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Pyrazolidine-3,5-dione-based inhibitors ofphosphoenolpyruvate carboxylase as a new class ofpotential C4 plant herbicidesMarkus Dick1, German Erlenkamp1, Giang T.T. Nguyen2, Kerstin F€orster2, Georg Groth2 andHolger Gohlke1
1 Institute of Pharmaceutical and Medicinal Chemistry and Bioeconomy Science Center (BioSC), Heinrich-Heine-Universit€at D€usseldorf,
Germany
2 Institute of Biochemical Plant Physiology and Bioeconomy Science Center (BioSC), Heinrich-Heine-Universit€at D€usseldorf, Germany
Correspondence
H. Gohlke, Institute of Pharmaceutical and
Medicinal Chemistry and Bioeconomy
Science Center (BioSC), Heinrich-Heine-
Universit€at D€usseldorf, 40225 D€usseldorf,
Germany
Fax: +49(0)221-81-13847
Tel: +49(0)221-81-13662
E-mail: gohlke@uni-duesseldorf.de
(Received 28 July 2017, revised 1
September 2017, accepted 5 September
2017, available online 24 September 2017)
doi:10.1002/1873-3468.12842
Edited by Richard Cogdell
Phosphoenolpyruvate carboxylase (PEPC) is a key enzyme in the C4 photosyn-
thetic pathway of many of the world’s worst weeds and a valuable target to
develop C4 plant-selective herbicides. By virtual screening, analog synthesis,
and in vitro validation, we identified pyrazolidine-3,5-diones as a new class of
small molecules with inhibitory potential down to the submicromolar range
against C4 PEPC and a selectivity factor of up to 16 over C3 PEPC. No other
biological activity has yet been reported for the best compound, (3-bromophe-
nyl)-4-(3-hydroxybenzylidene)-pyrazolidine-3,5-dione. A systematic variation
in the substituents allowed the derivation of a qualitative structure–activity rela-
tionship. These findings make this compound class highly interesting for further
investigations toward generating potent, C4 plant-selective herbicides with a
low potential for unwanted effects.
Keywords: C4 photosynthesis; phosphoenolpyruvate; pyrazolidine-3, 5-diones;
selective C4 herbicides; virtual screening
The development of herbicides against weeds has
become a global challenge in agriculture as weeds com-
pete with crops for water, sunlight, and soil nutrients.
Additionally, the rapid development of resistances
against established herbicides demands to develop
bioactive compounds for new targets. For this, one
can exploit that many of the worst weeds are C4
plants, whereas the majority of crops use C3 photosyn-
thesis [1,2]. Hence, one should be able to identify C4
plant-selective herbicides by targeting enzymes of such
plants. In C4 photosynthesis, initially, inorganic car-
bon is fixed by the enzyme phosphoenolpyruvate
(PEP) carboxylase (PEPC). PEPC catalyzes the car-
boxylation of PEP to the four-carbon molecule
oxaloacetate [3], which is reduced to aspartate or
malate, or transaminated to asparagine [4]. Structural
and biochemical studies have revealed that residue
R884 of PEPC of the C3 plant Flaveria pringlei assists
in binding malate; malate then acts as a feedback inhi-
bitor. R884 is conserved in all typical C3 crop plants
(Fig. S1). In contrast, in C4 weeds, the homolog resi-
due often corresponds to glycine, serine, glutamate, or
glutamine, besides arginine (Fig. S2). The smaller resi-
dues have been linked with a weaker feedback inhibi-
tor-binding site [5], for example, G884 in PEPC of the
C4 plant Flaveria trinervia does not show any interac-
tion with the inhibitor [6]. Recently, we used the
molecular difference in the feedback inhibitor-binding
site of PEPC between C3 and C4 plants to develop
potential C4 plant-selective herbicides with a novel
mode of action [7,8]. These studies verified that the
identified chalcones, quinoxalines, and catechins are
Abbreviations
PEP, phosphoenolpyruvate; PEPC, phosphoenolpyruvate carboxylase; RMSD, root mean square deviation.
3369FEBS Letters 591 (2017) 3369–3377 ª 2017 Federation of European Biochemical Societies
potent inhibitors of C4 PEPC (low micromolar to sub-
micromolar range) and show selectivity factors over C3
PEPC up to 27. However, chalcones are known to
have a wide range of biological activities [9] such as
antibacterial [10], antioxidant [11], antifungal [12], and
anticancer [13] effects. Quinoxalines also display a
broad spectrum of biological activities [8], and cate-
chins are known to be antioxidants [14] and antifungal
molecules [15]. Hence, identifying alternative molecule
classes that serve as unique inhibitors for C4 PEPC
but show no/less effects on other targets remains an
important task. Here, we identified, by repetitive
rounds of ligand- and structure-based virtual screening
on the ZINC database, analog synthesis, and in vitro
validation, pyrazolidine-3,5-dione-based selective C4
PEPC inhibitors with a so far unexplored chemotype
for C4 PEPC inhibition. These inhibitors are compara-
ble in affinity and selectivity to the previous inhibitors
but, to our knowledge, no other biological activity has
yet been reported for them.
Materials and methods
Protein and ligand structure preparation
The crystal structures of PEPC of the C4 plant F. trinervia
(PDB ID 3ZGE) and the C3 plant F. pringlei (PDB ID
3ZGB) [16] were retrieved from the Protein Data Bank [17].
Both structures were preprocessed with the Protein Prepara-
tion Wizard [18] of Schr€odinger’s Maestro suite. Thereby,
bond orders were assigned, hydrogen was added, the H-
bond network was optimized, and missing side chains were
added using Prime [19,20]. Finally, the systems were energy
minimized using the OPLS 2005 force field, resulting in a
root mean square deviation (RMSD) of 0.3 �A with respect
to chain A of the crystal structure [21]. In both crystal struc-
tures, PEPC forms a homo 4-mer. Since the allosteric-bind-
ing site is not affected by the presence of the other
monomer, we only used one monomer for further analysis
[22,23]. 3D structures of ligands were generated with the
LigPrep [24] module of the Schr€odinger suite.
Virtual screening with ROCS and FRED
The ZINC database [25,26] was initially screened for inhibi-
tor candidates applying rules that describe favorable phy-
sico-chemical properties of herbicides [27]. The program
Omega [28] was used to generate up to 100 conformations of
each remaining compound. These conformations were
screened with the combined shape query created from previ-
ously identified active compounds [8] using ROCS [29]. The
default settings of ROCS were used for this screening step,
and only the best fitting conformation for each compound
was saved. Hits from this step were then docked by FRED
[30–33] into C3 and C4 PEPC. For this, the box was centered
on the cocrystallized aspartate of PDB ID 3ZGE, and the
dimensions of the box were set to 18.00, 14.67, and 17.00 �A.
Docking with AutoDock
AUTODOCK 3.0 [34] in combination with DrugScore [35] was
utilized to identify common binding modes of hits using
the Lamarckian genetic algorithm with default parameters.
The box was again centered on the cocrystallized aspartate.
The dimension of the box was set to 60 �A in each direc-
tion. Hundred independent docking runs were performed
for each compound, with a maximum of 500 000 energy
evaluations. A clustering RMSD cutoff of 2.0 �A was cho-
sen, and the docking solution with the lowest energy was
taken if the configuration was found within a cluster cover-
ing more than 20% of all docking solutions.
Synthesis of new pyrazolidine-3,5-diones
All compound syntheses were performed by Taros Chemi-
cals, Dortmund. The syntheses were performed according
to Koo et al. [36]. Analytic data of the final products are
provided as Data S1.
Chemicals for in vitro assays
Chemicals were acquired from Sigma-Aldrich (St Louis,
USA) if not stated otherwise.
Cloning, protein expression, and purification
His-tagged recombinant PEPC of C4 plant F. trinervia and
C3 plant F. pringlei cloned in bacterial expression vector
pETEV16b (Novagene, Darmstadt, Germany) were
expressed in Escherichia coli and purified by immobilized-
metal affinity chromatography (IMAC) on Ni2+-nitrilotria-
cetic acid agarose (GE Healthcare, Munchen, Germany)
according to the protocol described in Paulus et al. [6]. Pur-
ity of recombinant proteins was confirmed by SDS/PAGE
and Colloidal Coomassie Staining. Protein concentrations
were determined by UV absorption at 280 nm on a Tecan
Infinite M-200 (Tecan Group Ltd., M€annedorf, Switzerland)
using a molar absorptivity value of 119 930 M�1�cm�1 for
F. trinervia PEPC or 125 430 M�1�cm�1 for F. pringlei
PEPC, respectively. Purified proteins were concentrated to
5–15 mg�mL�1 and stored at �80 °C, respectively.
PEPC-coupled spectrophotometric assay
Inhibition of purified recombinant PEPCs by pyrazolidine-
3,5-diones was measured in a coupled spectrophotometric
assay at 25 °C in a Beckman DU-800 spectrophotometer as
described previously [37]. Reaction mixture contained
3370 FEBS Letters 591 (2017) 3369–3377 ª 2017 Federation of European Biochemical Societies
Pyrazolidine-3,5-diones as C4 plant herbicides M. Dick et al.
purified C3 or C4 PEPC (0.05 U), NADH (150 lM), malate
dehydrogenase (2 U), and the pyrazolidine-3,5-diones stud-
ied in 50 mM HEPES/KOH pH 7.5, 10 mM MgCl2, 10 mM
KHCO3. Catalytic turnover was started by adding PEP at
concentrations corresponding to two-fold Km of the recom-
binant PEPC. The IC50 of selected pyrazolidine-3,5-diones
was determined by varying the inhibitor concentration from
0.01 to 200 lM in the coupled spectrophotometric assay.
Data were analyzed using GRAPHPAD Prism (GraphPad Soft-
ware, Inc., La Jolla, CA, USA).
Results
We performed a ligand-based virtual screening on a
subset of 15 000 molecules of the ZINC database
filtered such that they comply with rules for favorable
physico-chemical properties of herbicides [27] (see
Fig. 1A). Our search query was built based on two
types of selective C4 PEPC inhibitors, catechins and
quinoxalines, identified previously by us [8]. To do so,
we used Rapid Overlay of Chemical Structures (ROCS
[29]) to create a 3D overlay considering molecular
shape and acceptor, donor, cationic, anionic, aromatic,
and hydrophobic properties of these active compounds
(Fig. 1B). Applying this query with ROCS to the gen-
erated conformations of the 15 000 molecules yielded
7000 candidates fulfilling the characteristics of the 3D
ROCS overlay. The candidates were then docked with
FRED [30–33] into the feedback inhibitor-binding
Fig. 1. Workflow for structure-based screening for PEPC inhibitors. (A) Based on 20 million compounds from the ZINC database and two
filtering steps, 7000 compounds were docked into the binding pocket of PEPC. Out of 700 hits, 10 were used for in vitro tests resulting in
one active compound. In a second run, 15 000 compounds that fulfill the rules for bioavailability were screened for ligands with a
pyrazolidine-3,5-dione core, and 20 hits were tested. In addition, ten potential inhibitors that only vary in ring B (compared to the initial hit)
were designed, synthesized, and tested. (B) Shape- and properties-based query for a ROCS search based on an overlay of known inhibitors
of C4 PEPC [8]. Colored spheres represent ring structures (green), acceptor (blue), or donor atoms (red).
3371FEBS Letters 591 (2017) 3369–3377 ª 2017 Federation of European Biochemical Societies
M. Dick et al. Pyrazolidine-3,5-diones as C4 plant herbicides
pocket of C4 PEPC from F. trinervia. From the first
700 best scored molecules, 10 were selected by visual
inspection for in vitro activity tests (Fig. 1A). One
active compound with an IC50 value of 2.79 lM for C4
PEPC and 13.98 lM for C3 PEPC (resulting in a selec-
tivity factor of 5.01) was identified (compound 1–1,Table 1, Fig. S3). It contains a pyrazolidine-3,5-dione
core with a phenyl substituent at position 2 and a ben-
zylidene one at position 4 (referred to as ring A and
ring B hereafter).
Based on this initial hit, we performed a similarity
search (2D using ROCS) to retrieve all pyrazolidine-
3,5-diones from the 15 000 compounds. Twenty-two
compounds were chosen for a second round of in vitro
Table 1. Inhibitory effect of pyrazolidine-3,5-diones on PEPC from Flaveria trinervia (C4 plant) and Flaveria pringlei (C3 plant).
Molecule IC50 values (lM)
Structure Vendor ID C4 C3 Ratio C3/C4
1–1a
NHN
O
O
Br
O
Amb3596945 2.79 � 0.04 13.98 � 0.03 5.01
2–1a
NHN
O
O
Br
Cl
O
Amb3455285 0.90 � 0.04 4.80 � 0.02 5.33
2–2
NHN
O
O
BrCl
O
Amb3455286 1.20 � 0.04 4.90 � 0.20 4.08
2–3
NHN
O
O
O Br Amb8583694 1.20 � 0.04 2.60 � 0.10 2.17
2–4
NHN
O
O
O
Br
Amb21992151 0.56 � 0.04 0.52 � 0.60 0.93
3–1
NHN
O
O
Br
O2N
Taro27483 24.09 � 2.14 103.07 � 6.81 4.28
3–2
NHN
O
O
BrO2N Taro27484 1.26 � 0.19 2.06 � 0.22 1.63
3–3
NHN
O
O
Br
O2N Taro27485 2.85 � 0.42 2.59 � 0.28 0.91
3372 FEBS Letters 591 (2017) 3369–3377 ª 2017 Federation of European Biochemical Societies
Pyrazolidine-3,5-diones as C4 plant herbicides M. Dick et al.
testing based on visual inspection. A first activity test
revealed that 10 of the 22 compounds had an inhibi-
tory effect (> 60%, Fig. S4). For the best four hits (in-
hibitory effect > 80%), the IC50 values were measured
for both C3 and C4 PEPC (Table 1, compounds 2–1 to
2–4; see also Fig. S4). All four molecules have IC50
values in the range of 0.56–4.9 lM and selectivity fac-
tors of 0.93–5.33. Compound 2–4 is the most potent
C4 PEPC inhibitor known to date but lacks selectivity.
Notably, of all five molecules identified so far, it is the
only one that does not have a bromide substitution at
ring A. Thus, in order to improve the selectivity, we
decided to perform a screen for differently substituted
aromatic rings B while keeping the 2-bromophenyl
substituent as ring A. To be not limited by the pool of
commercially available molecules, the compounds of
interest were newly synthetized (compounds 3–1 to 3–10 in Table 1). The best compound 3–5 had an IC50
value of 1.96 lM toward C4 PEPC, a selectivity factor
of 16.6, and a 2-hydroxyl-benzylidene substituent as
Table 1. (Continued).
Molecule IC50 values (lM)
Structure Vendor ID C4 C3 Ratio C3/C4
3–4
NHN
O
O
Br
HO
Taro27486 13.94 � 0.94 72.58 � 6.79 5.21
3–5a
NHN
O
O
BrHO Taro27487 1.96 � 0.17 32.59 � 1.94 16.63
3–6
NHN
O
O
Br
HO ChEMBLl1533094 18.99 � 2.12 72.53 � 2.22 3.82
3–7
NHN
O
O
Br
N
N Taro27489 39.57 � 9.23 131.39 � 47.83 3.32
3–8
NHN
O
O
Br
N
O ChEMBL1434855 63.95 � 14.97 149.00 � 28.29 2.33
3–9
NHN
O
O
Br
HO
OTaro27491 11.62 � 0.99 105.94 � 3.07 9.12
3–10
NHN
O
O
BrO
HO
Taro27492 11.46 � 1.53 144.98 � 68.24 12.65
a IC50 measurements for inhibition of C4 and C3 PEPC are shown as examples in Fig. S3.
3373FEBS Letters 591 (2017) 3369–3377 ª 2017 Federation of European Biochemical Societies
M. Dick et al. Pyrazolidine-3,5-diones as C4 plant herbicides
ring B. To investigate its binding mode, 3–5 was
docked into the binding sites of C3 and C4 PEPC
using Autodock with DrugScore potentials [38,39].
The predicted binding pose in C4 PEPC is shown in
Fig. 2. Ring B is located close to R641 and R888,
forming cation–p interactions and a hydrogen bond
between the 2-hydroxyl group and R641. A similar
interaction pattern has been described for chalcone-
based inhibitors of PEPC [7]. Ring A is buried in the
hydrophobic part of the binding pocket in between
I113, L881, and A132. The comparison with the dock-
ing result in C3 PEPC revealed a nearly identical bind-
ing mode. The observed selectivity, thus, cannot
simply be explained by a different shape matching.
Discussion
Phosphoenolpyruvate carboxylase is a crucial enzyme
for carbon fixation in photosynthesis. The structural
differences in PEPC of C3 and C4 plants make it an
attractive target for C4 plant-selective herbicides. In
this study, we used a repetitive ligand- and structure-
based virtual screening approach to identify and char-
acterize small molecules with a pyrazolidine-3,5-dione
core as selective inhibitors of C4 PEPC. Specifically,
we identified 2-(3-bromophenyl)-4-(3-hydroxybenzyli-
dene)-pyrazolidine-3,5-dione (compound 3–5) with an
IC50 value of 1.96 lM and a selectivity factor of 16.6
over C3 PEPC. The inhibitor furthermore complies
with rules for favorable physico-chemical properties of
herbicides [27]. Both the inhibitory potential and the
selectivity factor of 3–5 are comparable with those
identified for the most promising chalcone-based
inhibitors [7] and superior to those identified for
catechine-based inhibitors [8]. With respect to quinoxa-
line-based inhibitors [8], the inhibitory potential of 3–5is higher by a factor of at least 70. In addition, for the
identified pyrazolidine-3,5-diones, other biological
activities have rarely been mentioned so far: A similar-
ity search for compound 3–5 (Tanimoto similarity
score > 90%) using SciFinder [40] or ChEMBL [41]
did not reveal any literature entry related to a known
other biological activity (databases accessed in July
2017).
From our in vitro activity data and the predicted
binding mode, a qualitative structure–activity relation-
ship for the investigated pyrazolidine-3,5-diones can be
derived. Bulky and rigid substituents in ring B such as
4-morpholino have a negative effect on the inhibitory
potential (compounds 3–7, 3–8), which may be
rationalized by steric clashes as identified in the dock-
ing experiment. Interestingly, bulky but more flexible
residues such as benzyloxy (2–3) or phenylethyloxy
(2–4) lowered the IC50 to a submicromolar range.
However, this increase in inhibitory potential toward
C4 PEPC was accompanied by a loss in selectivity over
C3 PEPC. This loss is probably caused by a different
binding mode (shown for 2–4 in Fig. S5), where a new
Fig. 2. Predicted binding pose of compound 3–5 within C4 PEPC. The conformation with the lowest energy in the largest cluster is shown.
(A) 3D representation of the binding pocket. The bound inhibitor is represented in space-filling mode (carbon: green, nitrogen: blue, oxygen:
red, bromide: light red), while the residues of PEPC are shown as sticks (carbon: light blue, nitrogen: blue, oxygen: red, polar hydrogen:
white). (B) 2D scheme of the binding pose. Red arrows represent hydrogen bond formation. Protein residues are labeled in blue (pos.
charge), red (neg. charge), light blue (polar), or green (hydrophobic).
3374 FEBS Letters 591 (2017) 3369–3377 ª 2017 Federation of European Biochemical Societies
Pyrazolidine-3,5-diones as C4 plant herbicides M. Dick et al.
orientation of both ring A and ring B enable a cation–p interaction of the benzyloxy moiety with the nearby
R687. A 3-hydroxyl group at ring B yielded both a
good inhibitory potential and selectivity (3–5), likely
because it allows the formation of a hydrogen bond
with either R888 or N964, which appears unlikely to
form with hydroxyl groups in positions 2 or 4 due to a
larger distance to those amino acids (resulting in
higher IC50 values). In support of this hypothesis, a
similar effect was detected when the hydroxyl group
was exchanged by a nitro group (compounds 3–1 to 3–3) or ether moiety (3–9 and 3–10), which can function
as (weak) hydrogen bond acceptors [42].
Finally, as to selectivity-determining factors, the
binding pockets of our C3 and C4 PEPC differ only in
position 884 (arginine in C3 PEPC instead of glycine
in C4 PEPC). Multiple sequence alignments reveal that
amino acids are highly conserved in the feedback inhi-
bitor-binding pocket (Figs S1 and S2), with R884 in
C3 PEPC being fully conserved and glycine being the
most common amino acid in C4 PEPC at position 884
that is different from the arginine found in C3 PEPC.
Hence, the PEPC investigated here are good represen-
tatives of their families. As almost all our compounds
show a selectivity toward C4 PEPC, apparently, disfa-
vorable steric interactions of R884 in C3 PEPC with
ring B in the identified binding mode outweigh poten-
tially favorable cation–p or polar interactions.
As to in vivo experiments, only a preliminary study
has been carried out on the effect of the identified
pyrazolidine-3,5-dione inhibitors on C4 plants. No
obvious damage or growth-inhibitory effect was
observed with the C4 weed Amaranthus retroflexus
when sprayed at single dose at 3 mM concentration.
However, previous weed control and herbicide
research projects have already shown that herbicidal
activities critically depend on formulation and applica-
tion of the active compound [43]. Consequently, fur-
ther plant uptake studies will address if higher dose,
repetitive spraying, or the addition of surfactants can
promote foliar absorption and herbicidal activities of
pyrazolidine-3,5-diones.
In conclusion, we identified pyrazolidine-3,5-diones
(Fig. 3) as a new class of small molecules with inhibi-
tory potential in the low micromolar to submicromolar
range against C4 PEPC and a selectivity factor of up
to 16 with respect to binding to C3 PEPC. To the best
of our knowledge, no other biological activity has yet
been reported for our best compound, 3–5. A system-
atic variation of substituents at ring B allowed deriving
a qualitative structure–activity relationship. Together,
these findings make this compound class highly inter-
esting for further investigations toward generating
potent, C4 plant-selective herbicides with a low poten-
tial for unwanted effects.
Acknowledgements
This study was funded within the Bioeconomy Science
Center (BioSC) by the boost fund ‘C4-PSH’ granted to
HG and GG. The scientific activities of BioSC were
financially supported by the Ministry of Innovation,
Science, and Research within the framework of the
NRW Strategieprojekt BioSC (No. 313/323-400-002
13). We are grateful to the ‘Zentrum f€ur Informations-
und Medientechnologie (ZIM)’ at Heinrich Heine
University D€usseldorf for providing computational
support.
Authors contribution
HG and GG conceived and supervised the study; MD
and GE performed in silico experiments; GN and KF
performed in vitro tests; MD and HG wrote the manu-
script; GG, GN, KF, and GE made manuscript revi-
sions.
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Supporting information
Additional Supporting Information may be found
online in the supporting information tab for this
article:Fig. S1. C3 PEPC sequences according to Paulus et al.
[1] aligned with the C3 PEPC from Flaveria pringlei
Fig. S2. C4 PEPC sequences according to Paulus et al.
[1] aligned with the C4 PEPC from Flaveria triniervia.
Fig. S3. Assay for C4 and C3 PEPC inhibition by dif-
ferent pyrazolidine-3,5-dione-based inhibitors (A to D:
compounds 1–1, 2–1, 2–4 and 3–5).Fig. S4. Activity assay to determine the inhibitory
effect of selected compounds (second screening round
of Fig. 1) on the catalytic activity of PEPC from
Flaveria trinervia.
Fig. S5. 2D schemes of the predicted binding modes of
(A) compound 2–4 (selectivity < 1) and (B) 3–5 (selec-
tivity 16.6) within PEPC from Flaveria trinervia (C4
plant).
Data S1. Analytic data for compounds 3–1 to 3–10provided by Taros Chemicals, Dortmund.
3377FEBS Letters 591 (2017) 3369–3377 ª 2017 Federation of European Biochemical Societies
M. Dick et al. Pyrazolidine-3,5-diones as C4 plant herbicides