A safer treatment for toxoplasmosis would be achieved by improving the selectivity and potency of dihydrofolate reductase (DHFR) inhibitors, such as pyrimethamine (1), for Toxoplasma gondii DHFR ( TgDHFR) relative to human DHFR ( hDHFR). We previously reported on the identification of meta-biphenyl analog 2, designed by in silico modeling of key differences in the binding pocket between TgDHFR and hDHFR. Compound 2 improves TgDHFR selectivity 6.6-fold and potency 16-fold relative to 1. Here, we report on the optimization and structure-activity relationships of this arylpiperazine series leading to the discovery of 5-(4-(3-(2-methoxypyrimidin-5-yl)phenyl)piperazin-1-yl)pyrimidine-2,4-diamine 3. Compound 3 has a TgDHFR I

Barks, Jennifer

Brockman, Adam

Gould, Julie

Hopper, Allen T

Radke, Joshua B

Sibley, L. David

Thomas, Stephen

Wise, Andy

Zou, Yongmao

English

Digital Commons@Becker

S1Supporting InformationDiscovery of Selective Toxoplasma gondii Dihydrofolate Reductase Inhibitors for the Treatment of ToxoplasmosisAllen T. Hopper*,a,  Adam Brockmana, Andy Wiseb, Julie Gouldb, Jennifer Barksc, Joshua B. Radkec, L. David Sibleyc, Yongmao Zoud, and Stephen ThomasaPurification of T. gondii DHFR-thymidylate synthase:The T. gondii DHFR-thymidylate synthase (4KYA) construct with the loop truncated (residues deleted: 49-73 and 201-219) and crossover helix deletion (residues 291-296) was produced from expression in E.Coli  and crystallized as described previously1 with some modification to the purification and crystallization conditions. Briefly, the cells were lysed by sonicating in 25 mM Tris-HCl, pH 7.3 and 100 mM NaCl and purified over a methotrexate agarose affinity column.  The affinity purified protein was further purified by size exclusion chromatography (SEC) over a Superdex 200 column in SEC buffer (pH 7.3 consisting of 25 mM Tris-HCl, 10 mM DTT and 10% glycerol). The SEC pooled TgDHFR-thymidylate synthase protein (>95% purity) was concentrated to 13.2 mg/mL.Crystallization:Compound 29: Compound 29 and NADPH, along with the thymidylate synthase inhibitor N10-propargyl-5,8-dideazafolate (PDDF, provided by the WuXi chemical synthesis group) and dUMP were combined with protein and then mixed with 0.1 M potassium formate buffer with 16% PEG3350.  Needle crystals grew at 293K using the sitting drop vapor diffusion method. Data collection was carried out at the Shanghai synchrotron radiation facility (SSRF). The three-dimensional crystal structure was solved to 3.0Å.  A homodimer was in the asymmetric unit and both monomers with ligand adopt similar conformations.Compound 3 was crystallized in a similar manner except using 0.2M diammonium citrate pH 4.6 and 15% PEG3350.  Although this structure was solved at 3.5 Å, the electron density for the compound was observed in the binding pocket.  S2Table S1.    Diffraction and refinement statistics for 29 and 3Compound Name 29 3Data collection   Resolution (Å) 50.0-3.0 50.0-3.5Space group P212121 P212121a 53.689     53.209     b 145.522  144.343 c 175.922 174.189 No. of total reflections 117,211 54799No. of unique reflections 25,031 11564Completeness (%) 87.8 (90.7) 62.7 (66.2) 9.4 (2.8) 12.0 (5.0)Redundancy 4.9 (4.8) 4.7 (4.4)Rmerge (%) 14.7 (45.2) 13.8 (52.3)Refinement   Rwork/Rfree (%) 21.36/26.40 19.82/26.37RMSbond/angel 0.005/1.085 0.007/1.096  Kinetic solubility Kinetic solubility was determined by the shake flask method from 10 mM stock solutions of test compounds in DMSO, which were diluted to final test concentrations of 200 μM in 50 mM phosphate buffer, pH 7 and shaken for 24 h.  The samples were filtered, and concentrations determined by UV detection, calibrated by a 3-point standard curve (1, 20, 200 µM).Log P Measured Log P was performed at pH 11.0 in octanol/buffer.  Buffer: Acetic acid (1.20 g), boric acid (1.24 g), phosphoric acid (1.96 g) dissolved in 250 mL of purified water. The pH of the final solution was adjusted to 11 with 4M sodium hydroxide solution.  Compounds were added as 10 S3mM stock solutions in DMSO to give a final compound concentration of 67 μM in 1.0% DMSO.  Log P was determined by MRM, calculated based on internal standard. The buffer-layer sample was diluted by a factor of 20-fold and octanol-layer sample by a factor of 200-fold.Clearance in human and mouse liver microsomesHuman and mouse liver microsome intrinsic clearance (Clint) was determined by assessing the disappearance of test compounds at six-time points over a 60 min incubation.  In 96 well plate format, 10 μL of 10 μM test compounds or controls in 100 mM potassium phosphate buffer containing 9.9% MeOH was added to all plates except the matrix blank.  Then 80 μL/well human or mouse microsomes, at a final concentration of 0.5 mg protein/mL, was added and the mixture of microsome solutions and compounds were incubated at 37℃ for about 10 min.  After pre-warming, 10 μL/well NADPH regenerating system was added, and the timer started.  At each time point (T0, T5, T10, T20, T30, T60), 300 μL/well stop solution (Stop solution: Cold ACN containing 100 ng/mL Tolbutamide and 100 ng/mL Labetalol as internal standard (IS) at 4℃) was added to terminate the reaction.  The sampling plates were shaken for 10 min.   Samples were centrifuged at 4000 rpm for 20 min at 4℃.  Then 100 μL of the supernatant from each well was transferred to a new 96-well plate containing 300 μL HPLC water per well and the samples analyzed by LC/MS/MS.Data was analyzed based on first order kinetics to calculate t1/2 and Clint(mic): Human and mouse CLint was determined using the in vitro T1/2 method.  To calculate T1/2, test compound/internal standard peak height ratios were converted to percentage compound remaining in the incubation volume by normalizing the ratios to initial concentration (C0 at t=0).  Then, using a linear regression plot of log (Ln) percentage compound remaining versus incubation time (Ln C = Ln S4C0 – Kt), the slope corresponding to elimination rate (-K) was computed. Since T½=0.693/K, the CLint was then determined by: CLint = 0.693  X  Incubation Volume (mL)                 T1/2             Microsomal Protein (mg)MDCK-MDR-1 permeabilityMDCK-MDR1 cells (obtained from the Netherlands Cancer Institute, Amsterdam, The Netherlands) were seeded onto polyethylene membranes (PET) in 96-well BD insert systems at 2.5 x 105 cells/ mL and maintained for 4-7 days until confluent cell monolayer formation2-3.    Test compounds were diluted with the transport buffer (HBSS with 10 mM Hepes, pH 7.4) from 10 mM DMSO stock solution to a concentration of 2 µM (DMSO: 0.4 %) and applied to the apical or basolateral side of the cell monolayer.  Permeation of the test compounds from A to B or B to A direction was determined in duplicate over a 150-minute incubation at 37°C and 5% CO2 with a relative humidity of 95%. Test and reference compounds were quantified by LC/MS/MS analysis based on the peak area ratio of analyte/IS.  The B:A to A:B apparent permeability coefficient ratio was used to determine the extent of efflux or Pgp substrate specificity.  After the transport assay, a lucifer yellow rejection assay was applied to determine the cell monolayer integrity, where in the data was rejected if the transport of lucifer yellow was greater than 2%. The apparent permeability coefficient Papp (cm/s) was calculated using the equation:          Papp = (dCr/dt) x Vr / (A x C0) Where dCr/dt is the cumulative concentration of compound in the receiver chamber as a function of time (µM/s); Vr is the solution volume in the receiver chamber (0.075 mL on the apical side, S50.25 mL on the basolateral side); A is the surface area for the transport, i.e. 0.0804 cm2 for the area of the monolayer; C0 is the initial concentration in the donor chamber (µM). The efflux ratio was calculated using the equation:          Efflux Ratio = Papp (BA) / Papp (AB)Percent recovery was calculated using the equation:        % Recovery = 100 x [(Vr x Cr) + (Vd x Cd)] / (Vd x C0)Where Vd is the volume in the donor chambers (0.075 mL on the apical side, 0.25 mL on the basolateral side); Cd and Cr are the final concentrations of transport compound in donor and receiver chambers, respectively. Percent of lucifer yellow in basolateral well is calculated using the equation:where RFUApical and RFUBasolateral are the relative fluorescence unit values of lucifer yellow in the apical and basolateral wells, respectively; VApical and VBasolateral are the volume of apical and basolateral wells (0.075 mL and 0.25 mL), respectively.  100×RFUVRFUVRFUVYellowLucifer%lBasolateralBasolateraApicalApicallBasolateralBasolateraS6CEREP 44 Screening Results:S7Molecular Formula StringsCompound SMILE1 Clc1ccc(cc1)c2c(CC)nc(N)nc2N2 Nc1nc(N)c(cn1)N2CCN(CC2)c3cc(ccc3)c4ccccc43 COc1ncc(cn1)c2cc(ccc2)N3CCN(CC3)c4c(N)nc(N)nc44 COc1c(OC)c(OC)cc(Cc2c(N)nc(N)nc2)c15 OC(=O)CC[C@@H](C(O)=O)NC(=O)c1ccc(cc1)N(C)Cc2nc3c(nc2)nc(N)nc3N6 COc1c(OC)cc(NCc2c(C)c3c(nc(N)nc3N)cc2)cc1OC7 Nc1nc(N)c(cn1)N2CCN(CC2)c3ccccc38 Nc1nc(N)c(cn1)N2CCN(CC2)c3c(cccc3)c4ccccc49 Nc1nc(N)c(cn1)N2CCN(CC2)c3ccc(cc3)c4ccccc410 Nc1nc(N)c(cn1)N2CCN(CC2)c3c(C)cccc311 Cc1cc(ccc1)N2CCN(CC2)c3c(N)nc(N)nc312 Cc1ccc(cc1)N2CCN(CC2)c3c(N)nc(N)nc313 Nc1nc(N)c(cn1)N2CCN(CC2)c3c(Cl)cccc314 Clc1cc(ccc1)N2CCN(CC2)c3c(N)nc(N)nc315 Clc1ccc(cc1)N2CCN(CC2)c3c(N)nc(N)nc316 COc1cc(ccc1)N2CCN(CC2)c3c(N)nc(N)nc317 Nc1nc(N)c(cn1)N2CCN(CC2)c3cc(ccc3)C(F)(F)F18 Nc1nc(N)c(cn1)N2CCN(CC2)c3cc(ccc3)OC(F)(F)F19 Nc1nc(N)c(cn1)N2CCN(CC2)c3cc(ccc3)C4CC420 Nc1nc(N)c(c(C)n1)N2CCN(CC2)c3cc(ccc3)c4ccccc421 CCc1c(c(N)nc(N)n1)N2CCN(CC2)c3cc(ccc3)c4ccccc422 Nc1nc(N)c(cn1)N2CCN(CC2)c3cc(ccc3)c4ncccc4S823 Nc1nc(N)c(cn1)N2CCN(CC2)c3cc(ccc3)c4cnccc424 Nc1nc(N)c(cn1)N2CCN(CC2)c3cc(ccc3)c4ccncc425 Nc1nc(N)c(cn1)N2CCN(CC2)c3cc(ccc3)c4ncccn426 Nc1nc(N)c(cn1)N2CCN(CC2)c3cc(ccc3)c4cncnc427 Nc1nc(N)c(cn1)N2CCN(CC2)c3cc(ccc3)c4nccnc428 Nc1nc(N)c(cn1)N2CCN(CC2)c3cc(ccc3)c4cnncc429 Cc1ncc(cn1)c2cc(ccc2)N3CCN(CC3)c4c(N)nc(N)nc430 Nc1nc(N)c(cn1)N2CCN(CC2)c3cc(ccc3)c4cnc(nc4)C(F)(F)F31 Nc1nc(N)c(cn1)N2CCN(CC2)c3cc(ccc3)c4cnc(nc4)C5CC532 Brc1cc(ccc1)N2CCN(CC2)c3c(N)nc(N)nc3References1. Sharma, H.; Landau, M. J.; Vargo, M. A.; Spasov, K. A.; Anderson, K. S., First Three-Dimensional Structure of Toxoplasma gondii Thymidylate Synthase-Dihydrofolate Reductase: Insights for Catalysis, Interdomain Interactions, and Substrate Channeling. Biochemistry 2013, 52 (41), 7305-7317.2. Wang, Q.; Rager, J. D.; Weinstein, K.; Kardos, P. S.; Dobson, G. L.; Li, J.; Hidalgo, I. J., Evaluation of the MDR-MDCK cell line as a permeability screen for the blood-brain barrier. Int. J. Pharm. 2005, 288 (2), 349-359.3. Troutman, M. D.; Thakker, D. R., Novel Experimental Parameters to Quantify the Modulation of Absorptive and Secretory Transport of Compounds by P-Glycoprotein in Cell Culture Models of Intestinal Epithelium. Pharm. Res. 2003, 20 (8), 1210-1224.

Discovery of selective Toxoplasma gondii dihydrofolate reductase inhibitors for the treatment of toxoplasmosis

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Discovery of selective Toxoplasma gondii dihydrofolate reductase inhibitors for the treatment of toxoplasmosis

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