FXR activation relative to the activity of 3 μM GW4064 which was defined as 100 % activation. The activity of 311 on FXR has been previously reported[25]. Data are the mean±S.E.M., n≥3. [b] LTA4H inhibition was determined on recombinant protein using L‐arginine‐7‐amino‐4‐methylcoumarine as fluorogenic substrate. Maximum inhibition (max. inhib.) refers to LTA4H inhibition at the highest tested concentration. Data are the mean±S.E.M., n=3.