PRMT5-IN-19 (Compound 41) is an selective orally active non-nucleosidePRMT5inhibitor withIC₅₀values of 23.9 nM (radioactive biochemical assay) and 47 nM (AlphaLISA assay). PRMT5-IN-19 can occupy theSAM-binding pocketinPRMT5and block methyltransferase activity, which displays good selectivity over other PRMTs and PKMTs. PRMT5-IN-19 inhibits cell proliferation by inducing cellapoptosis, and can be used for cancer-related research^[1].

PRMT5-IN-19 (Compound 41, 5 days) has strong anti-proliferative effects against the A375 cell with anIC₅₀value of 1.36 μM^[1].
PRMT5-IN-19 shows higher selectivity for PRMT5 (IC₅₀value of 23.9 nM) than other histone methyltransferases (PRMT1 and PRMT4), and PKMTS (EZH2, NSD2, MLL1, and MLL4)^[1].
PRMT5-IN-19 binds with the SAM-binding pocket in PRMT5^[1].
PRMT5-IN-19 (4-5 days) Inhibits proliferation of multiple cancer cell lines (A-375, CHL-1, SNU-423, SNU-449, MDA-MB-231, MDA-MA-453, MV-4-11, MOLM13) with IC₅₀value ranging from 1.08 to 3.45 μM^[1].
PRMT5-IN-19 inhibits arginine symmetrical dimethylation in A375 cells^[1].
PRMT5-IN-19 (0-4 μM, 48 h) suppresses A375 cell proliferation by inducing apoptosis in a concentration-dependent manner^[1].

PRMT5-IN-19 (Compound 41, A375 xenograft model, 75 mg/kg/d, p.o., 19 days) has good PK properties and significant antitumor efficacy, without the obvious loss of body weight and visible toxicity^[1].